Fusion proteins and use thereof for preparing vaccines

The present invention is applicable to new fusion proteins and use thereof for preparing vaccines.

The Zika virus (ZIKV) was first detected in a monkey in Uganda in 1947. The first human cases were identified in the 1970s in Africa (Uganda, Tanzania, Egypt, Central African Republic, Sierra Leone, Gabon and Senegal), then in certain Asian countries (India, Malaysia, Philippines, Thailand, Vietnam and Indonesia).

Many cases have been confirmed today, e.g. 55,000 cases of Zika virus infections were identified in French Polynesia between 2013 and 2014. The Zika virus was also detected for the first time in Brazil in May 2015, and to date, between 440,000 and 1,500,000 suspected cases have been reported. Zika virus epidemics have thus intensified over the last few years, and the World Health Organization notably indicated in February 2016 that the Zika virus constituted a public health emergency of international concern.

The majority of people infected by the Zika virus do not develop any symptoms (approximately 70 to 80% of cases). In the rest of the population, the symptoms caused by the Zika virus resemble flu symptoms: fatigue, fever, headaches and muscle and joint pain. Rashes, conjunctivitis, pain behind the eyes, digestive disorders or even hand or foot edema may also occur, as well as serious post-infection neurological complications like Guillain-Barrè syndrome or fetal malformations in pregnant women.

At this time, there is no vaccine preventing the Zika virus infections, nor specific medication to treat said infections.

There is thus a real need to provide a means of preventing and/or treating Zika virus infections.

There is notably a real need to provide a vaccine against the Zika virus.

One of the objects of the invention is thus to provide a means of preventing and/or treating Zika virus infections.

One of the objects of the invention is thus to provide a vaccine against the Zika virus.

The present invention is based on the unexpected results of the Inventors, according to which Zika-HBV fusion proteins are capable of forming subviral, non-infectious and immunogenic particles that are well structured and efficaciously secreted and that can be used to prevent and/or treat Zika virus infections.

The interest in such fusion proteins lies in preventing and/or treating Zika virus infections and/or hepatitis B virus infections, i.e. inducing double immunization against the Zika virus and the hepatitis B virus.

An additional interest of the invention can be found in the fact that it can be easily adapted to existing industrial manufacturing chains for currently commercialized vaccines against hepatitis B.

This is why one of the objects of the invention is an immunogenic Zika-HBV fusion protein.

Another object of the invention is a nucleic acid molecule coding an immunogenic Zika-HBV fusion protein.

Another object of the invention is a vector comprising a nucleic acid molecule coding an immunogenic Zika-HBV fusion protein.

Another object of the invention is a subviral, non-infectious and immunogenic particle comprising at least one immunogenic Zika-HBV fusion protein.

Another object of the invention is an immunogenic Zika-HBV fusion protein for use as a medication.

Another object of the invention is an immunogenic Zika-HBV fusion protein for use in the prevention and/or treatment of hepatitis B and/or Zika virus infections.

Another object of the invention is a cellular line that expresses subviral, non-infectious and immunogenic particles comprising at least one immunogenic Zika-HBV fusion protein.

Finally, another object of the invention is a method for producing subviral, non-infectious and immunogenic particles comprising at least one immunogenic Zika-HBV fusion protein.

In a first embodiment, the invention thus relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S or the protein M of a human hepatitis B virus (HBV) isolate, which protein S or protein M is optionally deleted at the N-terminal end thereof, or
- an amino acid sequence with a percent identity of at least 91%, notably at least 93%, particularly at least 95% and more particularly at least 97%, with said amino acid sequence of the protein S or the protein M optionally deleted at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus, or,
- the amino acid sequence of a natural variant from another isolate of the HBV, or of a synthetic variant derived from said amino acid sequence of the protein S or the protein M optionally deleted at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the sequence of amino acids of at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate selected from the envelope protein,
- an amino acid sequence with a percent identity of at least 90%, notably at least 95%, with said amino acid sequence of at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another isolate of the Zika virus, or of a synthetic variant derived from said amino acid sequence of at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, said protein of a Zika virus isolate being chosen from among the envelope protein E or a fusion peptide comprising the envelope protein E and the protein prM.

The expression “fusion protein” refers to any artificial/chimeric protein comprising at least the protein S or the protein M of the HBV, optionally deleted at the N-terminal end thereof, and at least one transmembrane domain and the ectodomain of at least one envelope protein E of a Zika virus isolate. Examples of such fusion proteins are represented in FIGS. 8, 10, 12, 14, 16, 18, 20 and 22.

The term “protein S” or “wild-type protein S” or “S” or “HBs-S(HBV)” refers to:

- the envelope protein of an HBV isolate notably comprising 226 amino acids and comprising four transmembrane domains (FIG. 1), and notably the envelope protein of the HBVadw isolate, or
- any amino acid sequence with a percent identity of at least 91% with the amino acid sequence of the protein S of an HBV isolate, or
- the natural variant(s) of the protein S of all the HBV isolates, or the synthetic variant(s) of said protein S.

The wild-type protein S contains four transmembrane domains, but does not contain an ectodomain. It possesses an antigenic loop that corresponds to the amino acids situated between the transmembrane domains 2 and 3. The wild-type protein S is represented, for example, by SEQ ID NO. 2.

The term “protein M” or “wild-type protein M” or “M” or “HBs-M(HBV)” refers to:

- the envelope protein of an HBV isolate notably comprising 281 amino acids and comprising four transmembrane domains (FIGS. 2A and 2B), and notably the envelope protein of the HBVadw isolate, or
- any amino acid sequence with a percent identity of at least 91% with the amino acid sequence of the protein M of an HBV isolate, or
- the natural variant(s) of the protein M of all the HBV isolates, or the synthetic variant(s) of said protein M.

The protein M sequence differs from that of the protein S through the presence of the N-terminal end of 55 additional amino acids. These 55 amino acids correspond to the preS2 domain.

The wild-type protein M contains four transmembrane domains and a preS2 domain. The wild-type protein M is represented, for example, by SEQ ID NO. 4.

The expression “optionally deleted at the N-terminal end thereof” means that all (or nearly all) or part of the protein S or the protein M is used in the invention's fusion proteins. More precisely:

- if the protein S is not deleted at the N-terminal end thereof, all (or nearly all) of the protein S sequence, as defined above, is used in the invention's fusion proteins;
- if the protein S is deleted at the N-terminal end thereof, said protein S is deleted from its transmembrane domain located at the N-terminal end thereof and is named delete S in such a case. In such a case, said protein S is thus essentially constituted of its three transmembrane domains located at the C-terminal end thereof. Thus, this is also understood, in the protein S defined above, to be the deletion of the region from the amino acid in position 1 to that in position 23 of the protein S of an HBV isolate;
- if the protein M is not deleted at the N-terminal end thereof, all (or nearly all) of the protein M sequence, as defined above, is used in the invention's fusion proteins. In this particular embodiment, said protein M is thus not deleted in its preS2 domain;
- if the protein M is deleted at the N-terminal end thereof, said protein M is deleted from its preS2 domain (i.e. the domain constituted of the amino acids located position 1 to position 55 of the N-terminal end) and is named delete M in such a case. Thus, said protein M is deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof. A deletion of a sequence of 1 to 54 amino acids is understood to be a deletion of 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 31, 32, 33, 34, 35, 36, 37, 38, 39, 40, 41, 42, 43, 44, 45, 46, 47, 48, 49, 50, 51, 52, 53 and 54 amino acids. In a particular embodiment of the invention, said protein M is deleted from a sequence of 54 amino acids located at the N-terminal end thereof. In such a case, said protein M thus remains essentially constituted of its four transmembrane domains, despite the deletion. The protein M fully deleted from its preS2 domain corresponds to the non-deleted protein S.

A protein S deleted at the N-terminal end thereof is represented, for example, by SEQ ID NO. 1.

A protein M deleted at the N-terminal end thereof is represented, for example, by SEQ ID NO. 3.

In a particular embodiment of the invention, the deleted amino acids are contiguous.

The expression “nearly all” means that the proteins S or M may be deleted from some amino acids at the N or C-terminal ends thereof when they are present in the fusion proteins according to the invention. For example, the methionine (M) in position 1 of SEQ ID NO. 2 and SEQ ID NO. 4 may not be present in the fusion protein sequences according to the invention.

The expression “N-terminal end” is understood to be the “N-terminal side” or the “N-terminal.”

The expression “C-terminal end” is understood to be the “C-terminal side” or the “C-terminal.”

In the fusion proteins according to the invention, when said protein S is deleted at the N-terminal end thereof, the transmembrane domain of the protein of a Zika virus isolate, notably the envelope protein E, replaces the one deleted at the N-terminal of the HBV protein S.

Alternatively, in the fusion proteins according to the invention, when said protein S is not deleted at the N-terminal end thereof, the C-terminal end of the protein of a Zika virus isolate, and more particularly the second transmembrane domain of the envelope protein E of the Zika virus, is fused to the first amino acids at the N-terminal end of the HBV protein S.

Alternatively, in the fusion proteins according to the invention, when said protein M is deleted at the N-terminal end thereof, the transmembrane domain of the protein of a Zika virus isolate replaces the sequence deleted from 1 to 54 amino acids in the N-terminal of the HBV protein M.

Alternatively, in the fusion proteins according to the invention, when said protein M is not deleted at the N-terminal end thereof, the transmembrane domain of the protein of a Zika virus isolate is fused to the preS2 domain at the N-terminal end of the HBV protein M.

The expression “isolate of the human hepatitis B virus” or “isolate of the human HBV” means any isolate belonging to the family Hepadnaviridae and the genus Orthohepadnavirus, or any isolate classified by the International Committee for the Taxonomy of Viruses (ICTV) as being related to the HBV [Schaefer S. Hepatitis B virus taxonomy and hepatitis B virus genotypes. World J Gastroenterol. 2007 Jan. 7: 13(1):14-21].

In a particular embodiment, the human HBV isolate in the fusion protein mentioned above is the HBVadw isolate.

The term “Zika virus isolate” means any isolate belonging to the family Flaviviridae and the genus Flavivirus, or any isolate classified by the International Committee for the Taxonomy of Viruses (ICTV) as being related to the Zika virus.

In a particular embodiment, the Zika virus isolate in the fusion protein mentioned above is the isolate described under GenBank accession number KU312312.1 (Enfissi et al., Lancet. 2016 Jan. 16:387(10015):227-8. Doi: 10.1016/S0140-6736(16)00003). In a particular embodiment, said Zika virus isolate is represented by SEQ ID NO. 29.

In a particular embodiment, the Zika virus isolate in the fusion protein mentioned above is the isolate described under GenBank accession number KU321639 (First Complete Genome Sequence of Zika Virus (Flaviviridae, Flavivirus) from an Autochtonous Transmission in Brazil. Cunha M S, Esposito D L, Rocco I M, Maeda A Y, Vasami F G, Nogueira J S, de Souza R P, Suzuki A, Addas-Carvalho M, Barjas-Castro Mde L, Resende M R, Stucchi R S, Boin Ide F, Katz G, Angerami R N, da Fonseca B A. Genome Announc. 2016 Mar. 3:4(2). Pii: e00032-16. Doi: 0.1128/genomeA.00032-16). In a particular embodiment, said Zika virus isolate is represented by SEQ ID NO. 52. It is SEQ ID NO. 52 that was used to determine the cartography of Zika in the present invention.

In a particular embodiment of the invention, the Zika virus is the human Zika virus.

The expression “percent identity” means the percentage determined by the direct comparison of two sequences (nucleic or protein) by determining the number of nucleic acids or amino acid residues common to both sequences, then dividing this by the number of nucleic acids or amino acid residues in the longer of the two sequences and multiplying the result by 100.

The expression “at least 91%” means 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98%, 99% and 100%.

The expression “at least 90%” means 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98%, 99% and 100%.

The expression “maintains the ability to form subviral, non-infectious particles” refers to the ability of any protein, notably the protein S of the human HBV virus, particularly of the protein S deleted from its transmembrane domain at the N-terminal end thereof, and more particularly of a fusion protein of the invention comprising, for example, the protein S deleted at the N-terminal, to assemble in the presence of the wild-type protein S. This also refers to the ability of the wild-type proteins S to assemble themselves into filamentous or spherical subviral particles.

The protein M of the human HBV virus, optionally deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, also possesses the ability to assemble in the presence of the wild-type protein S.

The protein E of the Zika virus, optionally deleted from a transmembrane domain at the N-terminal end thereof, also possesses the ability to assemble in the presence of the wild-type protein S.

The protein prM of the Zika virus also possesses the ability to assemble in the presence of the wild-type protein S.

Said ability to form subviral particles may also be demonstrated through observation, notably through an electron microscope analysis, and notably through the test mentioned in examples 1 and 2.

The term “assemble” or “assembly” refers to the ability of a protein to form subviral particles by combining with the wild-type protein S. The term “self-assembly” is to be understood as the ability of a protein to form subviral particles by itself.

The term “immunogenic/immunogenic properties” means that the fusion proteins according to the invention are provided with antigenic properties and are capable of inducing a reaction or an immune response.

In particular, a protein is considered immunogenic to HBV if, after immunization, it induces an anti-S and/or anti-M humoral response, as detected, for example:

- according to a protocol described by Huzly et al., 2008 [Huzly D, Schenk T, Jilg W, Neumann-Haefelin D. Comparison of nine commercially available assays for quantification of antibody response to hepatitis B virus surface antigen. J Clin Microbiol. 2008 April, 46(4):1298-306], or
- by performing immunoblots associated with a revelation by an anti-HBs antibody (e.g. the R247 antibody, as mentioned by Jenna, S., and C. Sureau. Mutations in the carboxyl-terminal domain of the small hepatitis B virus envelope protein impair the assembly of hepatitis delta virus particles. J. Virol. 1999. 73: 3351-3358). Such an antibody may demonstrate a greater size of the fusion protein according to the invention. Such tests allow it to be determined, for example, whether the amino acid sequences or the fusion proteins according to the invention maintain the immunogenic properties against the human HBV.

A protein is considered immunogenic to Zika if, after immunization, it induces an anti-E and/or anti-prM humoral response, as detected, for example:

- by a sandwich ELISA test involving the 4G2 antibody (clone D1-4G2-4-15, commercialized by Millipore under the reference number MAB10216). This antibody is directed against Flavivirus antigens, and it thus allows the immunocapture of particles comprising such antigens and their detection using immunoenzymatic techniques; or
- by performing immunoblots associated with a revelation by an anti-Zika antibody commercialized by Biofront Technologies under the reference number BF-1176-56 (clone 0302156). Such tests allow it to be determined, for example, whether the amino acid sequences or the fusion proteins according to the invention maintain the immunogenic properties against the Zika virus.

The expression “natural variant” refers to all variability, all polymorphism, all diversity of a DNA sequence, of an allele, of a protein sequence, or more generally, of any protein or nucleic sequence, between the isolates of a single species or a single population. The percent of natural variability is determined through a direct comparison of two molecules (polypeptides or polynucleotides), derived from a wild-type reference molecule with biological properties of interest, such as immunogenic properties and/or the ability to form subviral particles. This is quantified by determining the exact number of amino acid or nucleic acid residues, identical between the two sequences, then dividing them by the number of amino acid or nucleic acid residues of the shorter of the two sequences and multiplying the result by 100.

The expression “synthetic variant” refers to any polypeptide molecule (amino acid sequence) or polynucleotide molecule (nucleic acid sequence), according to the invention, derived by recombining a wild-type reference molecule through addition, deletion or substitution of one or more nucleic acids or amino acids in said wild-type reference molecule, provided that it maintains the biological properties of interest, such as immunogenic properties and/or the ability to form subviral particles. The percent of synthetic variability is determined through a direct comparison of said molecule derived from said wild-type reference molecule, by determining the exact number of amino acid or nucleic acid residues, identical between the two sequences, with regard to their position and nature, then dividing them by the number of amino acid or nucleic acid residues of the shorter of the two sequences and multiplying the result by 100.

The term “envelope protein E” or “wild-type envelope protein E” or E(Zika) refers to the structural protein of a Zika virus isolate, and notably:

- the protein of a Zika virus isolate notably comprising 504 amino acids and consisting of two transmembrane domains (FIG. 3), and notably the protein of the Zika isolate with SEQ ID NO. 29 or SEQ ID NO. 52, or
- any amino acid sequence presenting a percent identity of at least 90% with the amino acid sequence of the envelope protein E of a Zika virus isolate, or
- the natural variant(s) of the envelope protein E of all the Zika virus isolates, or the synthetic variant(s) of the envelope protein E.

The wild-type protein E comprises 2 transmembrane domains and an ectodomain. The wild-type protein E is represented, for example, by SEQ ID NO. 15.

In one embodiment of the invention, in the above-mentioned fusion proteins, said envelope protein E comprises its two transmembrane domains.

In another embodiment of the invention, in the above-mentioned fusion proteins, said envelope protein E comprises only one of its two transmembrane domains. In such a case, it is always the second transmembrane domain of E (i.e. the one located at the C-terminal end thereof, from position 485 to position 504) that is deleted. In such a case, said envelope protein E is named deleted E. The first transmembrane domain of the envelope protein E is never involved in a deletion.

In one embodiment of the invention, the ectodomain of the envelope protein E is understood to be the amino acids in position 1 to the amino acids in position 455.

In one embodiment of the invention, the first transmembrane domain of the envelope protein E is understood to be the amino acids in position 456 to the amino acids in position 484. The last seven amino acids in the C-terminal position (i.e. the amino acids in positions 478 to 484) correspond to an extramembrane loop that binds the first and the second transmembrane domains.

In one embodiment of the invention, the second transmembrane domain of the envelope protein E is understood to be the amino acids in position 485 to the amino acids in position 504.

According to a particularly advantageous embodiment of the invention, the transmembrane domains of the envelope protein E are deleted from at least one of the last three amino acids, and notably from the last three amino acids, located in the C-terminal position. Said deletion of at least one of the three amino acids, and notably of the last three amino acids, in the C-terminal position presents the advantage of deactivating the peptidase cleavage site, which is necessary for the maturation of the Zika polyprotein, but which is not necessary in the scope of chimeric constructions of the present invention.

The term “protein prM” or “wild-type protein prM” refers to the structural protein of a Zika virus isolate, and notably:

- the protein of a Zika virus isolate notably comprising 164 amino acids and containing two transmembrane domains (FIG. 4), and notably the protein of the Zika virus isolate from SEQ ID NO. 29 or SEQ ID NO. 52, or
- any amino acid sequence presenting a percent identity of at least 90% with the amino acid sequence of the protein prM of a Zika virus isolate, or
- the natural variant(s) of the protein prM of all the Zika virus isolates, or the synthetic variant(s) of the protein prM.

The protein prM is in its native form in the polyprotein comprising the fusion proteins according to the invention: the sequence of the protein prM is complete/whole in the polyprotein comprising the fusion proteins according to the invention. In other words, the protein prM is never deleted from one or both transmembrane domains in the fusion proteins according to the invention.

The wild-type protein prM comprises 2 transmembrane domains and an ectodomain. The protein prM is constituted of a pro-peptide portion and an M portion (prM=pro-peptide (pr)+M). The protein pr/M undergoes two cleavages, one located at the junction between the pro-peptide and M, the second at the junction between M and E; these cleavages take place before assembly of the particle in the cell by two cellular proteases. In the present invention, the production of the protein prM in the context of the polyprotein containing the fusion protein is sought to allow the correct three-dimensional folding of the Zika envelope protein E included in the chimeric proteins. This three-dimensional folding is necessary to minimize the non-specific aggregation of the Zika protein E included in the chimeric protein, an incident capable of inducing the premature degradation of the chimeric protein by the proteasome. Likewise, the three-dimensional folding of the protein E under the dependence of prM allows an optimal presentation of the protein E included in the chimeric protein to the immune system in the scope of its use as an anti-Zika immunogen. The integral protein prM is considered a chaperone protein of the Zika protein E, as this function is described in the literature on flaviviruses (Roby J A, Setoh Y X, Hall R A, Khromykh A A, J Gen Virol. 2015 July: 96(Pt 7):1551-69. Doi: 10.1099/vir.0.000097).

In one embodiment of the invention, the ectodomain of the uncleaved protein prM is understood to be the amino acids in position 1 to the amino acids in position 123.

In one embodiment of the invention, the ectodomain of the cleaved protein prM is understood to be the amino acids in position 90 to the amino acids in position 123.

In one embodiment of the invention, the first transmembrane domain of the protein prM is understood to be the amino acids in position 124 to the amino acids in position 143 or from position 124 to 149 if the first transmembrane domain also comprises the amino acids in position 144 to 149 corresponding to the extramembrane loop that binds the first and second transmembrane domains.

In one embodiment of the invention, the second transmembrane domain of the protein prM is understood to be the amino acids in position 150 to the amino acids in position 164.

In one embodiment of the invention, the pro-peptide portion of the protein prM is understood to be the amino acids in position 1 to the amino acids in position 89. The pro-peptide portion is thus part of the ectodomain.

In one embodiment of the invention, the M portion of the protein prM is understood to be the amino acids in position 90 to the amino acids in position 164.

The wild-type protein prM is represented, for example, by SEQ ID NO. 50.

The interest in using the protein prM could, for example, be the improvement of the addressing and/or immunogenicity of the fusion proteins according to the invention.

The invention also relates to a fusion protein having an amino acid sequence presenting a percent identity of at least 83%, notably of at least 85%, particularly of at least 90%, and more particularly of at least 95% with the amino acid sequence of an above-mentioned fusion protein.

In a particular embodiment, in said above-mentioned fusion protein, the first peptide located on the C-terminal side is constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting a percent identity of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV, or,
- the amino acid sequence of a natural variant from another variant of the human HBV isolate, or of a synthetic variant derived from said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV.

In another particular embodiment, in said above-mentioned fusion protein, the first peptide located on the C-terminal side is constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is not deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting a percent identity of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV, or,
- the amino acid sequence of a natural variant from another variant of the human HBV isolate, or of a synthetic variant derived from said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV.

In another particular embodiment, in said above-mentioned fusion protein, the first peptide located on the C-terminal side is constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting a percent identity of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV, or,
- the amino acid sequence of a natural variant from another variant of the human HBV isolate, or of a synthetic variant derived from said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV.

In another particular embodiment, in said above-mentioned fusion protein, the first peptide located on the C-terminal side is constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting a percent identity of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV, or,
- the amino acid sequence of a natural variant from another variant of the human HBV isolate, or of a synthetic variant derived from said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV.

In another particular embodiment, in said above-mentioned fusion protein, the second peptide located on the N-terminal side is constituted of:

- the amino acid sequence of at least one transmembrane domain and the ectodomain of the envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of at least one transmembrane domain and the ectodomain of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of at least one transmembrane domain and the ectodomain of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus.

In another particular embodiment, in said above-mentioned fusion protein, the second peptide located on the N-terminal side is constituted of:

- the amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus.

In another particular embodiment, in said above-mentioned fusion protein, the second peptide located on the N-terminal side is constituted of:

- the amino acid sequence comprising both transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence comprising both transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising both transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus.

In another particular embodiment, in said above-mentioned fusion protein, the second peptide located on the N-terminal side is constituted of:

- the amino acid sequence of a fusion peptide comprising at least one transmembrane domain and the ectodomain of the envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus.

In another particular embodiment, in said above-mentioned fusion protein, the second peptide located on the N-terminal side is constituted of:

- the amino acid sequence of a fusion peptide comprising both transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus.

In another particular embodiment, in said above-mentioned fusion protein, the second peptide located on the N-terminal side is constituted of:

- the amino acid sequence of a fusion peptide comprising only one of the two transmembrane domains and the ectodomain of the envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus.

In a particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is not deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is not deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is not deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein S of a human HBV isolate, which protein S is not deleted from its transmembrane domain located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising only one of the two transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In another particular embodiment, the present invention relates to an immunogenic fusion protein comprising at least the two following peptides:

a) —on the C-terminal side, a first peptide constituted of:

- the amino acid sequence of the protein M of a human HBV isolate, which protein M is not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, or
- an amino acid sequence presenting an identity percentage of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, or
- the amino acid sequence of a natural variant from another human HBV virus isolate, or of a synthetic variant derived from said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV virus, and

b) —on the N-terminal side, a second peptide constituted of:

- the amino acid sequence of a fusion peptide comprising both transmembrane domains and the ectodomain of an envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, or
- an amino acid sequence presenting an identity percentage of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus, or
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human Zika virus.

In a particular embodiment, the present invention relates to an above-mentioned fusion protein, said protein also comprising another peptide at the N-terminal end thereof (i.e. at the N-terminal end of the second peptide) constituted of:

- the amino acid sequence of a transfer initiation peptide of a Zika virus isolate, or
- an amino acid sequence presenting an identity percent of at least 83%, notably of at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said amino acid sequence of the transfer initiation peptide of a Zika virus isolate, provided that said amino acid sequence maintains the properties of a transfer initiation peptide,
- the amino acid sequence of a natural variant from another Zika virus isolate, or of a synthetic variant derived from said amino acid sequence of said transfer initiation peptide, provided that said amino acid sequence maintains the properties of a transfer initiation peptide.

In a particular embodiment of the invention, the transfer initiation peptide sequence corresponds to the 19 C-terminal amino acids of the sequence coding the capsid (core) protein of the Zika virus, and is notably represented by SEQ ID NO. 25. The synthesis of this transfer initiation peptide (and consequently the fusion protein) is initiated by an initiation codon internal to the sequence coding the capsid protein (notably represented by SEQ ID NO. 27), located 17 codons before the first codon coding this transfer initiation peptide. Advantageously, a transfer initiation peptide of the art is used in the fusion proteins whose Zika virus isolate protein comprises a fusion peptide comprising the envelope protein E and the protein prM.

In another embodiment of the invention, the transfer initiation peptide sequence corresponds to the second transmembrane domain of prM, i.e. to the 15 amino acids located at the C-terminal end of prM, and is notably represented by SEQ ID NO. 26. The synthesis of this transfer initiation peptide is initiated by introduction through directed mutagenesis of an initiation codon (notably represented by SEQ ID NO. 28), located 9 codons before the first codon coding this transfer initiation peptide. Advantageously, a transfer initiation peptide of the art is used in the fusion proteins whose Zika virus isolate protein comprises only the envelope protein E.

The insertion of a transfer initiation peptide at the N-terminal end of the above-mentioned fusion protein is particularly advantageous in that it adds the properties of a transfer initiation peptide to the fusion peptide according to the invention. In particular, this allows co-translational address of the invention to the endoplasmic reticulum, such that it is correctly glycolyzed and that its three-dimensional conformation and/or that its antigenic qualities do not present substantial alterations with regards to the wild-type proteins.

In a particular embodiment, the present invention relates to the above-mentioned fusion protein in which the first and second peptides are contiguous and the C-terminal end of the second peptide is covalently bonded to the N-terminal end of the first peptide.

In a particular embodiment, the above-mentioned fusion protein is capable of forming spherical and/or filamentous subviral, non-infectious and immunogenic particles.

In a particular embodiment of the invention, a binding peptide binds the first and second peptides constituting the above-mentioned fusion protein, said binding peptide being constituted of 1 amino acid, or of 2 amino acids, or of 3 amino acids, or of 4 amino acids, or of 5 amino acids, provided that said fusion protein maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the first peptide in the C-terminal position is constituted of:

- an amino acid sequence defined by the contiguous amino acids located from position 24 to position 226 of the protein S of a human HBV isolate, notably the amino acid sequence represented by SEQ ID NO. 1, or
- an amino acid sequence presenting an identity percent of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus, or,
- the amino acid sequence of a natural variant from another isolate of the HBV, or of a synthetic variant derived from said amino acid sequence of the protein S deleted from its transmembrane domain at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus.

The term “position 24” refers to the amino acid 24 of the sequence of the protein S of the human HBV, the amino acid 1 being the first amino acid from the N-terminal side, and the amino acid 226 being the first amino acid from the C-terminal side.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the first peptide in the C-terminal position is constituted of:

- an amino acid sequence defined by the contiguous amino acids located from position 1 to position 226 of the protein S of a human HBV isolate, notably the amino acid sequence represented by SEQ ID NO. 2, or
- an amino acid sequence presenting an identity percent of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S not deleted from its transmembrane domain located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus, or,
- the amino acid sequence of a natural variant from another isolate of the HBV, or of a synthetic variant derived from said amino acid sequence of the protein S not deleted from its transmembrane domain at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus.

The sequence of the protein S not deleted at the N-terminal end thereof, SEQ ID NO. 2, corresponds to the complete sequence of the protein S, notably the protein S of the human HBVadw isolate.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the first peptide in the C-terminal position is constituted of:

- an amino acid sequence defined by the contiguous amino acids located from position 55 to position 281 of the protein M of a human HBV isolate, notably the amino acid sequence represented by SEQ ID NO. 3, or
- an amino acid sequence presenting an identity percent of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus, or,
- the amino acid sequence of a natural variant from another isolate of the HBV, or of a synthetic variant derived from said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the first peptide in the C-terminal position is constituted of:

- an amino acid sequence defined by the contiguous amino acids located from position 1 to position 281 of the protein M of a human HBV isolate, notably the amino acid sequence represented by SEQ ID NO. 4, or
- an amino acid sequence presenting an identity percent of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus, or,
- the amino acid sequence of a natural variant from another isolate of the HBV, or of a synthetic variant derived from said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus.

The sequence of the protein M not deleted from a sequence of 1 to 54 amino acids at the N-terminal end thereof, SEQ ID NO. 4, corresponds to the complete sequence of the protein M, notably the protein M of the human HBVadw isolate.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the second peptide in the N-terminal position is constituted of:

- an amino acid sequence defined by the contiguous amino acids located from position 1 to position 484 of the envelope protein E of a Zika virus isolate, notably the amino acid sequence represented by SEQ ID NO. 5, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, or,
- the amino acid sequence of a natural variant from another isolate of the Zika virus, or of a synthetic variant derived from said amino acid sequence of the envelope protein E of a Zika virus, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the second peptide in the N-terminal position is constituted of:

- an amino acid sequence defined by the contiguous amino acids located from position 1 to position 504 of the envelope protein E of a Zika virus isolate, notably the amino acid sequence represented by SEQ ID NO. 15, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, or,
- the amino acid sequence of a natural variant from another isolate of the Zika virus, or of a synthetic variant derived from said amino acid sequence of the envelope protein E of a Zika virus, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the second peptide in the N-terminal position is constituted of:

- an amino acid sequence of a fusion peptide comprising the contiguous amino acids located from position 1 to position 484 of the envelope protein E of a Zika virus isolate and the contiguous amino acids located from position 1 to position 164 of the protein prM of a Zika virus isolate, notably the amino acid sequence represented by SEQ ID NO. 6, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, or,
- the amino acid sequence of a natural variant from another isolate of the Zika virus, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus.

In another particular embodiment, the present invention relates to an above-mentioned fusion protein, in which the second peptide in the N-terminal position is constituted of:

- an amino acid sequence of a fusion peptide comprising the contiguous amino acids located from position 1 to position 504 of the envelope protein E of a Zika virus isolate and the contiguous amino acids located from position 1 to position 164 of the protein prM of a Zika virus isolate, notably the amino acid sequence represented by SEQ ID NO. 16, or
- an amino acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, or,
- the amino acid sequence of a natural variant from another isolate of the Zika virus, or of a synthetic variant derived from said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 7, or
- an amino acid sequence presenting an identity percent of at least 88%, notably of at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 7, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 7, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

As indicated in Table 1 of the present patent application, SEQ ID NO. 7 corresponds to the fusion protein sequence “deleted E+deleted S.” SEQ ID NO. 7 thus corresponds to the fusion of SEQ ID NO. 5 and SEQ ID NO. 1. However, it should be noted that in SEQ ID NO. 7, the last amino acid in the C-terminal (D, aspartic acid) of SEQ ID NO. 5 is not present. This presents the advantage of deactivating a peptidase cleavage site. This reasoning applies mutatis mutandis to the other fusion protein sequences according to the invention.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 7 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 17, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 17, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 17, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 8, or
- an amino acid sequence presenting an identity percent of at least 88%, notably at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 8, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 8, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 8 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 18, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 18, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 18, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 9, or
- an amino acid sequence presenting an identity percent of at least 88%, notably at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 9, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 9, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 9 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 19, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 19, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 19, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 10, or
- an amino acid sequence presenting an identity percent of at least 88%, notably at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 10, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 10, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 10 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 20, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 20, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 20, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 11, or
- an amino acid sequence presenting an identity percent of at least 88%, notably at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 11, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 11, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 11 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 21, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 21, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 21, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 12, or
- an amino acid sequence presenting an identity percent of at least 88%, notably at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 12, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 12, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 12 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 22, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 22, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 22, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 13, or
- an amino acid sequence presenting an identity percent of at least 88%, notably at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 13, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 13, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 13 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 23, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 23, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 23, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, a fusion protein such as those mentioned above comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 14, or
- an amino acid sequence presenting an identity percent of at least 88%, notably at least 89%, particularly of at least 92%, and more particularly of at least 95%, with said SEQ ID NO. 14, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 14, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the fusion protein of the above-mentioned SEQ ID NO. 14 also comprises a transfer initiation peptide located on the N-terminal side and comprises or is constituted of:

- the amino acid sequence represented by SEQ ID NO. 24, or
- an amino acid sequence presenting an identity percent of at least 83%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 24, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 24, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

Said SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23, SEQ ID NO. 24 also comprise, at the N-terminal ends thereof, the amino acid sequence allowing the synthesis of said transfer initiation peptide (and notably the initiation sequence of SEQ ID NO. 27 or SEQ ID NO. 28).

The initiating SEQ ID NO. 27 is more particularly used when the fusion protein according to the invention comprises the protein prM.

The initiating SEQ ID NO. 28 is more particularly used when the fusion protein according to the invention does not comprise the protein prM.

In a second embodiment, the present invention also relates to a nucleic acid molecule coding an above-mentioned fusion protein.

The expression “nucleic acid molecule” refers to a nucleic acid molecule comprising at least one sequence coding the protein S or the protein M of a human HBV isolate deleted at the N-terminal end thereof, and at least one sequence coding at least the transmembrane domain and the ectodomain of at least one envelope protein E of a Zika virus isolate, or any molecule from a molecule defined above and modified following the natural degeneration of its genetic code.

