Sodium ion-driven chloride /bi-carbonate exchanger

FIELD OF THE INVENTION

The present invention relates to human and mouse Na

+

-driven Cl—/HCO

3

— exchanger (sodium ion-driven chloride/bicarbonate exchanger) proteins, which are a class of proteins involved in intracellular pH regulation. More specifically, the present invention relates to sodium ion-driven chloride/bicarbonate exchanger proteins, cells designed to express one of the proteins, which cells are of a species different from the origin of the one of the proteins expressed, DNAs encoding the proteins, antibodies to the proteins, and a method for selecting agonists/antagonists of the sodium ion-driven chloride/bicarbonate exchanger proteins.

BACKGROUND OF THE INVENTION

Regulation of intracellular pH (pH

i

) in response to various stimuli is a critical one among a number of cellular functions. A family of bicarbonate transporters is a major pH

i

regulator under physiological conditions in animal cells. Bicarbonate (HCO

3

—) transporters are divided into four groups according to their functions [Boron, W. F. et al., J. Exp. Biol., 200:263-268(1997)]: Na

+

-independent Cl—/HCO

3

— exchanger (alternatively called an anion exchanger, AE), Na

+

—HCO

3

— cotransporter (NBC), K

+

—HCO

3

— cotransporter, and Na

+

-driven Cl—/HCO

3

— exchanger. Three AEs and three NBCs have been cloned and functionally characterized, but the molecular structure of the K

+

—HCO

3

— cotransporter and the Na

+

-driven Cl—/HCO

3

— exchanger have remained unknown.

A Na

+

-driven Cl—/HCO

3

— exchanger was first discovered in invertebrate neurons and was later found in vertebrate neurons as well as non-neuronal cells, including brain, vascular endothelial cells, sperm, kidney and pancreatic β-cells. Na

+

-driven Cl—/HCO

3

— exchanger is an intracellular pH regulator that transports extracellular Na

+

and HCO

3

— into the cells in exchange for intracellular Cl—, thereby playing an important role in cellular alkalinization.

In pancreatic β-cells, glucose is the most important physiological regulator of insulin secretion. Glucose metabolism induces an increase in intracellular pH in the pancreatic cells. It has been shown that this glucose-induced pH

i

rise is evoked primarily by the action of Na

+

-driven Cl—/HCO

3

— exchanger [Pace, C. S. et al., J. Membrane Biol., 73:39-43(1983)].

Na

+

-driven Cl—/HCO

3

— exchanger is thus an important intracellular pH regulator in various cells, but its molecular basis is not known. Analysis of the molecular structure and function of Na

+

-driven Cl—/HCO

3

— exchanger should be valuable not only for functional analysis of insulin secretion by pancreatic β-cells but also for screening as well as for drug designing based on its molecular structure aimed at the development of therapeutics of diabetes mellitus.

On the above background, the present invention has as its objective to clone Na

+

-driven Cl—/HCO

3

— exchangers, thereby obtaining their DNA for sequencing, providing cells of a different species expressing the DNAs, and determining the structure and function of the Na

+

-driven Cl—/HCO

3

— exchangers.

SUMMARY OF THE INVENTION

Thus, the present invention provides a Na

+

-driven Cl—/HCO

3

— exchanger protein comprising the amino acid sequence set forth as SEQ ID NO:2 or NO:4 in the Sequence Listing.

The present invention further provides a protein comprising an amino acid sequence having deletion, substitution, addition or insertion of one or more amino acids relative to the amino acid sequence set forth as SEQ ID NO:2 or NO:4 in the Sequence Listing and which, when expressed in a cell, functions as Na

+

-driven Cl—/HCO

3

— exchanger.

The present invention further provides an above protein wherein the Na

+

-driven Cl—/HCO

3

— exchanger, dependently upon both of extracellular bicarbonate and intracellular chloride ions, takes up extracellular sodium ion into the cell and transport intracellular sodium ion out of the cell.

The present invention further provides a cell in which one of the above proteins is expressed, wherein the cell is of a species different from the species of origin of the one of the proteins. Non-limiting examples of such cells of different species include

Xenopus laevis

oocytes and HEK293 cells. Expression of a Na

+

-driven Cl—/HCO

3

— exchanger in such cells of different species may be achieved by transfection of a DNA encoding the Na

+

-driven Cl—/HCO

3

— exchanger or by introduction of a cRNA corresponding to the Na

+

-driven Cl—/HCO

3

— exchanger.

The present invention further provides antibodies to the above proteins. The antibodies may be monoclonal or polyclonal.

The present invention further provides a method for selection of agonists and antagonists of Na

+

-driven Cl—/HCO

3

— exchanger, which method comprises bringing a cell of a different species expressing the protein into contact with a candidate compound, measuring the function of the Na

+

-driven Cl—/HCO

3

— exchanger, comparing the result thus obtained with a result obtained by measuring the function of the sodium ion-driven chloride/bicarbonate exchanger of the cell which has not been brought into contact with the candidate compound, and thereby determining whether or not the candidate compound enhances or inhibits the function.

The present invention further provides a DNA comprising the nucleotide sequence set forth as SEQ ID NO:1 or NO:3 in the Sequence Listing, a DNA >2 comprising a nucleotide sequence consisting of nucleotides 67 through 3330 in the nucleotide sequence set forth as SEQ ID NO:1 in the Sequence Listing, and a DNA comprising a nucleotide sequence consisting of the nucleotides 83 through 3346 in the nucleotide sequence set forth as SEQ ID NO:3 in the Sequence Listing.

The present invention further provides a DNA comprising a nucleotide sequence having deletion, substitution, addition or insertion of one or more nucleotides relative to a DNA comprising a nucleotide sequence consisting of the nucleotides 67 through 3330 in the nucleotide sequence set forth as SEQ ID NO:1 in the Sequence Listing, and encoding:

(1) a protein comprising the amino acid sequence set forth as SEQ ID NO:2 in the Sequence Listing, or

(2) a protein comprising an amino acid sequence having deletion, substitution, addition or insertion of one or more amino acids relative to the amino acid sequence set forth as SEQ ID NO:2 in the Sequence Listing, which protein, when expressed in a cell, functions as Na

+

-driven Cl—/HCO

3

— exchanger.

The present invention still further provides a DNA comprising a nucleotide sequence having deletion, substitution, addition or insertion of one or more nucleotides relative to a DNA comprising a nucleotide sequence consisting of the nucleotides 83 through 3346 in the nucleotide sequence set forth as SEQ ID NO:3 in the Sequence Listing, and encoding:

(1) a protein comprising the amino acid sequence set forth as SEQ ID NO:4 in the Sequence Listing, or

(2) a protein comprising an amino acid sequence having deletion, substitution, addition or insertion of one or more amino acids relative to the amino acid sequence set forth as SEQ ID NO:4 in the Sequence Listing, which protein, when expressed in a cell, functions as Na

+

-driven Cl—/HCO

3

— exchanger.

BRIEF DESCRIPTION OF THE FIGURES

FIG. 1

shows RNA blot analysis of NCBE mRNA in rat tissues and hormone-secreting cell lines (a) and RT-PCR detection of NCBE mRNA from mouse pancreatic islets (b).

FIG. 2

shows a graph illustrating the effect of extracellular Na

+

concentration on

22

Na

+

uptake.

FIG. 3

shows a graph illustrating the effect of extracellular HCO

3

concentration on

22

Na

+

uptake.

FIG. 4

shows a graph illustrating the effect of intracellular Cl— on

36

Cl— efflux.

FIG. 5

shows a graph illustrating the effect of DIDS on

22

Na

+

uptake.

FIG. 6

shows a graph illustrating the change in the intracellular pH in the presence and absence of 300 μM DIDS, along with the change in the intracellular pH in control (non-transfected) cells.

FIG. 7

shows a graph illustrating the change observed in the intracellular pH when the environment is switched from a Na

+

-free solution to a Na

+

-containing solution, under a HCO

3—

-free condition.

FIG. 8

shows a graph illustrating the change observed in the intracellular pH when the environment is switched from a Na

+

-free solution to a Na

+

-containing solution, under a Cl—-free condition.

DETAILED DESCRIPTION OF THE INVENTION

In the present invention, the cells of different species in which the protein of the present invention is expressed may be, for example,

Xenopus laevis

oocytes or HEK293 cells, and selected according to a given purpose from a variety of cells other than those from mouse or human. A conventional method well known in the art may be used for bringing about expression of a protein of the present invention in cells of species different from the species of origin of the protein.

In the present specification, the term “one or more” when used in the context of “an amino acid sequence having deletion, substitution, addition or insertion of one or more amino acids” means a number of one to ten in general, and preferably a number of one to a few (e.g., three or four).

Also in the present specification, the term “one or more” when used in the context of “a DNA comprising a nucleotide sequence having deletion, substitution, addition or insertion of one or more nucleotides” means a number of one to ten in general, and preferably a number of one to a few (e.g., three or four).

A variety of such mutant DNAs, as well as mutant proteins encoded by the DNAs, can be produced by means of recombinant DNA technology. First, mutations can be introduced into a cloned DNA fragment through any of different chemical or enzymatic processes. Mutant DNAs thus obtained are then sequenced for selection of particular mutants with intended merits. This method allows systematic preparation of different mutants regardless of their phenotypes. General methods for preparing mutant clones are as follows.

1. With the help of an oligonucleotide, substitution, deletion, insertion or addition of one or more nucleotides can be directly induced in a given DNA sequence. This method allows introduction of a number of mutations into a small region of a given DNA.

2. By using a relatively long oligonucleotide, a desired gene can be synthesized.

3. By means of region-specific mutagenesis, a desired mutation can be introduced into a large (1-3 kb) DNA region.

4. Linker-scanning mutagenesis of DNA is a method suitable to introduce a cluster point mutation into a relatively small (4-10 bp) DNA region.

5. PCR is also utilized as a method for directly introducing a mutation. [References: Current protocols in molecular biology. 3 vols., Edited by Ausubel F. M. et al., John Wiley & Sons, Inc., Current Protocols., Vol. 1, Chapter 8: Mutagenesis of cloned DNA, pages 8.0.1-8.5.10]

Also well known to those skilled in the art are methods for preparing plasmids or other vectors which can express a desired gene including different mutations obtained by the above methods. That is, by inserting a DNA comprising a desired gene into an expression vector DNA using a combination of restriction enzymes and a ligase, a recombinant plasmid is readily constructed which carries the desired gene. The recombinant plasmid thus obtained is then introduced into different cells to effect transfection, thereby producing transformed cells. A range of cells may be utilized, from prokaryotic cells, e.g.

