Claims
- 1. An isolated polypeptide having RA pathway activity comprising a polypeptide sequence selected from the group consisting of:
(a) the polypeptide sequence of Perturbagen R3 (FIG. 15(b)); (b) the polypeptide sequence of Perturbagen F802 (FIG. 13(a)); (c) the polypeptide sequence of Perturbagen F820 (FIG. 13(b)); (d) biologically active modifications of (a), (b) or (c); and (e) biologically active fragments of (a), (b) or (c).
- 2. The isolated polypeptide of claim 1 wherein said isolated polypeptide is (a) (b) or (c).
- 3. The isolated polypeptide of claim 1 consisting essentially of the sequence of Perturbagen R3 (FIG. 15(b)).
- 4. The isolated polypeptide of claim 3 wherein said isolated polypeptide comprises the amino acid sequence of Perturbagen R3 (FIG. 15(b)) except for one or more conservative amino acid substitutions.
- 5. The isolated polypeptide of claim 2 consisting of Perturbagen R3 (FIG. 15(b)).
- 6. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 99% identical to the amino acid sequence of Perturbagen R3 (FIG. 15(b)).
- 7. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 95% identical to the amino acid sequence of Perturbagen R3 (FIG. 15(b)).
- 8. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 90% identical to the amino acid sequence of Perturbagen R3 (FIG. 15(b)).
- 9. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 85% identical to the amino acid sequence of Perturbagen R3 (FIG. 15(b)).
- 10. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 80% identical to the amino acid sequence of Perturbagen R3 (FIG. 15(b)).
- 11. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a biologically active fragment of Perturbagen R3 (FIG. 15(b)) displaying a shift in RA-correlated reporter expression.
- 12. The isolated polypeptide of claim 1 wherein said isolated polypeptide is a closely related analog of Perturbagen R3 (FIG. 15(b)) wherein said analog displays biological activity of a shift in RA-correlated reporter expression.
- 13. The isolated polypeptide of claim 1 wherein said isolated polypeptide is an antigenic analog of Perturbagen R3 (FIG. 15(b)) wherein said analog binds to an antibody specific for the polypeptide of Perturbagen R3 (FIG. 15(b)).
- 14. The isolated polypeptide of claim 1 wherein said isolated polypeptide is an N-terminal fragment of Perturbagen R3 (FIG. 15(b)).
- 15. The isolated polypeptide of claim 14 wherein said N-terminal fragment comprises at least 10 amino acids of Perturbagen R3 (FIG. 15(b)).
- 16. The isolated polypeptide of claim 1 wherein said isolated polypeptide is a C-terminal fragment of Perturbagen R3 (FIG. 15(b)).
- 17. The isolated polypeptide of claim 16 wherein said C-terminal fragment comprises at least 10 amino acids of Perturbagen R3 (FIG. 15(b)).
- 18. The isolated polypeptide of claim 1 consisting essentially of the sequence of Perturbagen F802 (FIG. 13(a)).
- 19. The isolated polypeptide of claim 3 wherein said isolated polypeptide comprises the amino acid sequence of Perturbagen F802 (FIG. 13(a)) except for one or more conservative amino acid substitutions.
- 20. The isolated polypeptide of claim 2 consisting of Perturbagen F802 (FIG. 13(a)).
- 21. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 99% identical to the amino acid sequence of Perturbagen F802 (FIG. 13(a)).
- 22. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 95% identical to the amino acid sequence of Perturbagen F802 (FIG. 13(a)).
- 23. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 90% identical to the amino acid sequence of Perturbagen F802 (FIG. 13(a)).
- 24. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 85% identical to the amino acid sequence of Perturbagen F802 (FIG. 13(a)).
- 25. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 80% identical to the amino acid sequence of Perturbagen F802 (FIG. 13(a)).
- 26. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a biologically active fragment of Perturbagen F802 (FIG. 13(a)) displaying a shift in RA-correlated reporter expression.