In an embodiment of the invention, this nucleic acid molecule is a hybrid. In a particular embodiment, the nucleic acid molecule mentioned above, coding an above-mentioned fusion protein, comprises at least the following two nucleic acid sequences:

a) —on side 3′, a first constituted nucleic acid sequence coding the protein S or the protein M of a human hepatitis B virus (HBV) isolate, which protein S or protein M is optionally deleted at the N-terminal end thereof, or

- a nucleic acid sequence presenting an identity percent of at least 91%, notably of at least 93%, particularly of at least 95%, and more particularly of at least 97%, with said amino acid sequence of the protein S or the protein M optionally deleted at the N-terminal end thereof, provided that said protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV, or
- the nucleic acid sequence of a natural variant from another human HBV isolate, or of a synthetic variant derived from said nucleic acid sequence of the protein S or the protein M optionally deleted at the N-terminal end thereof, provided that said protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV, and

b) —on side 5′ of the first sequence, a second nucleic acid sequence coding at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate, or

- a nucleic acid sequence presenting an identity percent of at least 90%, notably of at least 95%, with said nucleic acid sequence coding at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate, provided that said at least one transmembrane domain and ectodomain coded by said nucleic acid sequence maintain the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, or
- the nucleic acid sequence of a natural variant from another Zika isolate, or of a synthetic variant derived from said nucleic acid sequence of at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate, provided that said at least one transmembrane domain and ectodomain coded by said nucleic acid sequence maintain the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, said protein of a Zika virus isolate being chosen from among the envelope protein E or a fusion peptide comprising the envelope protein E and the protein prM.

The nucleic acid molecule can also comprise, on the side 5′ of the second sequence, a nucleic acid sequence coding a transfer initiation peptide.

In another particular embodiment, the present invention relates to an above-mentioned nucleic acid molecule also comprising, at its end 5′ (i.e. at the end 5′ of the second peptide), another peptide constituted of:

- the nucleic acid sequence coding a transfer initiation peptide of a Zika virus isolate, or
- a nucleic acid sequence presenting an identity percentage of at least 83%, notably of at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said nucleic acid sequence coding a transfer initiation peptide of a Zika virus isolate,
- the nucleic acid sequence of a natural variant from another Zika isolate, or of a synthetic variant derived from said nucleic acid sequence coding a transfer initiation peptide, provided that said nucleic acid sequence maintains the properties of a transfer initiation peptide.

In a particular embodiment of the invention, the nucleic acid sequence coding a transfer initiation peptide corresponds to the 57 C-terminal nucleic acids of the sequence coding the capsid (core) protein of the Zika virus, and is notably represented by SEQ ID NO. 30. The synthesis of this transfer initiation peptide (and consequently of the fusion protein) is initiated by an initiation codon internal to the sequence coding the capsid protein (notably represented by SEQ ID NO. 32), located 17 codons before the first codon coding this transfer initiation peptide. Advantageously, a transfer initiation peptide of the art is used in the nucleic acid molecules coding the fusion protein whose protein of a Zika virus isolate comprises a fusion peptide comprising the envelope protein E and the protein prM.

In another embodiment of the invention, the transfer initiation peptide sequence corresponds to the second transmembrane domain of prM, i.e. to the 45 nucleic acids located at the C-terminal end of prM, and is notably represented by SEQ ID NO. 31. The synthesis of this transfer initiation peptide is initiated by introduction through directed mutagenesis of an initiation codon (notably represented by SEQ ID NO. 33), located 9 codons before the first codon coding this transfer initiation peptide. Advantageously, a transfer initiation peptide of the art is used in the nucleic acid molecules coding the fusion proteins whose Zika virus isolate protein comprises only the envelope protein E.

In one embodiment of the invention, the nucleic acid sequences coding the transmembrane domains, notably the nucleic acid sequences coding the transmembrane domains of the envelope protein E are deleted from one, two or three codons in position 3′ to delete one, two or three amino acids in the C-terminal position, which presents the advantage of deactivating the peptidase cleavage site, which is necessary for the maturation of the Zika polyprotein, but which is not necessary in the scope of chimeric constructions of the present invention.

In another embodiment of the invention, the first and second nucleic acid sequences of the above-mentioned nucleic acid molecule coding the above-mentioned immunogenic fusion protein are contiguous, and the end 5′ of the first nucleic acid sequence is covalently bonded to end 3′ of the second nucleic acid sequence.

The term “end 5′” is understood to be the position 5′ or the side 5′ of a nucleic acid sequence.

The term “end 3′” is understood to be the position 3′ or the side 3′ of a nucleic acid sequence.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 34, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 34, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 34, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

The expression “at least 80%” means 80%, 81%, 82%, 83%, 84%, 85%, 86%, 87%, 88%, 89%, 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98%, 99% and 100%.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 34 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 42, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 42, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 42, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

The expression “at least 78%” means 78%, 79%, 80%, 81%, 82%, 83%, 84%, 85%, 86%, 87%, 88%, 89%, 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98%, 99% and 100%.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 35, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 35, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 35, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 35 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 43, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 43, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 43, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 36, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 36, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 36, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 36 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 44, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 44, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 44, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 37, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 37, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 37, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 37 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 45, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 45, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 45, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 38, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 38, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 38, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 38 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 46, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 46, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 46, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 39, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 39, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 39, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 39 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 47, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 47, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 47, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 40, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 40, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 40, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 40 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 48, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 48, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 48, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, said nucleic acid molecule coding an above-mentioned fusion protein comprises or is constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 41, or
- a nucleic acid sequence presenting an identity percent of at least 80%, notably at least 85%, particularly of at least 90%, and more particularly of at least 95%, with said SEQ ID NO. 41, provided that the fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 41, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

In a particular embodiment, the nucleic acid molecule of the above-mentioned SEQ ID NO. 41 also comprises, on side 5′, a nucleic acid sequence coding a transfer initiation peptide, said nucleic acid molecule comprising or being thus constituted of:

- the nucleic acid sequence represented by SEQ ID NO. 49, or
- a nucleic acid sequence presenting an identity percent of at least 78%, notably at least 80%, particularly of at least 85%, and more particularly of at least 90%, with said SEQ ID NO. 49, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus, or
- the nucleic acid sequence of a synthetic variant derived from said SEQ ID NO. 49, provided that said fusion protein coded by said nucleic acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the human HBV and/or the Zika virus.

Said SEQ ID NO. 42, SEQ ID NO. 42, SEQ ID NO. 43, SEQ ID NO. 44, SEQ ID NO. 45, SEQ ID NO. 46, SEQ ID NO. 47, SEQ ID NO. 48, SEQ ID NO. 49 also comprises, at their end 5′, a nucleic acid sequence coding said transfer initiation peptide (and notably the initiation sequence of SEQ ID NO. 32 or SEQ ID NO. 33).

The initiation sequence of SEQ ID NO. 32 is used in nucleic acid molecules comprising the nucleic acid sequence coding the protein prM.

The initiation sequence of SEQ ID NO. 33 is used in the nucleic acid molecules not comprising the nucleic acid sequence coding the protein prM.

In a third embodiment, the present invention also relates to a vector comprising an above-mentioned nucleic acid molecule, coding an above-mentioned fusion protein, as well as the means necessary for its expression. Said means necessary for its expression are operationally bonded to said nucleic acid molecule.

In one embodiment of the invention, said molecule of nucleic acids comprised in an above-mentioned sector comprises SEQ ID NO. 34; SEQ ID NO. 35; SEQ ID NO. 36; SEQ ID NO. 37; SEQ ID NO. 38; SEQ ID NO. 39; SEQ ID NO. 40; SEQ ID NO. 41; SEQ ID NO. 42; SEQ ID NO. 43; SEQ ID NO. 44; SEQ ID NO. 45; SEQ ID NO. 46; SEQ ID NO. 47; SEQ ID NO. 48 and/or SEQ ID NO. 49.

The expression “means necessary for the expression” of a protein (the term protein being used for any amino acid molecule, such as a protein, fusion protein, protein fragment, peptide, polyprotein, polypeptide, etc.) is understood to be any means that allows the protein to be obtained, notably a promoter, a transcription terminator, a replication origin and preferably a selection marker. The means necessary for the expression of a peptide are operationally bonded to the nucleic acid sequence coding said peptide (of interest).

The means necessary for the expression of a peptide may be homologous means, i.e. included in the genome of the vector used, or heterologous. In the latter case, said means are cloned with the peptide of interest to be expressed.

The expression “operationally bonded” refers to a juxtaposition of said elements necessary for expression and of the gene coding said peptide (of interest), which are in a relationship such that it allows them to function in an expected way. For example, there may be additional bases between the promoter and the gene of interest so long as their functional relationship is maintained.

In a particular embodiment, said vector is chosen from among the plasmids, the lentiviral vectors, the Semliki vector, an adenovirus, a poxvirus, the virus of the vaccine, a baculovirus, Salmonella bacterial vectors and BCG.

In a particularly preferred embodiment, said vector is a lentiviral vector, notably the pLenti vector. This was previously described (Naldini, L., Blomer, U., Gallay, P., Ory, D., Mulligan, R., Gage, F. H., Verma, I. M., and Trono, D. (1996). In vivo gene delivery and stable transduction of nondividing cells by a lentiviral vector. Science 272(5259), 263-7).

In a particularly preferred embodiment, said vector is the Semliki vector.

In a particularly preferred embodiment, said vector is a defective viral vector derived from the genome of the Semliki Forest virus, notably the pSFV1 vector.

These viruses were previously described by Schlesinger, S., and T. M. Dubensky, Jr. 1999. Alphavirus vectors for gene expression and vaccines. Curr. Opin. Biotechnol. 10:434-439.

In a particular embodiment, the above-mentioned vector also comprises a promoter, notably a heterologous promoter, chosen from among:

- (i) viral promoters such as the SV40 promoter (simian virus 40), the promoter of the thymidine-kinase gene of the herpes simplex virus (TK-HSV-1), the LTR of Rous sarcoma virus (RSV), the promoter of the cytomegalovirus (CMV) and the adenovirus major late promoter (MLP);
- (ii) any cellular promoter that controls the transcription of genes coding four peptides in superior eukaryotes, such as the constitutive promoter of the phosphoglycerate-kinase (PGK) gene ((Adra et al., 1987, Gene, 60: 65-74)), the promoter of genes specific to the alpha-1 antitrypsine liver and FIX and the SM22 promoter specific to smooth muscle tissues (Moessler et al., 1996, Development, 122: 2415-2425).

In a preferred embodiment, the promoter is that of the cytomegalovirus (CMV).

In a fourth embodiment, the present invention also relates to a subviral, non-infectious and immunogenic particle comprising the following proteins:

- the protein constituted of the wild-type domain S of the surface antigen of a hepatitis B virus isolate, and
- at least one above-mentioned fusion protein.

In one embodiment, the invention also relates to a subviral, non-infectious and immunogenic particle comprising the following proteins:

- the protein constituted of the wild-type domain S of the surface antigen of a hepatitis B virus isolate, and
- at least one fusion protein represented by SEQ ID NO. 7, SEQ ID NO. 8, SEQ ID NO. 9, SEQ ID NO. 10, SEQ ID NO. 11, SEQ ID NO. 12, SEQ ID NO. 13, SEQ ID NO. 14, SEQ ID NO. 15, SEQ ID NO. 16, SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23 or SEQ ID NO. 24.

The particles according to the invention are thus well structured and efficaciously secreted and are capable of inducing a quality antigenic response.

The expression “subviral, non-infectious particle” refers to a filamentous or spherical particle, resulting from the assembly of the wild-type protein S of the HBV and/or the protein S deleted from its N-terminal transmembrane domain, said particle being devoid of viral genome, and notably synthesized and secreted in very great excess, and which can be analyzed by any protocol allowing demonstration of the absence of nucleotide fragments specific to HBV or Zika, such as the amplification by PCR or RT-PCR previously described:

- concerning Zika, by [Faye O1, Faye O, Dupressoir A, Weidmann M, Ndiaye M, Alpha Sall A. One-step RT-PCR for detection of Zika virus. J Clin Virol. 2008 September; 43 (1): 96-101];
- concerning HBV, by [Thibault V, Pichoud C, Mullen C, Rhoads J, Smith J B, Bitbol A, Thamm S, Zoulim F. Characterization of a new sensitive PCR assay for quantification of viral DNA isolated from patients with hepatitis B virus infections. J. Clin. Microbiol. 2007 December 45(12):2948-53];

and whose result is negative.

In a fifth embodiment, the invention also relates to an above-mentioned fusion protein for its use as a medication.

The invention also relates to an above-mentioned subviral particle for its use as a medication.

In a preferred embodiment, said medication is a vaccine.

In one embodiment, the invention also relates to a fusion protein represented by SEQ ID NO. 7, SEQ ID NO. 8, SEQ ID NO. 9, SEQ ID NO. 10, SEQ ID NO. 11, SEQ ID NO. 12, SEQ ID NO. 13, SEQ ID NO. 14, SEQ ID NO. 15, SEQ ID NO. 16, SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23 or SEQ ID NO. 24 for its use as a medication.

In another embodiment, the invention also relates to a subviral, non-infectious and immunogenic particle comprising the following proteins:

- the protein constituted of the wild-type domain S of the surface antigen of a hepatitis B virus isolate, and
- at least one fusion protein represented by SEQ ID NO. 7, SEQ ID NO. 8, SEQ ID NO. 9, SEQ ID NO. 10, SEQ ID NO. 11, SEQ ID NO. 12, SEQ ID NO. 13, SEQ ID NO. 14, SEQ ID NO. 15, SEQ ID NO. 16, SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23 or SEQ ID NO. 24
  
  for its use as a medication.

In a particular embodiment, the invention also relates to a composition comprising an above-mentioned fusion protein as an active substance.

The invention also relates to a composition comprising an above-mentioned subviral particle as an active substance.

In a preferred embodiment, said composition is a vaccine composition.

In one embodiment, the invention also relates to a composition comprising a fusion protein represented by SEQ ID NO. 7, SEQ ID NO. 8, SEQ ID NO. 9, SEQ ID NO. 10, SEQ ID NO. 11, SEQ ID NO. 12, SEQ ID NO. 13, SEQ ID NO. 14, SEQ ID NO. 15, SEQ ID NO. 16, SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23 or SEQ ID NO. 24 as an active substance.

In another embodiment, the invention also relates to a composition comprising, as an active substance, a subviral, non-infectious and immunogenic particle comprising the following proteins:

- the protein constituted of the wild-type domain S of the surface antigen of a hepatitis B virus isolate, and
- at least one fusion protein represented by SEQ ID NO. 7, SEQ ID NO. 8, SEQ ID NO. 9, SEQ ID NO. 10, SEQ ID NO. 11, SEQ ID NO. 12, SEQ ID NO. 13, SEQ ID NO. 14, SEQ ID NO. 15, SEQ ID NO. 16, SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23 or SEQ ID NO. 24.

In a sixth embodiment, the invention also relates to an above-mentioned fusion protein for its use in preventing and/or treating hepatitis B and/or Zika virus infections.

The invention also relates to an above-mentioned subviral particle for its use in preventing and/or treating hepatitis B and/or Zika virus infections.

The expression “Zika virus infections” is understood to be infections by the Zika virus or infections linked to Zika virus.

In another embodiment, the invention also relates to a subviral, non-infectious and immunogenic particle comprising the following proteins:

- the protein constituted of the wild-type domain S of the surface antigen of a hepatitis B virus isolate, and
- at least one fusion protein represented by SEQ ID NO. 7, SEQ ID NO. 8, SEQ ID NO. 9, SEQ ID NO. 10, SEQ ID NO. 11, SEQ ID NO. 12, SEQ ID NO. 13, SEQ ID NO. 14, SEQ ID NO. 15, SEQ ID NO. 16, SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23 or SEQ ID NO. 24
  
  for its use in preventing and/or treating hepatitis B and/or Zika virus infections.

In a seventh embodiment, the invention also relates to a cellular line that expresses above-mentioned subviral, non-infectious and immunogenic particles.

In one embodiment, the invention also relates to a cellular line that expresses a subviral, non-infectious and immunogenic particle comprising the following proteins:

- the protein constituted of the wild-type domain S of the surface antigen of a hepatitis B virus isolate, and
- at least one fusion protein represented by SEQ ID NO. 7, SEQ ID NO. 8, SEQ ID NO. 9, SEQ ID NO. 10, SEQ ID NO. 11, SEQ ID NO. 12, SEQ ID NO. 13, SEQ ID NO. 14, SEQ ID NO. 15, SEQ ID NO. 16, SEQ ID NO. 17, SEQ ID NO. 18, SEQ ID NO. 19, SEQ ID NO. 20, SEQ ID NO. 21, SEQ ID NO. 22, SEQ ID NO. 23 or SEQ ID NO. 24.

In a particular embodiment, said cellular line is chosen from among:

- yeasts, such as those from the following families: Saccharomyces, Schizosaccharomyces, Kluveromyces, Pichia, Hanseluna, Yarowia, Schwaniomyces, Zygosaccharomyces, Saccharomyces cerevisiae, Saccharomyces carlsbergensis and Kluveromyces lactis;
- bacteria, such as E. coli and those from the following families: Lactobillicus, Lactococcus, Salmonella, Streptococcus, Bacillus and Streptomyces.

In a particular embodiment, said cellular line is chosen from among the eukaryotic cells, notably the cells from animals like mammals, reptiles, insects and the equivalent, and more particularly:

- cells from Chinese hamsters (CHO cells);
- cells from monkeys (COS and Vero cells);
- cells from the dwarf hamster kidneys (BHK cells);
- cells from the pig kidneys (PK 15 cells);
- cells from rabbit kidneys (RK13 cells);
- the human cellular lines of osteosarcoma (143 B cells);
- HeLa human cellular cells;
- the human cellular lines of hepatoma (Hep G2 cells);
- insect cellular lines (e.g. from Spodoptera frugiperda).

In a particularly preferred embodiment, said cellular line is the ovary line of Chinese hamsters, called CHO. For more on this, see, for example, Michael ML, Pontisso P, Sobczak E, Malpièce Y, Streeck R E, Tiollais P. Synthesis in animal cells of hepatitis B surface antigen particles carrying a receptor for polymerized human serum albumin. Proc Natl Acad Sci USA. 1984 December; 81(24)7708-12.

In a particularly preferred embodiment, said cellular line is a yeast, notably Saccharomyces cerevisae.

In a particularly preferred embodiment, said cellular line is a cellular line from a newborn hamster kidney (BHK) and is particularly the cellular line from a newborn hamster kidney (BHK-21). For more on this, see, for example, Goldman R D, Follet E A. Birefringent filamentous organelle in BHK-21 cells and its possible role in cell spreading and motility. Science. 1970 Jul. 17; 169(942):286-8.

In an eighth embodiment, the present invention also relates to a method of producing the above-mentioned particles from an above-mentioned cellular line, comprising the following steps:

1—a step of TRANSDUCING the cells of the cellular line with a lentiviral vector comprising a nucleic acid sequence coding the wild-type protein S of a hepatitis B virus isolate,

2—a step of CULTIVATING said cells to produce a cellular line capable of expressing the subviral particles of wild-type envelope of the hepatitis B virus,

3—a step of SELECTING a clone presenting an optimal secretion of subviral particles of wild-type envelope of the hepatitis B virus,

4—a step of SUPERTRANSDUCING said clone with an above-mentioned vector,

5—a step of CULTIVATING said cells to produce a cellular line capable of expressing the above-mentioned subviral, non-infectious and immunogenic particles,

6—a step of SELECTING said cells capable of optimally secreting the above-mentioned subviral, non-infectious and immunogenic particles,

7—a step of CULTIVATING said cells to produce a the above-mentioned subviral, non-infectious and immunogenic particles, and

8—a step of PURIFYING the subviral particles from the collected culture environment (centrifugation, gradient ultracentrifugation, positive fraction collection for the chimeric subviral particles, dialysis).

Table 1 indicates the correspondence between the nucleic acid sequences and the amino acid sequences described in the present invention, as well as the genes/proteins associated with these sequences.

Nucleic

Gene/protein associated

sequence
Protein sequence
with these sequences

/
SEQ ID NO. 1
deleted S

/
SEQ ID NO. 2
S

/
SEQ ID NO. 3
deleted M

/
SEQ ID NO. 4
M

/
SEQ ID NO. 5
deleted E

/
SEQ ID NO. 6
prM + deleted E

SEQ ID NO. 34
SEQ ID NO. 7
deleted E + deleted S

(= SEQ ID NO. 5 +

SEQ ID NO. 1)

SEQ ID NO. 35
SEQ ID NO. 8
prM + deleted E + deleted S

SEQ ID NO. 36
SEQ ID NO. 9
E + S

SEQ ID NO. 37
SEQ ID NO. 10
prM + E + S

SEQ ID NO. 38
SEQ ID NO. 11
deleted E + M

SEQ ID NO. 39
SEQ ID NO. 12
prM + deleted E + M

SEQ ID NO. 40
SEQ ID NO. 13
E + M

SEQ ID NO. 41
SEQ ID NO. 14
prM + E + M

SEQ ID NO. 15
E

SEQ ID NO. 16
prM + E

SEQ ID NO. 42
SEQ ID NO. 17
TIP + deleted E + deleted S

SEQ ID NO. 43
SEQ ID NO. 18
TIP + prM + deleted E +

deleted S

SEQ ID NO. 44
SEQ ID NO. 19
TIP + E + S

SEQ ID NO. 45
SEQ ID NO. 20
TIP + prM + E + S

SEQ ID NO. 46
SEQ ID NO. 21
TIP + deleted E + M

SEQ ID NO. 47
SEQ ID NO. 22
TIP + prM + deleted E + M

SEQ ID NO. 48
SEQ ID NO. 23
TIP + E + M

SEQ ID NO. 49
SEQ ID NO. 24
TIP + prM + E + M

SEQ ID NO. 30
SEQ ID NO. 25
Transfer initiation peptide

SEQ ID NO. 31
SEQ ID NO. 26
Transfer initiation peptide

SEQ ID NO. 32
SEQ ID NO. 27
Initiation sequence

SEQ ID NO. 33
SEQ ID NO. 28
Initiation sequence

SEQ ID NO. 29
/
Zika virus, accession

number KU312312.1

/
SEQ ID NO. 50
prM

SEQ ID NO. 51

Synthesis gene (as represented

in FIG. 6) allowing the fusion

peptide prM + E to be obtained,

or allowing all the structural

peptides of Zika to be obtained

(the capsid protein C, the protein

prM and the envelope protein E).

SEQ ID NO. 52
/
Zika virus, accession number

KU32169

SEQ ID NO. 53
/
pSFV1-prM + E + S

SEQ ID NO. 54
/
pSFV1-prM + deleted

E + deleted S″

SEQ ID NO. 55
/
pSFV1-prM + E + S

SEQ ID NO. 56
/
pSFV1′^puro-HBV-prM + E + S

SEQ ID NO. 57
/
pSFV1′^puro-HBV-prM +

deleted E + deleted S

SEQ ID NO. 58
/
pSFV1′^puro-HBV-prM + E + M

SEQ ID NO. 59
/
Zika virus Polynesian

strain

The term “TIP” means that:

the initiation sequence (allowing the synthesis of the transfer initiation peptide) and the sequence of said transfer initiation peptide are present in the fusion protein sequences according to the invention, or

the sequence coding the initiation sequence and the sequence coding said transfer initiation peptide are present in the sequences coding the fusion proteins according to the invention.

SEQ ID NO. 34; SEQ ID NO. 35; SEQ ID NO. 36; SEQ ID NO. 37; SEQ ID NO. 38; SEQ ID NO. 39; SEQ ID NO. 40; SEQ ID NO. 41; SEQ ID NO. 42; SEQ ID NO. 43; SEQ ID NO. 44; SEQ ID NO. 45; SEQ ID NO. 46; SEQ ID NO. 47; SEQ ID NO. 48 and SEQ ID NO. 49 possess a “taa” stop codon at their end 3′.

TABLE 2

lists the sequences of the present invention:

SEQ
Riltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipi

ID
psswafakylwcwasvrfswlsllvpfvqwfvqlsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

NO:

1

SEQ
Menitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgns

ID
mfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

NO:

2

SEQ
nmenitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhspfscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgn

ID
smfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

NO:

3

SEQ
Mqwnstafhqtlqdprvrglylpaggsssgtvnpapniashissisartgdpvtnmenitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgy

ID
rwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmm

NO:
wywgpslysivspfipllpiffclwvyi

4

SEQ
ircigvsnrdfvegmsggtwvdvvlchggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfa

ID
cskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkewfhdiplpwhagadtgtphwnnke

NO:
alvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanp

5
vitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakmavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmnwlglnakngsd

SEQ
rrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyecpmldegvepddvdcwcnttstwvvygtchhkkgearrsrravtlpshstrklqtrsqtwlesreytkhlirve

ID
nwifrnpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgea

NO:
yldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyl

6
tmnnkhwlvhkcwfhdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgt

vtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgi

hqifgaafkslfggmswfsqiligtllmwlglnakngsd

SEQ
ircigvsnrdfvcgmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfa

ID
cskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkcwfhdiplpwhagadtgtphwnnke

NO:
alvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanp

7
vitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsrilt

ipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipss

wafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmvywgpslysivspfipllpiffclwvyi

SEQ
rrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyecpmldegvepddvdcwcnttstwvvygtchhkkgearrsrravtlpshstrklqtrsqtwlesreytkhlirve

ID
nwifrnpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgea

NO:
yldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyl

8
tmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgt

vtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgi

hqifgaafkslfggmswfsqiligtllmwlglnakngsriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgst

ttstgpcktcttpaqgasmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
ircigvsnrdvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfa

ID
cskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltmmnkhwlvhkewfhdiplpwhagadtglphwnnke

NO:
alvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanp

9
vitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsisl

mclalggvliflstavsaenitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgs

tttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
rrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyecpmldcgvepddvdcwcnttstwvygtchhkkgearrsrravtlpshstrklqtrsqtwlesreytkhlirve

ID
nwifrnpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgea

NO:
yldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyl

10
tmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqegavhtalagaleaeindgakgrlssghlkcrlkindklrlkgvsyslctaaftftkipaetlhgt

vtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkitlihwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgi

hqifgaafkslfggmswfsqiligtllmwlglnakngsislmclalggvliflstavsaenitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpg

yrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgmmfpsccctkptdgnctcipipsswafakylwcwasvrfswlsllvpfvqwfvglsptvwlsaiwm

mwywgpslysivspfipllpiffclwvyi

SEQ
ircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfa

ID
cskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspracatlggfgslgldccprtgldfsdlyyltmnnkhwlvhkewfhdiplpwhagadtgtphwnnkc

NO:
alvefkdahakrqtvwlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipactlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanp

11
vitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnalcngsq

wnstafhqtlqdprvrglylpaggsssgtvnpapniaslussisartgdpvtnmenitsgflgpllvlqagfnitriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrw

mclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwminw

ywgpslysivspfipllpiffclwvyi

SEQ
rrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyecpmldegvepddvdcwcnttstwvvygtchhkkgearrsrravtlpshstrklqtrsqtwlesreytkhlirve

ID
nwifrnpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgea

NO:
yldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrdkveitpnspraeatlggfgslgldceprtgldfsdlyyl

12
tmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgt

vtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgckkithhwhrsgstigkafcatvrgakrmavlgdtawdfgsvggalnslgkgi

hqifgaafkslfggmswfsqiligtllmwlglnakngsqwnstafhqtlqdprvrglylpaggsssgtvnpapniashissisartgdpvtnmenitsgflgpllvlqagfflltriltipqsldsw

wtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylw

ewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
ircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfa

ID
cskkmtgksiqpenleyrimlsvhgsqhsgmivndtghctdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkcwfhdiplpwhagadtgtphwnnke

NO:
alvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanp

13
vitestenskmmleldppfgdsyivigvgekkithliwhrsgstigkafeatvrgaknnavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsisl

mclalggvliflstavsaqwnstafliqtlqdprvrglylpaggsssgtvnpapmashissisartgdpvtnmenitsgflgpllvlqagllflltriltipqsldswwtslnflggspvclgqnsqspt

snhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfv

glsptvwlsaiwmmwywgpslysivspflpllpiffclwvyi

SEQ
rrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyecpmldegvepddvdcwcnttstwvvygtchhkkgcarrsrravtlpshstrklqtrsqtwlesreytkhlirve

ID
nwifmpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvniaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgea

NO:
yldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyl

14
tmrmkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqcgavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgt

vtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgi

liqifgaafkslfggmswfsqiligtllmwlglnakngsislmclalggvliflstavsaqwnstafhqtlqdprvrglylpaggsssgtvnpapniashissisartgdpvtnmenitsgflgpllv

lqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdg

nctcipipsswafakylwcwasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
ircigvsnrdfvegmsggtwvdvvldiggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvteakfa

ID
cskkmtgksiqpenleyrimlsvhgsqhsgmradtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltnmnkhwlvhkewfhdiplpwhagadtgtphwnnke

NO:
alvcfkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanp

15
vitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsisl

mclalggvliflstavsa

SEQ
rrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyccpmldcgvepddvdcwcnttstwvvygtchhkkgearrsrravtlpshstrklqtrsqtwlesreytkhlirve

ID
nwifrnpgfaiaaaaiawllgsstsqkviylvmilliapaysircigvsnrdivegmsggtwvdvvlehggcvtvmaqdkptvdielvttlvsnmaevrsycyeasisdmasdsrcptqgea

NO:
yldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkrntgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyl

16
tmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvwlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgt

vtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafealvrgakrmavlgdtawdfgsvggalnslgkgi

liqifgaafkslfggmswfsqiligtllmwlglnakngsislmclalggvliflstavsa

SEQ
mlgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvrnaqdkptvdielvtttvsnmaevrsycyeasisdniasdsrcptqgeayldkqsdtqyvckrtlv

ID
drgwgngcglfgkgslvtcakfacskkmtgksiqpcnleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkewf

NO:
hdiplpwhagadtgtphwmikealvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipactlhgtvtvcvqyagtdgpck

17
vpaqmavdmqtltpvgrlitanpvitestenskninileldppfgdsyivigvgekkithhwhrsgstigkafcatvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggms

wfsqiligtllmwlglnakngsriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgn

smfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
mlriinarkekkrrgadtsvgivglllttamaaevtrrgsayymyldmdageaisfpttlgnmkcyiqimdlghtcdatmsyecpmldegvepddvdcwcnttstwvvygtchhkkgear

ID
rsrravtlpshstrklqtrsqtwlesreytkhlirvenwifrnpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvcgmsggtwvdvvlehggcvtvmaqdkptvdielvtt

NO:
tvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmnivndtghetdenrakve

18
itpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvwlgsqegavhtalagaleaemdgakgrlssghl

kcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdinqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithliwhrsgstigkafea

tvrgaknnavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmc

lrrfnflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwIsaiwmmwyw

gpslysivspfipllpiffclwvyi

SEQ
migsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlv

ID
drgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtgheldenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkcwf

NO:
hdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpck

19
vpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggms

wfsqiligtllmwlglnakngsislmclalggvliflstavsaenitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllcl

ifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfi

pllpiffclwvyi

SEQ
mlriinarkekkrrgadtsvgivglllttamaacvlrrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyecpmldegvcpddvdcwcnttstwvvygtdihkkgear

ID
rsrravtlpshstrklqtrsqtwlcsrcytkhlirvenwifrnpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdwlehggcvtvmaqdkptvdielvtt

NO:
tvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakve

20
itpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghl

kcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafea

tvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsislmclalggvliflstavsaenitsgflgpllvlqagfflltriltipqsldswwtsl

nflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgiismfpsccctkptdgiictcipipsswafakylwewa

svrfswlsllvpfVqwfVglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
mlgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgcayldkqsdtqyvckrtlv

ID
drgwgngcglfgkgslvtcakfacskkmtgksiqpcnlcyrimlsvhgsqhsgmivndtghctdcnrakveitpnspracatlggfgslgldccprtgldfsdlyyltmnnkhwlvhkewf

NO:
hdiplpwhagadtgtphwnnkealvefkdahakiqtvwlgsqegavhtalagalcaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaflftkipaetlhgtvtvevqyagtdgpck

21
vpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafeatvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggms

wfsqiligtllmwlglnakngsqwnstafliqtlqdprvrglylpaggsssgtvnpapniashissisarfgdpvtnmenitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqn

sqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfv

qwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
mlriinarkekkngadtsvgivglllttamaaevtrrgsayymyldrndageaisfpttlginnkcyiqimdlghtcdatmsyecpmldegvepddvdcwcnttstwvvygtchhkkgear

ID
rsrravtlpshstrklqtreqtwlesreytkhlirvenwifmpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqdkptvdielvtt

NO:
tvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlvdrgwgngcglfgkgslvtcakfkcskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdcnrakvc

22
itpnspraeatlggfgslgldceprtgldfsdlyyltmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqmvlgsqcgavhtalagalcacmdgakgrlssghl

kcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafea

tvrgakrmavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsqwnstafhqtlqdprvrglylpaggsssgtvnpapniashissisartgdpvtn

memtsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwniclrrfiiflfilllclifllvlldyqgmlpvcplipgstttstgpcktcttpaqgns

mfpsccctkptdgnctcipipsswafakylwewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
mlgsstsqkviylvmilliapaysircigvsnrdfvegmsggtwvdvvlehggcvtvmaqclkptvdielvtttvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckrtlv

ID
drgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrimlsvhgsqhsgmivndtghetdenrakveitpnspraeatlggfgslgldceprtgldfsdlyyltmimkhwlvhkewf

NO:
hdiplpwhagadtgtphwnnkealvefkdahakrqtvwlgsqegavhtalagaleaemdgakgrlssghlkcrlkmdklrlkgvsyslctaaftftkipaetlhgtvtvevqyagtdgpck

23
vpaqinavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhisgstigkafeatvrgaknnavlgdtawdfgsvggalnslgkgihqifgaafkslfggins

wfsqiligtllmwlglnakngsislmclalggvliflstovsaqwnstafliqtlqdpmglylpaggsssgtvnpapniashissisartgdpvtnmenitsgflgpllvlqagfflltriltipqslds

wwtslnflggspvclgqnsqsptsnhsptscppicpgyrwniclrrfiiflfilllclifllvlldyqginlpvcplipgsttlstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakyl

wewasvrfswlsllvpfvqwfvglsptvwlsaiwmmwywgpslysivspfipllpiffclwvyi

SEQ
mlriinarkekkrrgadtsvgivglllttamaaevtrrgsayymyldrndageaisfpttlgmnkcyiqimdlghtcdatmsyccpmldegvepddvdcwcnttstwwygtchhkkgcar

ID
rsrravtlpslistrklqtrsqtwlesrcytkhlirvenwifrnpgfalaaaaiawllgsstsqkviylvmilliapaysircigvsnrdfvcgmsggtwvdwlchggcvtvmaqdkptvdielvtt