E. coli,

to yeast, insect, plant and animal cells.

[Reference: Vectors essential data. Gacesa P. and Ramji D. P. 166 pages. BIOS Scientific Publishers Limited 1994., John Wiley & Sons in association with BIOS Scientific Publishers Ltd. Expression vectors, pages 9-12.]

Introduction of a recombinant plasmid into host cells may be carried out by calcium chloride method or by electroporation. Calcium chloride method is an efficient way for achieving transformation and it does not requires any apparatus specially designed for it. If still higher efficiency is needed, electroporation is recommended.

[References: Current Protocols in Molecular Biology, 3 Vols. Edited by Ausbel F. M. et al., John Wiley & Sons, Inc., Current Protocols, Vol. 1, unit 1.8: Introduction of Plasmid DNA into Cells, pages 1.8.1-1.8.10]

There are known two types of transfection generally carried out on animal cell lines, i.e., a transient type and a stable and permanent type. In transient transfection, transformed cells are cultured for 1-4 days to allow transcription and replication of the introduced gene, and then the cells are harvested and their DNA analyzed. In many studies, alternatively, a stable transformant cell line is produced, in which the introduced gene is incorporated into the chromosomes. Examples of the method for transfection include calcium phosphate method, electroporation, and liposome fusion method. [Reference: Current protocols in molecular biology. 3 vols. Edited by Ausubel F. M. et al., John Wiley & Son, Inc., Current Protocols. Vol. 1, chapter 9: Introduction of DNA into mammalian cells, pages 9.0.1-9.17.3.]

Polyclonal and monoclonal antibodies to the Na

+

-driven Cl—/HCO

3

— exchanger proteins of the present invention, or to their fragments or their analogues, are readily prepared using technologies well known in the art. Antibodies thus obtained may be used, for example, in immunohistochemistry of Na

+

-driven Cl—/HCO

3

— exchanger protein expressed in cells of different species or for inhibition of its function by blocking the protein. Cells of different species in which the function of Na

+

-driven Cl—/HCO

3

— exchanger is inhibited are used as a control in selection of agonists/antagonists of the protein.

A general method for preparing a monoclonal antibody in mg-scale directed to the Na

+

-driven Cl—/HCO

3

— exchanger proteins of the present invention is as follows: Mice are inoculated with one of the antigen proteins to immunize. The spleen is removed from the mice exhibiting a sufficient antibody titer. The spleen cells are dissociated and B cells are selected and fused with myeloma cells of B cell origin to form hybridoma cells secreting the antibody. The monoclonal antibody secreted by the hybridoma cells is purified from the culture medium by using an affinity column, or by ion-exchange or gel filtration, etc. Polyclonal antibody of the present invention may also be prepared by a conventional method: using rabbits, horses, mice or guinea pigs as immunized animals, the antigen protein is inoculated along one of the schedules known in the art to immunize the animals, and then an immunoglobulin such as IgG is isolated from the collected serum.

[Reference: Current protocols in molecular biology, 3 vols. Edited by Ausubel F. M. et al., John Wiley & Sons, Inc., Current Protocols, Vol. 2, chapter 11: Immunology, pages 11.0.1-11.16.13.]

EXAMPLES

The present invention is described in further details with reference to examples. However, it is not intended that the present invention be limited to the examples.

To determine its structure and functional role, the present inventors cloned a Na

+

-driven Cl—/HCO

3

— exchanger (designated NCBE) from cDNA library from MIN6, an insulin secreting mouse cell line. The primary structure, tissue distribution and functional characterization of Na

+

-driven chloride (Cl—)/bicarbonate (HCO

3

—) exchanger (NCBE) will be described below.

It was revealed that the mouse NCBE protein (SEQ ID NO:2) consists of 1,088 amino acids and has 65, 65 and 41% amino acid identity to the sodium bicarbonate cotransporter from human muscle, retina and kidney, respectively. The mouse NCBE has was found to have ten putative membrane spanning regions and the conserved 4,4′-diisothiocyanostilbene-2,2′-disulfonic acid (DIDS)-binding motif characteristic of anion exchangers and sodium bicarbonate cotransporters. NCBE mRNA is was shown to be expressed at high levels in the brain and in a mouse insulinoma cell line MIN6, and, though at low levels, also in pituitary, testis, kidney, and ileum. Through functional analysis of NCBE protein expressed in

Xenopus laevis

oocytes and HEK293 cells, it was demonstrated that the protein causes a rise in intracellular pH by transporting extracellular Na

+

and HCO

3

— into cells in exchange for intracellular Cl—. Based on the findings, the present inventors concluded that the cloned NCBE is the Na

+

-driven Cl—/HCO

3

— exchanger that regulates intracellular pH in native cells.

Then, to also identify a human NCBE, a partial sequence (2,746 bp) of the mouse Na

+

-driven Cl—/HCO

3

— exchanger cDNA obtained above was first amplified by PCR. For this amplification, a DNA fragment having the sequence consisting of the nucleotides 250-270 of the sequence set forth as SEQ ID NO:1 in the Sequence Listing was used as a sense primer, and, as an antisense primer, a DNA fragment having a sequence complementary to the sequence consisting of the nucleotides 2976-2995 of the sequence set forth as SEQ ID NO:1 in the Sequence Listing. PCR conditions were as follows:

Initial denaturation:94° C., 2 min

Amplification (20 cycles)

denaturation:94° C., 15 sec

annealing:60° C., 30 sec

extension:72° C., 2 min

Final extension:72° C., 7 min

The PCR product thus obtained was labeled with

32

P-dCTP by nick translation and used to screen about 1 million phages from a human fetal brain cDNA library (Clontech). Four positive phage clones were obtained and their DNAs were digested with EcoRI. After agarose electrophoresis, corresponding bands were excised, and respective DNAs extracted to obtain inserts. Separately, pGEM7Z (Promega) was digested with EcoRI and treated with alkaline phosphatase. To this, the inserts obtained from the positive phages were ligated, respectively, for subcloning. The respective inserts were then sequenced on an autosequencer (ABI 310), and, based on the sequences thus obtained, the cDNA nucleotide sequence corresponding to human NCBE protein was determined (set forth as SEQ ID NO:3). According to the result, the sequence of human NCBE protein then was determined (set forth as SEQ ID NO:4 in the Sequence Listing).

The methods and results of the above experiments will be described below, focusing on the procedures followed and results obtained with mouse NCBE.

[Materials and Methods]

<cDNA Cloning>

A partial cDNA fragment of human kidney NBC cDNA [Burnham, C. E., et al., J. Biol. Chem., 272:19111-19114(1997)] amplified by PCR, using a human kidney cDNA as a template. The sense and antisense primers used in this were 5′-TTTGGAGAAAACCCCTGGT-3′ (nt 2232-2250) (SEQ ID NO:5) and 5′-TGACATCATCCAGGAAGCTG-3′ (nt 2912-2931) (SEQ ID NO:6). PCR was performed up to 40 cycles under the following conditions: denaturation at 94° C. for 15 sec, annealing at 60° C. for 30 sec, and extension at 72° C. for 45 sec in a thermal cycler GeneAmp PCR system 9600 (PE Applied Biosystems, Foster, Calif.). The 700 bp-PCR product was subjected to screening of a MIN6 cDNA library [Inagaki, N., et al., Proc. Natl. Acad. Sci. USA, 91:2679-2683(1994)] as a probe under a low stringent condition previously described [Fukumoto, H. et al., Proc. Natl. Acad. Sci. USA, 85:5434-5438(1988)]. Positive clones were subcloned in pGEM-3Z vector (Promega, Madison, Wis.) and sequenced in both directions using ABI PRISM ™ 377 DNA sequencer (PE Applied Biosystems).

<RNA blot analysis>

RNA blot analysis was performed using 10 μg of total RNA from various tissues and cells. The RNAs were denatured with formaldehyde, electrophoresed on 1% agarose gel, and transferred onto a nylon membrane. The blots were probed with NCBE cDNA under a standard condition previously described [Wang, C -Z. et al., Biochem. Biophys. Res. Commun., 220: 196-202(1996)]. Before autoradiography, the blots were washed with 0.1×SSC and 0.1% SDS at room temperature for one hr and then at 50° C. for another hour.

Reverse Transcription Polymerase Chain Reaction (RT-PCR)

Total RNA was prepared from isolated mouse pancreatic islets with TRIZOL Reagent (Life Technologies, Inc., Rockvill, Md.). First-strand cDNA (10 ng) was generated using Superscript™ II reverse transcriptase (Life Technologies) with random primers. PCR was performed with Expand High Fidelity PCR System (Roch Diagnostics, Mannheim, Germany) using about 1 ng of template DNA in a 20 μl reaction volume under a standard condition. The sense and antisense primers used were 5′-GTCATGTTAGACCAACAGGT-3′ (nt 4283-4302) (SEQ ID NO:7) and 5′-GTTGTAATAGCGACACTC-3′ (nt 4911-4928) (SEQ ID NO:8). The PCR product was resolved on 1% agarose gel and confirmed by DNA sequencing.

Functional Analysis of NCBE in

Xenopus laevis

oocytes

The coding sequence of NCBE in pSD5 was linearized by digestion with FspI and in vitro transcribed with SP6 RNA polymerase as previously described (Wang, C -Z. et al., Biochem. Biophys. Res. Commun., 220:196-202(1996)). Defolliculated oocytes were injected with NCBE cRNA (50 nl, 0.5 μg/μl) or water and incubated in 1×MBS medium (88 mM NaCl, 1 mM KCl, 0.8 mM MgCl

2

, 0.4 mM CaCl

2

, 0.3 mM Ca(NO

3

)

2

, 2.4 mM NaHCO

3

and 7.5 mM Tris, pH 7.4) for 3-5 days at 18° C. before the studies. The oocytes were preincubated for one hr at 18° C. in the standard solution (100 mM NaCl, 2 mM KCl, 1 mM MgCl

2

, 1 mM CaCl

2

, and 8 mM NaHCO

3

, pH 7.4).