- 27. The isolated polypeptide of claim 1 wherein said isolated polypeptide is a closely related analog of Perturbagen F802 (FIG. 13(a)) wherein said analog displays biological activity of a shift in RA-correlated reporter expression.
- 28. The isolated polypeptide of claim 1 wherein said isolated polypeptide is an antigenic analog of Perturbagen F802 (FIG. 13(a)) wherein said analog binds to an antibody specific for the polypeptide of Perturbagen F802 (FIG. 13(a)).
- 29. The isolated polypeptide of claim 1 wherein said isolated polypeptide is an N-terminal fragment of Perturbagen F802 (FIG. 13(a)).
- 30. The isolated polypeptide of claim 29 wherein said N-terminal fragment comprises at least 10 amino acids of Perturbagen F802 (FIG. 13(a)).
- 31. The isolated polypeptide of claim 1 wherein said isolated polypeptide is a C-terminal fragment of Perturbagen F802 (FIG. 13(a)).
- 32. The isolated polypeptide of claim 31 wherein said C-terminal fragment comprises at least 10 amino acids of Perturbagen F802 (FIG. 13(a)).
- 33. The isolated polypeptide of claim 1 consisting essentially of the sequence of Perturbagen F820 (FIG. 13(b)).
- 34. The isolated polypeptide of claim 3 wherein said isolated polypeptide comprises the amino acid sequence of Perturbagen F820 (FIG. 13(b)) except for one or more conservative amino acid substitutions.
- 35. The isolated polypeptide of claim 2 consisting of Perturbagen F820 (FIG. 13(b)).
- 36. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 99% identical to the amino acid sequence of Perturbagen F820 (FIG. 13(b)).
- 37. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 95% identical to the amino acid sequence of Perturbagen F820 (FIG. 13(b)).
- 38. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 90% identical to the amino acid sequence of Perturbagen F820 (FIG. 13(b)).
- 39. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 85% identical to the amino acid sequence of Perturbagen F820 (FIG. 13(b)).
- 40. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a sequence at least 80% identical to the amino acid sequence of Perturbagen F820 (FIG. 13(b)).
- 41. The isolated polypeptide of claim 1 wherein said isolated polypeptide comprises a biologically active fragment of sequence Perturbagen F820 (FIG. 13(b)) displaying a shift in RA-correlated reporter expression.
- 42. The isolated polypeptide of claim 1 wherein said isolated polypeptide is a closely related analog of Perturbagen F820 (FIG. 13(b)) wherein said analog displays biological activity of a shift in RA-correlated reporter expression.
- 43. The isolated polypeptide of claim 1 wherein said isolated polypeptide is an antigenic analog of Perturbagen F820 (FIG. 13(b)) wherein said analog binds to an antibody specific for the polypeptide of Perturbagen F820 (FIG. 13(b)).
- 44. The isolated polypeptide of claim 1 wherein said isolated polypeptide is an N-terminal fragment of Perturbagen F820 (FIG. 13(b)).
- 45. The isolated polypeptide of claim 44 wherein said N-terminal fragment comprises at least 10 amino acids of Perturbagen F820 (FIG. 13(b)).
- 46. The isolated polypeptide of claim 1 wherein said isolated polypeptide is a C-terminal fragment of Perturbagen F820 (FIG. 13(b)).
- 47. The isolated polypeptide of claim 46 wherein said C-terminal fragment comprises at least 10 amino acids of Perturbagen F820 (FIG. 13(b)).
- 48. The polypeptide of claim 1 wherein said polypeptide is fused to heterologous sequence.
- 49. The polypeptide of claim 48 wherein said heterologous sequence is a scaffold.
- 50. The polypeptide of claim 49 wherein said scaffold is a fluorescent protein.
- 51. The polypeptide of claim 1 wherein said polypeptide is chemically modified.
- 52. The polypeptide of claim 51 wherein said polypeptide is radio labeled.