NO:
tvsnmaevrsycyeasisdmasdsrcptqgeayldkqsdtqyvckillvdrgwgngcglfgkgslvtcakfacskkmtgksiqpenleyrinilsvhgsqhsgmivndtghetdenrakve

24
itpnspraeatlggfgslgldccprtgldfsdlyyltmnnkhwlvhkewfhdiplpwhagadtgtphwnnkealvefkdahakrqtvvvlgsqegavhtalagaleaemdgakgrlssghl

kcrllamdklrlkgvsyslctaaflftkipaetlhgtvtvevqyagtdgpckvpaqmavdmqtltpvgrlitanpvitestenskmmleldppfgdsyivigvgekkithhwhrsgstigkafea

tvrgaknnavlgdtawdfgsvggalnslgkgihqifgaafkslfggmswfsqiligtllmwlglnakngsislmclalggvliflstavsaqwnstafhqtlqdprvrglylpaggsssgtvnpa

pniashissisartgdpvtnnienitsgflgpllvlqagfflltriltipqsldswwtslnflggspvclgqnsqsptsnhsptscppicpgyrwmclrrfiiflfilllclifllvlldyqgmlpvcplipg

stttstgpcktcttpaqgnsmfpsccctkptdgnctcipipsswafakylwcwasvrfswlsllvpfVqwfvglsptvwlsaiwminwywgpslysivspfipllpiffclwvyi

SEQ
Tsvgivglllttamaaevt

ID

NO:

25

SEQ
viylvmilliapays

ID

NO:

26

SEQ
Mlriinarkekkrrgad

ID

NO:

27

SEQ
mlgsstsqk

ID

NO:

28

SEQ
acaggtttta ttttggattt ggaaacgaga gtttctggtc atgaaaaacc caaaaaagaa atccggagga ttccggattg tcaatatgct aaaacgcgga gtagcccgtg tgagcccctt

ID
tgggggcttg aagaggctgc cagccggact tctgctgggt catgggccca tcaggatggt cttggcgatt ctagcctttt tgagattcac ggcaatcaag ccatcactgg gtctcatcaa

NO:
tagatggggt tcagtgggga aaaaagaggc tatggaaata ataaagaagt tcaagaaaga tctggctgcc atgctgagaa taatcaatgc taggaaggag aagaagagac

29
gaggcgcaga tactagtgtc ggaattgttg gcctcctgct gaccacagct atggcagcgg aggtcactag acgtgggagt gcatactata tgtacttgga cagaaacgat

gctggggagg ccatatcttt tccaaccaca ttggggatga ataagtgtta tatacagatc atggatcttg gacacacgtg tgatgccacc atgagctatg aatgccctat gctggatgag

ggggtggaac cagatgacgt cgattgttgg tgcaacacga cgtcaacttg ggttgtgtac ggaacctgcc atcacaaaaa aggtgaagca cggagatcta gaagagctgt

gacgctcccc tcccattcca ctaggaagct gcaaacgcgg tcgcaaacct ggttggaatc aagagaatac acaaagcact tgattagagt cgaaaattgg atattcagga accctggctt

cgcgttagca gcagctgcca tcgcttggct tttgggaagc tcaacgagcc aaaaagtcat atacttggtc atgatactgc tgattgcccc ggcatacagc atcaggtgca taggagtcag

caatagggac tttgtggaag gtatgtcagg tgggacttgg gttgatgttg tcttggaaca tggaggttgt gtcactgtaa tggcacagga caaaccgact gtcgacatag agctggttac

aacaacagtc agcaacatgg cggaggtaag atcctactgc tatgaggcat caatatcaga catggcttcg gacagccgct gcccaacaca aggtgaagcc taccttgaca

agcaatcaga cactcaatat gtctgcaaaa gaacgttagt ggacagaggc tggggaaatg gatgtggact ttttggcaaa gggagcctgg tgacatgcgc taagtttgca tgctccaaga

aaatgaccgg gaagagcatc cagccagaga atctggagta ccggataatg ctgtcagttc atggctccca gcacagtggg atgatcgtta atgacacagg acatgaaact

gatgagaata gagcgaaagt tgagataacg cccaattcac caagagccga agccaccctg ggggggtttg gaagcctagg acttgattgt gaaccgagga caggccttga

cttttcagat ttgtattact tgactatgaa taacaagcac tggctggttc acaaggagtg gttccacgac attccattac cttggcacgc tggggcagac accggaactc cacactggaa

caacaaagaa gcactggtag agttcaagga cgcacatgcc aaaaggcaaa ctgtcgtggt tctagggagt caagaaggag cagttcacac ggcccttgct ggagctctgg

aggctgagat ggatggtgca aagggaaggc tgtcctctgg ccacttgaaa tgtcgcctga aaatggataa acttagattg aagggcgtgt catactcctt gtgtactgca gcgttcacat

tcaccaagat cccggctgaa acactgcacg ggacagtcac agtggaggta cagtacgcag ggacagatgg accttgcaag gttccagctc agatggcggt ggacatgcaa

actctgaccc cagttgggag gttgataacc gctaaccccg taatcactga aagcactgag aactctaaga tgatgctgga acttgatcca ccatttgggg actcttacat tgtcatagga

gtcggggaga agaagatcac ccaccactgg cacaggagtg gcagcaccat tggaaaagca tttgaagcca ctgtgagagg tgccaagaga atggcagtct tgggagacac

agcctgggac tttggatcag ttggaggcgc tctcaactca ttgggcaagg gcatccatca aatctttgga gcagctttca aatcattgtt tggaggaatg tcctggttct cacaaattct

cattggaacg ttgctgatgt ggttgggtct gaacgcaaag aatggatcta tttcccttat gtgcttggcc ttagggggag tgttgatctt cttatccaca gccgtctctg ctgatgtggg

gtgctcggtg gacttctcaa agaaggagac gagatgcggt acaggggtgt tcgtctataa cgacgttgaa gcctggaggg acaggtacaa gtaccatcct gactcccccc

gtagattggc agcagcagtc aagcaagcct gggaagatgg tatctgcggg atctcctctg tttcaagaat ggaaaacatc atgtggagat cagtagaagg ggagctcaac

gcaatcctgg aagagaatgg agttcaactg acggtcgttg tgggatctgt aaaaaacccc atgtggagag gtccacagag attgcccgtg cctgtgaacg agctgcccca

cggctggaag gcttggggga aatcgtactt cgtcagagca gcaaagacaa ataacagctt tgtcgtggat ggtgacacac tgaaggaatg cccactcaaa catagagcat

ggaacagctt tcttgtggag gatcatgggt tcggggtatt tcacactagt gtctggctca aggttagaga agattattca ttagagtgtg atccagccgt tattggaaca gctgttaagg

gaaaggaggc tgtacacagt gatctaggct actggattga gagtgagaag aatgacacat ggaggctgaa gagggcccat ctgatcgaga tgaaaacatg tgaatggcca

aagtcccaca cattgtggac agatggaata gaagagagtg atctgatcat acccaagtct ttagctgggc cactcagcca tcacaatacc agagagggct acaggaccca

aatgaaaggg ccatggcaca gtgaagagct tgaaattcgg tttgaggaat gcccaggcac taaggtccac gtggaggaaa catgtggaac gagaggacca tctctgagat

caaccactgc aagcggaagg gtgatcgagg aatggtgctg cagggagtgc acaatgcccc cactgtcgtt ccgggctaaa gatggctgtt ggtatggaat ggagataagg

cccaggaaag aaccagaaag caacttagta aggtcaatgg tgactgcagg atcaactgat cacatggacc acttctccct tggagtgctt gtgattctgc tcatggtgca ggaagggttg

aagaagagaa tgaccacaaa gatcatcata agcacatcaa tggcagtgct ggtagctatg atcctgggag gattttcaat gagtgacctg gctaagcttg caattttgat gggtgccacc

ttcgcggaaa tgaacactgg aggagatgta gctcatctgg cgctgatagc ggcattcaaa gtcagaccag cgttgctggt atctttcatc ttcagagcta attggacacc ccgtgaaagc

atgctgctgg ccttggcctc gtgtcttttg caaactgcga tctccgcctt ggaaggcgac ctgatggttc tcatcaatgg ttttgctttg gcctggttgg caatacgagc gatggttgtt

ccacgcactg ataacatcac cttggcaatc ctggctgctc tgacaccact ggcccggggc acactgcttg tggcgtggag agcaggcctt gctacttgcg gggggtttat gctcctctct

ctgaagggaa aaggcagtgt gaagaagaac ttaccatttg tcatggccct gggactaacc gctgtgaggc tggtcgaccc catcaacgtg gtgggactgc tgttgctcac

aaggagtggg aagcggagct ggccccctag cgaagtactc acagctgttg gcctgatatg cgcattggct ggagggttcg ccaaggcaga tatagagatg gctgggccca

tggccgcggt cggtctgcta attgtcagtt acgtggtctc aggaaagagt gtggacatgt acattgaaag agcaggtgac atcacatggg aaaaagatgc ggaagtcact

ggaaacagtc cccggctcga tgtggcgcta gatgagagtg gtgatttctc cctggtggag gatgacggtc cccccatgag agagatcata ctcaaggtgg tcctgatgac catctgtggc

atgaacccaa tagccatacc ctttgcagct ggagcgtggt acgtatacgt gaagactgga aaaaggagtg gtgctctatg ggatgtgcct gctcccaagg aagtaaaaaa

gggggagacc acagatggag tgtacagagt aatgactcgt agactgctag gttcaacaca agttggagtg ggagttatgc aagagggggt ctttcacact atgtggcacg

tcacaaaagg atccgcgctg agaagcggtg aagggagact tgatccatac tggggagatg tcaagcagga tctggtgtca tactgtggtc catggaagct agatgccgcc

tgggacgggc acagcgaggt gcagctcttg gccgtgcccc ccggagagag agcgaggaac atccagactc tgcccggaat atttaagaca aaggatgggg acattggagc

ggttgcgctg gattacccag caggaacttc aggatctcct atcctagaca agtgtgggag agtgatagga ctttatggca atggggtcgt gatcaaaaat gggagttatg ttagtgccat

cacccaaggg aggagggagg aagagactcc tgttgagtgc ttcgagcctt cgatgctgaa gaagaagcag ctaactgtct tagacttgca tcctggagct gggaaaacca

ggagagttct tcctgaaata gtccgtgaag ccataaaaac aagactccgt actgtgatct tagctccaac cagggttgtc gctgctgaaa tggaggaggc ccttagaggg cttccagtgc

gttatatgac aacagcagtc aatgtcaccc actctggaac agaaatcgtc gacttaatgt gccatgccac cttcacttcg cgtctactac agccaatcag agtccccaac tataatctgt

atattatgga tgaggcccac ttcacagatc cctcaagtat agcagcaaga ggatacattt caacaagggt tgagatgggc gaggcggccg ccatcttcat gaccgccacg

ccaccaggaa cccgtgacgc atttccggac tccaactcac caattatgga caccgaagtg gaagtcccag agagagcctg gagctcaggc tttgattggg tgacggatca

ttctggaaaa acagtttggt ttgttccaag cgtgaggaac ggcaatgaga tcgcagcttg tctgacaaag gctggaaaac gggtcataca gctcagcaga aagacttttg agacagagtt

ccagaaaaca aaacatcaag agtgggactt tgtcgtgaca actgacattt cagagatggg cgccaacttt aaagctgacc gtgtcataga ttccaggaga tgcctaaagc cggtcatact

tgatggcgag agagtcattc tggctggacc catgcctgtc acacatgcca gcgctgccca gaggaggggg cgcataggca ggaatcccaa caaacctgga gatgagtatc

tgtatggagg tgggtgcgca gagactgacg aagaccatgc acactggctt gaagcaagaa tgctccttga caatatttac ctccaagatg gcctcatagc ctcgctctat cgacctgagg

ccgacaaagt agcagccatt gagggagagt tcaagcttag gacggagcaa aggaagacct ttgtggaact catgaaaaga ggagatcttc ctgtttggct ggcctatcag gttgcatctg

ccggaataac ctacacagat agaagatggt gctttgatgg cacgaccaac aacaccataa tggaagacag tgtgccggca gaagtgtgga ccagacacgg agagaaaaga

gtgctcaaac cgaggtggat ggacgccaga gtttgttcag atcatgcggc cctgaagtca ttcaaggagt ttgccgctgg gaaaagagga gcggcttttg gagtgatgga

agccctggga acactgccag gacacatgac agagagattc caggaagcca ttgacaacct cgctgtgctc atgcgggcag agactggaag caggccttac aaagccgcgg

cggcccaatt gccggagacc ctagagacca ttatgctttt ggggttgctg ggaacagtct cgctgggaat cttcttcgtc ttgatgagga acaagggcat agggaagatg ggctttggaa

tggtgactct tggggccagc gcatggctca tgtggctctc ggaaattgag ccagccagaa ttgcatgtgt cctcattgtt gtgttcctat tgctggtggt gctcatacct gagccagaaa

agcaaagatc tccccaggac aaccaaatgg caatcatcat catggtagca gtaggtcttc tgggcttgat taccgccaat gaactcggat ggttggagag aacaaagagt gacctaagcc

atctaatggg aaggagagag gagggggcaa ccataggatt ctcaatggac attgacctgc ggccagcctc agcttgggcc atctatgctg ccttgacaac tttcattacc ccagccgtcc

aacatgcagt gaccacctca tacaacaact actccttaat ggcgatggcc acgcaagctg gagtgttgtt tggtatgggc aaagggatgc cattctacgc atgggacttt ggagtcccgc

tgctaatgat aggttgctac tcacaattaa cacccctgac cctaatagtg gccatcattt tgctcgtggc gcactacatg tacttgatcc cagggctgca ggcagcagct gcgcgtgctg

cccagaagag aacggcagct ggcatcatga agaaccctgt tgtggatgga atagtggtga ctgacattga cacaatgaca attgaccccc aagtggagaa aaagatggga

caggtgctac tcatagcagt agccgtctcc agcgccatac tgtcgcggac cgcctggggg tggggggagg ctggggccct gatcacagcc gcaacttcca ctttgtggga

aggctctccg aacaagtact ggaactcctc tacagccact tcactgtgta acatttttag gggaagttac ttggctggag cttctctaat ctacacagta acaagaaacg ctggcttggt

caagagacgt gggggtggaa caggagagac cctgggagag aaatggaagg cccgcttgaa ccagatgtcg gccctggagt tctactccta caaaaagtca ggcatcaccg

aggtgtgcag agaagaggcc cgccgcgccc tcaaggacgg tgtggcaacg ggaggccatg ctgtgtcccg aggaagtgca aagctgagat ggttggtgga gcggggatac

ctgcagccct atggaaaggt cattgatctt ggatgtggca gagggggctg gagttactac gccgccacca tccgcaaagt tcaagaagtg aaaggataca caaaaggagg

ccctggtcat gaagaacccg tgttggtgca aagctatggg tggaacatag tccgtcttaa gagtggggtg gacgtctttc atatggcggc tgagccgtgt gacacgttgc tgtgtgacat

aggtgagtca tcatctagtc ctgaagtgga agaagcacgg acgctcagag tcctctccat ggtgggggat tggcttgaaa aaagaccagg agccttttgt ataaaagtgt tgtgcccata

caccagcact atgatggaaa ccctcgagcg actgcagcgt aggtatgggg gaggactggt cagagtgcca ctctcccgca actctacaca tgagatgtac tgggtctctg

gagcgaaaag caacaccata aaaagtgtgt ccaccacgag ccagctcctc ttggggcgca tggacgggcc taggaggcca gtgaaatatg aggaggatgt gaatctcggc

tctggcacgc gggctgtggt aagctgcgct gaagctccca acatgaagat cattggtaac cgcattgaaa ggatccgcag tgagcacgcg gaaacgtggt tctttgacga

gaaccaccca tataggacat gggcttacca tggaagctat gaggccccca cacaagggtc agcgtcctct ctaataaacg gggttgtcag gctcctgtca aaaccctggg

atgtggtgac tggagtcaca ggaatagcca tgaccgacac cacaccgtat ggtcagcaaa gagttttcaa ggaaaaagtg gacactaggg tgccagaccc ccaagaaggc

actcgtcagg ttatgagcat ggtctcttcc tggttgtgga aagagctagg caaacacaaa cggccacgag tctgtaccaa agaagagttc atcaacaagg ttcgtagcaa tgcagcatta

ggggcaatat ttgaagagga aaaagagtgg aagactgcag tggaagctgt gaacgatcca aggttctggg ctctagtgga caaggaaaga gagcaccacc tgagaggaga

gtgccagagt tgtgtgtaca acatgatggg aaaaagagaa aagaaacaag gggaatttgg aaaggccaag ggcagccgcg ccatctggta tatgtggcta ggggctagat

ttctagagtt cgaagccctt ggattcttga acgaggatca ctggatgggg agagagaact caggaggtgg tgttgaaggg ctgggattac aaagactcgg atatgtccta gaagagatga

gtcgtatacc aggaggaagg atgtatgcag atgacactgc tggctgggac acccgcatta gcaggtttga tctggagaat gaagctctaa tcaccaacca aatggagaaa

gggcacaggg ccttggcatt ggccataatc aagtacacat accaaaacaa agtggtaaag gtccttagac cagctgaaaa agggaaaaca gttatggaca ttatttcgag

acaagaccaa agggggagcg gacaagttgt cacttacgct cttaacacat ttaccaacct agtggtgcaa ctcattcgga atatggaggc tgaggaagtt ctagagatgc aagacttgtg

gctgctgcgg aggtcagaga aagtgactaa ctggttgcag agcaacggat gggataggct caaacgaatg gcagtcagtg gagatgattg cgttgtgaag ccaattgatg

ataggtttgc acatgccctc aggttcttga atgatatggg aaaagttagg aaggacacac aagagtggaa accctcaact ggatgggaca actgggaaga agttccgttt tgctcccacc

acttcaacaa gctccatctc aaggacggga ggtccattgt ggttccctgc cgccaccaag atgaactgat tggccgggcc cgcgtctctc caggggcggg atggagcatc

cgggagactg cttgcctagc aaaatcatat gcgcaaatgt ggcagctcct ttatttccac agaagggacc tccgactgat ggccaatgcc atttgttcat ctgtgccagt tgactgggtt

ccaactggga gaactacctg gtcaatccat ggaaagggag aatggatgac cactgaagac atgcttgtgg tgtggaacag agtgtggatt gaggagaacg accacatgga

agacaagacc ccagttacga aatggacaga cattccctat ttgggaaaaa gggaagactt gtggtgtgga tctctcatag ggcacagacc gcgcaccacc tgggctgaga

acattaaaaa cacagtcaac atggtgcgca ggatcatagg tgatgaagaa aagtacatgg actacctatc cacccaagtt cgctacttgg gtgaagaagg gtctacacct ggagtgctgt

aagcaccaat cttaatgttg tcaggcctgc tagtcagcca cagcttgggg aaagctgtgc agcc

SEQ
acaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcact

ID

NO:

30

SEQ
Gtcatatacttggtcatgatactgctgattgccccggcatacagc

ID

NO:

31

SEQ
atgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagat

ID

NO:

32

SEQ
Atgttgggaagctcaacgagccaaaaa

ID

NO:

33

SEQ
atcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacat

ID
agagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagc

NO:
aatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccg

34
ggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgag

ataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactg

gctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaagg

caaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaa

aatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacaga

tggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaactt

gatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgocaagag

aatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggtt

ctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatggatctagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctccc

gtgtgtcttggccaaaaucgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctc

atcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccct

catgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgt

tcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtat

acatttaa

SEQ
agacgtgggagtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgcc

ID
accatgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacg

NO:
gagatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcag

35
gaaccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggag

tcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaaca

acagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatat

gtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagcc

agagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcacc

aagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagt

ggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttcta

gggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagatt

gaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagsgacagatggaccttgcaaggttc

cagctcagatggcggtggacatgcaaactctgaaccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttgggga

ctcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttggga

gacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattgg

aacgttgctgatgtggttgggtctgaacgcaaagaatggatctagaatcctcctcaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaatt

cgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttct

tctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaac

ctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggct

ttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacat

ID
agagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagc

NO:
aatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccg

36
ggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgag

ataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactg

gctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaagg

caaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaa

aatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacaga

tggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaactt

gatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagag

aatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggtt

ctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctgagaacatc

acatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtg

tcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatct

tcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgt

tgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagt

ggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacat

ttaa

SEQ
agacgtgggagtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgcc

ID
accatgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacg

NO:
gagatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcag

37
gaaccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggag

tcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaaca

acagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatat

gtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagcc

agagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcacc

aagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagt

ggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttcta

gggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagatt

gaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttc

cagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttgggga

ctcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttggga

gacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattgg

aacgttgctgatgtggttgggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctgagaacatcacatcaggattcctagg

acccctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgca

gtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctg

gattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctac

ggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcc

cccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacat

ID
agagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagc

NO:
aatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccg

38
ggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgag

ataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactg

gctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaagg

caaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaa

aatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgncacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacaga

tggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaactt

gatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagag

aatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggtt

ctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatggatctcagtggaattccactgccttccaccaaactctgcaggatcccagagtcaggggtctgtatcttcctgct

ggtggctccagttcaggaacagtaaaccctgctccgaatattgcctctcacatctcgtcaatctccgcgaggactggggaccctgtgacgaacatggagaacatcacatcaggattcctaggacccc

tgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccc

caacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggatta

tcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatg

gaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccac

tgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttatctaccgctgttaccaatttttctttttgtctctgggtatacatttaa

SEQ
agacgtgggagtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgcc

ID
accatgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacg

NO:
gagatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcag

39
gaaccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggag

tcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaagacaaaccgactgtcgacatagagctggttacaaca

acagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatat

gtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagcc

agagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcacc

aagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagt

ggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttcta

gggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagatt

gaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttc

cagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataactgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgataaccatttgggga

ctcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttggga

gacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattgg

aacgttgctgatgtggttgggtctgaacgcaaagaatggatctcagtggaattccactgccttccaccaaactctgcaggatcccagagtcaggggtctgtatcttcctgctggtggctccagttcagg

aacagtaaaccctgctccgaatattgcctctcacatctcgtcaatctccgcgaggactggggaccctgtgacgaacatggagaacatcacatcaggattcctaggacccctgctcgtgttacaggcg

gggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactca

ccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccg

tttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtatt

cccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctat

atggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacat

ID
agagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagc

NO:
aatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccg

40
ggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgag

ataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactg

gctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaagg

caaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaa

aatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacaga

tggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaactt

gatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagag

aatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggtt

ctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctcagtggaat

tccactgccttccaocaaactctgcaggatcccagagtcaggggtctgtatcttcctgctggtggctccagttcaggaacagtaaaccctgctccgaatattgcctctcacatctcgtcaatctccgcga

ggactggggaccctgtgacgaacatggagaacatcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtg

gtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcg

ttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacc

tgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagt

ccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtcccttta

taccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
agacgtgggagtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgcc

ID
accatgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacg

NO:
gagatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcag

41
gaaccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggag

tcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaaca

acagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatat

gtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagcc

agagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcacc

aagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagt

ggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttcta

gggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagatt

gaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttc

cagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttgggga

ctcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttggga

gacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattgg

aacgttgctgatgtggttgggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctcagtggaattccactgccttccacca

aactctgcaggatcccagagtcaggggtctgtatcttcctgctggtggctccagttcaggaacagtaaaccctgctccgaatattgcctctcacatctcgtcaatctccgcgaggactggggaccctgt

gacgaacatggagaacatcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaatttt

ctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcat

cctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaagg

caactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagt

ttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaatttt

cttttgtctctgggtatacatttaa

SEQ
atgttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtggga

ID
cttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctat

NO:
gaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaa

42
atggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatgg

ctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagccta

ggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcag

acaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctg

gagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcaca

ttcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccag

ttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacc

caccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctca

actcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatgga

tctagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcc

tccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctajgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaatt

ccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgt

cctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagfgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtg

gtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcat

ID
actatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatg

NO:
ccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctg

43
tgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgtt

agcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttg

tggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggc

ggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgtt

agtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtac

cggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccac

cctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattcca

ttaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaagga

gcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatact

ccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtg

gacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcatagga

gtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggacttt

ggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttg

ggtctgaacgcaaagaatggatctagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctcc

aatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggta

tgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgc

acctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggct

ttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atgttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtggga

ID
cttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctat

NO:
gaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaa

44
atggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagwagagaatctggagtaccggataatgctgtcagttcatgg

ctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagccta

ggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcag

acaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctg

gagctctggaggctgagatggatttgtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcaca

ttcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccag

ttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacc

caccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctca

actcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatgga

tctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctgagaacatcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaa

gaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctcc

aatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattcca

ggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctg

ggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtatt

gggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcat

ID
actatatgtacttggacagaaacgatgctggggaggccatatctttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatg

NO:
ccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctg

45
tgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaattaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgtt

agcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttg

tggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggc

ggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgtt

agtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtac

cggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccac

cctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattcca

ttaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaagga

gcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatact

ccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtg

gacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcatagga

gtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggacttt

ggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttg

ggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctgagaacatcacatcaggattcctaggacccctgctcgtgttaca

ggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatc

actcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttg

cccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctg

tattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcag

ctatatggatgatgtggtattggcggccaagtctgtacastcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atgttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtggga

ID
cttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctat

NO:
gaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatattttctgcaaaagaacgttagtggacasaggctggggaa

46
atggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatgg

ctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagccta

ggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcag

acaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctg

gagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcaca

ttcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccag

ttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacc

caccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctca

actcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatgga

tctcagtggaattccactgccttccaccaaactctgcaggatcccagagtcaggggtctgtatcttcctgctggtggctccagttcaggaacagtaaaccctgctccgaatattgcctctcacatctcgt

caatctccgcgaggactggggaccctgtgacgaacatggagaacatcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagag

tctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatg

tgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggacc

atgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcocatcgtcctgggctttcgcaaaatacctatggga

gtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatc

gtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcat

ID
actatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatg

NO:
ccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctg

47
tgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgtt

agcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttg

tggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggc

ggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgtt

agtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtac

cggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccac

cctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattcca

ttaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaagga

gcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatact

ccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtg

gacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatcgaccatttggggactcttacattgtcatagga

gtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggacttt

ggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttg

ggtctgaacgcaaagaatggatctcagtggaattccactgccttccaccaaactctgcaggatcccagagtcaggggtctgtatcttcctgctggtggctccagttcaggaacagtaaaccctgctcc

gaatattgcctctcacatctcgtcaatctccgcgaggactggggaccctgtgacgaacatggagaacatcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaag

aatcctcacaaraccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaa

tttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccagg

atcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctggg

ctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgg

gggccaagtctatacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctaggtatacatttaa

SEQ
atgttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatatagcatcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtggga

ID
cttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctat

NO:
gaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaa

48
atggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatgg

ctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagccta

ggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcag

acaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctg

gagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcaca

ttcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccag

ttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacc

caaactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctca

actcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatgga

tctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctcagtggaattccactgccttccaccaaactctgcaggatcccagagtcaggggtctgtatcttcctg

ctggtggctccagttcaggaacagtaaaccctgctccgaatattgcctctcacatctcgtcaatctccgcgaggactggggaccctgtgacgaacatggagaacatcacatcaggattcctaggacc

cctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtc

cccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggat

tatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacgga

tggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttccccca

ctgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaa

SEQ
atgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcat

ID
actatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatg

NO:
ccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctg

49
tgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgtt

agcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttg

tggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggc

ggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagaGactcaatatgtctgcaaaagaacgtt

agtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtac

cggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccac

cctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattcca

ttaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaagga

gcagttcacacggcccttttctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaattggcgtgtcatact

ccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtg

gacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcatagga

gtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggacttt

ggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttg

ggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctcagtggaattccactgccttccaccaaactctgcaggatcccag

agtcaggggtctgtatcttcctgctggtggctccagttcaggaacagtaaaccctgctccgaatattgcctctcacatctcgtcaatctccgcgaggactggggaccctgtgacgaacatggagaaca

tcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgt

gtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatc

ttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatg

ttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcag

tggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacat

ttaa

SEQ
Rrgsayymyldmdageaisfpttlgmnkcyiqimdlghtcdatmsyecpmldegvcpddvdcwcnltstwvvygtchhkkgearrsrravtlpshstrklqtrsqtwlesreytklilirve

ID
nwifrnpgfalaaaaiawllgsstsqkviylvmilliapays

NO:

50

SEQ
cccgggatcc atgaaaaacc caaaaaagaa atccggagga ttccggattg tcaatatgct aaaacgcgga gtagcccgtg tgagcccctt tgggggcttg aagaggctgc

ID
cagccggact tctgctgggt catgggccca tcaggatggt cttggcgatt ctagcctttt tgagattcac ggcaatcaag ccatcactgg gtctcatcaa tagatggggt tcagtgggga

NO:
aaaaagaggc tatggaaata ataaagaagt tcaagaaaga tctggctgcc atgctgagaa taatcaatgc taggaaggag aagaagagac gaggcgcaga tacaagtgtc

51
ggaattgttg gcctcctgct gaccacagct atggcagcgg aggtcactag acgtgggagt gcatactata tgtacttgga cagaaacgat gctggggagg ccatatcttt tccaaccaca

ttggggatga ataagtgtta tatacagatc atggatcttg gacacacgtg tgatgccacc atgagctatg aatgccctat gctggatgag ggggtggaac cagatgacgt cgattgttgg

tgcaacacga cgtcaacttg ggttgtgtac ggaacctgcc atcacaaaaa aggtgaagca cggagatcta gaagagctgt gacgctcccc tcccattcca ctaggaagct

gcaaacgcgg tcgcaaacct ggttggaatc aagagaatac acaaagcact tgattagagt cgaaaattgg atattcagga accctggctt cgcgttagca gcagctgcca tcgcttggct

tttgggaagc tcaacgagcc aaaaagtcat atacttggtc atgatactgc tgattgcccc ggcatacagc atcaggtgca taggagtcag caatagggac tttgtggaag gtatgtcagg

tgggacttgg gttgatgttg tcttggaaca tggaggttgt gtcactgtaa tggcacagga caaaccgact gtcgacatag agctggttac aacaacagtc agcaacatgg cggaggtaag

atcctactgc tatgaggcat caatatcaga catggcttcg gacagccgct gcccaacaca aggtgaagcc taccttgaca agcaatcaga cactcaatat gtctgcaaaa gaacgttagt

ggacagaggc tggggaaatg gatgtggact ttttggcaaa gggagcctgg tgacatgcgc taagtttgca tgctccaaga aaatgaccgg gaagagcatc cagccagaga

atctggagta ccggataatg ctgtcagttc atggctccca gcacagtggg atgatcgtta atgacacagg acatgaaact gatgagaata gagcgaaagt tgagataacg cccaattcac

caagagccga agccaccctg ggggggtttg gaagcctagg acttgattgt gaaccgagga caggccttga cttttcagat ttgtattact tgactatgaa taacaagcac tggctggttc

acaaggagtg gttccacgac attccattac cttggcacgc tggggcagac accggaactc cacactggaa caacaaagaa gcactggtag agttcaagga cgcacatgcc

aaaaggcaaa ctgtcgtggt tctagggagt caagaaggag cagttcacac ggcccttgct ggagctctgg aggctgagat ggatggtgca aagggaaggc tgtcctctgg

ccacttgaaa tgtcgcctga aaatggataa acttagattg aagggcgtgt catactcctt gtgtactgca gcgttcacat tcaccaagat cccggctgaa acactgcacg ggacagtcac

agtggaggta cagtacgcag ggacagatgg accttgcaag gttccagctc agatggcggt ggacatgcaa actctgaccc cagttgggag gttgataacc gctaaccccg

taatcactga aagcactgag aactctaaga tgatgctgga acttgatcca ccatttgggg actcttacat tgtcatagga gtcggggaga agaagatcac ccaccactgg cacaggagtg

gcagcaccat tggaaaagca tttgaagcca ctgtgagagg tgccaagaga atggcagtct tgggagacac agcctgggac tttggatcag ttggaggcgc tctcaactca

ttgggcaagg gcatccatca aatctttgga gcagctttca aatcattgtt tggaggaatg tcctggttct cacaaattct cattggaacg ttgctgatgt ggttgggtct gaacgcaaag

aatggatcta tttcccttat gtgcttggcc ttagggggag tgttgatctt cttatccaca gccgtctctg ctgatgtggg gtagctcsag gatcccggg

SEQ
gttgttactgttgctgactcagactgcgacagttcgagtttgaagcgaaagctagcaacagtatcaacaggttttatttggatttggaaacgagagtttctggtcatgaaaaacccaaaa

ID
ttagaaatccggaggattccggattgtcaatatgctaaaacgcggagtagcccgtgtgagcccctttgggggcttgaagaggctgccagccggacttctgctgggtcatgggcccatcaggatggt

NO:
cttggcaattctagcctttttgagattcacggcaatcaagccatcactgggtctcatcaatagatggggttcagtggggaaaaaagaggctatggaaataataaagaagttcaagaaagatctggctg