For studies of dependency on extracellular Na

+

concentration, the oocytes were then incubated in 1.4 ml of either 1, 10, 30 or 100 mM Na

+

solution bubbled with 1.5% CO

2

, pH 7.4 with 0.074 MBq of

22

Na+ (NEN™ Life Science Products, Boston, Mass.). In each solution, the Na

+

in the standard solution was substituted with an equal molar amount of choline. A ten μl aliquot was removed from the incubation solution for later determination of

22

Na

+

-specific activity. After 15 min,

22

Na

+

uptake was terminated by three washes with an ice-cold solution containing 1, 10, 30 or 100 mM Na

+

, pH 7.4, respectively, and the oocytes were then lyzed in 0.5 ml of 5% SDS and 4.5 ml of Aqueous Counting Scintillant (Amersham Pharmacia Biotech) was added.

22

Na

+

uptake was performed in either Cl—-free 1, 10, 30 or 100 mM Na

+

solution (pH 7.4). Extracellular Cl— was substituted with an equal molar amount of gluconic acid, and extracellular Na

+

was substituted with an equal molar amount of N-methyl-D-glucamine (NMG). The

22

Na

+

uptake for 15 min was also examined in the presence or absence of 300 μM 4,4′-diisothiocyanostilbene-2,2′-disulfonic acid (DIDS, Sigma), an inhibitor of anion-transporters in the standard solution.

For the study of dependency on extracellular HCO

3

— concentration, Na

+

uptake experiments were performed in 1, 3, 10 or 30 mM HCO

3

— solutions bubbled with 1.5% CO

2

at 18° C., pH 7.4, including 0.074 MBq of

22

Na

+

. The solutions contained 2 mM KCl, 1 mM MgCl

2

and 1 mM CaCl

2

, pH 7.4, and further 107 mM NaCl and 1 mM NaHCO

3

for 1 mM HCO

3

— solution, 105 mM NaCl and 3 mM NaHCO

3

for 3 mM HCO

3

— solution, 98 mM NaCl and 10 mM NaHCO

3

for 10 mM HCO

3

— solution, and 78 mM NaCl and 30 mM NaHCO

3

for 30 mM HCO

3

— solution.

For

36

Cl— efflux experiment, the oocytes were preincubated for one hour in the Cl—-free solution for depletion of intracellular Cl—, or Cl— containing standard solution. The oocytes were incubated in 0.074 MBq of

36

Cl—-containing solution (NEN™ Life Science Products) at 18° C. for one hour bubbling with 1.5% CO

2

. The oocytes were rapidly washed three times with the corresponding, respective solutions and then transferred into 1.5 ml of each a Cl—-free solution bubbled with 1.5% CO

2

, pH 7.4. A 10-μl aliquot was removed from the incubation solution for later determination of

36

Cl— specific activity.

36

Cl— activities in the solution were measured at 0, 5, 15, 25 and 35 min. The oocytes were treated as described above for the measurement of the remaining intracellular

36

Cl—. Portions of the medium from respective time points were counted and the values were summed to determine flux.

36

C— efflux was presented as a percent relative to the total cellular

36

Cl— released.

22

Na

+

and

36

Cl— activities were measured with beta scintillation counter (Aloka, Japan).

<Functional Analysis of NCBE in HEK293 Cells>

HEK293 cells were plated at a density of 3×10

5

cells per 3.5 cm-diameter dish containing a coverslip, and cultured in Dulbecco's modified Eagle's medium (DMEM, high glucose) supplemented with 10% fetal bovine serum, streptomycin (60.5 μg/ml), and penicillin (100 μg/ml) at 37° C. under a humidified condition of 95% air and 5% CO

2

. Cells were transfected with 1 μg of the full-length NCBE cDNA in the pcDNA3.1 vector (Invitrogen, Groningen, The Netherlands) using Lipofectamine, Lipofectamine Plus, and Opti-MEM I reagents (Life Technologies, Gaithersburg, Md.) according to the manufacturer's instructions. The cells were studied 48-72 hours after transfection. Changes in intracellular pH were monitored using 2′,7′-bis-(2-carboxyethyl)-5-(6)-carboxyfluorescein, acetoxymethyl ester (BCECF-AM, Molecular Probe, Eugene, Oreg.) (Burnham, C. E., et al., J. Biol. Chem., 272:19111-19114(1997)). HEK293 cells were loaded with 1 μM BCECF-AM for one hour and monitored for changes in intracellular pH by dual-excitation wavelength method with a computerized image processor (490 nm/450 nm; 520-560 nm emission) (Argus-50; Hamamatsu Photonics, Hamamatsu, Japan). ΔpH

i

was determined as the difference between the intracellular pH before and 10 min after switching to the test solution. The pH

i

calibration curve was generated using KCl/nigericin technique (Thomas, J. A. et al., Biochemistry 18:2210-2218(1979)). In all the experiments, the cells were first acidified by NH

4

+

-prepulse with 40 mM NH

4

Cl-containing solution for 5 min before switching to the Na

+

-containing respective test solutions (Burnham, C. E., et al., J. Biol. Chem., 272:19111-19114(1997)).

To estimate Na

+

-dependency of the intracellular pH (ΔpH

i

) recovery from intracellular acidification, a Na

+

-free solution (115 mM tetramethylammonium chloride (TMA-Cl), 25 mM KHCO

3

, 0.8 mM K

2

HPO

4

, 0.2 mM KH

2

PO

4

, 1 mM CaCl

2

, 1 mM MgCl

2

, 10 mM HEPES) and a Na

+

-containing solution (TMA-Cl and KHCO

3

in the Na

+

-free solution were replaced with 90 mM NaCl, 25 mM KCl, and 25 mM NaHCO

3

) were used.

To test for HCO—-dependency, a HCO

3

—-free, Na

+

-free solution (115 mM TMA-Cl, 0.8 mM K

2

HPO

4

, 0.2 mM KH

2

PO

4

, 1 mM CaCl

2

, 1 mM MgCl

2

, 10 mM HEPES) and a HCO

3

—-free, Na

+

-containing solution (in which TMA-Cl in the HCO

3

—-free, Na

+

-free solution was replaced with 90 mM NaCl and 25 mM KCl) were used.

To determine Cl—-dependency, a Cl—-free, Na

+

-free solution (25 mM KHCO

3

, 0.8 mM K

2

HPO

4

, 0.2 mM KH

2

PO

4

, 10 mM HEPES, 115 mM NMG-gluconate) and a Cl—-free, Na

+

-containing solution (in which NMG-gluconate was replaced with 115 mM sodium gluconate) were used and the results were compared with each other.

All the solutions were bubbled with 95% O

2

and 5% CO

2

, and their pH adjusted to 7.4. The osmolarity of each solution was adjusted with sucrose. The assays were carried out at 37° C.

<Statistical Analysis>

The results were expressed as means ± SE. Statistical significance between experiments was determined by Student's t test.

[Results and Discussion]

NCBE is structurally related to Na

+

—HCO

3

— transporters.

As described above, the cDNA encoding Na

+

-driven Cl—/HCO

3

— exchanger (NCBE) was cloned from a MIN6 cDNA by screening it using a partial human kidney Na

+

—HCO

3

— cotransporter (NBC) cDNA as a probe. The thus determined nucleotide sequence (NCBE) is set forth as SEQ ID NO:1 in the Sequence Listing. The composite 5,385-bp nucleotide sequence contains an open reading frame, which follows an in-frame termination signal upstream of the “ATG” and encodes a protein of 1,088 amino acids set forth as SEQ ID NO:1 having a predicted molecular weight of 122 kDa. A hydrophobicity analysis indicates that the amino acid sequence has putative membrane spanning segments (TM1 to TM10) at the following positions, respectively.

TM 1: amino acids 479˜499

TM2: amino acids 514˜534

TM3: amino acids 564˜584

TM4: amino acids 693˜713

TM5: amino acids 733˜753

TM6: amino acids 780˜800

TM7: amino acids 826˜846

TM8: amino acids 882˜901

TM9: amino acids 905˜924

TM10: amino acids 972˜992

In the amino acid sequence, there are three potential N-linked glycosylation sites in the extracellular loops between the third (TM3) and fourth (TM4) spanning region (Asn-647, Asn-657 and Asn-667). Putative DIDS-binding motif is at amino acids 815-818.

Comparison of amino acid sequence between NCBE and other NBCs showed that NCBE has 65%, 65% and 41% amino acid identity to human muscle NBC [Pushkin, A. et al., J. Biol. Chem., 274:16569-16575(1999)], human retina NBC [Ishibashi, K. et al., Biochem. Biophys. Res. Commun., 24:535-538(1998)], and human kidney NBC [Burnham, C. E., et al., J. Biol. Chem., 272:19111-19114(1997)], respectively. This indicates that NCBE represents a novel bicarbonate transporter. The amino acid sequences in the putative transmembrane regions and DIDS-binding motif Lys Leu Lys Lys (residue 815-818) are well conserved in NCBE, while those in the intracellular amino- and carboxyl-terminal regions and in the large extracellular loop between the third and the fourth membrane spanning regions are rather divergent.

NCBE is expressed at high levels in the brain and insulin-secreting clonal pancreatic β-cells.

RNA blot analysis revealed a 5.5 kb NCBE mRNA is expressed at high levels in brain and the insulin secreting cell line MIN6 cells and expressed at low levels in pituitary, testis, kidney, and ileum (

FIG. 1

,

a

). RT-PCR analysis shows that NCBE is also expressed in pancreatic islets (

FIG. 1

,

b

).

In the figure, “a” represents the result of the RNA blot analysis of NCBE mRNA in rat tissues and hormone-secreting cell lines. The size of hybridized transcripts is indicated. “b” represents the results of RT-PCR detection of NCBE mRNA in mouse pancreatic islets. DNA length markers and RT-PCR products are shown in lanes

1

and

2

, respectively.

NCBE is a Na

+

-driven Cl—/HCO

3

— exchanger that regulates intracellular pH (pH

i

).

The present inventors examined the functional properties of NCBE using

Xenopus laevis

oocyte system.