- 53. The polypeptide of claim 51 wherein said modification is selected from the group consisting of acetylation, glycosylation, or fluorescent tagging.
- 54. The polypeptide of claim 1 wherein said polypeptide is chemically synthesized.
- 55. An isolated polynucleotide encoding a polypeptide of claim 1.
- 56. The isolated polynucleotide of claim 55, wherein said polypeptide encodes sequences (a) (b) or (c).
- 57. An isolated polynucleotide encoding a polypeptide of claim 3, 18 or 33.
- 58. An isolated polynucleotide encoding a polypeptide of claim 4, 19 or 34.
- 59. An isolated polynucleotide encoding a polypeptide of claim 5, 20 or 35.
- 60. An isolated polynucleotide encoding a polypeptide of claim 6, 21 or 36.
- 61. An isolated polynucleotide encoding a polypeptide of claim 7, 22 or 37.
- 62. An isolated polynucleotide encoding a polypeptide of claim 8, 23 or 38.
- 63. An isolated polynucleotide encoding a polypeptide of claim 9, 24 or 39.
- 64. An isolated polynucleotide encoding a polypeptide of claim 10, 25 or 40.
- 65. An isolated polynucleotide encoding a polypeptide of claim 14, 29 or 44.
- 66. An isolated polynucleotide encoding a polypeptide of claim 16, 31 or 46.
- 67. An isolated polynucleotide comprising the DNA sequence selected from a group consisting of:
(a) Perturbagen R3 (FIG. 15(b)); (b) Perturbagen F802 (FIG. 13(a)); and (c) Perturbagen F820 (FIG. 13(b)).
- 68. An isolated polynucleotide of claim 67 wherein said isolated polynucleotide is (a).
- 69. An isolated polynucleotide of claim 67 wherein said isolated polynucleotide is (b).
- 70. An isolated polynucleotide of claim 67 wherein said isolated polynucleotide is (c).
- 71. An isolated polynucleotide consisting essentially of the sequence of Perturbagen R3 (FIG. 15(b)).
- 72. An isolated polynucleotide consisting essentially of the sequence of Perturbagen F802 (FIG. 13(a)).
- 73. An isolated polynucleotide consisting essentially of the sequence of Perturbagen F820 (FIG. 13(b)).
- 74. The isolated polynucleotide of any one of claims 68, 69 or 70 wherein said isolated polynucleotide comprises a sequence at least 99% identical to said polynucleotide.
- 75. The isolated polynucleotide of any one of claims 68, 69 or 70 wherein said isolated polynucleotide comprises a sequence at least 95% identical to said polynucleotide.
- 76. The isolated polynucleotide of any one of claims 68, 69 or 70 wherein said isolated polynucleotide comprises a sequence at least 90% identical to said polynucleotide.
- 77. The isolated polynucleotide of any one of claims 68, 69 or 70 wherein said isolated polynucleotide comprises a sequence at least 85% identical to said polynucleotide.
- 78. The isolated polynucleotide of any one of claims 68, 69 or 70 wherein said isolated polynucleotide comprises a sequence at least 80% identical to said polynucleotide.
- 79. A vector comprising the polynucleotide of any one of claims 55, 56, 67, 71, 72 or 73.
- 80. The vector of claim 79, wherein said vector provides inducible expression.
- 81. A gene therapy vector comprising the polynucleotide of claims 55, 56, 67, 71, 72 or 73.
- 82. A host cell comprising the vector of claim 79.
- 83. A polynucleotide that hybridizes under stringent conditions to the polynucleotide of any one of claims 55, 56, 67, 71, 72 or 73.
- 84. A method for producing a RA pathway related polypeptide comprising culturing a population of host cells of claim 82 under conditions suitable for the expression of an encoded polypeptide and recovering expressed polypeptide from the host cell culture.
- 85. A composition comprising the polypeptide of claims 1, 2, 3, 18 or 33 in a pharmaceutically acceptable carrier.
- 86. An antibody to the polypeptide of claims 1, 2, 3, 18 or 33.