52
ccatgctgagaataatcaatgctaggaaggagaagaagagacggggcgcagatactagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgc

atactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacatgtgtgatgccaccatgagctatgaat

gccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagct

gtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgt

tagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggacttt

gtggaaggtatgtcaggtgggacttgggttgatattgtcttggaacatggaggttgtgtcaccgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatgg

cggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgt

tagtggacagaggctggggaaatggatgtggactttttggcaaagggagtctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtac

cggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaggttgagataacgcccaattcaccaagagccgaagccac

cctggggggttttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggttggttcacaaggagtggttccacgacattccat

taccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggag

cagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatg

gataaacttagattgaagggcgtgtcatactccttgtgtaccgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatgga

ccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatc

caccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatg

gcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatttttggagcagctttcaaatcattgtttggaggaatgtcctggttctcac

aaattctcattggaacgttgctgatgtggttgggtctgaacacaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctgatgtggggtgctc

ggtggacttctcaaagaaggagacgagatgcggtacaggggtgttcgtctataacgacgttgaagcctggagggacaggtacaagtaccatcctgactccccccgtagattggcagcagcagtca

agcaagcctgggaagatggtatctgcgggatctcctctgtttcaagaatggaaaacatcatgtggagatcagtagaaggggagctcaacgcaatcctggaagagaatggagttcaactgacggtc

gttgtgggatctgtaaaaaaccccatgtggagaggtccacagagattgcccgtgcctgtgaacgagctgccccacggctggaaggcttgggggaaatcgcacttcgtcagagcagcaaagacaa

ataacagctttgtcgtggatggtgacacactgaaggaatgcocactcaaacatagagcatggaacagctttcttgtggaggatcatgggttcggggtatttcacactagtgtctggctcaaggttagag

aagattattcattagagtgtgatccagccgttattggaacagctgttaagggaaaggaggctgtacacagtgatctaggctactggattgagagtgagaagaatgacacatggaggctgaagaggg

cccatctgatcgagatgaaaacatgtgaatggccaaagtcccacacattgtggacagatggaatagaagagagtgatctgatcatacccaagtctttagctgggccactcagccatcacaataccag

agagggctacaggacccaaatgaaagggccatggcacagtgaagagcttgaaattcggtttgaggaatgcccaggcactaaggtccacgtggaggaaacatgtggaacaagaggaccatctct

gagatcaaccactgcaagcggaagggtgatcgaggaatggtgctgcagggagtgcacaatgcccccactgtcgttccgggctaaagatggctgttggtatggaatggagataaggcccaggaa

agaaccagaaagcaacttagtaaggtcaatggtgactgcaggatcaactgatcacatggatcacttctcccttggagtgcttgtgattctgctcatggtgcaggaagggctgaagaagagaatgacc

acaaagatcatcataagcacatcaatggcagtgctggtagctatgatcctgggaggattttcaatgagtgacctggctaagcttgcaattttgatgggtgccaccttcgcggaaatgaacactggagg

agatgtagctcatctggcgctgatagcggcattcaaagtcagaccagcgttgctggtatctttcatcttcagagctaattggacaccccgtgaaagcatgctgctggccttggcctcgtgtcttttgcaa

actgcgatctccgccttggaaggcgacctgatggttctcatcaatggttttgctttggcctggttggcaatacgagcgatggttgttccacgcactgataacatcaccttggcaatcctggctgctctgac

accactggcccggggcacactgcttgtggcgtggagagcaggccttgctacttgcggggggtttatgctcctctctctgaagggaaaaggcagtgtgaagaagaacttaccatttgtcatggccctg

ggactaaccgctgtgaggctggtcgaccccatcaacgtggtggggctgctgttgctcacaaggagtgggaagcggagctggccccctagcgaagtactcacagctgttggcctgatatgcgcatt

ggctggagggttcgccaaggcagatatagagatggctgggcccatggccgcggtcggtctgctaattgtcagttacgtggtctcaggaaagagtgtggacatgtacattgaaagagcaggtgaca

tcacatgggaaaaagatgcggaagtcactggaaacagtccccggctcgatgtggcgctagatgagagtggtgatttctccctggtggaggatgacggtccccccatgagagagatcatactcaag

gtggtcctgatgaccatctgtggcatgaacccaatagccataccctttgcagctggagcgtggtacgtatacgtgaagactggaaaaaggagtggtgctctatgggatgtgcctgctcccaaggaag

taaaaaagggggagaccacagatggagtgtacagagtaatgactcgtagactgctaggttcaacacaagttggagtgggagttatgcaagagggggtctttcacactatgtggcacgtcacaaaa

ggatccgcgctgagaagcggtgaagggagacttgatccatactggggagatgtcaagcaggatctggtgtcatactgtggtccatggaagctagatgccgcctgggacgggcacagcgaggtg

cagctcttggccgtgccccccggagagagagcgaggaacatccagactctgcccggaatatttaagacaaaggatggggacattggagcggttgcgctggattacccagcaggaacttcaggat

ctccaatcctagacaagtgtgggagagtgataggactttatggcaatggggtcgtgatcaaaaatgggagttatgttagtgccatcacccaagggaggagggaggaagagactcctgttgagtgctt

cgagccttcgatgctgaagaagaagcagctaactgtcttagacttgcatcctggagctgggaaaaccaggaga

gttcttcctgaaatagtccgtgaagccataaaaacaagactccgtactgtgatcttagctccaaccagggttgtcgctgctgaaatggaggaagcccttagagggcttccagtgcgttatatgacaaca

gcagtcaatgtcacccactctggaacagaaatcgtcgacttaatgtgccatgccaccttcacttcacgtctactacagccaatcagagtccccaactataatctgtatattatggatgaggcccacttca

cagatccctcaagtatagcagcaagaggatacatttcaacaagggttgagatgggcgaggcggctgccatcttcatgaccgccacgccaccaggaacccgtgacgcatttccggactccaactca

ccaattatggacaccgaagtggaagtcccagagagagcctggagctcaggctttgattgggtgacggattattctggaaaaacagtttggtttgttccaagcgtgaggaacggcaatgagatcgca

gcttgtctgacaaaggctggaaaacgggtcatacagctcagcagaaagacttttgagacagagttccagaaaacaaaacatcaagagtgggactttgtcgtgacaactgacatttcagagatgggc

gccaactttaaagctgaccgtgtcatagattccaggagatgcctaaagccggtcatacttgatggcgagagagtcattctggctggacccatgcctgtcacacatgccagcgctgcccagaggagg

gggcgcataggcaggaatcccaacaaacctggagatgagtatctgtatggaggtgggtgcgcagagactgacgaagaccatgcacactggcttgaagcaagaatgctccttgacaatatttacct

ccaagatggcctcatagcctcgctctatcgacctgaggccgacaaagtagcagccattgagggagagttcaagcttaggacggagcaaaggaagacctttgtggaactcatgaaaagaggagat

cttcctgtttggctggcctatcaggttgcatctgccggaataacctacacagatagaagatggtgctttgatggcacgaccaacaacaccataatggaagacagtgtgccggcagaggtgtggacca

gacacggagagaaaagagtgctcaaaccgaggtggatggacgccagagtttgttcagatcatgcggccctgaagtcattcaaggagtttgccgctgggaaaagaggagcggcttttggagtgat

ggaagccctgggaacactgccaggacacatgacagagagattccaggaagccattgacaacctcgctgtgctcatgcgggcagagactggaagcaggccttacaaagccgcggcggcccaat

tgccggagaccctagagaccattatgcttttggggttgctgggaacagtctcgctgggaatctttttcgtcttgatgaggaacaagggcatagggaagatgggctttggaatggtgactcttggggcc

agcgcatggctcatgtggctctcggaaattgagccagccagaattgcatgtgtcctcattgttgtgttcctattgctggtggtgctcatacctgagccagaaaagcaa

agatctccccaggacaaccaaatggcaatcatcatcatggtagcagtaggtcttctgggcttgattaccgccaatgaactcggatggttggagagaacaaagagtgacctaagccatctaatgggaa

ggagagaggagggggcaaccatgggattctcaatggacattgacctgcggccagcctcagcttgggccatctatgctgccttgacaactttcattaccccagccgtccaacatgcagtgaccacttc

atacaacaactactccttaatggcgatggccacgcaagctggagtgttgtttggtatgggcaaagggatgccattctacgcatgggactttggagtcccgctgctaatgataggttgctactcacaatt

aacgcccctgaccctaatagtggccatcattttgctcgtggcgcactacatgtacttgatcccagggctgcaggcagcagctgcgcgtgctgcccagaagagaacggcagctggcatcatgaaga

accctgttgtggatggaatagtggtgactgacattgacacaatgacaattgacccccaagtggagaaaaagatgggacaggtgctactcatggcagtagccgtctccagcgccatactgtcgcgga

ccgcctgggggtggggggaggctggggccctgatcacagccgcaacttccactttgtgggaaggctctccgaacaagtactggaactcctctacagccacttcactgtgtaacatttttaggggaa

gttacttggctggagcttctctaatctacacagtaacaagaaacgctggcttggtcaagagacgtgggggtggaacaggagagaccctgggagagaaatggaaggcccgcttgaaccagatgtc

ggccctggagttctactcctacaaaaagtcaggcatcaccgaggtgtgcagagaagaggcccgccgcgccctcaaggacggtgtggcaacgggaggccatgctgtgtcccgaggaagtgcaa

agctgagatggttggtggagcggggatacctgcagccctatggaaaggtcattgatcttggatgtggcagagggggctggagttactacgccgccaccatccgcaaagttcaagaagtgaaagg

atacacaaaaggaggccctggtcatgaagaacccgtgttggtgcaaagctatgggtggaacatagtccgtcttaagagtggggtggacgtctttcatatggcggctgagccgtgtgacacgttgctg

tgtgacataggtgagtcatcatctagtcctgaagtggaagaagcacggacgctcagagtcctctccatggtgggggattggcttgaaaaaagaccaggagccttttgtataaaagtgttgtgcccata

caccagcactatgatggaaaccctggagcgactgcagcgtaggtatgggggaggactggtcagagtgccactctcccgcaactctacacatgagatgtactgggtctctggagcgaaaagcaac

accataaaaagtgtgtccaccacgagccagctcctcttggggcgcatggacgggcctaggaggccagtgaaatatgaggaggatgtgaatctcggctctggcacgcgggctgtggtaagctgcg

ctgaagctcccaacatgaagatcattggtaaccgcattgaaaggatccgcagtgagcacgcggaaacgtggttctttgacgagaaccacccatataggacatgggcttaccatggaagctatgagg

cccccacacaagggtcagcgtcctctctaataaacggggttgtcaggctcctgtcaaaaccctgggatgtggtgactggagtcacaggaatagccatgaccgacaccacaccgtatggtcagcaa

agagttttcaaggaaaaagtggacactagggtgccagacccccaagaaggtactcgtcaggttatgagcatggtctcttcctggttgtggaaagagctaggcaaacacaaacggccacgagtctgt

accaaagaagagttcatcaacaaggttcgtagcaatgcagcattaggggcaatatttgaagaggaaaaagagtggaagactgcagtggaagctgtgaacgatccaaggttctgggctctagtgga

caaggaaagagagcaccacctgagaggagagtgccagagttgtgtgtacaacatgatgggaaaaagagaaaagaaacaaggggaatttggaaaggccaagggcagccgcgccatctggtata

tgtggctaggggctagatttctagagttcgaagcccttggattcttgaacgaggatcactggatggggagagagaactcaggaggtggtgttgaagggctgggattacaaagactcggatatgtcct

agaagagatgagtcgcataccaggaggaaggatgtatgcagatgacactgctggctgggacacccgcatcagcaggtttgatctggagaatgaagctctaatcaccaaccaaatggagaaaggg

cacagggccttggcattggccataatcaagtacacataccaaaacaaagtggtaaaggtccttagaccagctgaaaaagggaaaacagttatggacattatttcgagacaagaccaaagggggag

cggacaagttgtcacttacgctcttaacacatttaccaacctagtggtgcaactcattcggaatatggaggctgaggaagtcctagagatgcaagacttgtggctgctgcggaggtcagagaaagtg

accaactggttgcagagcaacggatgggataggctcaaacgaatggcagtcagtggagatgattgcgttgtgaagccaattgatgataggtttgcacatgccctcaggttcttgaatgatatgggaa

aagttaggaaggacacacaagagtggaaaccctcaactggatgggacaactgggaagaagttccgttttgctcccaccacttcaacaagctccatctcaaggacgggaggtccattgtggttccct

gccgccaccaagatgaactgattggccgggcccgcgtctctccaggggcgggatggagcatccgggagactgcttgcctagcaaaatcatatgcgcaaatgtggcagctcctttatttccacaga

agggacctccgactgatggccaatgccatttgttcatctgtgccagttgactgggttccaactgggagaactacctggtcaatccatggaaagggagaatggatgaccactgaagacatgcttgtggt

gtggaacagagtgtggattgaggagaacgaccacatggaagacaagaccccagttacgaaatggacagacattccctatttgggaaaaagggaagacttgtggtgtggatctctcatagggcaca

gaccgcgcaccacctgggctgagaacattaaaaacacagtcaacatggtgcgcaggatcataggtgatgaagaaaagtacatggactacctatccacccaagttcgctacttgggtgaagaaggg

tctacacctggagtgctgtaagcaccaatcttaatgttgtcaggcctgctagtcagccacagcttggggaaagctgtgcagcctgtgacccccccaggagaagctgggaaaccaagcctatagtca

ggccgagaacgccatggcacggaagaagaatgctgcctgtgagcccctcagaggacactgagtcaaaaaaccccacgcgcttggaggcgcaggatgggaaaagaaggtggcgaccttccc

cacccttcaatctggggcctgaactggagatcagctgtggatctccagaagagggactagtggttagaggaga

SEQ
gatggcggatgtgtgacatacacgacgccaaaagattttgttccagctcctgccacctccgctacgcgagagattaaccacccacgatggccgccaaagtgcatgttgatattgaggctgacagcc

ID
cattcatcaagtctttgcagaaggcatttccgtcgttcgaggtggagtcattgcaggtcacaccaaatgaccatgcaaatgccagagcattttcgcacctggctaccaaattgatcgagcaggagact

NO:
gacaaagacacactcatcttggatatcggcagtgcgccttccaggagaatgatgtctacgcacaaataccactgcgtatgccctatgcgcagcgcagaagaccccgaaaggctcgatagctacgc

53
aaagaaactggcagcggcctccgggaaggtgctggatagagagatcgcaggaaaaatcaccgacctgcagaccgtcatggctacgccagacgctgaatctcctaccttttgcctgcatacagac

gtcacgtgtcgtacggcagccgaaatggccgtataccaggacgtgtatgctgtacatgcaccaacatcgctgtaccatcaggcgatgaaaggtgtcagaacggcgtattggattgggtttgacacc

accccgtttatgtttgacgcgctagcaggcgcgtatccaacctacgccacaaactgggccgacgagcaggtgttacaggccaggaacataggactgtgtgcagcatccttgactgagggaagact

cggcaaactgtccattctccgcaagaagcaattgaaaccttgcgacacagtcatgttctcggtaggatctacattgtacactgagagcagaaagctactgaggagctggcacttaccctccgtattcc

acctgaaaggtaaacaatcctttacctgtaggtgcgataccatcgtatcatgtgaagggtacgtagttaagaaaatcactatgtgccccggcctgtacggtaaaacggtagggtacgccgtgacgtat

cacgcggagggattcctagtgtgcaagaccacagacactgtcaaaggagaaagagtctcattccctgtatgcacctacgtcccctcaaccatctgtgatcaaatgactggcatactagcgaccgac

gtcacaccggaggacgcacagaagttgttagtgggattgaatcagaggatagttgtgaacggaagaacacagcgaaacactaacacgatgaagaactatctgcttccgattgtggccgtcgcat

ttagcaagtgggcgagggaatacaaggcagaccttgatgatgaaaaacctctgggtgtccgagagaggtcacttacttgctgctgcttgtgggcatttaaaacgaggaagatgcacaccatgtaca

agaaaccagacacccagacaatagtgaaggtgccttcagagtttaactcgttcgtcatcccgagcctatggtctacaggcctcgcaatcccagtcagatcacgcattaagatgcttttggccaagaag

accaagcgagagttaatacctgttctcgacgcgtcgtcagccagggatgctgaacaagaggagaaggagaggttggaggccgagctgactagagaagccttaccacccctcgtccccatcgcg

ccggcggagacgggagtcgtcgacgtcgacgttgaagaactagagtatcacgcaggtgcaggggtcgtggaaacacctcgcagcgcgttgaaagtcaccgcacagccgaacgacgtactact

aggaaattacgtagttctgtccccgcagaccgtgctcaagagctccaagttggcccccgtgcaccctctagcagagcaggtgaaaataataacacataacgggagggccggcggttaccaggtc

gacggatatgacggcagggtcctactaccatgtggatcggccattccggtccctgagtttcaagctttgagcgagagcgccactatggtgtacaacgaaagggagttcgtcaacaggaaactatac

catattgccgttcacggaccgtcgctgaacaccgacgaggagaactacgagaaagtcagagctgaaagaactgacgccgagtacgtgttcgacgtagataaaaaatgctgcgtcaagagagagg

aagcgtcgggtttggtgttggtgggagagctaaccaaccccccgttccatgaattcgcctacgaagggctgaagatcaggccgtcggcaccatataagactacagtagtaggagtctttggggttat

gggatcacgcaagtctgctattattaagagcctcgtcaccaaacacaatctgatcaccaacagcaacaaagagaactgccaggaaatagttaacgacgtgaagaagcaccgcgggaaggg

gacaagtagggaaaacagtgactccatcctgctaaacgggtgtcgtcgtgccgtggacatcctatatgtggacgaggctttcgcttgccattccggtactctgctggccctaattgctcttgttaaacct

cggagcaaagtggtgttatgcggagaccccaagcaatgcggattcttcaatatgatgcagcttaaggtgaacttcaaccacaacatctgcactgaagtatgtcataaaagtatatccagacgttgcac

gcgtccagtcacggccatcgtgtctttcgttgcactacggaggcaagatgcgcacgaccaacccgtgcaacaaacccataatcatagacaccacaggacagaccaagcccaagccaggagacat

cgtgttaacatgcttccgaggctgggcaaagcagctgcsgttggactaccgtggacacgaagtcatgacagcagcagcatctcagggcctcacccgcaaaggggtatacgccgtaaggcagaa

ggtgaatgaaaatcccttgttttgcocctgcgtcggagcacgtgaatgtactgctgacgcgcactgaggataggctggtgtggaaaacgctggccggcgatactggattaaggtcctatcaaacat

tccacagggtaactttacggccacattggaagaatggcaagaagaacacgacaaaataatgaaggtgattgaaggaccggctgcgcctgtggacgcgttccagaacaaagcgaacgtgtgttgg

gcgaaaagcctggtgcctgtcctggacactgccggaatcagattgacagcagaggagtggagcaccataattacagcatttaaggaggacagagcttactctccagtggtggccttgaatgaaattt

gcaccaagtactatggagttgacctggacagtggcctgttttctgccccgaaggtgtccctgtattacgagaacaaccactgggataacagacctggtggaaggatgtatggattcaatgccgcaac

agctgccaggctggaagctagacataccttcctgaaggggcagtggcatacgggcaagcaggcagttatcgcagaaagaaaaatccaaccgctttctgtgctggacaatgtaattcctatcaaccg

caggctgccgcacgccctggtggctgagtacaagacggttaaaggcagtagggttgagtggctggtcaataaagtaagagggtaccacgtcctgctggtgagtgagtacaacctggctttgcctc

gacgcagggtcacttggttgtcaccgctgaatgtcacaggcgccgataggtgctacgacctaagtttaggactgccggctgacgccggcaggttcgacttggtctttgtgaacattcacacggaatt

cagaatccaccactaccagcagtgtgtcgaccacgccatgaagctgcagatgcttgggggagatgcgctacgactgctaaaacccggcggcatcttgatgagagcttacggatacgccgataaaa

tcagcgaagccgttgtttcctccttaagcagaaagttctcgtctgcaagagtgttgcgcccggattgtgtcaccagcaatacagaagtgttcttgctgttctccaactttgacaacggaaagagaccctc

tacgctacaccagatgaataccaagctgagtgccgtgtatgccggagaagccatgcacacggccgggtgtgcaccatcctacagagttaagagagcagacatagccacgtgcacagaagcggc

tgtggttaacgcagctaacgcccgtggaactgtaggggatggcgtatgcagggccgtggcgaagaaatggccgtcagcctttaagggagcagcaacaccagtgggcacaattaaaacagtcatg

tgcggctcgtaccccgtcatccacgctgtagcgcctaatttctctgccacgactgaagcggaaggggaccgcgaattggccgctgtctaccgggcagtggccgccgaagtaaacagactgtcact

gagcagcgtagccatcccgctgctgtccacaggagtgttcagcggcggaagagataggctgcagcaatccctcaaccatctattcacagcaatggacgccacggacgctgacgtgaccatctact

ggagagtcaaaagttgggagaagaaaatccaggaasccattgacatgaggacggctgtggagtrgctcaatgatgacgtggagctgaccacagacttggtgagagtgcacccggacagcagcc

tggtgggtcgtaagggctacagtaccactgacgggtcgctgtactcgtactttgaaggtacgaaattcaaccaggctgctattgatatggcagagatactgacgttgtggcccagactgcaagaggc

aaacgaacagatatgcctatacgcgctgggcgaaacaatggacaacatcagatccaaatgtccggtgaacgattccgattcatcaacacctcccaggacagtgccctgcctgtgccgctacgcaat

gacagcagaacggatcgcccgccttaggtcacaccaagttaaaagcatggtggtttgctcatcttttcccctcccgaaataccatgtagatggggtgcagaaggtaaagtgcgagaaggttctcctgt

tcgacccgacggtaccttcagtggttagtccgcggaagtatgccgcatctacgacggaccactcagatcggtcgttacgagggtttgacttggactggaccaccgactcgtcttccactgccagcga

taccatgtagctacccagtttgcagtcgtgtgacatcgactcgatctacgagccaatggctcccatagtagtgacggctgacgtacaccctgaacccgcaggcatcgcggacctggcggcagatgt

gcaccctgaacccgcagaccatgtggacctcgagaacccgattcctccaccgcgcccgaagagagctgcataccttgcctcccgcgcggcggagcgaccggtgccggcgccgagaaagccg

acgcctgccccaaggactgcgtttaggaacaagctgcctttgacgttcggcgactttgacgagcacgaggtcgatgcgttggcctocgggattactttcggagacttcgacgacgtcctgcgactag

gccgcgcgggtgcatatattttctcctcggacactggcagcggacatttacaacaaaaatccgttaggcagcacaatctccagtgcgcacaactggatgcggtccaggaggagaaaatgtacccg

ccaaaattggatactgagagggagaagctgttgctgctgaaaatgcagatgcacccatcggaggctaataagagtcgataccagtctcgcaaagtggagaacatgaaagccacggtggtggaca

ggctcacatcgggggccagattgtacacgggagcggacgtaggccgcataccaacatacgcggttcggtacccccgccccgtgtactcccctaccgtgatcgaaagattctcaagccccgatgta

gcaatcgcagcgtgcaacgaatacctatccagaaattacccaacagtggcgtcgtaccagataacagatgaatacgacgcatacttggacatggttgacgggtcggatagttgcttggacaga

gcgacatctgcccggcgaagctccggtgctacccgaaacatcatgcgtaccaccagccgactgtacgcagtgccgtcccgtcaccctttcagaacacactacagaacgtgctagcggccgcca

ccaagagaaactgcaacgtcacgcaaatgcgagaactacccaccatggactcggcagtgttcaacgtggagtgcttcaagcgctatgcctgctccggagaatattgggaagaatatgctaaacaa

cctatccggataaccactgagaacatcactacctatgtgaccaaattgaaaggcccgaaagctgctgccttgttcgctaagacccacaacttggttccgctgcaggaggttcccatggacagattcac

ggtcgacatgaaacgagatgtcaaagtcactccagggacgaaacacacagaggaaagacccaaagtccaggtaattcaagcagcggagccaftggcgaccgcttacctgtgcg

gcatccacagggaattagtaaggagactaaatgctgtgttacgccctaacgtgcacacattgtttgatatgtcggccgaagactttgacgcgatcatcgcctctcacttccacccaggagacccggtt

ctagagacggacattgcatcattcoacaaaagccaggacgactccttggctcttacaggtttaatgatcctcgaagatctaggggtggatcagtacctgctggacttgatcgaggcagcctttgggga

aatatccagctgtcacctaccaactggcacgcgcttcaagttcggagctatgatgaaatcgggcatgtttctgactttgtttattaacactgttttgaacatcaccatagcaagcagggtactggagcag

agactcactgactccgcctgtgcggccttcatcggcgacgacaacatcgttcacggagtgatctccgacaagctgatggcggagaggtgcgcgtcgtgggtcaacatggaggtgaagatcattga

cgctgtcatgggcgaaaaacccccatatttttgtgggggattcatagtttttgacagcgtcacacagaccgcctgccgtgtttcagacccacttaagcgcctgttcaagttgggtaagccgctaacagc

tgaagacaagcaggacgaagacaggcgacgagcactgagtgacgaggttagcaagtggttccggacaggcttgggggccgaactggaggtggcactaacatctaggtatgaggtagagggct

gcaaaagtatcctcatagccatggccaccttggcgagggacattaaggcgtttaagaaattgagaggacctgttatacacctctacggcggtcctagattggtgcgttaatacacagaattctgattgg

atcccgggctcgagatgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactag

acgtgggagtgcatactatatgtacttggctcagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccac

catgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacgga

gatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaa

ccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtca

gcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaaca

gtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtc

tgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccag

agaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaa

gagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtgg

ttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagg

gagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaa

gggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccag

ctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactc

ttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagac

acagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaac

gttgctgatgtggttgggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagccgtctctgctgagaacatcacatcaggattcctaggacc

cctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtc

cccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggat

tatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacgga

tggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttccccca

ctgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaactcgagcccgggatcccg

ggtaattaattgaattacatccctacgcaaacgttttacggccgccggtggcgcccgcgcccggcggcccgtccttggccgttgcaggccactccggtggctcccgtcgttcccgacttccaggcc

cagcagatgcagcaactcatcagcgccgtaaatgcgctgacaatgagacagaacgcaattgctcctgctaggcctcccaaaccaaagaagaagaagacaaccaaaccaaagccgaaaacgca

gcccaagaagatcaacggaaaaacgcagcagcaaaagaagaaagacaagcaagccgacaagaagaagaagaaacccggaaaaagagaaagaatgtgcatgaagattgaaaatgactgtatc

ttcgtatgcggctagccacagtaacgtagtgtttccagacatgtcgggcaccgcactatcatgggtgcagaaaatctcgggtggtctgggggccttcgcaatcggcgctatcctggtgctggttgtgg

tcacttgcattgggctccgcagataagttagggtaggcaatggcattgatatagcaagaaaattgaaaacagaaaaagttagggtaagcaatggcatataaccataactgtataacttgtaacaaagc

gcaacaagacctgcgcaattggccccgtggtccgcctcacggaaactcggggcaactcatattgacacattaattggcaataattggaagcttacataagcttaattcgacgaataattggatttttattt

tattttgcaattggtttttaatatttccaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaattcgaaactagtctgcattaatgaatcggcca

acgcgcggggagaggttggtttgcgtattgggcgctcttccgcttcctcgctcactgactcgctgcgctcggtcgttcggctgcggcgagcggtatcagctcactcaaaggcggtaatacggttatcc

acagaatcaggggataacgcaggaaagaacatgtgagcaaaaggccagcaaaaggccaggaaccgtaaaaaggccgcgttgctggcgtttttccataggctccgcccccctgacgagcatcac

aaaaatcgacgctcaagtcagaggtggcgaaacccgacaggactataaagataccaggcgtttccccctggaagctccctcgtgcgctctcctgttccgaccctgccgcttaccggatacctgtcc

gcctttctcccttcgggaagcgtggcgctttctcaatgctcgcgctgtaggtatctcagttcggtgtaggtcgttcgctccaagctgggctgtgtgcacgaaccccccgttcagcccgaccgctgcgc

cttatccggtaactatcgtcttgagtccaacccggtaagacacgacttatcgccactggcagcagocactggtaacaggattagcagagcgaggtatgtaggcggtgctacagagttcttgaagtgg

tggcctaactacggctacactagaaggacagtatttggtatctgcgctctgctgaagccagttaccttcggaaaaagagttggtagctcttgatccggcaaacaaaccaccgctggtagcggtggtttt

tttgtttgcaagcagcagattacgcgcagaaaaaaaggatctcaagaagatcctttgatcttttctacggggtctgacgctcagtggaacgaaaactcacgttaagggattttggtcatgagattatcaa

aaaggatcttcacctagatccttttaaattaaaaatgaagttttaaatcaatctaaagtatatatgagtaaacttggtctgacagttaccaatgcttaatcagtgaggcacctatctcagcgatctgtctattt

cgttcatccatagttgcctgactccccgtcgtgtagataactacgatacgggagggcttaccatctggaccagtgctgcaatgataccgcgagacccacgctcaccggctccagatttatcagcaata

aaccagccagccggaagggccgagcgcagaagtggtcctgcaactttatccgcctccatccagtctattaattgttgccgggaagctagagtaagtagttcgccagttaatagtttgcgcaacgttgt

tgccattgctacaggcatcgtggtgtcacgctcgtcgtttggtatggcttcattcagctccggttcccaacgatcaaggcgagttacatgatcccccatgttgtgcaaaaaagcggttagctccttcggt

cctccgatcgttgtcagaagtaagttggccgcagtgttatcactcatggttatggcagcactgcataattctcttactgtcatgccatccgtaagatgcttttctgtgactggtgagtactcaaaaagtcat

tctgagaatagtgtatgcggcgaccgagttgctcttgcccggcgtcaatacgggataataccgcgccacatagcagaactttaaaagtgctcatcattggaaaacgttcttcggggcgaaaactctca

aggatcttaccgctgttgagatccagttcgatgtaacccactcgtgcacccaactgatcttcagcatcttttactttcaccagcgtttctgggtgagcaaaaacaggaaggcaaaatgccgcaaaaaag

ggaataagggcgacacggaaatgttgaatactcatactcttcctttttcaatattattgaagcatttatcagggttattgtctcatgagcggatacatatttgaatgtatttagaaaaataaacaaataggggt

tccgcgcacatttccccgaaaagtgccacctgacgtctaagaaaccattattatcatgacattaacctataaaaataggcgtatcacgaggccctttcgtctcgcgcgtttcggtgatgacggtgaaaa

cctctgacacatgcagctcccggagacggtcacagcttctgtctaagcggatgccgggagcagacaagcccgtcagggcgcgtcagcgggtgttggcgggtgtcggggctggcttaactatgcg

gcatcagagcagattgtactgagagtgcaccatatcgacgctctcccttatgcgactcctgcattaggaagcagcccagtactaggttgaggccgttgagcaccgccgccgcaaggaatggtgcat

gcaaggagatggcgcccaacagtcccccggccacggggcctgccaccatacccacgccgaaacaagcgctcatgagcccgaagtggcgagccogatcttocccatcggtgatgtcggcgata

taggcgccagcaaccgcacctgtggcgccggtgatgccggccacgatgcgtccggcgtagaggatctggctagcgatgaccctgctgattggttcgctgaccatttccggggtgcggaacggcg

ttaccagaaactcagaaggttcgtccaaccaaaccgactctgacggcagtttacgagagagatgatagggtctgcttcagtaagccagatgctacacaattaggcttgtacatattgtcgttagaacg

cggctacaattaatacataaccttatgtatcatacacatacgatttaggtgacactata

SEQ
gatggcggatgtgtgacatacacgacgccaaaagattttgttccagctcctgccacctccgctacgcgagagattaaccacccacgatggccgccaaagtgcatgttgatattgaggctgacagcc

ID
cattcatcaagtctttgcagaaggcatttccgtcgttcgaggtggagtcattgcaggtcacaccaaatgaccatgcaaatgccagagcattttcgcacctggctaccaaattgatcgagcaggagact

NO:
gacaaagacacactcatcttggatatcggcagtgcgccttccaggagaatgatgtctacgcacaaataccactgcgtatgccctatgcgcagcgcagaagaccccgaaaggctcgatagctacgc

