Claims
- 1. A fusion protein comprising:
(a) a first moiety that is a protein domain comprising an amino acid sequence foreign to a filamentous phage; and (b) a second moiety that comprises a mature filamentous phage coat protein.
- 2. The fusion protein of claim 1 wherein the mature phage coat protein is a mature filamentous phage gene VIII protein.
- 3. The fusion protein of claim 1 wherein the mature phage coat protein is a mature filamentous phage gene III protein.
- 4. The fusion protein of any of claims 1 to 3 wherein the second moiety is carboxy terminal to the first moiety.
- 5. The fusion protein of any of claims 1 to 3 wherein the protein domain is stable to a temperature of at least 40° C.
- 6. The fusion protein of any of claims 1 to 3 wherein the protein domain binds to a target other than an antibody with a dissociation constant of less than 10−6 moles/liter.
- 7. The fusion protein of any of claims 1 to 3 wherein the protein domain of the first moiety comprises an antibody domain.
- 8. The fusion protein of any of claims 1 to 3 wherein the first and second moieties are linked by a peptide or amino acid linker.
- 9. The fusion protein of any of claims 1 to 3 wherein the filamentous phage is M13, fd, or f1.
- 10. A fusion protein comprising:
(a) a first moiety that is a protein domain comprising an amino acid sequence foreign to a filamentous phage, the domain being stable to a temperature of at least 40° C., and binding a target other than an antibody with a dissociation constant of less than 10−6 moles/liter; and (b) a second moiety that comprises a mature filamentous phage gene III or gene VIII coat protein and is carboxy terminal to the first moiety.
- 11. A filamentous bacteriophage that comprises a chimeric binding protein that comprises (i) a proteinaceous binding domain which is sufficiently stable in structure to have a melting point of at least 40° C., said domain being foreign to filamentous bacteriophage, and (ii) a mature filamentous phage coat protein.
- 12. The bacteriophage of claim 11 wherein the mature phage coat protein comprises the mature gene VIII protein.
- 13. The bacteriophage of claim 11 wherein the mature phage coat protein mature gene III.
- 14. A filamentous bacteriophage that includes a chimeric binding protein that comprises (i) a proteinaceous binding domain which is sufficiently stable in structure to have a melting point of at least 40° C., said domain being foreign to filamentous bacteriophage, and (ii) a protein selected from the group consisting of: filamentous phage gene VI protein, gene VII protein, gene IX protein, and a carboxyl terminal fragment of filamentous phage gene III protein
- 15. The bacteriophage of claim 14 wherein the protein (ii) is a carboxyl terminal fragment of gene III protein that is functional for insertion into the coat of the bacteriophage.
- 16. The bacteriophage of claim 15 wherein the carboxyl terminal fragment comprises residues 275 to 424 of M13 gene III protein.
- 17. A variegated population of filamentous bacteriophage, each bacteriophage including, on its outer surface, a chimeric protein that comprises (a) a potential binding domain which is a mutant of a parental binding domain and (b) a mature gene VIII protein or a mature gene III protein, wherein the potential binding domains of the bacteriophage of the population comprise mutants of a parental binding domain at one or more predetermined amino acid positions of said parental binding domain.
- 18. The population of claim 17 wherein the chimeric protein comprises the mature gene VIII protein.
- 19. The population of claim 17 wherein the chimeric protein comprises the mature gene III protein.
- 20. The population of any of claims 17 to 19, wherein the parental binding domain comprises an antibody domain.
- 21. A library of replicable genetic packages, each package including (i) a potential binding domain, accessible to an affinity matrix and comprising an antibody domain, and (ii) a nucleic acid construct encoding the potential binding domain, and each package physically associating the potential binding domain and the nucleic acid construct encoding it, wherein
the library comprises a package for each of a plurality of different potential binding domains, the differentiation among said plurality of different potential binding domains comprises at least partially random variation of at least one amino acid position in a hypervariable region of the antibody domain, and the replicable genetic packages are filamentous bacteriophage.
- 22. A library of filamentous phage, each phage displaying an a proteinaceous potential binding domain that comprises an antibody domain and each phage comprising a nucleic acid construct encoding the potential binding domain, the library comprising a package for each of a plurality of different antibody domains, wherein the differentiation among said plurality of different potential binding domains comprises at least partially random variation of one or more predetermined amino acid positions of a hypervariable region of the antibody domains.
- 23. A library of filamentous phage, each phage (i) bearing on its outer surface a proteinaceous potential binding domain that comprises an antibody domain, the proteinaceous potential binding domain being foreign to the phage, and (ii) containing an expressible nucleic acid encoding the proteinaceous binding domain, the library comprising a plurality of different potential binding domains, wherein the differentiation among said plurality of different potential binding domains comprises at least partially random variation of one or more predetermined amino acid positions of a hypervariable region of the antibody domains.
- 24. The library of claim 21, 22, or 23 wherein the at least partially random variation is determined by selection from a set of at least two codons, the set being characterized by one or more of the following properties: (a) the set excludes all codons encoding cysteine, (b) the set includes a single codon for each encoded amino acid, and (c) the amino acids encoded by the set are represented at substantially equal frequency.
- 25. The library of claim 24 wherein the set excludes all codons encoding cysteine.
- 26. The library of claim 24 wherein the set includes a single codon for each encoded amino acid.
- 27. The library of claim 24 wherein the amino acids encoded by the set are represented at substantially equal frequency.
- 28. The library of claim 24 wherein the set is characterized by all three properties, (a), (b), and (c).
- 29. The library of claim 21, 22, or 23 wherein the filamentous phage is M13, fd, or f1.
- 30. A fusion protein comprising:
(a) a first moiety that is a protein domain comprising an amino acid sequence foreign to a filamentous phage; and (b) a second moiety that comprises a functional domain of a filamentous phage coat protein.
- 31. The fusion protein of claim 30 where said filamentous phage coat protein is a gene III coat protein.
- 32. The fusion protein of claim 30 where said filamentous phage coat protein is a gene VIII coat protein.
- 33. A filamentous bacteriophage that comprises a chimeric binding protein that comprises (i) a proteinaceous binding domain which is sufficiently stable in structure to have a melting point of at least 40° C., said domain being foreign to filamentous bacteriophage, and (ii) a functional domain of a filamentous phage coat protein.
- 34. The filamentous bacteriophage of claim 33 where said filamentous phage coat protein is a gene VIII coat protein.
- 35. The filamentous bacteriophage of claim 33 where said filamentous phage coat protein is a gene III coat protein.
- 36. A variegated population of filamentous bacteriophage, each bacteriophage including, on its outer surface, a chimeric protein that comprises (a) a potential binding domain which is a mutant of a parental binding domain and (b) a functional domain of a gene VIII protein or a gene III protein, wherein the potential binding domains of the bacteriophage of the population comprise mutants of a parental binding domain at one or more predetermined amino acid positions of said parental binding domain.
- 37. The population of claim 36 where said filamentous phage coat protein is a gene VIII coat protein.
- 38. The population of claim 36 where said filamentous phage coat protein is a gene III coat protein.
Priority Claims (1)
Number |
Date |
Country |
Kind |
PCT/US89/03731 |
Sep 1989 |
US |
|
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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Jan 1993 |
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Continuations (3)
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Continuation in Parts (2)
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