22

Na

+

uptake and

36

Cl— efflux were measured 3-5 days after injection of the cRNAs or water (control). Bubbling with 1.5% CO

2

to acidify the oocytes, the present inventors first examined the effect of extracellular Na

+

concentration on

22

Na

+

uptake. The results are shown in FIG.

3

.

FIG. 3

illustrates the relation between

22

Na

+

uptake (nmol/oocyte/hour) and extracellular Na

+

concentration. In the figure, ▪ and &Circlesolid; indicate the results obtained with the cells injected with NCBE cRNA, and □ and ◯ the results obtained with the cells injected with water. ▪ and □ indicate the results obtained using Cl—-containing extracellular solutions, and &Circlesolid; and ◯ indicate the results obtained using Cl—-free extracellular solutions. The respective data represent the mean ±SE (standard error) for 7 to 16 oocytes from two independent experiments. * and † (p<0.05) indicate the presence/absence of statistical significance in the difference from water-injected cells and from incubation in Cl—-free extracellular solutions, respectively, with 10, 30 or 100 mM Na

+

.

As shown in

FIG. 2

, the increase in

22

Na

+

uptake was dependent on extracellular Na

+

concentrations, with a linear pattern observed in NCBE cRNA-injected oocytes over the physiological range of Na

+

concentrations. The water-injected oocytes showed no increase in

22

Na

+

uptake. Comparison of Na

+

uptake between the results obtained with Cl—-containing and Cl—-free solutions showed significantly higher Na

+

uptake in the presence of extracellular Cl— than the in the absence of extracellular Cl— (FIG.

2

). These results indicate that NCBE transports extracellular Na

+

into the cells and that extracellular Cl— participates in acceleration of the NCBE's activity.

The present inventors, then, examined the effect of extracellular bicarbonate ion on

22

Na

+

uptake. The results are shown in FIG.

3

. The respective data represent the mean±SE (standard error) for 11 to 16 oocytes from two independent experiments. * (p<0.05) indicates comparison with water-injected cells. As evident from the figure, increased extracellular bicarbonate ion significantly boosted Na

+

uptake in a concentration-dependent manner in the NCBE cRNA-injected oocytes, while the water-injected oocytes did not show any such change in Na

+

uptake. These results indicate that extracellular bicarbonate ion is necessary in transporting Na

+

into the cells.

To determine whether Cl— is transported into or out of the cells by NCBE, the present inventors examined

36

Cl— efflux from

Xenopus laevis

oocytes. As

36

Cl— influx was not detected in water-injected oocytes, analysis was made only for

36

Cl— efflux from NCBE cRNA-injected oocytes. The rate (%) of

36

Cl— efflux from NCBE cRNA-injected oocytes was measured from 0 to 35 min under the intracellular Cl—-depleted condition by preincubation with a Cl—-free solution and under the intracellular Cl— non-depleted condition by preincubation with Cl—-containing solution. The results are shown in FIG.

4

. In the figure, &Circlesolid; indicates the results obtained with cells under the intracellular Cl— non-depleted condition (preincubation in the Cl—-containing solution), and ▴ indicates the results obtained with cells under the intracellular Cl—-depleted condition (preincubation in the Cl—-free solution). The data represent the mean ±SE (standard error) for 16 to 17 oocytes from three independent experiments. * (p<0.05) indicates comparison with intracellular Cl—-depleted cells, at 5, 15, 25, and 35 min.

Comparison made among results of

36

Cl— efflux under the different conditions indicates that NCBE transports intracellular Cl— out of the cells. Taken together, these results demonstrate that NCBE exchanges extracellular Na

+

and bicarbonate ion with intracellular Cl—.

The present inventors also examined the effect of DIDS, an inhibitor of anion-transporter, on

22

Na

+

uptake. Expression was assessed in the absence or presence of 0.3 mM DIDS. The results are shown in FIG.

5

. The data represent the mean ±SE (standard error) for 21 to 22 oocytes from three independent experiments. * (p<0.05) indicates comparison with cRNA+DIDS.

While the

22

Na

+

uptake in NCBE cRNA-injected oocytes was 31.4±2.1 nmol/oocyte/hour (n=21) in the absence of DIDS, it was 6.0±0.7 nmol/oocyte/hour (n=14) in the presence of 300 μM DIDS. In water-injected oocytes, the uptake was 1.6±0.3 (n=22) and 2.1±0.4 (n=19) nmol/oocytes/hour in the absence and presence of DIDS, respectively. Thus, DIDS was shown to partially inhibit

22

Na

+

uptake by NCBE (FIG.

5

).

To clarify the role of NCBE in the regulation of intracellular pH, changes in intracellular pH were measured under various conditions using HEK293 cells transiently transfected with NCBE. All the experiments were performed under conditions where the intracellular pH was acidified with NH

4

+prepulse. To determine whether the change in the intracellular pH is dependent on extracellular Na

+

, the environment of the cells was switched from a Na

+

-free solution to a Na

+

-containing solution. The results are shown in FIG.

6

.

FIG. 6

is a graph illustrates a trace of control (non-transfected) cells and NCBE-transfected cells with or without 300 μM DIDS. The environment of the cells was switched from a Na

+

-free solution to a Na

+

-containing solution.

As shown in the figure, a rapid recovery of intracellular pH (ΔpH

i

) was observed only in the NCBE-transfected cells in the presence of 1 mM 5-(N-ethyl-N-isopropyl)-amiloride (EIPA), a specific inhibitor of Na

+

/H+exchanger (ΔpH

i

was 0.239±0.028 (n=97) in the NCBE-transfected cells and 0.003±0.015 (n=70) in the control. p<0.05) (FIG.

6

). This recovery in intracellular pH was partially inhibited by 300 μM DIDS (ΔpH

i

was 0.023±0.042 (n=89). p<0.05).

To determine whether this change in intracellular pH is bicarbonate ion-dependent, the environment of the NCBE-transfected cells was switched from a HCO

3

—-free, Na

+

-free solution to a HCO

3

—-free but Na

+

-containing solution, in the presence of 1 mM EIPA. However, as shown in

FIG. 7

, no recovery of intracellular pH was detected (ΔpH

i

was 0.002±0.014 (n=71)).

Finally, an examination for Cl— dependency was also made by the present inventors. NCBE-transfected cells were kept in a Cl—-free solution (under an intracellular Cl—-depletion condition) throughout the experiments. Under this condition, the environment of the cells was switched from a Na

+

-free solution to a Na

+

-containing solution. In the presence of 1 mM EIPA, as shown in

FIG. 8

, no recovery of intracellular pH was detected [ΔpH, was 0.067±0.012 (n=95)].

These results indicate that recovery of intracellular pH from intracellular acidification is detected only where extracellular Na

+

and HCO

3

— and intracellular Cl— are present.

The studies of the function of NCBE heterologously expressed in

Xenopus laevis

oocytes and HEK293 cells show that NCBE allows intracellular pH to recover from acute intracellular acidification, by transporting extracellular Na

+

and HCO

3

— in exchange for intracellular Cl— (FIGS.

3

and

4

). NCBE is functionally distinct from so far reported anion exchangers and Na

+

—HCO

3

— cotransporters. This is because: 1) NCBE, expressed in

Xenopus laevis,

exhibited a Na

+

uptake increase dependent on intracellular Cl—, 2) it shows the ability of exporting Cl— out of the cells, and, furthermore, 3) the NCBE, expressed in HEK239 cells, elevates intracellular pH in a manner dependent upon extracellular Na

+

and HCO

3

—, and intracellular Cl—. These properties are similar to those of Na

+

-driven Cl—/HCO

3

— exchanger described in native cells. The cloned NCBE, therefore, is concluded to be a Na

+

-driven Cl—/HCO

3

— exchanger.

Possible physiological relevance of NCBE. That NCBE mRNA is expressed in insulin secreting cell line MIN6 and pancreatic islets implies its physiological relevance. It has been shown that glucose-induced insulin secretion is accompanied by a rise in intracellular pH in pancreatic β-cells. While several intracellular pH regulators have been suggested to be present in pancreatic β-cells, their molecular basis has not been known so far. NCBE is the first intracellular pH-regulating exchanger whose primary structure and functional properties have been determined. NCBE most likely contributes to the process for recovery of intracellular pH in pancreatic β-cells that have been acidified by glucose metabolism. NCBE mRNA occurs also in the testis, although its expression level is low. It has been shown that intracellular pH regulates many functions in sperm including sperm capacitation. As sperm capacitation results in the increase in intracellular pH, which requires functional Na

+

, Cl— and HCO

3

—-dependent acid-efflux pathway, NCBE could participate in the process of sperm capacitation. NCBE mRNA is also expressed at high levels in the brain. Though physiological studies suggests that NCBE is present in hippocampal neurons and astrocytes, its physiological significance of such cells remains unknown at present.

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Glu Asp Val Arg His Arg Val His Glu Ala Le

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His Gln Asn Gln Lys Lys Leu Ala Asn Arg Il

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Val Asp Leu His Phe Met Lys Lys Ile Pro Pr

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Asn Ile Leu Val Gly Glu Leu Glu Phe Leu As

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#40 3

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Gly Gln Gln Tyr His Glu Ile Gly Arg Ser Il

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# 360

# 365

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Asp Glu Val Phe His Asp Val Ala Tyr Lys Al

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# 375

# 380

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Leu Val Ser Gly Ile Asp Glu Phe Leu Asp Gl

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# 390

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# 405

# 410

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Pro Ser Gln Glu Lys Arg Lys Ile Pro Ala Va

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Ala His Gly Glu Ala Glu Pro His Gly Gly Hi

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# 440

# 445

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Gln Arg Thr Gly Arg Ile Phe Gly Gly Leu Me

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# 455

# 460

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Lys Ala Pro Phe Phe Trp Ser Asp Phe Arg As

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# 470

# 475

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Cys Leu Ala Ser Phe Leu Phe Leu Tyr Cys Al

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# 485

# 490

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Ile Thr Phe Gly Gly Leu Leu Gly Glu Ala Th

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#05 5

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Ala Ile Glu Ser Leu Phe Gly Ala Ser Met Th

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# 520

# 525

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Leu Phe Gly Gly Gln Pro Leu Thr Ile Leu Gl

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# 535

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Leu Val Phe Glu Lys Ile Leu Phe Lys Phe Cy