54
aaagaaactggcagcggcctccgggaaggtgctggatagagagatcgcaggaaaaatcaccgacctgcagaccgtcatggctacgccagacgctgaatctcctaccttttgcctgcatacagac

gtcacgtgtcgtacggcagccgaagtggccgtataccaggacgtgtatgctgtacatgcaccaacatcgctgtaccatcaggcgatgaaaggtgtcagaacggcgtattggattgggtttgacacc

accccgtttatgtttgacgcgctagcaggcgcgtatccaacctacgccacaaactgggccgacgagcaggtgttacaggccaggaacataggactgtgtgcagcatccttgactgagggaagact

cggcaaactgtccattctccgcaagaagcaattgaaaccttgcgacacagtcatgttctcggtaggatctacattgtacactgagagcagaaagctactgaggagctggcacttaccctccgtattcc

acctgaaaggtaaacaatcctttacctgtaggtgcgataccatcgtatcatgtgaagggtacgtagttaagaaaatcactatgtgccccggcctgtacggtaaaacggtagggtacgccgtgacgtat

cacgcggagggactcctagtgtgcaagaccacagacactgtcaaaggagaaagagtctcattccctgtatgcacctacgtcccctcaaccatctgtgatcaaatgactggcatactagcgaccgac

gtcacaccggaggacgcacagaagttgttagtgggattgaatcagaggatagttgtgaacggaagaacacagcgaaacactaacacgatgaagaactatctgcttccgattgtggccgtcgcat

ttagcaagtgggcgagggaatacaaggcagaccttgatgatgaaaaacctctgggtgtccgagagaggtcacttacttgctgctgcttgtgggcatttaaaacgaggaagatgcacaccatgtaca

agaaaccagacacccagacaatagtgaaggtgccttcagagtttaactcgttcgtcatcccgagcctatggtctacaggcctcgcaatcccagtcagatcacgcattaagatgcttttggccaagaag

accaagcgagagttaatacctgttctcgacgcgtcgtcagccagggatgctgaacaagaggagaaggagaggttggaggccgagctgactagagaagccttaccacccctcgtccccatcgcg

ccggcggagacgggagtcgtcgacgtcgacgttgaagaactagagtatcacgcaggtgcaggggtcgtggaaacacctcgcagcgcgttgaaagtcaccgcacagccgaacgacgtactact

aggaaattacgtagttctgtccccgcagaccgtgctcaagagctccaagttggcccccgtgcaccctctagcagagcaggtgaaaataataacacataacgggagggccggcggttaccaggtc

gacggatatgacggcagggtcctactaccatgtggatcggccattccggtccctgagtttcaagctttgagcgagagcgccactatggtgtacaacgaaagggagttcgtcaacaggaaactatac

catattgccgttcacggaccgtcgctgaacaccgacgaggagaactacgagaaagtcagagctgaaagaactgacgccgagtacgtgttcgacgtagataaaaaatgctgcgtcaagagagagg

aagcgtcgggtttggtgttggtgggagagctaaccaaccccccgttccatgaattcgcctacgaagggctgaagatcaggccgtcggcaccatataagactacagtagtaggagtctttggggttcc

gggatcaggcaagtctgctattattaagagcctcgtgaccaaacacgatctggtcaccagcggcaagaaggagaactgccaggaaatagttaacgacgtgaagaagcaccgcgggaaggggac

aagtagggaaaacagtgactccatcctgctaaacgggtgtcgtcgtgccgtggacatcctatatgtggacgaggctttcgcttgccattccggtactctgctggccctaattgctcttgttaaacctcgg

agcaaagtggtgttatgcggagaccccaagcaatgcggattcttcaatatgatgcagcttaaggtgaacttcaaccacaacatctgcactgaagtatgtcataaaagtatatccagacgttgcacgcgt

ccagtcacggccatcgtgtctacgttgcactacggaggcaagatgcgcacgaccaacccgtgcaacaaacccataatcatagacaccacaggacagaccaagcccaagccaggagacatcgtg

ttaacatgcttccgaggctgggcaaagcagctgcagttggactaccgtggacacgaagtcatgacagcagcagcatctcagggcctcacccgcaaaggggtatacgccgtaaggcagaaggtg

aatgaaaatcccttgtatgcccctgcgtcggagcacgtgaatgtactgctgacgcgcactgaggataggctggtgtggaaaacgctggccggcgatccctggattaaggtcctatcaaacattccac

agggtaactttacggccacattggaagaatggcaagaagaacacgacaaaataatgaaggtgattgaaggaccggctgcgcctgtggacgcgttccagaacaaagcgaacgtgtgttgggcgaa

aagcctggtgcctgtcctggacactgccggaatcagattgacagcagaggagtggagcaccataattacagcatttaaggaggacagagcttactctccagtggtggccttgaatgaaatttgcacc

aagtactatggagttgacctggacagtggcctgttttctgccccgaaggtgtccctgtattacgagaacaaccactgggataacagacctggtggaaggatgtatggattcaatgccgcaacagctg

ccaggctggaagctagacataccttcctgaaggggcagtggcatacgggcaagcaggcagttatcgcagaaagaaaaatccaaccgctttctgtgctggacaatgtaattcctatcaaccgcagg

ctgccgcacgccctggtggctgagtacaagacggttaaaggcagtagggttgagtggctggtcaataaagtaagagggtaccacgtcctgctggtgagtgagtacaacctggctttgcctcg

acgcagggtcacttggttgtcaccgctgaatgtcacaggcgccgataggtgctacgacctaagtttaggactgccggctgacgccggcaggttcgacttggtctttgtgaacattcacacggaattca

gaatccaccactaccagcagtgtgtcgaccacgccatgaagctgcagatgcttgggggagatgcgctacgactgctaaaacccggcggcatcttgatgagagcttacggatacgccgataaaatc

agcgaagccgttgtttcctccttaagcagaaagttctcgtctgcaagagtgttgcgcccggattgtgtcaccagcaatacagaagtgttcttgctgttctccaactttgacaacggaaagagaccctcta

cgctacaccagatgaataccaagctgagtgccgtgtatgccggagaagccatgcacacggccgggtgtgcaccatcctacagagttaagagagcagacatagccacgtgcacagaagcggctg

tggttaacgcagctaacgcccgtggaactgtaggggatggcgtatgcagggccgtggcgaagaaatggccgtcagcctttaagggagcagcaacaccagtgggcacaattaaaacagtcatgtg

cggctcgtaccccgtcatccacgctgtagcgcctaatttctctgccacgactgaagcggaaggggaccgcgaattggccgctgtctaccgggcagtggccgccgaagtaaacagactgtcactga

gcagcgtagccatcccgctgctgtccacaggagtgttcagcggcggaagagataggctgcagcaatccctcaaccatctattcacagcaatggacgccacggacgctgacgtgaccatctactgc

agagacaaaagttgggagaagaaaatccaggaagccattgacatgaggacggctgtggagttgctcaatgatgacgtggagctgaccacagacttggtgagagtgcacccggacagcagcctg

gtgggtcgtaagggctacagtaccactgacgggtcgctgtactcgtactttgaaggtacgaaattcaaccaggctgctattgatatggcagagatactgacgttgtggcccagactgcaagaggcaa

acgaacagatatgcctatacgcgctgggcgaaacaatggacaacatcagatccaaatgtccggtgaacgattccgattcatcaacacctcccaggacagtgccctgcctgtgccgctacgcaatga

cagcagaacggatcgcccgccttaggtcacaccaagttaaaagcatggtggtttgctcatcttttcccctcccgaaataccatgtagatggggtgcagaaggtaaagtgcgagaaggttctcctgttc

gacccgacggtaccttcagtggttagtccgcggaagtatgccgcatctacgacggaccactcagatcggtcgctacgagggtttgacttggactggaccaccgactcgtcttccactgccagcgata

ccatgtcgctacccagtttgcagtcgtgtgacatcgactcgatctacgagccaatggctcccatagtagtgacggctgacgtacaccctgaacccgcaggcatcgcggacctggcggcagatgtgc

accctgaacccgcagaccatgtggacctcgagaacccgattcctccaccgcgcccgaagagagctgcataccttgcctcccgcgcggcggagcgaccggtgccggcgccgagaaagccgac

gcctgccccaaggactgcgtttaggaacaagctgcctttgacgttcggcgactttgacgagcacgaggtcgatgcgttggcctccgggattactttcggagacttcgacgacgtcctgcgactaggc

cgcgcgggtgcatatattttctcctcggacactggcagcggacatttacaacaaaaatccgttaggcagcacaatctccagtgcgcacaactggatgcggtccaggaggagaaaatgtacccgcca

aaactggatactgagagggagaagctgttgctgctgaaaatgcagatgcacccatcggaggctaataagagtcgataccagtctcgcaaagtggagaacatgaaagccacggtggtggacaggc

tcacatcgggggccagactgtacacgggagcggacgtaggccgcataccaacatacgcggctcggtacccccgccccgtgtactcccctaccgtgatcgaaagactctcaagccccgatgtagca

atcgcagcgtgcaacgaatacctattcagaaactacccaacagtggcgtcgtaccagataacagatgaatacgacgcatacctggacatggttgacgggtcggatagctgcctggacagagcgaca

ttctgcccggcgaagctccggtgctacccgaaacatcatgcgtaccaccagccgactgtacgcagtgccgtcccgtcaccctttcagaacacactacagaacgtgctagcggccgccaccaaga

gaaactgcaacgtcacgcaaatgcgagaactacccaccatggactcggcagtgttcaacgtggagtgcttcaagcgctatgcctgctccggagaatattgggaagaatatgctaaacaacctatcc

ggataaccactgagaacatcactacctatgtgaccaaattgaaaggcccgaaagctgctgccttgttcgctaagacccacaacttggttccgctgcaggaggttcccatggacagattcacggtcga

catgaaacgagatgtcaaagtcactccagggacgaaacacacagaggaaagacccaaagtccaggtaattcaagcagcggagccattggcgaccgcttacctgtgcggcatccacagggaatt

agtaaggagactaaatgctgtgttacgccctaacgtgcacacattgtttgatatgtcggccgaagactttgacgcgatcatcgcctctcactttccacccaggagacccggttctagagacggacattg

catcattcgacaaaagccaggacgactccttggctcttacaggtttaatgatcctcgaagatctaggggtggatcagtacctgctggacttgatcgaggcagcctttggggaaatatccagctgtcac

ctaccaactggcacgcgcttcaagttcggagctatgatgaaatcgggcatgtttctgactttgtttattaacactgttttgaacatcaccatagcaagcagggtactggagcagagactcactgactccg

cctgtgcggccttcatcggcgacgacaacatcgttcacggagtgatctccgacaagctgatggcggagaggtgcgcgtcgtgggtcaacatggaggtgaagatcattgacgctgtcatgggcgaa

aaacccccatatttttgtgggggattcatagtttttgacagcgtcacacagaccgcctgccgtgtttcagacccacttaagcgcctgttcaagttgggtaagccgctaacagctgaagacaagcagga

cgaagacaggcgacgagcactgagtgacgaggttagcaagtggttccggacaggcttgggggccgaactggaggtggcactaacatctaggtatgaggtagagggctgcaaaagtatcctcat

agccatggccaccttggcgagggacattaaggcgtttaagaaattgagaggacctgttatacacctctacggcggtcctagattggtgcgttaatacacagaattctgattggatcccgggctcgaga

tgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcata

ctatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatgc

cctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctgt

gacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgtta

gcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgt

ggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcg

gaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgtta

gtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtacc

ggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccacc

ctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattcc

attaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaagg

agcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcata

ctccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcgg

tggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcatag

gagtcggggagaagaagatcacccaccactgacacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggac

tttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtgg

ttgggtctgaacgcaaagaatggatctagaatcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacct

ccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaagg

tatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaatt

gcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttgg

ctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaactcgagcccgggatcccgggtaatta

attgaattacatccctacgcaaacgttttacggccgccggtggcgcccgcgcccggcggcccgtccttggccgttgcaggccactccggtggctcccgtcgtccccgacttccaggcccagcagat

gcagcaactcatcagcgccgtaaatgcgctgacaatgagacagaacgcaattgctcctgctaggcctcccaaaccaaagaagaagaagacaaccaaaccaaagccgaaaacgcagcccaaga

agatcaacggaaaaacgcagcagcaaaagaagaaagacaagcaagccgacaagaagaagaagaaacccggaaaaagagaaagaatgtgcatgaagattgaaaatgactgtatcttcgtatgc

ggctagccacagtaacgtagtgtttccagacatgtcgggcaccgcactatcatgggtgcagaaaatctcgggtggtctgggggccttcgcaatcggcgctatcctggtgctggttgtggtcacttgc

attgggctccgcagataagttagggtaggcaatggcattgatatagcaagaaaattgaaaacagaaaaagttagggtaagcaatggcatataaccataactgtataacttgtaacaaagcgcaacaa

gacctgcgcaattggccccgtggtccgcctcacggaaactcggggcaactcatattgacacattaattggcaataattggaagcttacataagcttaattcgacgaataattggatttttattttattttgca

attggtttttaatatttccaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaattcgaaactagtctgcattaatgaatcggccaacgcgcg

gggagaggcggtttgcgtattgggcgctcttccgcttcctcgctcactgactcgctgcgctcggtcgttcggctgcggcgagcggtatcagctcactcaaaggcggtaatacggttatccacagaat

caggggataacgcaggaaagaacatgtgagcaaaaggccagcaaaaggccaggaaccgtaaaaaggccgcgttgctggcgtttttccataggctccgcccccctgacgagcatcacaaaaatc

gacgctcaagtcagaggtggcgaaacccgacaggactataaagataccaggcgtttccccctggaagctccctcgtgcgctctcctgttccgaccctgccgcttaccggatacctgtccgcctttct

cccttcgggaagcgtggcgctttctcaatgctcgcgctgtaggtatctcagttcggtgtaggtcgttcgctccaagctgggctgtgtgcacgaaccccccgttcagcccgaccgctgcgccttatccg

gtaactatcgtcttgagtccaacccggtaagacacgacttatcgccactggcagcagccactggtaacaggattagcagagcgaggtatgtaggcggtgctacagagttcttgaagtggtggccta

actacggctacactagaaggacagtatttggtatctgcgctctgctgaagccagttaccttcggaaaaagagttggtagctcttgatccggcaaacaaaccaccgctggtagcggtggtttttttgtttg

caagcagcagattacgcgcagaaaaaaaggatctcaagaagatcctttgatcttttctacggggtctgacgctcagtggaacgaaaactcacgttaagggattttggtcatgagattatcaaaaagga

tcttcacctagatccttttaaattaaaaatgaagttttaaatcaatctaaagtatatatgagtaaacttggtctgacagttaccaatgcttaatcagtgaggcacctatctcagcgatctgtctatttcgttca

tccatagttgcctgactccccgtcgtgtagataactacgatacgggagggcttaccatctggccccagtgctgcaatgataccgcgagacccacgctcaccggctccagatttatcagcaataaaccag

ccagccggaagggccgagcgcagaagtggtcctgcaactttatccgcctccatccagtctattaattgttgccgggaagctagagtaagtagttcgccagttaatagtttgcgcaacgttgttgccatt

gctacaggcatcgtggtgtcacgctcgtcgtttggtatggcttcattcagctccggttcccaacgatcaaggcgagttacatgatcccccatgttgtgcaaaaaagcggttagctccttcggtcctccga

tcgttgtcagaagtaagttggccgcagtgttatcactcatggttatggcagcactgcataattctcttactgtcatgccatccgtaagatgcttttctgtgactggtgagtactcaaccaagtcattctgaga

atagtgtatgcggcgaccgagttgctcttgcccggcgtcaatacgagataataccgcgccacatagcagaactttaaaagtgctcatcattggaaaacgttcttcggggcgaaaactctcaaggatct

taccgctgttgagatccagttcgatgtaacccactcgtgcacccaactgatcttcagcatcttttactttcaccagcgtttctgggtgagcaaaaacaggaaggcaaaatgccgcaaaaaagggaata

agggcgacacggaaatgttgaatactcatactcttcctttttcaatattattgaagcatttatcagggttattgtctcatgagcggatacatatttgaatgtatttagaaaaataaacaaataggggttccgcg

cacatttccccgaaaagtgccacctgacgtctaagaaaccattattatcatgacattaacctataaaaataggcgtatcacgaggccctttcgtctcgcgcgtttcggtgatgacggtgaaaacctctga

cacatgcagctcccggagacggtcacagcttctgtctaagcggatgccgggagcagacaagcccgtcagggcgcgtcagcgggtgttggcgggtgtcggggctggcttaactatgcggcatca

gagcagattgtactgagagtgcaccatatcgacgctctcccttatgcgactcctgcattaggaagcagcccagtactaggttgaggccgttgagcaccgccgccgcaaggaatggtgcatgcaag

gagatggcgcccaacagtcccccggccacggggcctgccaccatacccacgccgaaacaagcgctcatgagcccgaagtggcgagcccgatcttccccatcggtgatgtcggcgatataggc

gccagcaaocgcacctgtggcgccggtgatgccggccacgatgcgtccggcgtagaggatctggctagcgatgaccctgctgattggttcgctgaccatttccggggtgcggaacggcgttacc

agaaactcagaaggttcgtccaaccaaaccgactctgacggcagtttacgagagagatgatagggtctgcttcagtaagccagatgctacacaattaggcttgtacatattgtcgttagaacgcggct

acaattaatacataaccttatgtatcatacacatacgatttaggtgacactata

SEQ
gatggcggatgtgtgacatacacgacgccaaaagattttgttccagctcctgccacctccgctacgcgagagattaaccacccacgatggccgccaaagtgcatgttgatattgaggctgacagcc

ID
cattcatcaagtctttgcagaaggcatttccgtcgttcgaggtggagtcattgcaggtcacaccaaatgaccatgcaaatgccagagcattttcgcacctggctaccaaattgatcgagcaggagact

NO:
gacaaagacacactcatcttggatatcggcagtgcgccttccaggagaatgatgtctacgcacaaataccactgcgtatgccctatgcgcagcgcagaagaccccgaaaggctcgatagctacgc

55
aaagaaactggcagcggcctccgggaaggtgctggatagagagatcgcaggaaaaatcaccgacctgcagaccgtcatggctacgccagacgctgaatctcctaccttttgcctgcatacagac

gtcacgtgtcgtacggcagccgaagtggccgtataccaggacgtgtatgctgtacatgcaccaacatcgctgtaccatcaggcgatgaaaggtgtcagaacggcgtattggattgggtttgacacc

accccgtttatgtttgacgcgctagcaggcgcgtatccaacctacgccacaaactgggccgacgagcaggtgttacaggccaggaacataggactgtgtgcagcatccttgactgagggaagact

cggcaaactgtccattctccgcaagctagcaattgaaaccttgcgacacagtcatgttctcggtaggatctacattgtacactgagagcagaaagctactgaggagctggcacttaccctocgtattcc

acctgaaaggtaaacaatcctttacctgtaggtgcgataccatcgtatcatgtgaagggtacgtagttaagaaaatcactatgtgccccggcctgtacggtaaaacggtagggtacgccgtgacgtat

cacgcggagggattcctagtgtgcaagaccacagacactgtcaaaggagaaagagtctcattccctgtatgcacctacgtcccctcaaccatctgtgatcaaatgactggcatactagcgaccgac

gtcacaccggaggacgcacagaagttgttagtgggattgaatcagaggatagttgtgaacggaagaacacagcgaaacactaacacgatgaagaactatctgcttccgattgtggccgtcgcat

ttagcaagtgggcgagggaatacaaggcagaccttgatgatgaaaaacctctgggtgtccgagagaggtcacttacttgctgctgcttgtgggcatttaaaacgaggaagatgcacaccatgtaca

agaaaccagacacccagacaatagtgaaggtgccttcagagtttaactcgttcgtcatcccgagcctatggtctacaggcctcgcaatcccagtcagatcacgcattaagatgcttttggccaagaag

accaagcgagagttaatacctgttctcgacgcgtcgtcagccagggatgctgaacaagaggagaaggagaggttggaggccgagctgactagagaagccttaccacccctcgtccccatcgcg

ccggcggagacgggagtcgtcgacgtcgacgttgaagaactagagtatcacgcaggtgcaggggtcgtggaaacacctcgcagcgcgttgaaagtcaocgcacagccgaacgacgtactact

aggaaattacgtagttctgtccccgcagaccgtgctcaagagctccaagttggcccccgtgcaccctctagcagagcaggtgaaaataataacacataacgggagggccggcggttaccaggtc

gacggatatgacggcagggtcctactaccatgtggatcggccattccggtccctgagtttcaagctttgagcgagagcgccactatggtgtacaacgaaagggagttcgtcaacaggaaactatac

catattgccgttcacggaccgtcgctgaacaccgacgaggagaactacgagaaagtcagagctgaaagaactgacgccgagtacgtgttcgacgtagataaaaaatgctgcgtcaagagagagg

aagcgtcgggtttggtgttggtgggagagctaaccaaccccccgttccatgaattcgcctacgaagggctgaagatcaggccgtcggcaccatataagactacagtagtaggagtctttggggtta

gggatcaggcaagtctgctattattaagagcctcgtgaccaaacacgatctggtcaccagcggcaagaaggagaactgccaggaaatagttaacgacgtgaagaagcaccgcgggaaggggac

aagtagggaaaacagtgactccatcctgctaaacgggtgtcgtcgtgccgtggacatcctatatgtggacgaggctttcgcttgccattccggtactctgctggccctaattgctcttgttaaacctcgg

agcaaagtggtgttatgcggagaccccaagcaatgcggattcttcaatatgatgcagcttaaggtgaacttcaaccacaacatctgcactgaagtatgtcataaaagtatatccagacgttgcacgcgt

ccagtcacggccatcgtgtctacgttgcactacggaggcaagatgcgcacgaccaacccgtgcaacaaacccataatcatagacaccacaggacagaccaagcccaagccaggagacatcgtg

ttaacatgcttccgaggctgggcaaagcagctgcagttggactaccgtggacacgaagtcatgacagcagcagcatctcagggcctcacccgcaaaggggtatacgccgtaaggcagaaggtg

aatgaaaatcccttgtatgcccctgcgtcggagcacgtgaatgtactgctgacgcgcactgaggataggctggtgtggaaaacgctggccggcgatccctggattaaggtcctatcaaacat

tccacagggtaactttacggccacattggaagaatggcaagaagaacacgacaaaataatgaaggtgattgaaggaccggctgcgcctgtggacgcgttccagaacaaagcgaacgtgtgttgg

gcgaaaagcctggtgcctgtcctggacactgccggaatcagattgacagcagaggagtggagcaccataattacagcatttaaggaggacagagcttactctccagtggtggccttgaatgaaattt

gcaccaagtactatggagttgacctggacagtggcctgttttctgccccgaaggtgtccctgtattacgagaacaaccactgggataacagacctggtggaaggatgtatggattcaatgccgcaac

agctgccaggctggaagctagacataccttcctgaaggggcagtggcatacgggcaagcaggcagttatcgcagaaagaaaaatccaaccgctttctgtgctggacaatgtaattcctatcaaccg

caggctgccgcacgccctggtggctgagtacaagacggttaaaggcagtagggttgagtggctggtcaataaagtaagagggtaccacgtcctgctggtgagtgagtacaacctggctttgcctc

gacgcagggtcacttggttgtcaccgctgaatgtcacaggcgccgataggtgctacgacctaagtttaggactgccggctgacgccggcaggttcgacttggtctttgtgaacattcacacggaatt

cagaatccaccactaccagcagtgtgtcgaccacgccatgaagctgcagatgcttgggggagatgcgctacgactgctaaaacccggcggcatcttgatgagagcttacggatacgccgataaaa

tcagcgaagccgttgtttcctccttaagcagaaagttctcgtctgcaagagtgctgcgcccggattgtgtcaccagcaatacagaagtgttcttgctgttctccaactttgacaacggaaagagaccctc

tacgctacaccagatgaataccaagctgagtgccgtgtatgccggagaagccatgcacacggccgggtgtgcaccatcctacagagttaagagagcagacatagccacgtgcacagaagcggc

tgtggttaacgcagctaacgcccgtggaactgtaggggatggcgtatgcagggccgtggcgaagaaatggccgtcagcctttaagggagcagcaacaccagtgggcacaattaaaacagtcatg

tgcggctcgtaccccgtcatccacgctgtagcgcctaatttctctgccacgactgaagcggaaggggaccgcgaattggccgctgtctaccgggcagtggccgccgaagtaaacagactgtcact

gagcagcgtagccatcccgctgctgtccacaggagtgttcagcggcggaagagataggctgcagcaatccctcaaccatctattcacagcaatggacgccacggacgctgacgtgaccatctact

gcagagacaaaagttgggagaagaaaatccaggaagccattgacatgaggacggctgtggagttgctcaatgatgacgtggagctgaccacagacttggtgagagtgcacccggacagcagcc

tggtgggtcgtaagggctacagtaccactgacgggtcgctgtactcgtactttgaaggtacgaaattcaaccaggctgctattgatatggcagagatactgacgttgtggcccagactgcaagaggc

aaacgaacagatatgcctatacgcgctgggcgaaacaatggacaacatcagatccaaatgtccggtgaacgattccgattcatcaacacctcccaggacagtgccctgcctgtgccgctacgcaat

gacagcagaacggatcgcccgccttaggtcacaccaagttaaaagcatggtggtttgctcatcttttcccctcccgaaataccatgtagatggggtgcagaaggtaaagtgcgagaaggttctcctgt

tcgacccgacggtaccttcagtggttagtccgcggaagtatgccgcatctacgacggaccactcagatcggtcgttacgagggtttgacttggactggaccaccgactcgtcttccactgccagcga

taccatgtcgctacccagtttgcagtcgtgtgacatcgactcgatctacgagccaatggctcccatagtagtgacggctgacgtacaccctgaacccgcaggcatcgcggacctggcggcagatgt

gcaccctgaacccgcagaccatgtggacctcgagaacccgattcctccaccgcgcccgaagagagctgcataccttgcctcccgcgcggcggagcgaccggtgccggcgccgagaaagccg

acgcctgccccaaggactgcgtttaggaacaagctgcctttgacgttcggcgactttgacgagcacgaggtcgatgcgttggcctccgggattactttcggagacttcgacgacgtcctgcgactag

gccgcgcgggtgcatatattttctcctcggacactggcagcggacatttacaacaaaaatccgttaggcagcacaatctccagtgcgcacaactggatgcggtccaggaggagaaaatgtacccg

ccaaaactggatactgagagggagaagctgctgctgctgaaaatgcagatgcacccatcggaggctaataagagtcgataccagtctcgcaaagtggagaacatgaaagccacggtggtggaca

ggctcacatcgggggccagattgtacacgggagcggacgtaggccgcataccaacatacgcggttcggtacccccgccccgtgtactcccctaccgtgatcgaaagattctcaagccccgatgta

gcaatcgcagcgtgcaacgaatacctatccagaaattacccaacagtggcgtcgtaccagataacagatgaatacgacgcatacttggacatggttgacgggtcggatagttgcttggacagagcg

acattctgcccggcgaagctccggtgctacccgaaacatcatgcgtaccaccagccgactgtacgcagtgccgtcccgtcaccctttcagaacacactacagaacgtgctagcggccgccaccaa

gagaaactgcaacgtcacgcaaatgcgagaactacccaccatggactcggcagtgttcaacgtggagtgcttcaagcgctatgcctgctccggagaatattgggaagaatatgctaaacaacctat

ccggataaccactgagaacatcactacctatgtgaccaaattgaaaggcccgaaagctgctgccttgttcgctaagacccacaacttggttccgctgcaggaggttcccatggacagattcacggtc

gacatgaaacgagatgtcaaagtcactccagggacgaaacacacagaggaaagacccaaagtccaggtaactcaagcagcggagccactggcgaccgcttacctgtgcggcatccacaggga

attagtaaggagactaaatgctgtgttacgccctaacgtgcacacattgtttgatatgtcggccgaagactttgacgcgatcatcgcctctcacttccacccaggagacccggttctagagacggac

attgcatcattcgacaaaagccaggacgactccttggctcttacaggtttaatgatcctcgaagatctaggggtggatcagtacctgctggacttgatcgaggcagcctttggggaaatatccagctgt

cacctaccaactggcacgcgcttcaagttcggagctatgatgaaatcgggcatgtttctgactttgtttattaacactgttttgaacatcaccatagcaagcagggtactggagcagagactcactgact

ccgcctgtgcggccttcatcggcgacgacaacatcgttcacggagtgatctccgacaagctgatggcggagaggtgcgcgtcgtgggtcaacatggaggtgaagatcattgacgctgtcatgggc

gaaaaacccccatatttttgtgggggattcatagtttttgacagcgtcacacagaccgcctgccgtgtttcagacccacttaagcgcctgttcaagttgggtaagccgctaacagctgaagacaagca

ggacgaagacaggcgacgagcactgagtgacgaggttagcaagtggttccggacaggcttgggggccgaactggaggtggcactaacatctaggtatgaggtagagggctgcaaaagt

atcctcatagccatggccaccttggcgagggacattaaggcgtttaagaaattgagaggacctgttatacacctctacggcggtcctagattggtgcgttaatacacagaattctgattggatcccggg

ctcgagatgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtggga

gtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagcta

tgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaa

gagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccct

ggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaa

tagggaccttgtggaaggtatgtcaggtgggacctgggctgatgttgtcctggaacatggaggctgtgtcactgtaatggcacaggacaaaccgactgtcgacatagagctggctacaacaacagtca

gcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgca

aaagaacgctagtggacagaggctggggaaatggatgtggacctcttggcaaagggagcctggtgacatgcgctaagcttgcatgctccaagaaaatgaccgggaagagcatccagccagagaa

tctggagtaccggataatgctgtcagctcatggctcccagcacagtgggatgatcgctaatgacacaggacatgaaactgatgagaatagagcgaaagctgagataacgcccaactcaccaaga

gccgaagccaccctgggggggcttggaagcctaggacctgattgtgaaccgaggacaggccctgacctctcagatctgtattacctgactatgaataacaagcactggctggctcacaaggagtggctc

cacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctaggga

gtcaagaaggagcagctcacacggcccctgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacctgaaatgtcgcctgaaaatggataaacctagattgaagg

gcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctc

agatggcggtggacatgcaaactctgaccccagttgggaggctgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccacttggggactct

tacactgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccactggaaaagcatctgaagccactgtgagaggtgccaagagaatggcagtcctgggagaca

cagcctgggaccttggatcagctggaggcgctctcaactcactgggcaagggcatccatcaaatccttggagcagccttcaaatcactgcttggaggaatgtcctggctctcacaaactctcattggaacg

ctgctgatgtggctgggtctgaacgcaaagaatggatctattttccctatgtgcctggccctagggggagtgctgatcctcttatccacagccgtctctgctcagtggaactccactgccctccaccaaactc

tgcaggatcccagagtcaggggtctgtatcctcctgctggtggctccagctcaggaacagtaaaccctgctccgaatactgcctctcacatctcgtcaatctccgcgaggactggggaccctgtgacg

aacatggagaacatcacatcaggattcctaggacccctgctcgtgctacaggcggggttcttcctgttgacaagaatcctcacaataccgcagagtctagactcgtggtggacctctctcaactctctagg

gggatctcccgtgtgtcctggccaaaactcgcagtocccaacctccaatcactcaccaacctcctgtcctccaatctgtcctggttatcgctggatgtgtctgcggcgttctatcatattcctcttcatcctgc

tgctatgcctcatcttcttattggctcctctggattatcaaggtatgctggcgtctgtcctctaactccaggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggca

actctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagttt

actagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttct

tttgtctctgggtatacatttaactcgagcccgggatcccgggtaattaattgaattacatccctacgcaaacgttttacggccgccggtggcgcccgcgcccggcggcccgtccttggccgttgcagg

ccactccggtggctcccgtcgtccccgacttccaggcccagcagatgcagcaactcatcagcgccgtaaatgcgctgacaatgagacagaacgcaattgctcctgctaggcctcccaaaccaaag

aagaagaagacaaccaaactaaagccgaaaacgcagcccaagaagatcaacggaaaaacgcagcagcaaaagaagaaagacaagcaagccgacaagaagaagaagaaacccggaaaaa

gagaaagaatgtgcatgaagattgaaaatgactgtatcttcgtatgcggctagccacagtaacgtagtgtttccagacatgtcgggcaccgcactatcatgggtgcagaaaatctcgggtggtctgg

gggccttcgcaatcggcgctatcctggtgctggttgtggtcacttgcattgggctccgcagataagttagggtaggcaatggcattgatatagcaagaaaattgaaaacagaaaaagttagggtaag

caatggcatataaccataactgtataacttgtaacaaagcgcaacaagacctgcgcaattggccccgtggtccgcctcacggaaactcggggcaactcatattgacacattaattggcaataattgga

agcttacataagcttaattcgacgaataattggatttttattttattttgcaattggtttttaatatttccaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaaa

aaaaaaaattcgaaactagtctgcattaatgaatcggccaacgcgcggggagaggcggtttgcgtattgggcgctcttccgcttcctcgctcactgactcgctgcgctcggtcgttcggctgcggcg

agcggtatcagctcactcaaaggcggtaatacggttatccacagaatcaggggataacgcaggaaagaacatgtgagcaaaaggccagcaaaaggccaggaaccgtaaaaaggccgcgttgct

ggcgtttttccataggctccgcccccctgacgagcatcacaaaaatcgacgctcaagtcagaggtggcgaaacccgacaggactataaagataccaggcgtttccccctggaagctccctcgtgc

gctctcctgttccgaccctgccgcttaccggatacctgtccgcctttctcccttcgggaagcgtggcgctttctcaatgctcgcgctgtaggtatctcagttcggtgtaggtcgttcgctccaagctggg

ctgtgtgcacgaaccccccgttcagcccgaccgctgcgccttatccggtaactatcgtcttgagtccaacccggtaagacacgacttatcgccactggcagcagccactggtaacaggattagcag

agcgaggtatgtaggcggtgctacagagttcttgaagtggtggcctaactacggctacactagaaggacagtatttggtatctgcgctctgctgaagccagttaccttcggaaaaagagttggtagct

cttgatccggcaaacaaaccaccgctggtagcggtggtttttttgtttgcaagcagcagattacgcgcagaaaaaaaggatctcaagaagatcctttgatcttttctacggggtctgacgctcagtgga

acgaaaactcacgttaagggattttggtcatgagattatcaaaaaggatcttcacctagatccttttaaattaaaaatgaagttttaaatcaatctaaagtatatatgagtaaacttggtctgacagtt

accaatgcttaatcagtgaggcacctatctcagcgatctgtctatttcgttcatccatagttgcctgactccccgtcgtgtagataactacgatacgggagggcttaccatctggccccagtgctgcaat

gataccgcgagacccacgctcaccggctccagatttatcagcaataaaccagccagccggaagggccgagcgcagaagtggtcctgcaactttatccgcctccatccagtctattaattgttgccg

ggaagctagagtaagtagttcgccagttaatagtttgcgcaacgttgttgccattgctacaggcatcgtggtgtcacgctcgtcgtttggtatggcttcattcagctccggttcccaacgatcaaggcga

gttacatgatcccccatgttgtgcaaaaaagcggttagctccttcggtcctccgatcgttgtcagaagtaagttggccgcagtgttatcactcatggttatggcagcactgcataattctcttactgtcatg

ccatccgtaagatgcttttctgtgactggtgagtactcaaccaagtcattctgagaatagtgtatgcggcgaccgagttgctcttgcccggcgtcaatacgggataataccgcgccacatagcagaact

ttaaaagtgctcatcattggaaaacgttcttcggggcgaaaactctcaaggatcttaccgctgttgagatccagttcgatgtaacccactcgtgcacccaactgatcttcagcatcttttactttcaccagc

gtttctgggtgagcaaaaacaggaaggcaaaatgccgcaaaaaagggaataagggcgacacggaaatgttgaatactcatactcttcctttttcaatattattgaagcatttatcagggttattgtctcat

gagcggatacatatttgaatgtatttagaaaaataaacaaataggggttccgcgcacatttccccgaaaagtgccacctgacgtctaagaaaccattattatcatgacattaacctataaaaataggcgt

atcacgaggccctttcgtctcgcgcgtttcggtgatgacggtgaaaacctctgacacatgcagctcccggagacggtcacagcttctgtctaagcggatgccgggagcagacaagcccgtcaggg

cgcgtcagcgggtgttggcgggtgtcggggctggcttaactatgcggcatcagagcagattgtactgagagtgcaccatatcgacgctctcccttatgcgactcctgcattaggaagcagcccagt

actaggttgaggccgttgagcaccgccgccgcaaggaatggtgcatgcaaggagatggcgcccaacagtcccccggccacggggcctgccaccatacccacgccgaaacaagcgctcatga

gcccgaagtggcgagcccgatcttccccatcggtgatgtcggcgatataggcgccagcaaccgcacctgtggcgccggtgatgccggccacgatgcgtccggcgtagaggatctggctagcga

tgaccctgctgattggttcgctgaccatttccggggtgcggaacggcgttaccagaaactcagaaggttcgtccaaccaaaccgactctgacggcagtttacgagagagatgatagggtctgcttca

gtaagccagatgctacacaattaggcttgtacatattgtcgttagaacgcggctacaattaatacataaccttatgtatcatacacatacgatttaggtgacactata

SEQ
ttaattccgtgtattctatagtgtcacctaaatcgtatgtgtatgatacataaggttatgtattaattgtagccgcgttctaacgacaatatgtacaagcctaattgtgtagcatctggcttactgaagcagac

ID
cctatcatctctctcgtaaactgccggcagagtcggtttggttggacgaaccttctgagtttctggtaacgccgtcccgcacccggaaatggtcagcgaaccaatcagcagggtcatcgctagccagat

NO:
cctctacgccggacgcatcgtggccggcatcaccggcgccacaggtgcggttgctggcgcctatatcgccgacatcaccgatggggaagatcgggctcgccacttcgggctcatgagcgcttgtt

