Claims
- 1. A method of recovering a nucleic acid encoding a proteinaceous binding domain, the method comprising:
providing a variegated population of filamentous phage, each phage including a proteinaceous potential binding domain and a nucleic acid construct comprising a nucleic acid sequence that encodes it, wherein each phage physically associates the potential binding domain with the particular nucleic acid sequence that encodes it, the [encoded] potential binding domains differing through the at least partially random variegation of one or more predetermined amino acid positions of a parental binding domain; contacting the phage with a target material such that the potential binding domain and the particular DNA molecule which encodes it remain physically associated, and such that the potential binding domains and the target material may interact; isolating at least one binding domain that binds to the target material; and recovering the particular nucleic acid construct that was physically associated with the at least one isolated binding domain during the contacting, wherein the parental binding domain comprises an antibody domain, and at least one of said variegated amino acid positions is within a hypervariable region of the antibody domain.
- 2. The method of claim 1 wherein the variegation excludes cysteines.
- 3. The method of claim 1 wherein the parental binding domain is a domain of a naturally occurring protein.
- 4. The method of claim 1 wherein the parental binding domain is a non-naturally occurring domain which substantially corresponds in sequence to a naturally occurring domain.
- 5. The method of claim 4 wherein the parental binding domain differs from the corresponding naturally occurring domain in sequence by one or more substitutions, insertions, or deletions.
- 6. The method of claim 1 wherein the parental binding domain substantially corresponds in sequence to a hybrid of subsequences of two or more naturally occurring proteins.
- 7. The method of claim 1 wherein the recovering comprises removing the at least one isolated binding domain from the filamentous phage that physically associated the at least one isolated binding domain with the particular nucleic acid construct that encodes it during the contacting.
- 8. A method of recovering a nucleic acid encoding a binding domain, the method comprising:
providing a variegated population of filamentous phage, each phage including a potential binding domain that comprises an antibody domain and a nucleic acid construct comprising a nucleic acid sequence that encodes the potential binding domain, wherein each phage physically associates each potential binding domain with the particular nucleic acid sequence that encodes the potential binding domain, the encoded potential binding domains differ from one another through the at least partially random variation of one or more predetermined amino acids corresponding to a hypervariable region, and the random variation of at least one of the predetermined amino acid positions is by random selection of the codon encoding the amino acid at said position from a set of codons, the set being characterized by one or more of the following properties:
(a) the set includes at least one codon for each of at least two different amino acids other than cysteine, and excludes all codons encoding cysteine, (b) the set provides a single codon for each encoded amino acid, and (c) the amino acids encoded by the set are represented at substantially equal frequency; contacting the phage with a predetermined target material such that the potential binding domains and the target material may interact while each potential binding domain and the particular DNA molecule which encodes it remain physically associated; isolating a binding domain that binds to the target material; and recovering the particular nucleic acid construct that was physically associated with the isolated binding domain during the contacting.
- 9. The method of claim 8 wherein the set excludes all codons encoding cysteine.
- 10. The method of claim 8 wherein the set provides a single codon for each encoded amino acid.
- 11. The method of claim 8 wherein the amino acids encoded by the set are represented at substantially equal frequency.
- 12. The method of claim 8 wherein the set is characterized by all three properties, (a), (b), and (c).
- 13. A process for determining a binding property of a proteinaceous domain, the process comprising:
mutagenizing a gene encoding an antibody domain to form a gene encoding a potential binding domain, wherein at least one codon encoding an amino acid in a hypervariable region is mutagenized; displaying the potential binding domain on the outer surface of an amplifiable genetic package, wherein said amplifiable genetic package is a filamentous bacteriophage that contains the gene encoding said potential binding domain, contacting the package with the target material, and determining whether the package displaying the potential binding domain binds to said target material.
- 14. The process of claim 13 wherein the at least one codon is a codon selected from a set of codons, the set excluding all codons encoding cysteine.
- 15. A method of isolating a binding protein, the method comprising:
preparing a variegated population of filamentous phage, each phage including a nucleic acid construct that encodes a chimeric protein that comprises a potential binding domain and a polypeptide encoded by a filamentous phage gene VIII or a filamentous phage gene III, the encoded potential binding domains differ through the at least partially random variation of one or more predetermined amino acid positions of a parental binding domain; expressing the potential binding domains encoded by the nucleic acid constructs of the phage population; and isolating at least one phage from the population, the isolated phage including a nucleic acid construct that encodes a potential binding domain that binds to the target material with at least a predetermined affinity; and recovering the nucleic acid construct from the isolated phage.
- 16. The method of claim 15 wherein the chimeric protein comprises a potential binding domain and a mature filamentous phage gene VIII protein.
- 17. The method of claim 15 wherein the chimeric protein comprises a potential binding domain and a mature filamentous phage gene III protein.
Priority Claims (1)
Number |
Date |
Country |
Kind |
PCT/US89/03731 |
Sep 1989 |
WO |
|
CROSS-REFERENCE TO RELATED APPLICATIONS
[0001] This application is a continuation-in-part of Ladner, Guterman, Roberts, and Markland, Ser. No. 07/487,063, filed Mar. 2, 1990, now pending, which is a continuation-in-part of Ladner and Guterman, Ser. No. 07/240,160, filed Sep. 2, 1988, now pending. Ser. No. 07/487,063 claimed priority under 35 U.S.C. 119 from PCT Application No. PCT/US89/03731, filed Sep. 1, 1989. All of the foregoing applications are hereby incorporated by reference.
[0002] The following related and commonly-owned applications are also incorporated by reference:
[0003] Robert Charles Ladner, Sonia Kosow Guterman, Rachael Baribault Kent, and Arthur Charles Ley are named as joint inventors on U.S. Ser. No. 07/293,980, filed Jan. 8, 1989, and entitled GENERATION AND SELECTION OF NOVEL DNA-BINDING PROTEINS AND POLYPEPTIDES. This application has been assigned to Protein Engineering Corporation.
[0004] Robert Charles Ladner, Sonia Kosow Guterman, and Bruce Lindsay Roberts are named as a joint inventors on a U.S. Ser. No. 07/470,651 filed Jan. 26, 1990, entitled “PRODUCTION OF NOVEL SEQUENCE-SPECIFIC DNA-ALTERING ENZYMES”, likewise assigned to Protein Engineering Corp.
[0005] Ladner, Guterman, Kent, Ley, and Markland, Ser. No. 07/558,011 is also assigned to Protein Engineering Corporation.
Divisions (1)
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07664989 |
Mar 1991 |
US |
Child |
08009319 |
Jan 1993 |
US |
Continuations (3)
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08993776 |
Dec 1997 |
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10126544 |
Apr 2002 |
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08415922 |
Apr 1995 |
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08993776 |
Dec 1997 |
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08009319 |
Jan 1993 |
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08415922 |
Apr 1995 |
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Continuation in Parts (2)
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07487063 |
Mar 1990 |
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07664989 |
Mar 1991 |
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07240160 |
Sep 1988 |
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07487063 |
Mar 1990 |
US |