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# 550

# 555

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Ser Tyr Leu Ser Leu Arg Ala Ser Ile Gly Le

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# 565

# 570

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Cys Ile Ile Leu Val Ala Thr Asp Ala Ser Se

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#80 5

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Thr Arg Phe Thr Glu Glu Ala Phe Ala Ser Le

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# 600

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Ile Tyr Glu Ala Leu Glu Lys Leu Phe Glu Le

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# 615

# 620

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# 630

# 635

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# 650

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#60 6

#65 6

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# 680

# 685

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His Gly His Pro Tyr Val Pro Asp Val Leu Ph

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# 695

# 700

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Phe Phe Ser Thr Val Thr Met Ser Ala Thr Le

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# 710

# 715

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Ser Arg Tyr Phe Pro Thr Lys Val Arg Ser Il

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720

# 725

# 730

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Val Phe Leu Thr Ile Leu Cys Met Val Leu Il

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735 7

#40 7

#45 7

#50

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Ile Pro Ser Pro Lys Leu Gln Val Pro Ser Va

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755

# 760

# 765

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Tyr Asp Arg Gly Trp Phe Val Thr Pro Leu Gl

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770

# 775

# 780

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Thr Ile Ile Ala Ala Ile Ile Pro Ala Leu Le

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785

# 790

# 795

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Phe Met Asp Gln Gln Ile Thr Ala Val Ile Il

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800

# 805

# 810

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#20 8

#25 8

#30

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Val Met Leu Gly Val Cys Ser Ile Met Gly Le

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835

# 840

# 845

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Ala Thr Val Leu Ser Ile Thr His Val Asn Se

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850

# 855

# 860

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865

# 870

# 875

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Gln Arg Val Thr Gly Leu Met Ile Phe Ile Le

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880

# 885

# 890

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Phe Met Thr Ser Ile Leu Lys Phe Ile Pro Me

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895 9

#00 9

#05 9

#10

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Val Phe Leu Tyr Met Gly Ala Ser Ser Leu Ly

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915

# 920

# 925

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Asp Arg Ile Lys Leu Phe Trp Met Pro Ala Ly

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930

# 935

# 940

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Ile Tyr Leu Arg His Val Pro Leu Arg Lys Va

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945

# 950

# 955

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Ile Gln Met Ser Cys Leu Gly Leu Leu Trp Il

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960

# 965

# 970

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Ala Ala Ile Val Phe Pro Met Met Val Leu Al

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975 9

#80 9

#85 9

#90

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Lys Leu Met Asp Phe Leu Phe Thr Lys Arg Gl

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995

# 1000

# 1005

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#t gaa gat gct gag aaa 3132

Asp Leu Met Pro Glu Ser Lys Lys Lys Lys Le

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1010

# 1015

# 1020

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Glu Glu Glu Gln Ser Met Leu Ala Met Glu As

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1025

# 1030

# 1035

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Leu Pro Leu Glu Gly His Tyr Arg Asp Asp Pr

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1040

# 1045

# 1050

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Ser Asp Glu Met Ser Lys Thr Ala Met Trp Gl

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1055 1060

# 1065

# 1070

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Ala Asp Asn Ser Lys Glu Lys Glu Ser Arg Ph

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1075

# 1080

# 1085

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Pro Ser

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taatgcaaga gtctccagtg ttactgccgt aagacattcg ccaacacagg at