56
tcggcgtgggtatggtggcaggccccgtggccgggggactgttgggcgccatctccttgcatgcaccattccttgcggcggcggtsctcaacggcctcaacctactactgggctgcttcctaatgc

aggagtcgcataagggagagcgtcgaatggtgcactctcagtacaatctgctctgatgccgcatagttaagccagccccgacacccgccaacacccgctgacgcgccctgacgggc

ttgtctgctcccggcatccgcttacagacaagctgtgaccgtctccgggagctgcatgtgtcagaggttttcaccgtcatcaccgaaacgcgcgagacgaaagggcctcgtgatacgcctatttttat

aggttaatgtcatgataataatggtttcttagacgtcaggtggcacttttcggggaaatgtgcgcggaacccctatttgtttatttttctaaatacattcaaatatgtatccgctcatgagacaataaccctga

taaatgcttcaataatattgaaaaaggaagagtatgagtactcaacatttccgtgtcgcccttattcccttttttgcggcattttgccttcctgtttttgctcacccagaaacgctggtgaaagtaaaagatgc

tgaagatcagttgggtgcacgagtgggttacatcgaactggatctcaacagcggtaagatccttgagagttttcgccccgaagaacgttttccaatgatgagcacttttaaagttctgctatgtggcgcg

gtattatcccgtattgacgccgggcaagagcaactcggtcgccgcatacactattctcagaatgacttggttgagtactcaccagtcacagaaaagcatcttacggatggcatgacagtaagagaatt

atgcagtgctgccataaccatgagtgataacactgcggccaacttacttctgacaacgatcggaggaccgaaggagctaaccgcttttttgcacaacatgggggatcatgtaactcgccttgatcgtt

gggaaccggagctgaatgaagccataccaaacgacgagcgtgacaccacgatgcctgtagcaatggcaacaacgttgcgcaaactattaactggcgaactacttactctagcttcccggcaacaa

ttaatagactggatggaggcggataaagttgcaggaccacttctgcgctcggcccttccggctggctggtttattgctgataaatctggagccggtgagcgtgggtctcgcggtatcattgcagcact

ggggccagatggtaagccctcocgtatcgtagttatctacacgacggggagtcaggcaactatggatgaacgaaatagacagatcgctgagataggtgcctcactgattaagcattggtaactgtca

gaccaagtttactcatatatactttagattgatttaaaacttcatttttaatttaaaaggatctaggtgaagatcctttttgataatctcatgaccaaaatcccttaacgtgagttttcgttccactgagcgt

cagaccccgtagaaaagatcaaaggatcttcttgagatcctttttttctgcgcgtaatctgctgcttgcaaacaaaaaaaccaccgctaccagcggtggtttgtttgccggatcaagagctaccaactctttt

tccgaaggtaactggcttcagcagagcgcagataccaaatactgtccttctagtgtagccgtagttaggccaccacttcaagaactctgtagcaccgcctacatacctcgctctgctaatcctgttaccagt

ggctgctgccagtggcgataagtcgtgtcttaccgggttggactcaagacgatagttaccggataaggcgcagcggtcgggctgaacggggggttcgtgcacacagcccagcttggagcg

aacgacctacaccgaactgagatacctacagcgtgagcattgagaaagcgccacgcttcccgaagggagaaaggcggacaggtatccggtaagcggcagggtcggaacaggagagcgcac

gagggagcttccagggggaaacgcctggtatctttatagtcctgtcgggtttcgccacctctgacttgagcgtcgatttttgtgatgctcgtcaggggggcggagcctatggaaaaacgccagcaac

gcggcctttttacggttcctggccttttgctggccttttgctcacatgttctttcctgcgttatcccctgattctgtggataaccgtattaccgcctttgagtgagctgataccgctcgccgcagccgaacga

ccgagcgcagcgagtcagtgagcgaggaagcggaagagcgcccaatacgcaaaccgcctctccccgcgcgttggccgattcattaatgcagctgtggaatgtgtgtcagttagggtgtggaaag

tccccaggctccccagcaggcagaagtatgcaaagcatgcatctcaattagtcagcaaccaggtgtggaaagtccccaggctccccagcaggcagaagtatgcaaagcatgcatctcaattagtc

agcaaccatagtcccgcccctaactccgcccatcccgcccctaactccgcccagttccgcccattctccgccccatggctgactaattttttttatttatgcagaggccgaggccgcctcggcctctga

gctattccagaagtagtgaggaggcttttttggaggcctaggcttttgcaaaaagcttggacacaagacaggcttgcgagatatgtttgagaataccactttatcccgcgtcagggagaggcagtgcg

taaaaagacgcggactcatgtgaaatactggtttttagtgcgccagatctctataatctcgcgcaacctattttcccctcgaacactttttaagccgtagataaacaggctgggacacttcacatgagcg

aaaaatacatcgtcacctgggacatgttgcagatccatgcacgtaaactcgcaagccgactgatgccttctgaacaatggaaaggcattattgccgtaagccgtggcggtctgtaccgggtgcgtta

ctggcgcgtgaactgggtattcgtcatgtcgataccgtttgtatttccagctacgatcacgacaaccagcgcgagcttaaagtgctgaaacgcgcagaaggcgatggcgaaggcttcatcgttattga

tgacctggtggataccggtggtactgcggttgcgattcgtgaaatgtatccaaaagcgcactttgtcaccatcttcgcaaaaccggctggtcgtccgctggttgatgactatgttgttgatatcccgca

agatacctggattgaacagccgtgggatatgggcgtcgtattcgtcccgccaatctccggtcgctaatcttttcaacgcctggcactgccgggcgttgttctttttaacttcaggcgggttacaatagttt

ccagtaagtattctggaggctgcatccatgacacaggcaaacctgagcgaaaccctgttcaaaccccgctttaaacatcctgaaacctcgacgctagtccgccgctttaatcacggcgcacaaccg

cctgtgcagtcggcccttgatggtaaaaccatccctcactggtatcgcatgattaaccgtctgatgtggatctggcgcggcattgacccacgcgaaatcctcgacgtccaggcacgtattgtgatgag

cgatgccgaacgtaccgacgatgatttatacgatacggtgattggctaccgtggcggcaactggatttatgagtgggccccggatctttgtgaaggaaccttacttctgtggtgtgacataattggaca

aactacctacagagatttaaagctctaaggtaaatataaaatttttaagtgtataatgtgttaaactactgattctaattgtttgtgtattttagattccaacctatggaactgatgaatgggagcagtggtgg

aatgcctttaatgaggaaaacctgttttgctcagaagaaatgccatctagtgatgatgaggctactgctgactctcaacattctactcctccaaaaaagaagagaaaggtagaagaccccaaggactttc

cttcagaattgctaagttttttgagtcatgctgtgtttagtaatagaactcttgcttgctttgctatttacaccacaaaggaaaaagctgcactgctatacaagaaaattatggaaaaatattctgtaacct

ttataagtaggcataacagttataatcataacatactgttttttcttactccacacaggcatagagtgtctgctattaataactatgctcaaaaattgtgtacctttagctttttaatttgtaaaggggttaa

taaggaatatttgatgtatagtgccttgactagagatcataatcagccataccacatttgtagaggttttacttgctttaaaaaacctcccacacctccccctgaacctgaaacataaaatgaatgcaattgtt

gttgttaacttgtttattgcagcttataatggttacaaataaagoaatagcatcacaaatttcacaaataaagcatttttttcactgcattctagttgtggtttgtccaaatttcatcaatgtatcttatcatg

tctggatcaactggataactcaagctaaccaaaatcatcccaaacttcccaccccataccctattaccactgccaattacctagtggtttcatttactctaaacctgtgattcctctgaattattttcatttta

aagaaattgtatttgttaaatatgtactacaaacttagtagttggaagggctaattcactcccaaagaagacaagatatccttgatctgtggatctaccacacacaaggctacttccctgattagcagaacta

cacaccagggccaggggtcagatatccactgacctttggatggtgctacaagctagtaccagttgagccagataaggtagaagaggccaataaaggagagaacaccagcttgttacaccctgtgagcctgcat

gggatggatgacccggagagagaagtgttagagtggaggtttgacagccgcctagcatttcatcacgtggcccgagagctgcatccggagtacttcaagaactgctgatatcgagcttgctacaag

ggactttccgctggggactttccagggaggcgtggcctgggcgggactggggagtggcgagccctcagatcctgcatataagcagctgctttttgcctgtactgggtctctctggttagaccag

atctgagcctgggagctctctggctaactagggaacccactgcttaagcctcaataaagcttgccttgagtgcttcaagtagtgtgtgcccgtctgttgtgtgactctggtaactagagatccctcagac

ccttttagtcagtgtggaaaatctctagcagtggcgcccgaacagggacttgaaagcgaaagggaaaccagaggagctctctcgacgcaggactcggcttgctgaagcgcgcacggcaagagg

cgaggggcggcgactggtgagtacgccaaaaattttgactagcggaggctagaaggagagagatgggtgcgagagcgtcagtattaagcgggggagaattagatcgcgatgggaaaaaattc

ggttaaggccagggggaaagaaaaaatataaattaaaacatatagtatgggcaagcagggagctagaacgattcgcagttaatcctggcctgttagaaacatcagaaggctgtagacaaatactgg

gacagctacaaccatcccttcagacaggatcagaagaacttagatcattatataatacagtagcaaccctctattgtgtgcatcaaaggatagagataaaagacaccaaggaagctttagacaagata

gaggaagagcaaaacaaaagtaagaccaccgcacagcaagcggccgctgatcttcagacctggaggaggagatatgagggacaattggagaagtgaattatataaatataaagtagtaaaaatt

gaaccattaggagtagcacccaccaaggcaaagagaagagtggtgcagagagaaaaaagagcagtgggaataggagctttgttccttgggttcttgggagcagcaggaagcactatgggcgca

gcgtcaatgacgctgacggtacaggccagacaattattgtctggtatagtgcagcagcagaacaatttgctgagggctattgaggcgcaacagcatctgttgcaactcacagtctggggcatcaagc

agctccaggcaagaatcctggctgtggaaagatacctaaaggatcaacagctcctggggatttggggttgctctggaaaactcatttgcaccactgctgtgccttggaatgctagttggagtaataaat

ctctggaacagatttggaatcacacgacctggatggagtgggacagagaaattaacaattacacaagcttaatacactccttaattgaagaatcgcaaaaccagcaagaaaagaatgaacaagaatt

attggaattagataaatgggcaagtttgtggaattggtttaacataacaaattggctgtggtatataaaattattcataatgatagtaggaggcttggtaggtttaagaatagtttttgctgtactttctatag

tgaatagagttaggcagggatattcaccattatcgtttcagacccacctcccaaccccgaggggacccgacaggcccgaaggaatagaagaagaaggtggagagagagacagagacagatccatt

cgattagtgaacggatctcgacggtatcgccgaattcacaaatggcagtattcatccacaattttaaaagaaaaggggggattggggggtacagtgcaggggaaagaatagtagacataatagcaa

cagacatacaaactaaagaattacaaaaacaaattacaaaaattcaaaattttcgggtttattacagggacagcagagatccactttatcgataagcttgggagttccgcgttacataacttacggtaaat

ggcccgcctggctgaccgcccaacgacccccgcccattgacgtcaataatgacgtatgttcccatagtaacgccaatagggactttccattgacgtcaatgggtggaatatttacggtaaactgccc

acttggcagtacatcaagtgtatcatatgccaagtacgccccctattgacgtcaatgacggtaaatggcccgcctggcattatgcccagtacatgaccttacgggactttcctacttggcagtacatc

tacgtattagtcatcgctattaccatggtgatgcggttttggcagtacaccaatgggcgtggatagcggtttgactcacggggatttccaagtctccaccccattgacgtcaatgggagtttgttttggca

ccaaaatcaacgggactttccaaaatgtcgtaacaactccgccccattgacgcaaatgggcggtaggcgtgtacggtgggaggtctata!aagcagagctcgtttagtgaaccg!cagatcgcctg

gagacgccatccacgctgttttgacctccatagaagacaccgactctagctagaggatcccgggctcgagatgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagataca

agtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacatt

ggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacg

acgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggtt

ggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatat

acttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtg

tcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagcc

gctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtg

acatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacaca

ggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgact

tttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaa

gcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagg

gaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacggg

acagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcac

tgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattgg

aaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttgg

agcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagt

gttgatcttcttatccacagccgtctctgctgagaacatcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaagaatcctcacaataccgcagagtctagactcgt

ggtggacttctctcaattttctagggggatotcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgcggc

gttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaaac

ctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggcctca

gtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtccctt

tataccgctgttaccaattttcttttgtctctgggtatacatttaactcgagcccgggatccggactagtaactcgaggcccctctccctcccccccccctaacgttactggccgaagccgcttggaataa

ggccggtgtgcgtttgtctatatgttattttccaccatattgccgtcttttggcaatgtgagggcccggaaacctggccctgtcttcttgacgagcattcctaggggtctttcccctctcgccaaaggaatg

caaggtctgttgaatgtcgtgaaggaagcagttcctctggaagcttcttgaagacaaacaacgtctgtagcgaccctttgcaggcagcggaaccccccacctggcgacaggtgcctctgcggccaa

aagccacgtgtataagatacacctgcaaaggcggcacaaccccagtgccacgttgtgagttggatagttgtggaaagagtcaaatggctctcctcaagcgtattcaacaaggggctgaaggatgcc

cagaaggtaccccattgtatgggatctgatctggggcctcggtacacatgctttacatgtgtttagtcgaggttaaaaaaacgtctaggccccccgaaccacggggacgtggttttcctttgaaaaaca

cgatgataatatggccacaaccttggatgaccgagtacaagcccacggtgcgcctcgccacccgcgacgacgtcccccgggccgtacgcaccctcgccgccgcgttcgccgactaccccgcca

cgcgccacaccgtcgacccggaccgccacatcgagcgggtcaccgagctgcaagaactcttcctcacgcgcgtcgggctcgacatcggcaaggtgtgggtcgcggacgacggcgccgcggt

ggcggtctggaccacgccggagagcgtcgaagcgggggcggtgttcgccgagatcggcccgcgcatggccgagttgagcggttcccggctggccgcgcagcaacagatggaaggcctcct

ggcgccgcaccggcccaaggagcccgcgtggttcctggccaccgtcggcgtctcgcccgaccaccagggcaagggtctgggcagcgccgtcgtgctccccggagtggaggcggccgagcg

cgccggggtgcccgccttcctggagacctccgcgccccgcaacctcccctttctacgagcggctcggcttcaccgtcaccgccgacgtcgaggtgcccgaaggaccgcgcacctggtgcatgac

ccgcaagcccggtgcctgataaggtacctttaagaccaatgacttacaaggcagctgtagatcttagccactttttaaaagaaaaggggggactggaagggctaattcactcccaacgaagacaag

atctttttgcttgtactgggtctctctggttagaccagatctgagcctgggagctctctggctaactagggaacccactgcttaagcctcaataaagcttgccttgagtgcttcaagtagtgtgtgcccgtc

tgttgtgtgactctggtaactagagatccctcagacccttttagtcagtgtggaaaatctctaga

SEQ
ttaattccgtgtattctatagtgtcacctaaatcgtatgtgtatgatacataaggttatgtattaattgtagccgcgttctaacgacaatatgtacaagcctaattgtgtagcatctggcttactgaagcagac

ID
cctatcatctctctcgtaaactgccgtcagagtcggtttggttggacgaaccttctgagtttctggtaacgccgtcccgcacccggaaatggtcagcgaaccaatcagcagggtcatcgctagccagat

NO:
cctctacgccggacgcatcgtggccggcatcaccggcgccacaggtgcggttgctggcgcctatatcgccgacatcaccgatggggaagatcgggctcgccacttcgggctcatgagcgcttgtt

57
tcggcgtgggtatggtggcaggccccgtggccgggggactgttgggcgccatctccttgcatgcaccattccttgcggcggcggtgctcaacggcctcaacctactactgggctgcttcctaatgc

aggagtcgcataagggagagcgtcgaatggtgcactctcagtacaatctgctctgatgccgcatagttaagccagccccgacacccgccaacacccgctgacgcgccctgacgggcttgtctgct

cccggcatccgcttacagacaagctgtgaccgtctccgggagctgcatgtgtcagaggttttcaccgtcatcaccgaaacgcgcgagacgaaagggcctcgtgatacgcctatttttataggttaatg

tcatgataataatggtttcttagacgtcaggtggcacttttcggggaaatgtgcgcggaacccctatttgtttatttttctaaatacattcaaatatgtatccgctcatgagacaataaccctgataaatgctt

caataatattgaaaaaggaagagtatgagtattcaacatttccgtgtcgcccttattcccttttttgcggcattttgccttcctgtttttgctcacccagaaacgctggtgaaagtaaaagatgctgaagatca

gttgggtgcacgagtgggttacatcgaactggatctcaacagcggtaagatccttgagagttttcgccccgaagaacgttttccaatgatgagcacttttaaagttctgctatgtggcgcggtattatcc

cgtattgacgccgggcaagagcaactcggtcgccgcatacactattctcagaatgacttggttgagtactcaccagtcacagaaaagcatcttacggatggcatgacagtaagagaattatgcagtg

ctgccataaccatgagtgataacactgcggccaacttacttctgacaacgatcggaggaccgaaggagctaaccgcttttttgcacaacatgggggatcatgtaactcgccttgatcgttgggaacc

ggagctgaatgaagccataccaaacgacgagcgtgacaccacgatgcctstagcaatggcaacaacgttgcgcaaactattaactggcgaactacttactctagcttcccggcaacaattaataga

ctggatggaggcggataaagttgcaggaccacttctgcgctcggcccttccggctggctggtttattgctgataaatctggagccggtgagcgtgggtctcgcggtatcattgcagcactggggcca

gatggtaagccctcccgtatcgtagttatctacacgacggggagtcaggcaactatggatgaacgaaatagacagatcgctgagataggtgcctcactgattaagcattggtaactgtcagaccaag

tttactcatatatactttagattgatttaaaacttcatttttaatttaaaaggatctaggtgaagatcctttttgataatctcatgaccaaaatcccttaacgtgagttttcgttccactgagcgtcagacccc

gtagaaaagatcaaaggatcttcttgagatcctttttttctgcgcgtaatctgctgcttgcaaacaaaaaaaccaccgctaccagcggtggtttgtttgccggatcaagagctaccaactctttttccgaaggt

aactggcttcagcagagcgcagataccaaatactgtccttctagtgtagccgtagttaggccaccacttcaagaactctgtagcaccgcctacatacctcgctctgctaatcctgttaccagtggctgct

gccagtggcgataagtcgtgtcttaccgggttggactcaagacgatagttaccggataaggcgcagcggtcgggctgaacggggggttcgtgcacacagcccagcttggagcgaacgacctac

accgaactgagatacctacagcgtgagcattgagaaagcgccacgcttcccgaagggagaaaggcggacaggtatccggtaagcggcagggtcggaacaggagagcgcacgagggagctt

ccagggggaaacgcctggtatctttatagtcctgtcgggtttcgccacctctgacttgagcgtcgatttttgtgatgctcgtcaggggggcggagcctatggaaaaacgccagcaacgcggccttttt

acggttcctggccttttgctggccttttgctcacatgttctttcctgcgttatcccctgattctgtggataaccgtattaccgcctttgagtgagctgataccgctcgccgcagccgaacgaccgagcgca

gcgagtcagtgagcgaggaagcggaagagcgcccaatacgcaaaccgcctctccccgcgcgttggccgattcattaatgcagctgtggaatgtgtgtcagttagggtgtggaaagtccccaggc

tccccagcaggcagaagtatgcaaagcatgcatctcaattagtcagcaaccaggtgtggaaagtccccaggctccccagcaggcagaagtatgcaaagcatgcatctcaattagtcagcaaccat

agtcccgcccctaactccgcccatcccgcccctaactccgcccagttccgcccattctccgccccatggctgactaattttttttatttatgcagaggccgaggccgcctcggcctctgagctattccag

aagtagtgaggaggcttttttggaggcctaggcttttgcaaaaagcttggacacaagacaggcttgcgagatatgtttgagaataccactttatcccgcgtcagggagaggcagtgcgtaaaaagac

gcggactcatgtgaaatactggtttttagtgcgccagatctctataatctcgcgcaacctattttcccctcgaacactttttaagccgtagataaacaggctgggacacttcacatgagcgaaaaatacat

cgtcacctgggacatgttgcagatccatgcacgtaaactcgcaagccgactgatgccttctgaacaatggaaaggcattattgccgtaagccgtggcggtctgtaccgggtgcgttactggcgcgtg

aactgggtattcgtcatgtcgataccgtttgtatttccagctacgatcacgacaaccagcgcgagcttaaagtgctgaaacgcgcagaaggcgatggcgaaggcttcatcgttattgatgacctggtg

gataccggtggtactgcggttgcgattcgtgaaatgtatccaaaagcgcactttgtcaccatcttcgcaaaaccggctggtcgtccgctggttgatgactatgttgttgatatcccgcaagatacctgga

ttgaacagccgtgggatatgggcgtcgtattcgtcccgccaatctccggtcgctaatcttttcaacgcctggcactgccgggcgttgttctttttaacttcaggcgggttacaatagtttccagtaagt

attctggaggctgcatccatgacacaggcaaacctgagcgaaaccctgttcaaaccccgctttaaacatcctgaaacctcgacgctagtccgccgctttaatcacggcgcacaaccgcctgtgcagt

cggcccttgatggtaaaaccatccctcactggtatcgcatgattaaccgtctgatgtggatctggcgcggcattgacccacgcgaaatcctcgacgtccaggcacgtattgtgatgagcgatgccga

acgtaccgacgatgatttatacgatacggtgattggctaccgtggcggcaactggatttatgagtgggccccggatctttgtgaaggaaccttacttctgtggtgtgacataattggacaaactacctac

agagatttaaagctctaaggtaaatataaaatttttaagtgtataatgtgttaaactactgattctaattgtttgtgtattttagattccaacctatggaactgatgaatgggagcagtggtggaatgccttta

atgaggaaaacctgttttgctcagaagaaatgccatctagtgatgatgaggctactgctgactctcaacattctactcctccaaaaaagaagagaaaggtagaagaccccaaggactttccttcagaatt

gctaagttttttgagtcatgctgtgtttagtaatagaactcttgcttgctttgctatttacaccacaaaggaaaaagctgcactgctatacaagaaaattatggaaaaatattctgtaacctttataagtaggc

ataacagttataatcataacatactgttttttcttactccacacaggcatagagtgtctgctattaataactatgctcaaaaattgtgtacctttagctttttaatttgtaaaggggttaataaggaatatttg

atgtatagtgccttgactagagatcataatcagccataccacatttgtagaggttttacttgctttaaaaaacctcccacacctccccctgaacctgaaacataaaatgaatgcaattgttgttgttaacttgt

ttattgcagcttataatggttacaaataaagcaatagcatcacaaatttcacaaataaagcatttttttcactgcattctagttgtggtttgtccaaactcatcaatgtatcttatcatgtctggatcaactgg

ataactcaagctaaccaaaatcatcccaaacttcccaccccataccctattaccactgccaattacctagtggtttcatttactctaaacctgtgattcctctgaattattttcattttaaagaaattgtattt

gttaaatatgtactacaaacttagtagttggaagggctaattcactcccaaagaagacaagatatccttgatctgtggatctaccacacacaaggctacttccctgattagcagaactacacaccagggccagg

ggtcagatatccactgacctttggatggtgctacaagctagtaccagttgagccagataaggtagaagaggccaataaaggagagaacaccagcttgttacaccctgtgagcctgcatgggatgga

tgacccggagagagaagtgttagagtggaggtttgacagccgcctagcatttcatcacgtggcccgagagctgcatccggagtacttcaagaactgctgatatcgagcttgctacaagggactttcc

gctggggactttccagggaggcgtggcctgggcgggactggggagtggcgagccctcagatcctgcatataagcagctgctttttgcctgtactgggtctctctggttagaccag

atctgagcctgggagctctctggctaactagggaacccactgcttaagcctcaataaagcttgccttgagtgcttcaagtagtgtgtgcccgtctgttgtgtgactctggtaactagagatccctcagac

ccttttagtcagtgtggaaaatctctagcagtggcgcccgaacagggacttgaaagcgaaagggaaaccagaggagctctctcgacgcaggactcggcttgctgaagcgcgcacggcaagagg

cgaggggcggcgactggtgagtacgccaaaaattttgactagcggaggctagaaggagagagatgggtgcgagagcgtcagtattaagcggggagaattagatcgcgatgggaaaaaattc

ggttaaggccagggggaaagaaaaaatataaattaaaacatatagtatgggcaagcagggagctagaacgattcgcagttaatcctggcctgttagaaacatcagaaggctgtagacaaatactgg

gacagctacaaccatcccttcagacaggatcagaagaacttagatcattatataatacagtagcaaccctctattgtgtgcatcaaaggatagagataaaagacaccaaggaagctttagacaagata

gaggaagagcaaaacaaaagtaagaccaccgcacagcaagcggccgctgatcttcagacctggaggaggagatatgagggacaattggagaagtgaattatataaatataaagtagtaaaaatt

gaaccattaggagtagcacccaccaaggcaaagagaagagtggtgcagagagaaaaaagagcagtgggaataggagctttgttccttgggttcttgggagcagcaggaagcactatgggcgca

gcgtcaatgacgctgacggtacaggccagacaattattgtctggtatagtgcagcagcagaacaatttgctgagggctattgaggcgcaacagcatctgttgcaactcacagtctggggcatcaagc

agctccaggcaagaatcctggctgtggaaagatacctaaaggatcaacagctcctggggatttggggttgctctggaaaactcatttgcaccactgctgtgccttggaatgctagttggagtaataaat

ctctggaacagatttggaatcacacgacctggatggagtgggacagagaaattaacaattacacaagcttaatacactccttaattgaagaatcgcaaaaccagcaagaaaagaatgaacaagaatt

attggaattagataaatgggcaagtttgtggaattggtttaacataacaaattggctgtggtatataaaattattcataatgatagtaggaggcttggtaggtttaagaatagtttttgctgtactttctatag

tgaatagagttaggcagggatattcaccattatcgtttcagacccacctcccaaccccgaggggacccgacaggcccgaaggaatagaagaagaaggtggagagagagacagagacagatccatt

cgattagtgaacggatctcgacggtatcgccgaattcacaaatggcagtattcatccacaattttaaaagaaaaggggggattggggggtacagtgcaggggaaagaatagtagacataatagcaa

cagacatacaaactaaagaattacaaaaacaaattacaaaaattcaaaatt!tcgggtttattacagggacagcagagatccactttatcgataagcttgggagttccgcgttacataacttacggtaaat

ggcccgcctggctgaccgcccaacgacccccgcccattgacgtcaataatgacgtatgttcccatagtaacgccaatagggactttccattgacgtcaatgggtggagtatttacggtaaactgccc

acttggcagtacatcaagtgtatcatatgccaagtacgccccctattgacgtcaatgacggtaaatggcccgcctggcattatgcccagtacatgaccttacgggactttcctacttggcagtacatc

tacgtattagtcatcgctattaccatggtgatgcggttttggcagtacaccaatgggcgtggatagcggtttgactcacggggatttccaagtctccaccccattgacgtcaatgggagtttgttttggca

ccaaaatcaacgggactttccaaaatgtcgtaacaactccgccccattgacgcaaatgggcggtaggcgtgtacggtgggaggtctatataagcagagctcgtttagtgaaccgtcagatcgcctg

gagacgccatccacgctgttttgacctccatagaagacaccgactctagctagaggatcccgggctcgagatgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagataca

agtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacatt

ggggatgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacg

acgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggtt

ggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatat

acttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtg

tcactgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagcc

gctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttctggcaaagggagcctggtg

acatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacaca

ggacatgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgact

tttcagatttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactagaacaacaaagaa

gcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagg

gaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacggg

acagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcac

tgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattgg

aaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttgg

agcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatggatctagaatcctcacaataccgcagagtctagact

cgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctccaatttgtcctggttatcgctggatgtgtctgc

ggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattccaggatcaacaacaaccagtacgggaccatgcaaa

acctgcacgactcctgctcaaggcaactctatgtttccctcatattgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctgggctttcgcaaaatacctatgggagtgggc

ctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtattgggggccaagtctgtacagcatcgtgagtc

cctttataccgctgttaccaattttcttttgtctctgggtatacatttaactcgagcccgggatccggactagtaactcgaggcccctctccctcccccccccctaacgttactggccgaagccgcttgga

ataaggccggtgtgcgtttgtctatatgttattttccaccatattgccgtcttttggcaatgtgagggcccggaaacctggccctgtcttcttgacgagcattcctaggggtctttcccctctcgccaaagg

aatgcaaggtctgttgaatgtcgtgaaggaagcagttcctctggaagcttcttgaagacaaacaacgtctgtagcgaccctttgcaggcagcggaaccccccacctggcgacaggtgcctctgcgg

ccaaaagccacgtgtataagatacacctgcaaaggcggcacaaccccagtgccacgttgtgagttggatagttgtggaaagagtcaaatggctctcctcaagcgtattcaacaaggggctgaagg

atgcccagaaggtaccccattgtatgggatctgatctggggcctcggtacacatgctttacatgtgtttagtcgaggttaaaaaaacgtctaggccccccgaaccacggggacgtggttttcctttgaa

aaacacgatgataatatggccacaaccttggatgaccgagtacaagcccacggtgcgcctcgccacccgcgacgacgtcccccgggccgtacgcaccctcgccgccgcgttcgccgactaccc

cgccacgcgaacaccgtcgacccggaccgccacatcgagcgggtcaccgagctgcaagaactcttcctcacgcgcgtcgggctcgacatcggcaaggtgtgggtcgcggacgacggcgcc

gcggtggcggtctggaccacgccggagagcgtcgaagcgggggcggtgttcgccgagatcggcccgcgcatggccgagttgagcggttcccggctggccgcgcagcaacagatggaaggc

ctcctggcgccgcaccggcccaaggagcccgcgtggttcctggccaccgtcggcgtctcgcccgaccaccagggcaagggtctgggcagcgccgtcgtgctccccggagtggaggcggccg

agcgcgccggggtgcccgccttcctggagacctccgcgccccgcaacctccccttctacgagcggctcggcttcaccgtcaccgccgacgtcgaggtgcccgaaggaccgcgcacctggtgc

atgacccgcaagcccggtgcctgataaggtacctttaagaccaatgacttacaaggcagctgtagatcttagccactttttaaaagaaaaggggggactggaagggctaattcactcccaacgaag

acaagatctttttgcttgtactgggtctctctggttagaccagatctgagcctgggagctctctggctaactagggaacccactgcttaagcctcaataaagcttgccttgagtgcttcaagtagtgtgtg

cccgtctgttgtgtgactctggtaactagagatccctcagacccttttagtcagtgtggaaaatctctaga

SEQ
ttaattccgtgtattctatagtgtcacctaaatcgtatgtgtatgatacataaggttatgtattaattgtagccgcgttctaacgacaatatgtacaagcctaattgtgtagcatctggcttactgaagcagac

ID
cctatcatctctctcgtaaactgccgtcagagtcggtttggttggacgaaccttctgagtttctggtaacgccgtcccgcacccggaaatggtcagcgaaccaatcagcagggtcatcgctagccagat

NO:
cctctacgccggacgcatcgtggccggcatcaccggcgccacaggtgcggttgctggcgcctatatcgccgacatcaccgatggggaagatogggctcgccacttcgggctcatgagcgcttgtt

58
tcggcgtgggtatggtggcaggccccgtggccgggggactgttgggcgccatctccttgcatgcaccattccttgcggcggcggtgctcaacggcctcaacctactactgggctgcttcctaatgc

aggagtcgcataagggagagcgtcgaatggtgcactctcagtacaatctgctctgatgccgcatagttaagccagccccgacacccgccaacacccgctgacgcgccctgacgggcttgtctgct

cccggcatccgcttacagacaagctgtgaccgtctccgggagctgcatgtgtcagaggttttcaccgtcatcaccgaaacgcgcgagacgaaagggcctcgtgatacgcctatttttataggttaatg

tcatgataataatggtttcttagacgtcaggtggcacttttcggggaaatgtgcgcggaacccctatttgtttatttttctaaatacattcaaatatgtatccgctcatgagacaataaccctgataaatgctt

caataatattgaaaaaggaagagtatgagtattcaacatttccgtgtcgcccttattcccttttttgcggcattttgccttcctgtttttgctcacccagaaacgctggtgaaagtaaaagatgctgaagatca

gttgggtgcacgagtgggttacatcgaactggatctcaacagcggtaagatccttgagagttttcgccccgaagaacgttttccaatgatgagcacttttaaagttctgctatgtggcgcggtattatcc

cgtattgacgccgggcaagagcaactcggtcgccgcatacactattctcagaatgacttggttgagtactcaccagtcacagaaaagcatcttacggatggcatgacagtaagagaattatgcagtg

ctgccataaccatgagtgataacactgcggccaacttacttctgacaacgatcggaggaccgaaggagctaaccgcttttttgcacaacatgggggatcatgtaactcgccttgatcgttgggaacc

ggagctgaatgaagccataccaaacgacgagcgtgacaccacgatgcctgtagcaatggcaacaacgttgcgcaaactattaactggcgaactacttactctagcttcccggcaacaattaataga

ctggatggaggcggataaagttgcaggaccacttctgcgctcggcccttccggctggctggtttattgctgataaatctggagccggtgagcgtgggtctcgcggtatcattgcagcactggggcca

gatggtaagccctcccgtatcgtagttatctacacgacggggagtcaggcaactatggatgaacgaaatagacagatcgctgagataggtgcctcactgattaagcattggtaactgtcagaccaag

tttactcatatatactttagattgatttaaaacttcatttttaatttaaaaggatctaggtgaagatcctttttgataatctcatgaccaaaatcccttaacgtgagttttcgttccactgagcgtcagaccc

cgtagaaaagatcaaaggatcttcttgagatcctttttttctgcgcgtaatctgctgcttgcaaacaaaaaaaccaccgctaccagcggtggtttgtttgccggatcaagagctaccaactctttttccgaagg

taactggcttcagcagagcgcagataccaaatactgtccttctagtgtagccgtagttaggccaccacttcaagaactctgtagcaccgcctacatacctcgctctgctaatcctgttaccagtggctgct

gccagtggcgataagtcgtgtcttaccgggttggactcaagacgatagttaccggataaggcgcagcggtcgggctgaacggggggttcgtgcacacagcccagcttggagcgaacgacctac

accgaactgagatacctacagcgtgagcattgagaaagcgccacgcttcccgaagggagaaaggcggacaggtatccggtaagcggcagggtcggaacaggagagcgcacgagggagctt

ccagggggaaacgcctggtatctttatagtcctgtcgggtttcgccacctctgacttgagcgtcgatttttgtgatgctcgtcaggggggcggagcctatggaaaaacgccagcaacgcggccttttt

acggttcctggccttttgctggccttttgctcacatgttctttcctgcgttatcccctgattctgtggataaccgtattaccgcctttgagtgagctgataccgctcgccgcagccgaacgaccgagcgca

gcgagtcagtgagcgaggaagcggaagagcgcccaatacgcaaaccgcctctccccgcgcgttggccgattcattaatgcagctgtggaatgtgtgtcagttagggtgtggaaagtccccaggc

tccccagcaggcagaagtatgcaaagcatgcatctcaattagtcagcaaccaggtgtggaaagtccccaggctccccagcaggcagaagtatgcaaagcatgcatctcaattagtcagcaaccat

agtcccgcccctaactccgcccatcccgcccctaactccgcccagttccgcccattctccgccccatggctgactaattttttttatttatgcagaggccgaggccgcctcggcctctgagctattccag

aagtagtgaggaggcttttttggaggcctaggcttttgcaaaaagcttggacacaagacaggcttgcgagatatgtttgagaataccactttatcccgcgtcagggagaggcagtgcgtaaaaagac

gcggactcatgtgaaatactggtttttagtgcgccagatctctataatctcgcgcaacctattttcccctcgaacactttttaagccgtagataaacaggctgggacacttcacatgagcgaaaaatacat

cgtcacctgggacatgttgcagatccatgcacgtaaactcgcaagccgactgatgccttctgaacaatggaaaggcattattgccgtaagccgtggcggtctgtaccgggtgcgttactggcgcgtg

aactgggtattcgtcatgtcgataccgtttgtatttccagctacgatcacgacaaccagcgcgagcttaaagtgctgaaacgcgcagaaggcgatggcgaaggcttcatcgttattgatgacctggtg

gataccggtggtactgcggttgcgattcgtgaaatgtatccaaaagcgcactttgtcaccatcttcgcaaaaccggctggtcgtccgctggttgatgactatgttgttgatatcccgcaagatacctgga

ttgaacagccgtgggatatgggcgtcgtattcgtcccgccaatctccggtcgctaatcttttcaacgcctggcactgccgggcgttgttctttttaacttcaggcgggttacaatagtttccagtaagt

attctggaggctgcatccatgacacaggcaaacctgagcgaaaccctgttcaaaccccgctttaaacatcctgaaacctcgacgctagtccgccgctttaatcacggcgcacaaccgcctgtgcagt

cggcccttgatggtaaaaccatccctcactggtatcgcatgattaaccgtctgatgtggatctggcgcggcattgacccacgcgaaatcctcgacgtccaggcacgtattgtgatgagcgatgccga

acgtaccgacgatgatttatacgatacggtgattggctaccgtggcggcaactggatttatgagtgggccccggatctttgtgaaggaaccttacttctgtggtgtgacataattggacaaactacctac

agagatttaaagctctaaggtaaatataaaatttttaagtgtataatgtgttaaactactgattctaattgtttgtgtattttagattccaacctatggaactgatgaatgggagcagtggtggaatgccttta

atgaggaaaacctgttttgctcagaagaaatgccatctagtgatgatgaggctactgctgactctcaacattctactcctccaaaaaagaagagaaaggtagaagaccccaaggactttccttcagaatt

gctaagttttttgagtcatgctgtgtttagtaatagaactcttgcttgctttgctatttacaccacaaaggaaaaagctgcactgctatacaagaaaattatggaaaaatattctgtaacctttataagtaggc

ataacagttataatcataacatactgttttttcttactccacacaggcatagagtgtctgctattaataactatgctcaaaaattgtgtacctttagctttttaatttgtaaaggggttaataaggaatatttg

atgtatagtgccttgactagagatcataatcagccataccacatttgtagaggttttacttgctttaaaaaacctcccacacctccccctgaacctgaaacataaaatgaatgcaattgttgttgttaacttgt

ttattgcagcttataatggttacaaataaagcaatagcatcacaaatttcacaaataaagcatttttttcactgcattctagttgtggtttgtccaaactcatcaatgtatcttatcatgtctggatcaactgg

ataactcaagctaaccaaaatcatcccaaacttcccaccccataccctattaccactgccaattacctagtggtttcatttactctaaacctgtgattcctctgaattattttcattttaaagaaattgtattt

gttaaatatgtactacaaacttagtagttggaagggctaattcactcccaaagaagacaagatatccttgatctgtggatctaccacacacaaggctacttccctgattagcagaactacacaccagggccagg

ggtcagatatccactgacctttggatggtgctacaagctagtaccagttgagccagataaggtagaagaggccaataaaggagagaacaccagcttgttacaccctgtgagcctgcatgggatgga

tgacccggagagagaagtgttagagtggaggtttgacagccgcctagcatttcatcacgtggcccgagagctgcatccggagtacttcaagaactgctgatatcgagcttgctacaagggactttcc

gctggggactttccagggaggcgtggcctgggcgggactggggagtggcgagccctcagatcctgcatataagcagctgctttttgcctgtactgggtctctctggttagaccagatctgagcctg

ggagctctctggctaactagggaacccactgcttaagcctcaataaagcttgccttgagtgcttcaagtagtgtgtgcccgtctgttgtgtgactctggtaactagagatccctcagacccttttagtc

agtgtggaaaatctctagcagtggcgcccgaacagggacttgaaagcgaaagggaaaccagaggagctctctcgacgcaggactcggcttgctgaagcgcgcacggcaagaggcgaggggc

ggcgactggtgagtacgccaaaaattttgactagcggaggctagaaggagagagatgggtgcgagagcgtcagtattaagcgggggagaattagatcgcgatgggaaaaaattcggttaaggc

cagggggaaagaaaaaatataaattaaaacatatagtatgggcaagcagggagctagaacgattcgcagttaatcctggcctgttagaaacatcagaaggctgtagacaaatactgggacagctac

aaccatcccttcagacaggatcagaagaacttagatcattatataatacagtagcaaccctctattgtgtgcatcaaaggatagagataaaagacaccaaggaagctttagacaagatagaggaaga

gcaaaacaaaagtaagaccaccgcacagcaagcggccgctgatcttcagacctggaggaggagatatgagggacaattggagaagtgaattatataaatataaagtagtaaaaattgaaccatta

ggagtagcacccaccaaggcaaagagaagagtggtgcagagagaaaaaagagcagtgggaataggagctttgttccttgggttcttgggagcagcaggaagcactatgggcgcagcgtcaatg

acgctgacggtacaggccagacaattattgtctggtatagtgcagcagcagaacaatttgctgagggctattgaggcgcaacagcatctgttgcaactcacagtctggggcatcaagcagctccag

gcaagaatcctggctgtggaaagatacctaaaggatcaacagctcctggggatttggggttgctctggaaaactcatttgcaccactgctgtgocttggaatgctagttggagtaataaatctctggaa

cagatttggaatcacacgacctggatggagtgggacagagaaattaacaattacacaagcttaatacactccttaattgaagaatcgcaaaaccagcaagaaaagaatgaacaagaattattggaatt

agataaatgggcaagtttgtggaattggtttaacataacaaattggctgtggtatataaaattattcataatgatagtaggaggcttggtaggtttaagaatagtttttgctgtactttctatagtgaatag

agttaggcagggatattcaccattatcgtttcagacccacctcccaaccccgaggggacccgacaggcccgaaggaatagaagaagaaggtggagagagagacagagacagatccattcgatt

agtgaacggatctcgacggtatcgccgaattcacaaatggcagtattcatccacaattttaaaagaaaaggggggattggggggtacagtgcaggggaaagaatagtagacataatagcaacaga

catacaaactaaagaattacaaaaacaaattacaaaaattcaaaattttcgggtttattacagggacagcagagatccactttatcgataagcttgggagttccgcgttacataacttacggtaaatggcc

cgcctggctgaccgcccaacgacccccgcccattgacgtcaataatgacgtatgttcccatagtaacgccaatagggactttccattgacgtcaatgggtggagtatttacggtaaactgcccacttg

gcagtacatcaagtgtatcatatgccaagtacgccccctattgacgtcaatgacggtaaatggcccgcctggcattatgcccagtacatgaccttacgggactttcctacttggcagtacatctacgtat

tagtcatcgctattaccatggtgatgcggttttggcagtacaccaatgggcgtggatagcggtttgactcacggggatttccaagtctccaccccaKgacgtcaatgggagtttgttttggcaccaaaa

tcaacgggactttccaaaatgtcgtaacaactccgccccattgacgcaaatgggcggtaggcgtgtacggtgggaggtctatataagcagagctcgtttagtgaaccgtcagatcgcctggagacg

ccatccacgctgttttgacctccatagaagacaccgactctagctagaggatcccgggctcgagatgctgagaataatcaatgctaggaaggagaagaagagacgaggcgcagatacaagtgtc

ggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcatactatatgtacttggacagaaacgatgctggggaggccatatcttttccaaccacattgggga

tgaataagtgttatatacagatcatggatcttggacacacgtgtgatgccaccatgagctatgaatgccctatgctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtca

acttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctgtgacgctcccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatc

aagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgttagcagcagctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttgg

tcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgtggaaggtatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcactg

taatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggtaagatcctactgctatgaggcatcaatatcagacatggcttcggacagccgctgc

ccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgttagtggacagaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatg

cgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtaccggataatgctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggaca

tgaaactgatgagaatagagcgaaagttgagataacgcccaattcaccaagagccgaagccaccctgggggggtttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcag

atttgtattacttgactatgaataacaagcactggctggttcacaaggagtggttccacgacattccattaccttggcacgctggggcagacaccggaactccacactggaacaacaaagaagcact

ggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcacacggcccttgctggagctctggaggctgagatggatggtgcaaagggaag

gctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtactgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagt

cacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgcaaactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaa

gcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcggggagaagaagatcacccaccactggcacaggagtggcagcaccattggaaaag

catttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagttggaggcgctctcaactcattgggcaagggcatccatcaaatctttggagcag

ctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaacgcaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatc

ttcttatccacagccgtctctgctcagtggaattccactgccttccaccaaactctgcaggatcccagagtcaggggtctgtatcttcctgctggtggctccagttcaggaacagtaaaccctgctccga

atattgcctctcacatctcgtcaatctccgcgaggactggggaccctgtgacgaacatggagaacatcacatcaggattcctaggacccctgctcgtgttacaggcggggtttttcttgttgacaagaa

tcctcacaataccgcagagtctagactcgtggtggacttctctcaattttctagggggatctcccgtgtgtcttggccaaaattcgcagtccccaacctccaatcactcaccaacctcctgtcctc

caatttgtcctggttatcgctggatgtgtctgcggcgttttatcatattcctcttcatcctgctgctatgcctcatcttcttattggttcttctggattatcaaggtatgttgcccgtttgtcctctaattcca

ggatcaacaacaaccagtacgggaccatgcaaaacctgcacgactcctgctcaaggcaactctatgtttccctcatgttgctgtacaaaacctacggatggaaattgcacctgtattcccatcccatcgtcctg

ggctttcgcaaaatacctatgggagtgggcctcagtccgtttctcttggctcagtttactagtgccatttgttcagtggttcgtagggctttcccccactgtttggctttcagctatatggatgatgtggtatt

gggggccaagtctgtacagcatcgtgagtccctttataccgctgttaccaattttcttttgtctctgggtatacatttaactcgagcccgggatccggactagtaactcgaggcccctctccctccccccc

ccctaacgttactggccgaagccgcttggaataaggccggtgtgcgtttgtctatatgttattttccaccatattgccgtcttttggcaatgtgagggcccggaaacctggccctgtcttcttgacgagca

ttcctaggggtctttcccctctcgccaaaggaatgcaaggtctgttgaatgtcgtgaaggaagcagttcctctggaagcttcttgaagacaaacaacgtctgtagcgaccctttgcaggcagcggaac

cccccacctggcgacaggtgcctctgcggccaaaagccacgtgtataagatacacctgcaaaggcggcacaaccccagtgccacgttgtgagttggatagttgtggaaagagtcaaatggctctc

ctcaagcgtattcaacaaggggctgaaggatgcccagaaggtaccccattgtatgggatctgatctggggcctcggtacacatgctttacatgtgtttagtcgaggttaaaaaaacgtctaggccccc

cgaaccacggggacgtggttttcctttgaaaaacacgatgataatatggccacaaccttggatgaccgagtacaagcccacggtgcgcctcgccacccgcgacgacgtcccccgggccgtacgc

accctcgccgccgcgttcgccgactaccccgccacgcgccacaccgtcgacccggaccgccacatcgagcgggtcaccgagctgcaagaactcttcctcacgcgcgtcgggctcgacatcgg

caaggtgtgggtcgcggacgacggcgccgcggtggcggtctggaccacgccggagagcgtcgaagcgggggcggtgttcgccgagatcggcccgcgcatggccgagttgagcggttcccg

gctggccgcgcagcaacagatggaaggcctcctggcgccgcaccggcccaaggagcccgcgtggttcctggccaccgtcggcgtctcgcccgaccaccagggcaagggtctgggcagcgc

cgtcgtgctccccggagtggaggcggccgagcgcgccggggtgcccgccttcctggagacctccgcgccccgcaacctccccttctacgagcggctcggcttcaccgtcaccgccgacgtcg

aggtgcccgaaggaccgcgcacctggtgcatgacccgcaagcccggtgcctgataaggtacctttaagaccaatgacttacaaggcagctgtagatcttagccactttttaaaagaaaagggggg

actggaagggctaattcactcccaacgaagacaagatctggtgcttgtactgggtctctctggttagaccagatctgagcctgggagctctctggctaactagggaacccactgcttaagcctcaataa

agcttgccttgagtgcttcaagtagtgtgtgcccgtctgttgtgtgactctggtaactagagatccctcagacccttttagtcagtgtggaaaatctctaga

SEQ
agttgttgatctgtgtgaatcagactgcgacagttcgagtttgaagcgaaagctagcaacagtatcaacaggttttattttggatttggaaacgagagtttctggtcatgaaaaacccaaaaaagaaatc

ID
cggaggattccggattgtcaatatgctaaaacgcggagtagcccgtgtgagcccctttgggggcttgaagaggctgccagccggacttctgctgggtcatgggcccatcaggatggtcttggcgat

NO:
tctagcctttttgagattcacggcaatcaagccatcactgggtctcatcaatagatggggttcagtggggaaaaaagaggctatggaaataataaagaagttcaagaaagatctggctgccatgctga

59
gaataatcaatgctaggaaggagaagaagagacgaggcgcagatactagtgtcggaattgttggcctcctgctgaccacagctatggcagcggaggtcactagacgtgggagtgcatactatatg

tacttggacagaaacgacgctggggaggccatatcttttccaaccacattggggatgaataagtgttatatacagatcatggatcttggacacatgtgtgatgccaccatgagctatgaatgccctatg

ctggatgagggggtggaaccagatgacgtcgattgttggtgcaacacgacgtcaacttgggttgtgtacggaacctgccatcacaaaaaaggtgaagcacggagatctagaagagctgtgacgct

cccctcccattccactaggaagctgcaaacgcggtcgcaaacctggttggaatcaagagaatacacaaagcacttgattagagtcgaaaattggatattcaggaaccctggcttcgcgttagcagca

gctgccatcgcttggcttttgggaagctcaacgagccaaaaagtcatatacttggtcatgatactgctgattgccccggcatacagcatcaggtgcataggagtcagcaatagggactttgtggaagg

tatgtcaggtgggacttgggttgatgttgtcttggaacatggaggttgtgtcaccgtaatggcacaggacaaaccgactgtcgacatagagctggttacaacaacagtcagcaacatggcggaggta

agatcctactgctatgaggcatcaatatcggacatggcttcggacagccgctgcccaacacaaggtgaagcctaccttgacaagcaatcagacactcaatatgtctgcaaaagaacgttagtggac

agaggctggggaaatggatgtggactttttggcaaagggagcctggtgacatgcgctaagtttgcatgctccaagaaaatgaccgggaagagcatccagccagagaatctggagtaccggataat

gctgtcagttcatggctcccagcacagtgggatgatcgttaatgacacaggacatgaaactgatgagaatagagcgaaggttgagataacgcccaattcaccaagagccgaagccaccctgggg

ggttttggaagcctaggacttgattgtgaaccgaggacaggccttgacttttcagatttgtattacttgactatgaataacaagcactggttggttcacaaggagtggttccacgacattccattaccttgg

cacgctggggcagacaccggaactccacactggaacaacaaagaagcactggtagagttcaaggacgcacatgccaaaaggcaaactgtcgtggttctagggagtcaagaaggagcagttcac

acggcccttgctggagctctggaggctgagatggatggtgcaaagggaaggctgtcctctggccacttgaaatgtcgcctgaaaatggataaacttagattgaagggcgtgtcatactccttgtgtac

cgcagcgttcacattcaccaagatcccggctgaaacactgcacgggacagtcacagtggaggtacagtacgcagggacagatggaccttgcaaggttccagctcagatggcggtggacatgca

aactctgaccccagttgggaggttgataaccgctaaccccgtaatcactgaaagcactgagaactctaagatgatgctggaacttgatccaccatttggggactcttacattgtcataggagtcgggg

agaagaagatcacccaccactggcacaggagtggcagcaccattggaaaagcatttgaagccactgtgagaggtgccaagagaatggcagtcttgggagacacagcctgggactttggatcagt

tggaggcgctctcaactcattgggcaagggcatccatcaaatttttggagcagctttcaaatcattgtttggaggaatgtcctggttctcacaaattctcattggaacgttgctgatgtggttgggtctgaa

cacaaagaatggatctatttcccttatgtgcttggccttagggggagtgttgatcttcttatccacagctgtctctgctgatgtggggtgctcggtggacttctcaaagaaggagacgagatgcggtaca

ggggtgttcgtctataacgacgttgaagcctggagggacaggtacaagtaccatcctgactccccccgtagattggcagcagcagtcaagcaagcctgggaagatggtatctgtgggatc

tcctctgtttcaagaatggaaaacatcatgtggagatcagtagaaggggagctcaacgcaatcctggaagagaatggagttcaactgacggtcgttgtgggatctgtaaaaaaccccatgtggaga

ggtccacagagattgcccgtgcctgtgaacgagctgccccacggctggaaggcttgggggaaatcgtacttcgtcagagcagcaaagacaaataacagctttgtcgtggatggtgacacactgaa

ggaatgcccactcaaacatagagcatggaacagctttcttgtggaggatcatgggttcggggtatttcacactagtgtctggctcaaggttagagaagattattcattagagtgtgatccagccgttatt

ggaacagctgttaagggaaaggaggctgtacacagtgatctaggctactggattgagagtgagaagaatgacacatggaggttgaagagggcccatctgatcgagatgaaaacatgtgaatggc

caaagtcccacacattgtggacagatggaatagaagagagtgatctgatcatacccaagtctttagctgggccactcagccatcacaataccagagagggctacaggacccaaatgaaagggcca

tggcacagtgaagagcttgaaattcggtttgaggaatgcccaggcactaaggtccacgtggaggaaacatgtggaacaagaggaccatctctgagatcaaccactgcaagcggaagggtgatcg

aggaatggtgctgcagggagtgcacaatgcccccactgtcgttccgggctaaagatggctgttggtatggaatggagataaggcccaggaaagaaccagaaagtaacttagtaaggtcaatggtg

actgcaggatcaactgatcacatggatcacttctcccttggagtgcttgtgattctgctcatggtgcaggaagggctgaagaagagaatgaccacaaagatcatcataagcacatcgatggcagtgct

ggtagctatgatcctgggaggattttcaatgagtgacctggctaagcttgcaattttgatgggtgccaccttcgcggaaatgaacactggaggagatgtagctcatctggcgctgatagcggcattca

aagtcagaccagcgttgctggtatctttcatcttcagagctaattggacaccccgtgaaagcatgctgctggccttggcctcgtgtcttttgcaaactgcgatctccgccttggaaggcgacctgatggt

tctcatcaatggttttgctttggcctggttggcaatacgagcgatggttgttccacgcactgataacatcaccttggcaatcctggctgctctgacaccactggcccggggcacactgcttgtggcgtgg

agagcaggccttgctacttgcggggggtttatgctcctctctctgaagggaaaaggcagtgtgaagaagaacttaccatttgtcatggccctgggactaaccgctgtgaggctggtcgaccccatca

acgtggtgggactgctgttgctcacaaggagtgggaagcggagctggccccctagcgaagtactcacagctgttggcctgatatgcgcattggctggagggttcgccaaggcagatatagagatg

gctgggcccatggccgcggtcggtctgctaattgtcagttacgtggtctcaggaaagagtgtggacatgtacattgaaagagcaggtgacatcacatgggaaaaagatgcggaagtcactggaaa

cagtccccggctcgatgtggcgctagatgagagtggtgatttctccctggtggaggatgacggtccccccatgagagagatcatactcaaggtggtcctgatgaccatctgtggcatgaacccaata

gccataccctttgcagctggagcgtggtacgtatacgtgaagactggaaaaaggagtggtgctctatgggatgtgcctgctcccaaggaagtaaaaaagggggagaccacagatggagtgtaca

gagtaatgactcgtagactgctaggttcaacacaagttggagtgggagttatgcaagagggggtctttcacactatgtggcacgtcacaaaaggatccgcgctgagaagcggtgaagggagactt

gatccatactggggagatgtcaagcaggatctggtgtcatactgtggtccatggaagctagatgccgcctgggacgggcacagcgaggtgcagctcttggccgtgccccccggagagagagcg

aggaacatccagactctgcccggaatatttaagacaaaggatggggacattggagcggttgcgctggattacccagcaggaacttcaggatctccaatcctagacaagtgtgggagagtgatagg

actttatggcaatggggtcgtgatcaaaaatgggagttatgttagtgccatcacccaagggaggagggaggaagagactcctgttgagtgcttcgagccttcgatgctgaagaagaagcagcta

actgtcttagacttgcatcctggagctgggaaaaccaggagagttcttcctgaaatagtccgtgaagccataaaaacaagactccgtactgtgatcttagctccaaccagggttgtcgctgctgaaatg

gaggaagcccttagagggcttccagtgcgttatatgacaacagcagtcaatgtcacccactctggaacagaaatcgtcgacttaatgtgccatgccaccttcacttcacgtctactacagccaatcag

agtccccaactataatctgtatattatggatgaggcccacttcacagatccctcaagtatagcagcaagaggatacatttcaacaagggttgagatgggcgaggcggctgccatcttcatgaccgcca

cgccaccaggaacccgtgacgcatttccggactccaactcaccaattatggacaccgaagtggaagtcccagagagagcctggagctcaggctttgattgggtgacggatcattctggaaaaaca

gtttggtttgttccaagcgtgaggaacggcaatgagatcgcagcttgtctgacaaaggctggaaaacgggtcatacagctcagcagaaagacttttgagacagagttccagaaaacaaaacatcaa

gagtgggactttgtcgtgacaactgacatttcagagatgggcgccaactttaaagctgaccgtgtcatagattccaggagatgcctaaagccggtcatacttgatggcgagagagtcattctggctgg

acccatgcctgtcacacatgccagcgctgcccagaggagggggcgcataggcaggaatcccaacaaacctggagatgagtatctgtatggaggtgggtgcgcagagactgacgaagaccatg

cacactggcttgaagcaagaatgctccttgacaatatttacctccaagatggcctcatagcctcgctctatcgacctgaggccgacaaagtagcagccattgagggagagttcaagcttaggacgga

gcaaaggaagacctttgtggaactcatgaaaagaggagatcttcctgtttggctggcctatcaggttgcatctgccggaataacctacacagatagaagatggtgctttgatggcacgaccaacaac

accataatggaagacagtgtgccggcagaggtgtggaccagacacggagagaaaagagtgctcaaaccgaggtggatggacgccagagtttgttcagatcatgcggccctgaagtcatttt

aaggagtttgccgctgggaaaagaggagcggcttttggagtgatggaagccctgggaacactgccaggacacatgacagagagattccaggaagccattgacaacctcgctgtgctcatgcggg

cagagactggaagcaggccttacaaagccgcggcggcccaattgccggagaccctagagaccattatgcttttggggttgctgggaacagtctcgctgggaatctttttcgtcttgatgaggaacaa

gggcatagggaagatgggctttggaatggtgactcttggggccagcgcatggctcatgtggctctcggaaattgagccagccagaattgcatgtgtcctcattgttgtgttcctattgctggtggtgct

catacctgagccagaaaagcaaagatctccccaggacaaccaaatggcaatcatcatcatggtagcagtaggtcttctgggcttgattaccgccaatgaactcggatggttggagagaacaaagag

tgacctaagccatctaatgggaaggagagaggagggggcaaccataggattctcaatggacattgacctgcggccagcctcagcttgggccatctatgctgccttgacaactttcattacccca

gccgtccaacatgcagtgaccacttcatacaacaactactccttaatggcgatggccacgcaagctggagtgttgtttggtatgggcaaagggatgccattctacgcatgggactttggagtcccgct

gctaatgataggttgctactcacaattaacacccctgaccctaatagtggccatcattttgctcgtggcgcactacatgtacttgatcccagggctgcaggcagcagctgcgcgtgctgcccagaaga

gaacggcagctggcatcatgaagaaccctgttgtggatggaatagtggtgactgacattgacacaatgacaattgacccccaagtggagaaaaagatgggacaggtgctactcatagcagtagcc

gtctccagcgccatactgtcgcggaccgcctgggggtggggggaggctggggccctgatcacagcggcaacttccactttgtgggaaggctctccgaacaagtactggaactcctctacagcca

cttcactgtgtaacatttttaggggaagttacttggctggagcttctctaatctacacagtaacaagaaacgctggcttggtcaagagacgtgggggtggaacaggagagaccctgggagagaaa

tggaaggcccgcttgaaccagatgtcggccctggagttctactcctacaaaaagtcaggcatcaccgaggtgtgcagagaagaggcccgccgcgccctcaaggacggtgtggcaacgggagg

ccatgctgtgtcccgaggaagtgcaaagctgagatggttggtggagcggggatacctacagccctatggaaaggtcattgatcttggatgtggcagagggggctggagttactacgccgccacca

tccgcaaagttcaagaagtgaaaggatacacaaaaggaggccctggtcatgaagaacccatgttggtgcaaagctatgggtggaacatagtccgtcttaagagtggggtggacgtctttcatatgg

cggctgagccgtgtgacacgttgctgtgtgacataggtgagtcatcatctagtcctgaagtggaagaagcacggacgctcagagtcctctccatggtgggggattggcttgaaaaaagaccagga

gccttttgtataaaagtgttgtgcccatacaccagcactatgatggaaaccctggagcgactgcagcgtaggtatgggggaggactggtcagagtgccactctcccgcaactctacacatgagatgt

actgggtctctggagcgaaaagcaacaccataaaaagtgtgtccaccacgagccagctcctcttggggcgcatggacgggcccaggaggccagtgaaatatgaggaggatgtgaatctcggctc

tggcacgcgggctgtggtaagctgcgctgaagctcccaacatgaagatcattggtaaccgcattgaaaggatccgcagtgagcacgcggaaacgtggttctttgacgagaaccacccatatagga

catgggcttaccatggaagctatgaggcccccacacaagggtcagcgtcctctctaataaacggggttgtcaggctcctgtcaaaaccctgggatgtggtgactggagtcacaggaatagccatga

ccgacaccacaccgtatggtcagcaaagagttttcaaggaaaaagtggacactagggtgccagacccccaagaaggcactcgtcaggttatgagcatggtctcttcctggttgtggaaagagctag

gcaaacacaaacggccacgagtctgtaccaaagaagagttcatcaacaaggttcgtagcaatgcagcattaggggcaatatttgaagaggaaaaagagtggaagactgcagtggaagctgtgaa

cgatccaaggttctgggctctagtggacaaggaaagagagcaccacctgagaggagagtgccagagttgtgtgtacaacatgatgggaaaaagagaaaagaaacaaggggaatttggaaaggc

caagggcagccgcgccatctggtatatgtggctaggggctagatttctagagttcgaagcccttggattcttgaacgaggatcactggatggggagagagaactcaggaggtggtgttgaagggct

gggattacaaagactcggatatgtcctagaagagatgagtcgcataccaggaggaaggatgtatgcagatgacactgctggctgggacacccgcatcagcaggtttgatctggagaatgaagctc

taatcaccaaccaaatggagaaagggcacagggccttggcattggccataatcaagtacacataccaaaacaaagtggtaaaggtccttagaccagctgaaaaagggaagacagttatggacatt

atttcgagacaagaccaaagggggagcggacaagttgtcacttacgctcttaacacatttaccaacctagtggtgcaactcattcggaatatggaggctgaggaagttctagagatgcaagacttgtg

gctgctgcggaggtcagagaaagtgaccaactggttgcagagcaacggatgggataggctcaaacgaatggcagtcagtggagatgattgcgttgtgaagccaattgatgataggtttgcacatg

ccctcaggttcttgaatgatatgggaaaagttaggaaggacacacaagagtggaaaccctcaactggatgggacaactgggaagaagttccgttttgctcccaccacttcaacaagctccatctcaa

ggacgggaggtccattgtggttccctgccgccaccaagatgaactgattggccgggcccgcgtctctccaggggcgggatggagcatccgggagactgcttgcctagcaaaatcatatgcgcaa

atgtggcagctcctttatttccacagaagggacctccgactgatggccaatgccatttgttcatctgtgccagttgactgggttccaactgggagaactacctggtcaatccatggaaagggagaat

ggatgaccactgaagacatgcttgtggtgtggaacagagtgtggattgaggagaacgaccacatggaagacaagaccccagttacgaaatggacagacattccctatttgggaaaaagggaaga

cttgtggtgtggatctctcatagggcacagaccgcgcaccacctgggctgagaacattaaaaacacagtcaacatggtgcgcaggatcataggtgatgaagaaaagtacatggactacctatccac

ccaagttcgctacttgggtgaagaagggtctacacctggagtgctgtaagcaccaatcttagtgttgtcaggcctgctagtcagccacagcttggggaaagctgtgcagcctgtgacccccccagg

agaagctgggaaaccaagcctatagtcaggccgagaacgccatggcacggaagaagccatgctgcctgtgagcccctcagaggacactgagtcaaaaaaccccacgcgcttggaggcgcag

gatgggaaaagaaggtggcgaccttccccacccttcaatctggggcctgaactggagatcagctgtggatctccagaagagggactagtggttagaggagaccccccggaaaacgcaaaacag

catattgacgctgggaaagaccagagactccatgagtttccaccacgctggccgccaggcacagatcgccgaatagcggcggccggtgtggggaaatccatgggtct

The invention will be better illustrated through the following examples and Figures. The examples to follow aim to clarify the object of the invention and illustrate advantageous embodiments, but in no way intend to restrict the range of the invention.

FIGURE LEGEND

FIG. 1 illustrates the wild-type protein S of the HBV, which notably comprises four transmembrane domains, represented by black vertical rectangles; the N and C-terminal ends thereof are oriented towards the light of the endoplasmic reticulum (ER). In the case of the HBVadw isolate, this protein of approximately 45 kD comprises 226 amino acid residues.

FIG. 2A illustrates the wild-type protein M of the HBV, which notably comprises four transmembrane domains, represented by black vertical rectangles; the N and C-terminal ends thereof are oriented towards the light of the endoplasmic reticulum (ER). In the case of the HBVadw isolate, this protein of approximately 33 kD comprises 281 amino acid residues. This FIG. 2A presents a first transmembrane topology of the protein M.

FIG. 2B illustrates the protein M of the HBV, which comprises three transmembrane domains, represented by black vertical triangles; the C-terminal end thereof is oriented towards the light of the endoplasmic reticulum (ER). Unlike FIG. 2A, the N-terminal end is oriented towards the cytosol, and as a result thereof, the first transmembrane domain located on the N-terminal side is represented by a black horizontal rectangle. This FIG. 2B presents a second transmembrane typology of the protein M.

FIG. 3 illustrates the wild-type envelope protein E of the Zika virus, which notably comprises two transmembrane domains, represented by dark gray vertical rectangles; the N-terminal end thereof is in the light of the endoplasmic reticulum (ER), but is oriented towards the cytosol, and the C-terminal end thereof is oriented towards the light of the endoplasmic reticulum (ER). This protein of approximately 54 kD comprises 504 amino acid residues.

FIG. 4 illustrates the wild-type protein prM of the Zika virus, which notably comprises two transmembrane domain, represented by gray vertical rectangles; the N-terminal end thereof is in the light of the endoplasmic reticulum (ER) but is oriented towards the cytosol, and the C-terminal end thereof is oriented towards the light of the endoplasmic reticulum (ER). This protein of approximately 18 kD comprises 164 amino acid residues. The proteolytic cleavage site, allowing the pr portion and the M portion of the protein prM to be cleaved, is also indicated.

FIG. 5 illustrates the configuration of certain proteins of the Zika virus, and notably the configuration of the capsid protein (C), of the protein prM (pr and M) and of the envelope protein E (E) in relation to the membrane.

The capsid protein (C) comprises, on the C-terminal side, a transmembrane domain, represented by a light gray vertical rectangle; the N-terminal end thereof is oriented towards the cytosol.

The proteins E and prM are as described in the legends of FIGS. 3 and 4.

FIG. 6 illustrates the cartography of the synthesis gene allowing the fusion peptides prM+E to be obtained, i.e. a fusion peptide comprising the envelope protein E and the protein prM of Zika. The position of the transmembrane domains of the protein C, of the protein prM and of the envelope protein E is represented by short dark gray arrows.

FIG. 7 illustrates the cartography of the synthesis gene allowing the fusion protein “prM+deleted E+deleted S” to be obtained, i.e. the fusion protein comprising the protein prM, the protein E deleted from a transmembrane domain and the protein S deleted from a transmembrane domain, and notably the fusion protein represented by SEQ ID NO. 8 or SEQ ID NO. 35 or SEQ ID NO. 18 or SEQ ID NO. 43. The position of the transmembrane domains of the protein prM and of the envelope protein E is represented by short arrows (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a dark gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 8 illustrates the transmembrane topology of the fusion protein “prM+deleted E+deleted 5,” i.e. the fusion protein comprising the protein prM, the protein E deleted from a transmembrane domain and the protein S deleted from a transmembrane domain, and notably the fusion protein represented by SEQ ID NO. 8 or SEQ ID NO. 35 or SEQ ID NO. 18 or SEQ ID NO. 43.