#tctcattg 3680

ttgacattaa gagaacaaag ctttctttaa aagataagtt atatttgcct ag

#tttgtatt 3740

ttcctacctt agtaacctga agatgcctga taattttatt cagaagaatt tt

#gaaaggta 3800

gtcgtacttt ttatttttta tggcttagca ttcgttactg gttttgaaag ac

#ccaaatca 3860

aaaagttact ctgaaagcat ttttaataat tgtatttatg tatttccttg ac

#ttaatatg 3920

aaacatttaa tacttaataa ctgttacttc aagtcatttg agaaagagac ct

#gttcatat 3980

cttcttaaaa gacatactgc aaagagtcaa gtagtgttca cttagaattc aa

#gttgtaac 4040

catgcagtca aaaactaggc ttgtattaaa tgctttagag atatttgaag ag

#ttttgtgg 4100

ggcttttcat tttaaatctt taccagaaat atgctactga gtttctctcc ca

#ttgacaag 4160

ggttgcttcc cgaataagcc tatgacatac atacttacgg aatgccacat gg

#tgcaacat 4220

tgtacatttg atgccagccc tggcagctgt tctgctgacc atggtcatgt gc

#tgctaagt 4280

ttggttccta tcatgttgtc atgttagacc aacaggtctc caactgtatt tt

#gttttttt 4340

tgcaaagctc ttttccacat tttaactaaa tgcatgttgt ggaaaaatag tc

#tttgaaat 4400

aaaatttcag attttgttag aaaaggttat gtaaatactt cagtccatat ga

#aacagttc 4460

aactttattg aaacaggaag gagattatgg atttttgagt attactaaat at

#aaatttca 4520

tttaattttc aataaatgtg ctttaataca aaacaaaata tcataggggt ct

#tagttcct 4580

aaaaaagtat caatgattaa caaccttata atctttcaat gtccaggttt ag

#aaaaattc 4640

agagccttct gggttttata aattacatgt actctgtgta aatacacata at

#tagaaaaa 4700

tcctctttgc ttttaagcta atgaagacga gagacaacag agcctacata ac

#cttaatat 4760

tctgatatct tgaacaaaaa atttcctcag aatcctttca ggagccattt tt

#ttaatgag 4820

atatgagcca aaattgtgag aagaattttc agttcgtaaa gtctgtattt at

#aaatggta 4880

aagaaaaatg caaaattctt ttccaaatgt gctacctttg tgatagttgt aa

#tagcgaca 4940

ctctctctaa acattctcgc tgtctatgac ttagcaggcc aatccccaaa gc

#actctcct 5000

ggtgtctcta gagtgtcatg tctgttctgt tgaaatgacc agtgagtgac ac

#ttcacatg 5060

atcactggtt taaacaggca atcagcctat gaaattctgt atttctgaat at

#ttttatag 5120

taattttgtt cttgtgtgaa ttttaatgct atctctatct taatcttaat at

#tttgaaat 5180

cacataaaat ataagaaaat gtagtattct atatttactc taatttcaga tt

#cctggtca 5240

aaattactga atatcttgaa tgtaatttat tgcaatgttt aagtactgtg ta

#aatgtgac 5300

aggatattgt gtttttcaaa actaagaaat gttatgtgga aataaatatt ta

#tcctaaaa 5360

aaaaaaaaaa aaaaaaaaaa aaaaa

#

# 5385

<210> SEQ ID NO 2

<211> LENGTH: 1088

<212> TYPE: PRT

<213> ORGANISM: Mus musculus

<400> SEQUENCE: 2

Met Glu Ile Lys Asp Gln Gly Ala Gln Met Gl

#u Pro Leu Leu Pro Thr

1 5

# 10

# 15

Arg Asn Asp Glu Glu Ala Val Val Asp Arg Gl

#y Gly Thr Arg Ser Ile

20

# 25

# 30

Leu Lys Thr His Phe Glu Lys Glu Asp Leu Gl

#u Gly His Arg Thr Leu

35

# 40

# 45

Phe Ile Gly Val His Val Pro Leu Gly Gly Ar

#g Lys Ser His Arg Arg

50

# 55

# 60

His Arg His Arg Gly His Lys His Arg Lys Ar

#g Asp Arg Glu Arg Asp

65

#70

#75

#80

Ser Gly Leu Glu Asp Gly Arg Glu Ser Pro Se

#r Phe Asp Thr Pro Ser

85

# 90

# 95

Gln Arg Val Gln Phe Ile Leu Gly Thr Glu As

#p Asp Asp Glu Glu His

100

# 105

# 110

Leu Pro His Asp Leu Phe Thr Glu Leu Asp Gl

#u Ile Cys Trp Arg Glu

115

# 120

# 125

Gly Glu Asp Ala Glu Trp Arg Glu Thr Ala Ar

#g Trp Leu Lys Phe Glu

130

# 135

# 140

Glu Asp Val Glu Asp Gly Gly Glu Arg Trp Se

#r Lys Pro Tyr Val Ala

145 1

#50 1

#55 1

#60

Thr Leu Ser Leu His Ser Leu Phe Glu Leu Ar

#g Ser Cys Ile Leu Asn

165

# 170

# 175

Gly Thr Val Leu Leu Asp Met His Ala Asn Th

#r Ile Glu Glu Ile Ala

180

# 185

# 190

Asp Met Val Leu Asp Gln Gln Val Ser Ser Gl

#y Gln Leu Asn Glu Asp

195

# 200

# 205

Val Arg His Arg Val His Glu Ala Leu Met Ly

#s Gln His His His Gln

210

# 215

# 220

Asn Gln Lys Lys Leu Ala Asn Arg Ile Pro Il

#e Val Arg Ser Leu Ala

225 2

#30 2

#35 2

#40

Asp Ile Gly Lys Lys Gln Ser Glu Pro Asn Se

#r Met Asp Lys Asn Ala

245

# 250

# 255

Gly Gln Val Val Ser Pro Gln Ser Ala Pro Al

#a Cys Ala Glu Asn Lys

260

# 265

# 270

Asn Asp Val Ser Arg Glu Asn Ser Thr Val As

#p Phe Ser Lys Val Asp

275

# 280

# 285

Leu His Phe Met Lys Lys Ile Pro Pro Gly Al

#a Glu Ala Ser Asn Ile

290

# 295

# 300

Leu Val Gly Glu Leu Glu Phe Leu Asp Arg Al

#a Val Val Ala Phe Val

305 3

#10 3

#15 3

#20

Arg Leu Ser Pro Ala Val Leu Leu Gln Gly Le

#u Ala Glu Val Pro Ile

325

# 330

# 335

Pro Ser Arg Phe Leu Phe Ile Leu Leu Gly Pr

#o Leu Gly Lys Gly Gln

340

# 345

# 350

Gln Tyr His Glu Ile Gly Arg Ser Ile Ala Th

#r Leu Met Thr Asp Glu

355

# 360

# 365

Val Phe His Asp Val Ala Tyr Lys Ala Lys As

#p Arg Asn Asp Leu Val

370

# 375

# 380

Ser Gly Ile Asp Glu Phe Leu Asp Gln Val Th

#r Val Leu Pro Pro Gly

385 3

#90 3

#95 4

#00

Glu Trp Asp Pro Ser Ile Arg Ile Glu Pro Pr

#o Lys Asn Val Pro Ser

405

# 410

# 415

Gln Glu Lys Arg Lys Ile Pro Ala Val Pro As

#n Gly Thr Ala Ala His

420

# 425

# 430

Gly Glu Ala Glu Pro His Gly Gly His Ser Gl

#y Pro Glu Leu Gln Arg

435

# 440

# 445

Thr Gly Arg Ile Phe Gly Gly Leu Met Leu As

#p Ile Lys Arg Lys Ala

450

# 455

# 460

Pro Phe Phe Trp Ser Asp Phe Arg Asp Ala Ph

#e Ser Leu Gln Cys Leu

465 4

#70 4

#75 4

#80

Ala Ser Phe Leu Phe Leu Tyr Cys Ala Cys Me

#t Ser Pro Val Ile Thr

485

# 490

# 495

Phe Gly Gly Leu Leu Gly Glu Ala Thr Glu Gl

#y Arg Ile Ser Ala Ile

500

# 505

# 510

Glu Ser Leu Phe Gly Ala Ser Met Thr Gly Il

#e Ala Tyr Ser Leu Phe

515

# 520

# 525

Gly Gly Gln Pro Leu Thr Ile Leu Gly Ser Th

#r Gly Pro Val Leu Val

530

# 535

# 540

Phe Glu Lys Ile Leu Phe Lys Phe Cys Lys Gl

#u Tyr Gly Leu Ser Tyr

545 5

#50 5

#55 5

#60

Leu Ser Leu Arg Ala Ser Ile Gly Leu Trp Th

#r Ala Thr Leu Cys Ile

565

# 570

# 575

Ile Leu Val Ala Thr Asp Ala Ser Ser Leu Va

#l Cys Tyr Ile Thr Arg

580

# 585

# 590

Phe Thr Glu Glu Ala Phe Ala Ser Leu Ile Cy

#s Ile Ile Phe Ile Tyr

595

# 600

# 605

Glu Ala Leu Glu Lys Leu Phe Glu Leu Ser Gl

#u Thr Tyr Pro Ile Asn

610

# 615

# 620

Met His Asn Asp Leu Glu Leu Leu Thr Gln Ty

#r Ser Cys Asn Cys Met

625 6

#30 6

#35 6

#40

Glu Pro His Ser Pro Ser Asn Asp Thr Leu Ly

#s Glu Trp Arg Glu Ser

645

# 650

# 655

Asn Leu Ser Ala Ser Asp Ile Ile Trp Gly As

#n Leu Thr Val Ser Glu

660

# 665

# 670

Cys Arg Ser Leu His Gly Glu Tyr Val Gly Ar

#g Ala Cys Gly His Gly

675

# 680

# 685

His Pro Tyr Val Pro Asp Val Leu Phe Trp Se

#r Val Ile Leu Phe Phe

690

# 695

# 700

Ser Thr Val Thr Met Ser Ala Thr Leu Lys Gl

#n Phe Lys Thr Ser Arg

705 7

#10 7

#15 7

#20

Tyr Phe Pro Thr Lys Val Arg Ser Ile Val Se

#r Asp Phe Ala Val Phe

725

# 730

# 735

Leu Thr Ile Leu Cys Met Val Leu Ile Asp Ty

#r Ala Ile Gly Ile Pro

740

# 745

# 750

Ser Pro Lys Leu Gln Val Pro Ser Val Phe Ly

#s Pro Thr Ile Tyr Asp

755

# 760

# 765

Arg Gly Trp Phe Val Thr Pro Leu Gly Pro As

#n Pro Trp Trp Thr Ile

770

# 775

# 780

Ile Ala Ala Ile Ile Pro Ala Leu Leu Cys Th

#r Ile Leu Ile Phe Met

785 7

#90 7

#95 8

#00

Asp Gln Gln Ile Thr Ala Val Ile Ile Asn Ar

#g Lys Glu His Lys Leu

805

# 810

# 815

Lys Lys Gly Cys Gly Tyr His Leu Asp Leu Le

#u Met Val Ala Val Met

820

# 825

# 830

Leu Gly Val Cys Ser Ile Met Gly Leu Pro Tr

#p Phe Val Ala Ala Thr

835

# 840

# 845

Val Leu Ser Ile Thr His Val Asn Ser Leu Ly

#s Leu Glu Ser Glu Cys

850

# 855

# 860

Ser Ala Pro Gly Glu Gln Pro Lys Phe Leu Gl

#y Ile Arg Glu Gln Arg

865 8

#70 8

#75 8

#80

Val Thr Gly Leu Met Ile Phe Ile Leu Met Gl

#y Ser Ser Val Phe Met

885

# 890

# 895

Thr Ser Ile Leu Lys Phe Ile Pro Met Pro Va

#l Leu Tyr Gly Val Phe

900

# 905

# 910

Leu Tyr Met Gly Ala Ser Ser Leu Lys Gly Il

#e Gln Leu Phe Asp Arg

915

# 920

# 925

Ile Lys Leu Phe Trp Met Pro Ala Lys His Gl

#n Pro Asp Phe Ile Tyr

930

# 935

# 940

Leu Arg His Val Pro Leu Arg Lys Val His Le

#u Phe Thr Val Ile Gln

945 9

#50 9

#55 9

#60

Met Ser Cys Leu Gly Leu Leu Trp Ile Ile Ly

#s Val Ser Arg Ala Ala

965

# 970

# 975

Ile Val Phe Pro Met Met Val Leu Ala Leu Va

#l Phe Val Arg Lys Leu

980

# 985

# 990

Met Asp Phe Leu Phe Thr Lys Arg Glu Leu Se

#r Trp Leu Asp Asp Leu

995

# 1000

# 1005

Met Pro Glu Ser Lys Lys Lys Lys Leu Glu As

#p Ala Glu Lys Glu Glu

1010

# 1015

# 1020

Glu Gln Ser Met Leu Ala Met Glu Asp Glu Gl

#y Thr Val Gln Leu Pro

1025 1030

# 1035

# 1040

Leu Glu Gly His Tyr Arg Asp Asp Pro Ser Va

#l Ile Asn Ile Ser Asp

1045

# 1050

# 1055

Glu Met Ser Lys Thr Ala Met Trp Gly Asn Le

#u Leu Val Thr Ala Asp

1060

# 1065

# 1070

Asn Ser Lys Glu Lys Glu Ser Arg Phe Pro Se

#r Lys Ser Ser Pro Ser

1075

# 1080

# 1085

<210> SEQ ID NO 3

<211> LENGTH: 4138

<212> TYPE: DNA

<213> ORGANISM: Homo sapience

<400> SEQUENCE: 3

taagcagagc gagtgccggg ctgagtgtaa gacactgaag acactgcaga gc

#aaggtgct 60

tattccagag gcgttacaaa ac atg gag att aaa gac cag

# gga gcc caa atg 112

# Met Glu Ile Lys Asp Gln G

#ly Ala Gln Met

# 1

# 5

# 10

gag ccg ctg ctg cct acg aga aat gat gaa ga

#a gca gtt gtg gat aga 160

Glu Pro Leu Leu Pro Thr Arg Asn Asp Glu Gl

#u Ala Val Val Asp Arg

15

# 20

# 25

ggt gga act cgt tct att ctc aaa aca cac tt