FIG. 9 illustrates the cartography of the synthesis gene allowing the fusion protein “prM+E+5” to be obtained, i.e. the fusion protein comprising the protein prM, the protein E and the protein S, and notably the fusion protein represented by SEQ ID NO. 10 or SEQ ID NO. 37 or SEQ ID NO. 20 or SEQ ID NO. 45. The position of the transmembrane domains of the protein prM and the envelope protein E is represented by short arrows (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 10 illustrates the transmembrane topology of the fusion protein “prM+E+5,” i.e. the fusion protein comprising the protein prM, the protein E and the protein S, and notably the fusion protein represented by SEQ ID NO. 10 or SEQ ID NO. 37 or SEQ ID NO. 20 or SEQ ID NO. 45.

FIG. 11 illustrates the cartography of the synthesis gene allowing the fusion protein “prM+E+M” to be obtained, i.e. the fusion protein comprising the protein prM, the protein E and the protein M, and notably the fusion protein represented by SEQ ID NO. 14 or SEQ ID NO. 41 or SEQ ID NO. 24 or SEQ ID NO. 49. The position of the transmembrane domains of the protein prM and of the envelope protein E is represented by short arrows (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 12 illustrates the transmembrane topology of the fusion protein “prM+E+M,” i.e. the fusion protein comprising the protein prM, the protein E and the protein M, and notably the fusion protein represented by SEQ ID NO. 14 or SEQ ID NO. 41 or SEQ ID NO. 24 or SEQ ID NO. 49.

FIG. 13 illustrates the cartography of the synthesis gene allowing the fusion protein “prM+deleted E+M” to be obtained, i.e. the fusion protein comprising the protein prM, the protein E deleted from a transmembrane domain and the protein M, and notably the fusion protein represented by SEQ ID NO. 12 or SEQ ID NO. 39 or SEQ ID NO. 22 or SEQ ID NO. 47. The position of the transmembrane domains of the protein prM and of the envelope protein E is represented by short arrows (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 14 illustrates the transmembrane topology of the fusion protein “prM+deleted E+M,” i.e. the fusion protein comprising the protein prM, the protein E deleted from a transmembrane domain and the protein M, and notably the fusion protein represented by SEQ ID NO. 12 or SEQ ID NO. 39 or SEQ ID NO. 22 or SEQ ID NO. 47.

FIG. 15 illustrates the cartography of the synthesis gene allowing the fusion protein “deleted E+deleted 5” to be obtained, i.e. the fusion protein comprising the protein E deleted from a transmembrane domain and the protein S deleted from a transmembrane domain, and notably the fusion protein represented by SEQ ID NO. 7 or SEQ ID NO. 37 or SEQ ID NO. 17 or SEQ ID NO. 42. The position of the transmembrane domain of the envelope protein E is represented by a short arrow (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 16 illustrates the transmembrane topology of the fusion protein “deleted E+deleted 5,” i.e. the fusion protein comprising the protein E deleted from a transmembrane domain and the protein S deleted from a transmembrane domain, and notably the fusion protein represented by SEQ ID NO. 7 or SEQ ID NO. 34 or SEQ ID NO. 17 or SEQ ID NO. 42.

FIG. 17 illustrates the cartography of the synthesis gene allowing the fusion protein “E+5” to be obtained, i.e. the fusion protein comprising the protein E and the protein S, and notably the fusion protein represented by SEQ ID NO. 9 or SEQ ID NO. 36 or SEQ ID NO. 19 or SEQ ID NO. 44. The position of the two transmembrane domains of the envelope protein E is represented by short arrows (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 18 illustrates the transmembrane topology of the fusion protein “E+S,” i.e. the fusion protein comprising the protein E and the protein S, and notably the fusion protein represented by SEQ ID NO. 9 or SEQ ID NO. 36 or SEQ ID NO. 19 or SEQ ID NO. 44.

FIG. 19 illustrates the cartography of the synthesis gene allowing the fusion protein “E+M” to be obtained, i.e. the fusion protein comprising the protein E and the protein M, and notably the fusion protein represented by SEQ ID NO. 13 or SEQ ID NO. 40 or SEQ ID NO. 23 or SEQ ID NO. 48. The position of the two transmembrane domains of the envelope protein E is represented by short arrows (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 20 illustrates the transmembrane topology of the fusion protein “E+M,” i.e. the fusion protein comprising the protein E and the protein M, and notably the fusion protein represented by SEQ ID NO. 13 or SEQ ID NO. 40 or SEQ ID NO. 23 or SEQ ID NO. 48.

FIG. 21 illustrates the cartography of the synthesis gene allowing the fusion protein “deleted E+M” to be obtained, i.e. the fusion protein comprising the protein E deleted from a transmembrane domain and the protein M, and notably the fusion protein represented by SEQ ID NO. 11 or SEQ ID NO. 38 or SEQ ID NO. 21 or SEQ ID NO. 46. The position of the two transmembrane domains of the envelope protein E is represented by short arrows (indicated by the number 3 and in dark gray). The position of the initiation sequence is represented by a gray rectangle indicated by the number 1 and the position of the transfer initiation peptide is represented by a white arrow indicated by the number 2.

FIG. 22 illustrates the transmembrane topology of the fusion protein “deleted E+M,” i.e. the fusion protein comprising the protein E deleted from a transmembrane domain and the protein M, and notably the fusion protein represented by SEQ ID NO. 11 or SEQ ID NO. 38 or SEQ ID NO. 21 or SEQ ID NO. 46.

FIG. 23 illustrates the immunofluorescence of cells transfected by the RNA transcribed in vitro from the plasmids pSFV1-HBV-S and/or pSFV1-prM+deleted E+deleted S and revealed by an anti-HBV-S antibody (ADRI-2F3) or an anti-Zika antibody (D1-4G2-4-15). In particular, the chimeric protein HBV-Zika-deleted E+deleted S is detected with comparable efficacy either by the antibody recognizing the envelope protein of the Zika virus or by the antibody recognizing the protein HBV-S (line 2). These two fluorescence signals are perfectly co-localized, which shows that the chimeric protein HBV-Zika-deleted E+deleted S is not degraded or cleaved during its expression.

FIG. 24 illustrates the immunofluorescence of cells transfected by the RNA transcribed in vitro from the plasmids pSFV1-HBV-S and/or pSFV1-prM+E+S and revealed by an anti-HBV-S antibody (ADRI-2F3) or an anti-Zika antibody (D1-4G2-4-15). In particular, the chimeric protein HBV-Zika-E+S is detected with comparable efficacy either by the antibody recognizing the envelope protein of the Zika virus or by the antibody recognizing the protein HBV-S. These two fluorescence signals are perfectly co-localized, which shows that the chimeric protein HBV-Zika-E+S is not degraded or cleaved during its expression.

FIG. 25 illustrates a western blot revealed by the anti-Zika antibody D1-4G2-4-15 (A) or the anti-HBV-S antibody 70-HG15 (B), on the lysates of cells transfected by the RNA transcribed in vitro from the plasmids pSFV1-prM+E+S, pSFV1-HBV-S or pSFV3. The lysate CHO-S is used as a positive control. The two glycolized forms of the protein HBV-S (p24 and p27) are specifically detected on the immunoblot incubated with the anti-HBV-S antibody. The chimeric protein HBV-Zika-E+S is specifically detected by the two antibodies, with the expected theoretical size of 80 kDa (p80). This confirms a satisfactory production as well as the integration of the chimeric protein HBV-Zika-E+S, which does not undergo cleavage during its expression.

FIG. 26 illustrates a western blot revealed by the anti-HBV-S antibody (70-HG15) on the lysates of cells transfected by the RNA transcribed from the plasmids pSFV1-prM+deleted E+deleted S and/or pSFV1-HBV-S. The specific detection of the chimeric protein HBV-Zika-deleted E+deleted S with an expected theoretical size of 75 kDa (p75) shows that it is not degraded or cleaved during its expression. The protein HBV-S is also detected in its two glycosylation forms (p24 and p27).

FIG. 27 corresponds to an ELISA analysis (HBV-S detection) of the fractions collected after differential ultracentrifugation of the lysates of the cells expressing the RNA transcribed in vitro from the plasmids pSFV1-prM+E+S and pSFV1-HBV-S. The chimeric particle-enriched fractions 8 and 9 were collected, dialyzed then observed through negative staining (FIGS. 28 and 29).

FIG. 28 corresponds to a transmission electron microscopy observation with negative staining performed on the chimeric particles purified from the co-expression of the RNA transcribed from the plasmids pSFV-1-prM+E+S and pSFV1-HBV-S in BHK-21 cells. These chimeric particles are present in the form of bands and beads characteristic in size and structure of the assembly of the envelope proteins of the HBV (Patient R, Hourioux C, Sizaret P Y, Trassard S, Sureau C, Roingeard P. J Virol. 2007 April; 81(8):3842-51).

FIG. 29 corresponds to a transmission electron microscopy observation with negative staining performed on the chimeric particles purified from the co-expression of the RNA transcribed from the plasmids pSFV-1-prM+E+S and pSFV1-HBV-S in BHK-21 cells. Immunolabeling (immunogold) by the anti-Zika antibody D1-4G2-15 demonstrates the effective incorporation of the chimeric protein HBV-Zika-E+S in the vaccine particles (presence of gold beads at the surface of particles, arrows).

FIG. 30 illustrates a western blot revealed by the anti-HBV-S antibody 70-HG15 on the lysates of CHO-S cells transduced by pHR′^puro-HBV-Zika-prM+E+S, pHR′^puro-HBV-Zika-prM+deleted E+deleted S (clones 1 and 2) and pHR′^puro-HBV-Zika-prM+E+M (clones 1 and 2). The clone CHO-S is used as a positive control.

FIG. 31 illustrates a western blot revealed by the anti-HBV-S antibody 70-HG15 on the supernatants of CHO-S cells transduced by pHR′^puro-HBV-Zika-prM+E+S, pHR′^puro-HBV-Zika-prM+deleted E+deleted S (clones 1 and 2) and pHR′^puro-HBV-Zika-prM+E+M (clones 1 and 2). The clone CHO-S is used as a positive control.

EXAMPLES
Example 1: Stable Production of the Wild-Type Envelope Protein S of Wild-Type HBV-S and of the Chimeric Protein HBV-Zika in Clones of the Cellular Line CHO

Ovary cells of Chinese hamsters (CHO) are stably transduced using a strategy based on the lentiviral expression vector pHR′ (described by Dull et al., A third-generation lentivirus vector with a conditional packaging system, 1998, Journal of Virology, vol. 72, pp 8463-8471). The strategy based on the lentiviral expression vector pHR′ was described in the article Patient et al., Chimeric Hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies, 2009, New Biotechnology, vol. 25, no. 4, pp 226-234.

The DNA sequence of the chimeric HBV-Zika envelope proteins is transferred to the restriction site BamH1 and/or XH01 of the plasmid pHR′^gfp(constructed from the plasmid pHR′ and coding the GFP as a screening marker) to generate the plasmids pHR′^gfp-HBV-Zika. The lentiviruses are produced in the HEK-293T cells (human embryo kidney cells), kept in Dulbecco's Modified Eagle Medium (DMEM).

Twenty-four hours before the transfection, 3×10⁶cells are used to inoculate a culture dish measuring 75 cm²(Falcon®). The cells are transfected with an equimolar mixture (1 pmol of each) of plasmid pHR′^gfP-HBV-Zika, of plasmid pHCMVG (referenced in the ATCC under the reference pHCMV-G (ATCC® 754971) coding the VSV-G (envelope glycoprotein of the vesicular stomatitis virus) and the packaging construction p8.74 through the calcium phosphate method.

The following day, the transfection solution is eliminated and replaced with the fresh complete medium.

After 24 and 48 hours of culture, the supernatant is collected, filtered through a low protein binding filter with pores measuring 0.45 μm (Sartorius) and concentrated through centrifugation on a 20% saccharose cushion at 4° C. for 90 minutes at 100,000×g.

The residue is resuspended in 500 μL of PBS and stored at −80° C. until use.

The transduction unit (TU) titer is determined by quantifying the protein p24 (Innotest® HIV Antigen mAb Kit, Innogenetics).

The clone CHO-S (stably producing the protein HBV-S, previously described in the article Patient et al., Chimeric Hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies, 2009, New Biotechnology, vol. 25, no. 4, pp 226-234), cultivated in the DMEM-F12 (commercialized by Fisher Scientific) is transduced with the recombining lentivectors HRR′^gfp-HBV-Zika.

One day before transduction, 10⁵CHO-S cells/well are used to inoculate a six-well cellular culture plate (Falcon®).

The cells are incubated with the vectors HR′^gfp-HBV-Zika (infection multiplicity: 2.5) and 4 μg/mL of polybrene (Sigma) in the fresh complete medium.

Three days after transduction, the cells are used to inoculate a 96-well cellular culture plate (Falcon®) with a density of 1 cell/well.

The plates are incubated for 3 weeks.

The positive cellular clones of the GFP, named CHO-S+Zika-S or CHO-S+Zika-M are isolated and amplified.

The intracellular production of the proteins HBV-S and chimeric HBV-Zika is analyzed with a western blot of the cellular lysates, as previously described in the article Patient et al., Chimeric Hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies, 2009, New Biotechnology, vol. 25, no. 4, pp 226-234.

The membranes are incubated for one night at 4° C. with a polyclonal rabbit anti-HBsAg antibody (R247) or the monoclonal antibody directed to the Zika envelope protein (4G2).

Example 2: Analysis of the Supernatant of Cells Stably Coproducing the Envelope Proteins HBV-S and Chimeric HBV-Zika

The subviral envelope particles secreted are purified from the supernatant of the cells through gradient centrifugation of cesium chloride (CsCl), as previously described in the article Patient et al., Chimeric Hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies, 2009, New Biotechnology, vol. 25, no. 4, pp 226-234.

To summarize, 200 mL of supernatant are clarified and the total proteins are precipitated through the addition of a 45% solution of (NH₄)₂SO₄(pH 7.5).

The precipitate is collected through centrifugation at 4° C. for 15 minutes at 10,000×g and the residue is dissolved in a minimum volume of Tris-NaCl-EDTA (TNE) pad (10 mM Tris/HCl pH 7.5/100 mM NaCl/1 mM EDTA).

The solution is dialyzed against the TNE pad and cesium chloride is added until a density of 1.22 g/cm³is achieved.

Two successive cycles of isopycnic centrifugation are performed at 15° C. for 24 hours at 40,000 rpm in a 45Ti rotor (Beckman).

The fractions are collected from above and tested for the HBsAg antigen using an ELISA test. The peak fractions are collected and dialyzed at 4° C. against the TNE pad.

The final preparations are analyzed through negative staining electron microscopy and western blot as previously described.

Example 3: Transitory Production of the Wild-Type HBV Envelope Protein S (HBV-S) and the Chimeric HBV-Zika Protein (HBV-Zika-E+S, HBV-Zika-E+M or HBV-Zika-Deleted E+Deleted S) in Clones of the BKH-21 Cellular Line

I.1) Construction of the Plasmids pSFV1-prM+E+S and pSFV1-prM+Deleted E+Deleted S

The vector pSFV1 (Invitrogen) having a bicistronic structure of 11033 pb is used for the following constructions. This vector has a promoter sequence of SP6-ARN polymerase, inserted in 5′ of the first cistron, to initiate the synthesis of a complete RNA with a positive polarity (RNA named 42S(+)) through in-vitro transcription. After transfection into mammal cells, these recombining RNA capped in vitro self-replicate in the presence of the replicase nsP1-4 of the SFV (Semliki Forest Virus) and serve to produce proteins of interest through the intermediate secondary mRNA named 26S(+).

I.1.1) Cloning Sequences of Chimeric Proteins HBV-Zika-prM+E+S and HBV-Zika-prM+Deleted E+Deleted S in the Vector pSFV1

The fragments of hybrid nucleic acid molecules are cloned at the BamHI site of the plasmid pSFV1, previously linearized with this enzyme. The different plasmids comprising the fusion proteins of the invention (notably the plasmids pSFV1-prM+E+S and pSFV1-prM+deleted E+deleted S) are magnified through bacterial transformation, then purified with DNA Maxiprep using phenol/chloroform. The orientation of the insertion is verified through enzyme restriction and all of the constructions are verified through sequencing.

I.2) Obtaining of the Transitorily Transfected Cells by the RNA of Different Constructions Derived from the SFV

The newborn hamster kidney cell (BHK-21) culture procedures as well as the in-vitro transcription protocols of the matrix plasmids SFV and the transfection plasmids of the self-replicating recombining RNA are identical to those previously described [Patient, R., Hourioux, C., Sizaret, P. Y., Trassard, S., Sureau, C., and Roingeard, P., (2007) Hepatitis B Virus Subviral Envelope Particle Morphogenesis and Intracellular Trafficking J Virol, 81(8):3842-51]. The construction pSFV—HBV—S, expressing the wild-type HBV protein S and previously described in the aforementioned article, was used as a control.

I.3) Analysis of the Intracellular Production of the Wild-Type and Chimeric Envelope Proteins

The procedures for the biochemical analysis of the proteins of interest (notably HBV—S, HBV-Zika-E+S and HBV-Zika-deleted E+deleted S, HBV-Zika-E+M, etc.) through confocal microscopy immunofluorescence and western blot, the procedures for the ultrastructural analysis of the transfected cells with transmission electron microscopy as well as the procedures for the quantification (ELISA)/purification (sucrose gradient then dialysis) of the subviral particles of chimeric envelope HBV-Zika (HBV-Zika-E+S, HBV-Zika-deleted E+deleted S, HBV-Zika-E+M) are those previously described [Patient, R., Hourioux, C., Sizaret, P. Y., Trassard, S., Sureau, C., and Roingeard, P., (2007) Hepatitis B Virus Subviral Envelope Particle Morphogenesis and Intracellular Trafficking J Virol, 81(8):3842-51].

The proteins HBV-S, HBV-Zika-E+S, HBV-Zika-deleted E+deleted S were detected with the anti-HBV-S antibody 70-HG15 (interchim), the anti-Zika antibody D1-4G2-15 (millipore) for western blog analyses. The proteins HBV-S, HBV-Zika-E+S, HBV-Zika-deleted E+deleted S were detected with the anti-HBV-S antibody ADRI-2F3 (Cerino A. et al., 2015, 10(4): e0125704) and the anti-Zika antibody D1-4G2-15 for immunofluorescence analyses.

I.4) Analysis of the Culture Supernatant

After transfection, the culture supernatant of approximately 10⁷transfected cells is cleared via centrifugation for 10 minutes at 1500 g then ultracentrifuged at 4° C. for 16 hours at 35,000 rpm using an SW41 rotor (L70 Ultracentrifuge, Beckman). The residue is resuspended with 50 μL of the lysis pad, then analyzed with a western blot.

I.5) Production of the Fusion Proteins HBV-Zika-E+S and HBV-Zika-Deleted E+Deleted S of the Invention

Sixteen hours after the transfection by the SFV RNA comprising the hybrid nucleic acid molecules of the invention and transcribed from the plasmids pSFV1-prM+E+S and pSFV1-prM+deleted E+deleted S, the BHK-21 cells were lysed then analyzed with a western blot using the antibodies D1-4G2-4-15 and 70-HG15. After transitory production in the BHK-21 cell, the size of the fusion proteins HBV-Zika-E+S and HBV-Zika-deleted E+deleted S is detected at around 80 kD for the protein HBV-Zika-E+S and at around 75 kD for the protein HBV-Zika-deleted E+deleted S, i.e. precisely at the sizes corresponding to those theoretically determined. These results show, moreover, that the cleavage between prM and the chimeric proteins is efficacious. Furthermore, the perfect co-localization of the immunofluorescence signals obtained through the detection of said fusion proteins of the invention with the anti-HBV-S antibody ADRI-2F3 and anti-Zika antibody D1-4G2-15 show that they are correctly produced in the cells and do not or only slightly undergo internal cleavage to their sequence after their translation (FIGS. 23, 24, 25A and B and 26).

To restore the secretion abilities of the different fusion proteins of the invention (HBV-Zika-E+S and HBV-Zika-deleted E+deleted S), co-transfections are performed by providing the wild-type form of the protein HBV-S in trans to each of the fusion proteins of the invention (HBV-Zika-E+S and HBV-Zika-deleted E+deleted S). Sixteen hours after the transfection, the co-transfected cells are crushed and the intracellular subviral particles were purified through a sucrose gradient then affinity chromatography [Patient, R., Hourioux, C., Sizaret, P. Y., Trassard, S., Sureau, C., and Roingeard, P., (2007) Hepatitis B Virus Subviral Envelope Particle Morphogenesis and Intracellular Trafficking J Virol, 81(8):3842-51]. After detection through specific ELISA of the protein HBV-S and collection of the fractions enriched in subviral particles (FIG. 27), these particles are studied with a western blot using the anti-HBS antibody (70-HG-15) and electron microscopy with, if necessary, immunodetection using the antibody D1-4G2-1. The antibodies are as previously described in the example 1.3 (FIGS. 26, 28 and 29).

The transmission electron microscopy images show that in all these experiments co-producing the wild-type protein HBV-S with one of the fusion proteins from the invention (HBV-Zika-E+S and HBV-Zika-deleted E+deleted S), it is possible to produce a significant quantity of spherical and filamentous subviral particles (FIG. 28). The western blot analyses show that these more or less filamentous subviral particles are rich in fusion proteins from the invention (HBV-Zika-E+S, HBV-Zika-deleted E+deleted S), which is confirmed, moreover, by the anti-Zika immunostaining (immunogold) specifically observed on the negative stainings presented in FIG. 29.

The implementation of the present invention in an “SFV” system shows that the fusion proteins of the invention (HBV-Zika-E+S and HBV-Zika-deleted E+deleted S) containing nearly all or all of the protein E of the Zika virus gather into chimeric subviral particles of the same type as the subviral particles used in the production of vaccines against hepatitis B, thus facilitating the purification of said chimeric subviral particles from the invention and potentially the development of an industrial application of a vaccine against the Zika virus in perfect harmony with that of the vaccine against the HBV.

Example 4: Obtaining of Subviral Envelope Particles from the Zika Virus in a Lentiviral System

Chinese hamster ovary cells (CHO) are stably transduced using a strategy based on the lentiviral expression vector pHR′ (described by Dull et al., A third-generation lentivirus vector with a conditional packaging system, 1998, Journal of Virology, vol. 72, pp 8463-8471). The strategy based on the lentiviral expression vector pHR′ was described in the article Patient et al., Chimeric Hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies, 2009, New Biotechnology, vol. 25, no. 4, pp 226-234.

The DNA sequence of the chimeric envelope proteins HBV-Zika (prM+E+S, prM+E+M or prM+deleted E+deleted S) is introduced at the restriction site BamH1 of the linearized plasmid pHR,^puro(constructed from the plasmid pHR′, and coding the puromycin as a selection gene) to generate the chimeric plasmids pHR′^puro-HBV-Zika (pHR′^puro-HBV-prM+E+S, pHR′^puro-HBV-prM+deleted E+deleted S and pHR′^puro-HBV-prM+E+M). The lentiviruses are produced in the HEK-293T cells (human embryo kidney cells) and kept in the Dulbecco's Modified Eagle Medium (DMEM).

Twenty-four hours before transfection, 3×10⁶cells are used to inoculate a culture dish measuring 75 cm²(Falcon®). The cells are transfected with an equimolar mixture (1 pmol of each) of chimeric plasmid pHR′Puro_HBV-Zika (pHR′^puro-HBV-prM+E+S, pHR′^puro-HBV-prM+deleted E+deleted S and pHR′^puro-HBV-prM+E+M), of plasmid pHCMVG (referenced in the ATCC under the reference pHCMV-G (ATCC® 754971) coding the VSV-G (envelope glycoprotein of the vesicular stomatitis virus) and the encapsidation construction pCMVR8.74 (Addgene, reference #22036) using the calcium phosphate method.

The following day, the transfection solution is eliminated and replaced by a fresh complete medium.

The residue is resuspended in 500 μL of PBS and stored at −80° C. until use.

The transduction unit (TU) titer is determined by quantifying the protein p24 (Innotest® HIV Antigen mAb Kit, Innogenetics).

The clone CHO-S (stably producing the protein HBV-S, previously described in the article Patient et al., Chimeric Hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies, 2009, New Biotechnology, vol. 25, no. 4, pp 226-234), cultivated in the medium DMEM-F12 (commercialized by Fisher Scientific), is transduced with the recombining lentivectors chimeric HR′^puro-HBV-Zika (obtained from the plasmids pHR′^puro-HBV-prM+E+S, pHR′^puro-HBV-prM+deleted E+deleted S and pHR′^puro-HBV-prM+E+M).

One day before transduction, 10⁵CHO-S cells/well are used to inoculate a six-well cellular culture plate (Falcon®).

The cells are incubated with the vectors chimeric pHR′^puro-HBV-Zika defined above (infection multiplicity: 2.5) and 4 μg/mL of polybrene (Sigma) in the fresh complete medium.

Three days after transduction, the cells are used to inoculate a 96-well cellular culture plate (Falcon®) with a density of 1 cell/well.

The plates are incubated for 3 weeks with puromycin selection (2.5 μg/ml at the end in the culture supernatant).

The cellular clones from the puromycin selection, named CHO-S+Zika-prM+E+S, CHO-S+Zika-prM+deleted E+deleted S or CHO-S+Zika-prM+E+M are isolated and amplified. The expression of HBV-S and chimeric HBV-Zika (HBV-Zika+E+S, HBV-Zika-deleted E+deleted S and HBV-Zika-E+M) is analyzed using immunofluorescence with a human monoclonal anti-HBs antibody and an anti-Zika antibody, as described in example 1.3.

The intracellular production of the proteins HBV-S and chimeric HBV-Zika (HBV-Zika-E+S, HBV-Zika-deleted E+deleted S and HBV-Zika-E+M) is analyzed with a western blot of the cellular lysates, as previously described in the article Patient et al., Chimeric Hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies, 2009, New Biotechnology, vol. 25, no. 4, pp 226-234.

The membranes are incubated for one night at 4° C. with an anti-HBV-S antibody (70-HG15) or the monoclonal antibody directed at the Zika envelope protein (D1-4G2-4-15). The sizes of the fusion proteins HBV-Zika-E+S and HBV-Zika-deleted E+deleted S are approximately 80 kD for the protein HBV-Zika-E+S and approximately 75 kD for the protein HBV-Zika-deleted E+deleted S and 85 kD for the protein HBV-Zika-E+M. These results show, moreover, that the cleavage between prM and the chimeric proteins is efficacious. The protein HBV-S presents two sizes based on its level of glycosylation, one shape of 24 kD (non-glycosylated) and one of 27 kD (glycosylated). These results, correlated with the intense immunofluorescence obtained through the detection of said fusion proteins from the invention with the anti-HBV-S antibody (ADRI-2F3) show that they are correctly produced (FIG. 30).

Example 5: Analysis of the Supernatant of Cells Stably Coproducing the Envelope Proteins HBV-S and Chimeric HBV-Zika (HBV-Zika-E+S, HBV-Zika-E+M or HBV-Zika-Deleted E+Deleted S)

The supernatant is collected, filtered through a low protein binding filter with pores measuring 0.45 μm (Sartorius) and concentrated through centrifugation on a 20% saccharose cushion at 4° C. for 90 minutes at 26,000×g. The residue is resuspended in a minimum volume of PBS then undergoes a western blot analysis. The incubation of the antibody 70-HG15 shows that the chimeric proteins HBV-Zika are detected and consequently have co-assembled with the protein HBV-S into subviral particles (FIG. 31).

Example 6: Analysis of the Intracellular and Extracellular Production of Chimeric Envelope Proteins

The procedures for the biochemical analysis of the proteins of interest (notably HBV-Zika-E+S, HBV-Zika-deleted E+deleted S and HBV-Zika-E+M) through confocal microscopy immunofluorescence and western blot, the procedures for the ultrastructural analysis of the transfected cells with transmission electron microscopy as well as the procedures for the quantification (ELISA)/purification (sucrose gradient then affinity chromatography) of the subviral particles of chimeric envelope HBV-Zika (HBV-Zika-E+S, HBV-Zika-deleted E+deleted S and HBV-Zika-E+M) are evaluated for their reactivity towards anti-Zika envelope antibodies. For example, the antibodies commercialized by Biofront Technologies (http://www.biofronttech.com/), like the antibodies from family 1176 (1176-46, 1176-56, 1176-66, 1176-76, 1176-86), or the antibodies 7E5 or 7G6 are used for qualitative analyses (immunofluorescence, immunomicroscopy, electronic/immunogold), qualitative and semi-qualitative analyses using western blot tests (analysis of the size of the proteins of interest and their production level) and quantitative analysis using a sandwich ELISA test allowing the quantity of proteins of interest secreted in the culture supernatant to be determined. The detection of the dimeric conformation of the protein sequence of the Zika envelope is evaluated through immunofluorescence detection using specific reference antibodies 747(4)B7, 752-2C8, 753(3)C10 and 747(4)A11 commercialized by the company Absolute antibody (http://absoluteantibody.com). The detection of the protein prM in the cells producing the chimeric proteins or in the subviral chimeric envelope particles of chimeric HBV-Zika is notably evaluated with the antibody GTX133305 commercialized by GeneTex (http://www.genetex.com).

Example 7: Immunization Assay in Small Animals and Analysis of the Immune Response

A. Immunization Protocol

Immunizations are performed in GLP conditions (good laboratory practices). The New Zealand rabbits are naïve of all experimental protocols, in particular any previous immunization test. They are young and female, with homogeneous ages and weights. The animals are monitored with a daily clinical examination, monitoring of their mortality and weekly weighing.

Batches of six animals are immunized for each vaccine preparation comprising the chimeric HBV-Zika proteins (HBV-Zika-E+M), HBV-Zika-E+S and HBV-Zika-deleted E+deleted S). A batch of 6 animals is used as a control, 3 animals receiving only the adjuvant and three animals receiving the control vaccine constituted of a commercial anti-HBV vaccine (preparation with only HBV-S protein). The injection is performed subcutaneously with a maximum volume not exceeding 1 ml.

The vaccination schema comprises an initial injection on day 0 (D0) followed by two boosters on days D14 and D28. Three blood samples of at least 5 ml are taken from the animals before each injection; the sample on D0 is used as a negative control before immunization (pre-immune serum).

To complete the study of the immune response development kinetics, samples are taken on D42, D56 and D70. The two animals in each batch that respond best to the anti-Zika and/or anti-HBV-S antibodies receive a fourth vaccine injection on D70, then are exsanguinated on D85.

B. Analyses of the Anti-Zika and Anti-HBV Immune Response Induced in the Small Animal

The analysis of the immune response takes place in vitro using standardized productions of authentic Zika virus. The cross-neutralization with other flaviviruses is measured in the same way with preparations of authentic dengue and West Nile viruses.

1. Production of Standardized Batches of Zika, Dengue and West Nile Viruses on Vero Cells

These three viruses are produced in a BSL3 environment (Biosafety level 3). The Vero line (ATCC® CCL81™) is infected with each of the three viruses and the culture supernatants containing the virus are collected at different times ranging from 3 days (Zika virus), 4 days (West Nile virus) to 7 days for the dengue virus. For example, in the case of the Zika virus, the strain H/PF/2013 (genbank accession number: KJ776791) is used to infect sub confluent cells due to an MOI (multiplicity of infection) of 0.01 in the DMEM deprived of fetal bovine serum (FBS). After 24 h, the culture mediums are replaced by a complete nutritive medium (notably comprising 10% FBS). After 3 days of culture, the supernatants of these cells are collected, then clarified with centrifugation at 300×g, and finally possibly ultracentrifuged on a saccharose gradient. The viral titers are determined with the cellular method (determination of the viral dose infecting 50% of the cellular tissues; TCID5₀), according to the method described by Spearman-Karber (Kärber, G. Archiv f. experiment. Pathol. u. Pharmakol. 1931; 162: 480), possibly completed with a specific quantitative method Q-RT-PCR.

2. Kinetics Analysis of the Reactivity of the Antibodies Induced in the Small Animal.

The serums of the animals before and after immunization are dosed with the ELISA method to determine their reactivity to the Zika virus. For this, the ELISA anti-Zika virus test kit (IgA/IgG/IgM), commercialized by EUROIMMUN (euroimmun.com) is used to immunocapture anti-Zika antibodies in rabbits, which are then revealed using an anti-rabbit antibody coupled with peroxidase. The colorimetric revelation and the reading of the optical density (OD) allow the evolution of this anti-Zika response to be compared over time (D14 and D28, D42, D56, D70). The pre-immune serums as well as the serums of animals vaccinated only with the adjuvant or the anti-HBV commercial specialty are used as controls.

All of the rabbit serums are also dosed for their anti-HBV reactivity. This is achieved using the commercial anti-HBs Architect System kit (Abbott laboratories).

3. Analysis of the Neutralizing Ability of the Antibodies Induced in the Small Animal Against the Zika Virus Infection

Vero cells naïve of all infection are inoculated 24 h before infection onto a 96-well plate at 2×10³cells/well. Before infection, serum dilutions (e.g. ⅕, 1/25, 1/125, 1/625 and 1/3125) are incubated with constant virus quantities (1×10³) produced according to paragraph 1 for one hour at 37° C. These serum+virus mixtures are then deposited on the naïve Vero cells and then cultured for 72 h. For each of the infection conditions with virus+serum dilution mixtures, the effective infection of the cell layer is measured through visual determination of the cytopathogenic effect (presence of cell lysis plaques). The results of three independent experiments are then considered to determine the neutralization percentage. This neutralization percentage, determined for each serum dilution, is defined according to the following method: 100% neutralization is determined when no lysis plaque is detected in any of the wells for a single dilution; 50% neutralization corresponds to the identification of lysis plaques in 50% of the wells. When all of the wells present lysis plaques, the neutralization percentage is 0%. For these experiments, different controls are implemented, like virus pre-incubation in the presence of pre-immune serums, virus pre-incubation with the serums of rabbits immunized only with the adjuvant and infection of the cell layer with the virus in the absence of pre-incubation with rabbit serums.

Number	Name	Date	Kind
8765143	Roingeard et al.	Jul 2014	B2
20110150921	Roingeard	Jun 2011	A1

Fusion proteins and use thereof for preparing vaccines

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Cox et al. Predicting Zika virus structural biology: Challenges and opportunities for intervention. Antiviral Chemistry and Chemotherapy 2015, vol. 24(3-4) 118-126.
B. D. Cox et al: “Predicting Zika virus structural biology: Challenges and opportunities for intervention”, Antiviral Chemistry & Chemotherapy., vol. 24, No. 3-4, Aug. 1, 2015 (Aug. 1, 2015), GB, pp. 118-126, XP055328128, ISSN: 0956-3202, DOI: 10.1177/2040206616653873.
International Search Report, dated Sep. 27, 2017, from corresponding PCT/FR2017/051591 application.
FR Search Report, dated Dec. 22, 2016, from corresponding FR 1655677 application.