#t gag aaa gaa gat tta 208

Gly Gly Thr Arg Ser Ile Leu Lys Thr His Ph

#e Glu Lys Glu Asp Leu

30

# 35

# 40

gaa ggt cat cga aca cta ttt att gga gta ca

#t gtg ccc ttg gga gga 256

Glu Gly His Arg Thr Leu Phe Ile Gly Val Hi

#s Val Pro Leu Gly Gly

45

# 50

# 55

aga aaa agc cat cga cgt cac agg cat cgt gg

#t cat aaa cac aga aag 304

Arg Lys Ser His Arg Arg His Arg His Arg Gl

#y His Lys His Arg Lys

60

# 65

# 70

aga gac aga gaa aga gat tca gga tta gag ga

#t gga agg gag tca cct 352

Arg Asp Arg Glu Arg Asp Ser Gly Leu Glu As

#p Gly Arg Glu Ser Pro

75

#80

#85

#90

tct ttt gac acc cca tca cag agg gta cag tt

#t att ctt gga acc gag 400

Ser Phe Asp Thr Pro Ser Gln Arg Val Gln Ph

#e Ile Leu Gly Thr Glu

95

# 100

# 105

gat gat gac gag gaa cac att cct cat gac ct

#t ttc aca gaa ctg gat 448

Asp Asp Asp Glu Glu His Ile Pro His Asp Le

#u Phe Thr Glu Leu Asp

110

# 115

# 120

gag att tgt tgg cgt gaa ggt gag gac gct ga

#g tgg cga gaa aca gcc 496

Glu Ile Cys Trp Arg Glu Gly Glu Asp Ala Gl

#u Trp Arg Glu Thr Ala

125

# 130

# 135

agg tgg ttg aag ttt gaa gaa gat gtg gaa ga

#t gga gga gaa agg tgg 544

Arg Trp Leu Lys Phe Glu Glu Asp Val Glu As

#p Gly Gly Glu Arg Trp

140

# 145

# 150

agc aag cct tat gtg gct act ctt tca ttg ca

#c agc ttg ttt gaa ttg 592

Ser Lys Pro Tyr Val Ala Thr Leu Ser Leu Hi

#s Ser Leu Phe Glu Leu

155 1

#60 1

#65 1

#70

aga agt tgt att ctg aat gga act gtg ttg ct

#g gac atg cat gcc aac 640

Arg Ser Cys Ile Leu Asn Gly Thr Val Leu Le

#u Asp Met His Ala Asn

175

# 180

# 185

act tta gaa gaa att gca gat atg gtt ctt ga

#c caa caa gtg agc tca 688

Thr Leu Glu Glu Ile Ala Asp Met Val Leu As

#p Gln Gln Val Ser Ser

190

# 195

# 200

ggt cag ctg aat gaa gat gta cgc cat agg gt

#c cat gag gca ttg atg 736

Gly Gln Leu Asn Glu Asp Val Arg His Arg Va

#l His Glu Ala Leu Met

205

# 210

# 215

aaa cag cat cat cat cag aat cag aaa aaa ct

#c acc aac agg att ccc 784

Lys Gln His His His Gln Asn Gln Lys Lys Le

#u Thr Asn Arg Ile Pro

220

# 225

# 230

att gtt cgt tcc ttt gct gat att ggc aag aa

#a cag tca gaa cca aat 832

Ile Val Arg Ser Phe Ala Asp Ile Gly Lys Ly

#s Gln Ser Glu Pro Asn

235 2

#40 2

#45 2

#50

tcc atg gac aaa aat gca ggt cag gtt gtt tc

#t cct cag tct gct cca 880

Ser Met Asp Lys Asn Ala Gly Gln Val Val Se

#r Pro Gln Ser Ala Pro

255

# 260

# 265

gcc tgt gtt gaa aat aaa aat gat gtt agc ag

#a gaa aac agc act gtt 928

Ala Cys Val Glu Asn Lys Asn Asp Val Ser Ar

#g Glu Asn Ser Thr Val

270

# 275

# 280

gac ttt agc aag gtt gat ctg cat ttt atg aa

#a aag att cct cca ggt 976

Asp Phe Ser Lys Val Asp Leu His Phe Met Ly

#s Lys Ile Pro Pro Gly

285

# 290

# 295

gct gaa gca tcg aac atc tta ctg gga gaa ct

#g gag ttc ttg gat cga 1024

Ala Glu Ala Ser Asn Ile Leu Leu Gly Glu Le

#u Glu Phe Leu Asp Arg

300

# 305

# 310

aca gta gtt gcg ttt gtc agg ttg tct cca gc

#t gta ttg ctt caa gga 1072

Thr Val Val Ala Phe Val Arg Leu Ser Pro Al

#a Val Leu Leu Gln Gly

315 3

#20 3

#25 3

#30

ctg gct gaa gtc cca atc cca acc aga ttt tt

#g ttc att ctt ctg gga 1120

Leu Ala Glu Val Pro Ile Pro Thr Arg Phe Le

#u Phe Ile Leu Leu Gly

335

# 340

# 345

ccc ctg gga aag ggt caa cag tac cat gag at

#t ggc aga tca att gca 1168

Pro Leu Gly Lys Gly Gln Gln Tyr His Glu Il

#e Gly Arg Ser Ile Ala

350

# 355

# 360

acc cta atg aca gat gag gta ttt cat gat gt

#t gcc tat aaa gct aaa 1216

Thr Leu Met Thr Asp Glu Val Phe His Asp Va

#l Ala Tyr Lys Ala Lys

365

# 370

# 375

gat cgt aat gac ttg gta tca gga att gat ga

#g ttt ctg gat cag gtt 1264

Asp Arg Asn Asp Leu Val Ser Gly Ile Asp Gl

#u Phe Leu Asp Gln Val

380

# 385

# 390

act gtt ctc cct cct gga gaa tgg gat cca ag

#c att cga ata gag cct 1312

Thr Val Leu Pro Pro Gly Glu Trp Asp Pro Se

#r Ile Arg Ile Glu Pro

395 4

#00 4

#05 4

#10

ccc aaa aat gtt cct tcc cag gag aag agg aa

#g att cct gct gta cca 1360

Pro Lys Asn Val Pro Ser Gln Glu Lys Arg Ly

#s Ile Pro Ala Val Pro

415

# 420

# 425

aat gga aca gca gct cat ggg gaa gca gag cc

#c cac gga gga cat agt 1408

Asn Gly Thr Ala Ala His Gly Glu Ala Glu Pr

#o His Gly Gly His Ser

430

# 435

# 440

gga cct gaa ctc cag cga act gga agg att tt

#t ggg gga ctt att tta 1456

Gly Pro Glu Leu Gln Arg Thr Gly Arg Ile Ph

#e Gly Gly Leu Ile Leu

445

# 450

# 455

gat atc aaa aga aaa gct cca tac ttc tgg ag

#t gac ttc aga gat gct 1504

Asp Ile Lys Arg Lys Ala Pro Tyr Phe Trp Se

#r Asp Phe Arg Asp Ala

460

# 465

# 470

ttc agc ctg cag tgc tta gca tct ttt cta tt

#t ctc tac tgc gcg tgt 1552

Phe Ser Leu Gln Cys Leu Ala Ser Phe Leu Ph

#e Leu Tyr Cys Ala Cys

475 4

#80 4

#85 4

#90

atg tct cct gtc atc acg ttt gga gga ctg ct

#g gga gaa gca act gaa 1600

Met Ser Pro Val Ile Thr Phe Gly Gly Leu Le

#u Gly Glu Ala Thr Glu

495

# 500

# 505

ggg cgt ata agt gca att gaa tct ctc ttt gg

#a gca tcc atg acc ggg 1648

Gly Arg Ile Ser Ala Ile Glu Ser Leu Phe Gl

#y Ala Ser Met Thr Gly

510

# 515

# 520

ata gcc tat tct ctc ttt ggt gga cag cct ct

#t acc ata tta ggc agt 1696

Ile Ala Tyr Ser Leu Phe Gly Gly Gln Pro Le

#u Thr Ile Leu Gly Ser

525

# 530

# 535

aca gga cca gtt ttg gtg ttt gaa aag att tt

#g ttt aaa ttt tgc aaa 1744

Thr Gly Pro Val Leu Val Phe Glu Lys Ile Le

#u Phe Lys Phe Cys Lys

540

# 545

# 550

gaa tat ggg ctg tca tac cta tct tta aga gc

#t agc att gga ctt tgg 1792

Glu Tyr Gly Leu Ser Tyr Leu Ser Leu Arg Al

#a Ser Ile Gly Leu Trp

555 5

#60 5

#65 5

#70

act gca act cta tgt atc ata ctt gtg gcc ac

#a gat gct agt tcc ctt 1840

Thr Ala Thr Leu Cys Ile Ile Leu Val Ala Th

#r Asp Ala Ser Ser Leu

575

# 580

# 585

gtc tgc tac atc act cgg ttt act gaa gaa gc

#t ttt gct tcc ctg att 1888

Val Cys Tyr Ile Thr Arg Phe Thr Glu Glu Al

#a Phe Ala Ser Leu Ile

590

# 595

# 600

tgc atc att ttc att tat gag gcc ctg gag aa

#g ttg ttt gaa ctc agt 1936

Cys Ile Ile Phe Ile Tyr Glu Ala Leu Glu Ly

#s Leu Phe Glu Leu Ser

605

# 610

# 615

gaa gca tat cca atc aac atg cat aat gat ct

#g gaa ctg ctg aca caa 1984

Glu Ala Tyr Pro Ile Asn Met His Asn Asp Le

#u Glu Leu Leu Thr Gln

620

# 625

# 630

tac tcg tgt aac tgt gtg gaa ccg cat aat cc

#c agc aat ggc aca ttg 2032

Tyr Ser Cys Asn Cys Val Glu Pro His Asn Pr

#o Ser Asn Gly Thr Leu

635 6

#40 6

#45 6

#50

aag gaa tgg agg gaa tcc aat att tct gcc tc

#t gac ata att tgg gag 2080

Lys Glu Trp Arg Glu Ser Asn Ile Ser Ala Se

#r Asp Ile Ile Trp Glu

655

# 660

# 665

aac cta act gtg tca gaa tgc aaa tca ttg ca

#t gga gag tat gtt gga 2128

Asn Leu Thr Val Ser Glu Cys Lys Ser Leu Hi

#s Gly Glu Tyr Val Gly

670

# 675

# 680

cgg gcc tgt ggc cat gat cac cca tat gtt cc

#a gat gtt cta ttt tgg 2176

Arg Ala Cys Gly His Asp His Pro Tyr Val Pr

#o Asp Val Leu Phe Trp

685

# 690

# 695

tct gtg atc ctg ttc ttt tcc aca gtt act ct

#g tca gcc acc ctg aag 2224

Ser Val Ile Leu Phe Phe Ser Thr Val Thr Le

#u Ser Ala Thr Leu Lys

700

# 705

# 710

cag ttc aag act agc aga tat ttt cca acc aa

#g gtt cga tcc ata gtg 2272

Gln Phe Lys Thr Ser Arg Tyr Phe Pro Thr Ly

#s Val Arg Ser Ile Val

715 7

#20 7

#25 7

#30

agt gac ttt gct gtc ttt ctt aca att ctg tg

#t atg gtt tta att gac 2320

Ser Asp Phe Ala Val Phe Leu Thr Ile Leu Cy

#s Met Val Leu Ile Asp

735

# 740

# 745

tat gcc att ggg atc cca tct cca aaa cta ca

#a gta cca agt gtt ttc 2368

Tyr Ala Ile Gly Ile Pro Ser Pro Lys Leu Gl

#n Val Pro Ser Val Phe

750

# 755

# 760

aag ccc act aga gat gat cgt ggc tgg ttt gt

#t acg cct tta ggt cca 2416

Lys Pro Thr Arg Asp Asp Arg Gly Trp Phe Va

#l Thr Pro Leu Gly Pro

765

# 770

# 775

aac cca tgg tgg aca gta ata gct gct ata at

#t cca gct ctg ctt tgt 2464

Asn Pro Trp Trp Thr Val Ile Ala Ala Ile Il

#e Pro Ala Leu Leu Cys

780

# 785

# 790

act att cta att ttc atg gac caa cag att ac

#a gct gtc atc atc aac 2512

Thr Ile Leu Ile Phe Met Asp Gln Gln Ile Th

#r Ala Val Ile Ile Asn

795 8

#00 8

#05 8

#10

agg aaa gag cat aag cta aag aaa ggt tgt gg

#g tac cat ctg gac cta 2560

Arg Lys Glu His Lys Leu Lys Lys Gly Cys Gl

#y Tyr His Leu Asp Leu

815

# 820

# 825

tta atg gtg gct gtc atg ctc ggt gta tgc tc

#c atc atg ggc ctg cca 2608

Leu Met Val Ala Val Met Leu Gly Val Cys Se

#r Ile Met Gly Leu Pro

830

# 835

# 840

tgg ttt gtg gct gcc aca gtc ctc tcc atc ac

#t cat gtc aat agc cta 2656

Trp Phe Val Ala Ala Thr Val Leu Ser Ile Th

#r His Val Asn Ser Leu

845

# 850

# 855

aaa ctg gaa tca gaa tgc tca gct cca gga ga

#a caa ccc aaa ttt ctc 2704

Lys Leu Glu Ser Glu Cys Ser Ala Pro Gly Gl

#u Gln Pro Lys Phe Leu

860

# 865

# 870

ggc att cgg gag caa agg gtt act ggg ctt at

#g att ttt att ctt atg 2752

Gly Ile Arg Glu Gln Arg Val Thr Gly Leu Me

#t Ile Phe Ile Leu Met

875 8

#80 8

#85 8

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Gly Ser Ser Val Phe Met Thr Ser Ile Leu Ly

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895

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Val Leu Tyr Gly Val Phe Leu Tyr Met Gly Al

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Gln Pro Asp Phe Ile Tyr Leu Arg His Val Pr

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Leu Phe Thr Ile Ile Gln Met Ser Cys Leu Gl

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#65 9

#70

aaa gtt tca aga gct gct att gtc tct ccc at

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Lys Val Ser Arg Ala Ala Ile Val Ser Pro Me

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Val Phe Val Arg Lys Leu Met Asp Leu Leu Ph

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Cys Trp Leu Asp Asp Leu Met Pro Glu Ser Ly

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Tyr Ala Glu Lys Glu Glu Glu Gln Cys Val Le

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# 1030

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Gly Thr Val Gln Leu Pro Leu Glu Gly His Ty

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1035 1040

# 1045

# 1050

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#t gcc ttg tgg agg aac 3280

Val Ile Asn Ile Ser Asp Glu Met Ser Lys Th

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# 1060

# 1065

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Leu Leu Ile Thr Ala Asp Asn Ser Lys Asp Ly

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# 1075

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Ser Lys Ser Ser Pro Ser

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ttatttattt tatgcatagg aatattcatt ccggaattc

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Glu Asp Val Glu Asp Gly Gly Glu Arg Trp Se

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Thr Leu Ser Leu His Ser Leu Phe Glu Leu Ar

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Gly Thr Val Leu Leu Asp Met His Ala Asn Th

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Asp Met Val Leu Asp Gln Gln Val Ser Ser Gl

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Val Arg His Arg Val His Glu Ala Leu Met Ly

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Asn Gln Lys Lys Leu Thr Asn Arg Ile Pro Il

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Asp Ile Gly Lys Lys Gln Ser Glu Pro Asn Se

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Gly Gln Val Val Ser Pro Gln Ser Ala Pro Al

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Asn Asp Val Ser Arg Glu Asn Ser Thr Val As

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Leu His Phe Met Lys Lys Ile Pro Pro Gly Al

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Arg Leu Ser Pro Ala Val Leu Leu Gln Gly Le

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Pro Thr Arg Phe Leu Phe Ile Leu Leu Gly Pr

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Gln Tyr His Glu Ile Gly Arg Ser Ile Ala Th

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Val Phe His Asp Val Ala Tyr Lys Ala Lys As

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Ser Gly Ile Asp Glu Phe Leu Asp Gln Val Th

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Glu Trp Asp Pro Ser Ile Arg Ile Glu Pro Pr

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Gln Glu Lys Arg Lys Ile Pro Ala Val Pro As

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420

# 425

# 430

Gly Glu Ala Glu Pro His Gly Gly His Ser Gl

#y Pro Glu Leu Gln Arg

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# 445

Thr Gly Arg Ile Phe Gly Gly Leu Ile Leu As

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# 455

# 460

Pro Tyr Phe Trp Ser Asp Phe Arg Asp Ala Ph

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#80

Ala Ser Phe Leu Phe Leu Tyr Cys Ala Cys Me

#t Ser Pro Val Ile Thr

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# 490

# 495

Phe Gly Gly Leu Leu Gly Glu Ala Thr Glu Gl

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# 505

# 510

Glu Ser Leu Phe Gly Ala Ser Met Thr Gly Il

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Gly Gly Gln Pro Leu Thr Ile Leu Gly Ser Th

#r Gly Pro Val Leu Val

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Phe Glu Lys Ile Leu Phe Lys Phe Cys Lys Gl

#u Tyr Gly Leu Ser Tyr

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#50 5

#55 5

#60

Leu Ser Leu Arg Ala Ser Ile Gly Leu Trp Th

#r Ala Thr Leu Cys Ile

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# 570

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Ile Leu Val Ala Thr Asp Ala Ser Ser Leu Va

#l Cys Tyr Ile Thr Arg

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# 585

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Phe Thr Glu Glu Ala Phe Ala Ser Leu Ile Cy

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595

# 600

# 605

Glu Ala Leu Glu Lys Leu Phe Glu Leu Ser Gl

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# 615

# 620

Met His Asn Asp Leu Glu Leu Leu Thr Gln Ty

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#30 6

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#40

Glu Pro His Asn Pro Ser Asn Gly Thr Leu Ly

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# 650

# 655

Asn Ile Ser Ala Ser Asp Ile Ile Trp Glu As

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# 665

# 670

Cys Lys Ser Leu His Gly Glu Tyr Val Gly Ar

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# 680

# 685

His Pro Tyr Val Pro Asp Val Leu Phe Trp Se

#r Val Ile Leu Phe Phe

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# 695

# 700

Ser Thr Val Thr Leu Ser Ala Thr Leu Lys Gl

#n Phe Lys Thr Ser Arg

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#20

Tyr Phe Pro Thr Lys Val Arg Ser Ile Val Se

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# 730

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Leu Thr Ile Leu Cys Met Val Leu Ile Asp Ty

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Ser Pro Lys Leu Gln Val Pro Ser Val Phe Ly

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Arg Gly Trp Phe Val Thr Pro Leu Gly Pro As

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Ile Ala Ala Ile Ile Pro Ala Leu Leu Cys Th

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Asp Gln Gln Ile Thr Ala Val Ile Ile Asn Ar

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Lys Lys Gly Cys Gly Tyr His Leu Asp Leu Le

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Leu Gly Val Cys Ser Ile Met Gly Leu Pro Tr

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# 840

# 845

Val Leu Ser Ile Thr His Val Asn Ser Leu Ly

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# 855

# 860

Ser Ala Pro Gly Glu Gln Pro Lys Phe Leu Gl

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#70 8

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#80

Val Thr Gly Leu Met Ile Phe Ile Leu Met Gl

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885

# 890

# 895

Thr Ser Ile Leu Lys Phe Ile Pro Met Pro Va

#l Leu Tyr Gly Val Phe

900

# 905

# 910

Leu Tyr Met Gly Ala Ser Ser Leu Lys Gly Il

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915

# 920

# 925

Ile Lys Leu Phe Trp Met Pro Ala Lys His Gl

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930

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# 940

Leu Arg His Val Pro Leu Arg Lys Val His Le

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Met Ser Cys Leu Gly Leu Leu Trp Ile Ile Ly

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965

# 970

# 975

Ile Val Ser Pro Met Met Val Leu Ser Leu Va

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980

# 985

# 990

Met Asp Leu Leu Phe Thr Lys Arg Glu Leu Cy

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995

# 1000

# 1005

Met Pro Glu Ser Lys Lys Lys Lys Leu Glu Ty

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1010

# 1015

# 1020

Glu Gln Cys Val Leu Pro Met Glu Asp Glu Gl

#y Thr Val Gln Leu Pro

1025 1030

# 1035

# 1040

Leu Glu Gly His Tyr Arg Asp Asp Pro Ser Va

#l Ile Asn Ile Ser Asp

1045

# 1050

# 1055

Glu Met Ser Lys Thr Ala Leu Trp Arg Asn Le

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1060

# 1065

# 1070

Asn Ser Lys Asp Lys Glu Ser Ser Phe Pro Se

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#

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#

#

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<210> SEQ ID NO 8

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#

#

# 18

Number	Date	Country	Kind
2000-241775	Aug 2000	JP
2000-342911	Nov 2000	JP

Sodium ion-driven chloride /bi-carbonate exchanger

Information

Patent Number

Date Filed

Date Issued

Inventors

Original Assignees

Examiners

Agents

CPC

US Classifications

Field of Search

US

International Classifications

Term Extension

Abstract

Description

Claims

Priority Claims (2)

US Referenced Citations (1)

Foreign Referenced Citations (1)

Non-Patent Literature Citations (28)

Entry
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Database EM_HUM Online! EMBL; Dec. 2, 1998; Grichtchenko et al., Homo Sapiens Sodium.
Bicarbonate Cotransporter (NBC) mRNA, complete CDs. retrieved from EBI, accession No. AF069512, Database accession No. AF069512, XP00182615.
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Grichtchenko et al., “Cloning Characterization, and Chromosomal Mapping of a Human Electroneutral Na+-driven CI-HC02 Exchanger”, The Journal of Biological Chemistry, vol. 276, No. 11, published Mar. 16, 2001, pp. 8358-8363, XP002182612.
Database EM_RO Online! EMBL; Apr. 5, 2000; Wang et al., “Mus musculus sodium bicarbonate cotransporter isoform 3 kNBC-2 mRNA”, retrieved from EBI, accession No. AF224508, Database accession No. AF224508, XP002182617.
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Wang et al., “Mouse Na+:HC03-cotransporter isoform NBC-2 (kNBC-3): Cloning, expression, and renal distribution” Kidney International, vol. 59, 2001, pp. 1405-1414, XO002182613.
Burnham et al., “Cloning and functional expression of a human kidney Na+:”HC03-cotransporter, The Journal of Biological Chemistry, vol. 272, No. 31, Aug. 1, 1997, pp. 19111-19114, XP002076894.
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Database SWALL Online!; Mar. 1, 2001; Wang et al., “NCBE”, retrieved from EBI, accession No. Q9EST0, Database accession No. Q9EST0, XP002182620.
Database EM_HUM Online! EMBL; Nov. 21, 2000; Wang et al., “Homo sapiens SLC4A10 mRNA for NCBE, complete CDs” retrieved from EBI, accession no. AB040457, Database accession No. AB040457, XP002182621.
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