- 87. A method of identifying a cellular target that interacts with a RA pathway related polypeptide, comprising the steps of exposing a polypeptide of claim 1 to putative target molecules and identifying a polypeptide/target interaction pair.
- 88. The method of claim 87 wherein said step of exposing is performed in vitro and said step of identifying comprises detecting reporter expression, wherein said reporter expression is operatively linked to the formation of said interaction pair.
- 89. The method of claim 88 wherein said method is a yeast two-hybrid assay.
- 90. A method of screening for putative RA-related therapeutics, comprising the steps of:
a) exposing a polypeptide/target interaction pair obtained by the method of claim 87 to a plurality of agents; and b) recovering a subpopulation of disrupting agents which competitively displace said polypeptide from said target; wherein said disrupting agents are putative RA-related therapeutics.
- 91. The method of claim 90, wherein said plurality of agents is a combinatorial chemical library.
- 92. A method of treating an RA pathway related condition, comprising the step of administering a therapeutically effective amount of the polypeptide of claim 1, or a pharmaceutically acceptable salt thereof.
- 93. An isolated RA pathway polypeptide comprising the PAT1 polypeptide (FIG. 16(d).
- 94. An isolated RA pathway polypeptide consisting essentially of the PAT1 polypeptide (FIG. 16(d)).
- 95. The isolated polypeptide of claim 94 wherein said isolated polypeptide comprises the amino acid sequence of the PAT1 polypeptide (FIG. 16(d)) except for one or more conservative amino acid substitutions.
- 96. The isolated RA pathway polypeptide consisting of the PAT1 polypeptide (FIG. 16(d)).
- 97. The isolated polypeptide of claim 94 wherein said isolated polypeptide comprises a sequence at least 99% identical to the amino acid sequence of the PAT1 polypeptide (FIG. 16(d)).
- 98. The isolated polypeptide of claim 94 wherein said isolated polypeptide comprises a sequence at least 95% identical to the amino acid sequence of the PAT1 polypeptide (FIG. 16(d)).
- 99. The isolated polypeptide of claim 94 wherein said isolated polypeptide comprises a sequence at least 90% identical to the amino acid sequence of the PAT1 polypeptide (FIG. 16(d)).
- 100. The isolated polypeptide of claim 94 wherein said isolated polypeptide comprises a sequence at least 85% identical to the amino acid sequence of the PAT1 polypeptide (FIG. 16(d)).
- 101. The isolated polypeptide of claim 94 wherein said isolated polypeptide comprises a sequence at least 80% identical to the amino acid sequence of the PAT1 polypeptide (FIG. 16(d)).
- 102. An isolated polynucleotide encoding the polypeptide of claims 93, 94 or 96.
- 103. An isolated polynucleotide encoding the PAT1 polypeptide (FIG. 16(d)).
- 104. An isolated polynucleotide comprising the DNA sequence of PAT1 (FIG. 16 (c)).
- 105. An isolated polynucleotide consisting essentially of the DNA sequence of PAT1 (FIG. 16(c)).
- 106. An isolated polynucleotide consisting of the DNA sequence of PAT1 (FIG. 16 (c)).
- 107. A vector comprising the polynucleotide of claim 102.
- 108. A gene therapy vector comprising the polynucleotide of claim 102.
- 109. A host cell comprising the polynucleotide of claim 102.
- 110. A polynucleotide that hybridizes under stringent conditions to the polynucleotide of claim 102.
Parent Case Info
[0001] This application claims priority from, and is a continuation-in-part of, 08/812,994, now issued as U.S. Pat. No. 5,955,275, and U.S. application Ser. No. 60/249,768 (VEN007/00/P1, filed Nov. 17, 2000), the entire disclosures of which are specifically incorporated by reference herein in their entireties.
Provisional Applications (1)
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Number |
Date |
Country |
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60249468 |
Nov 2000 |
US |
Continuation in Parts (1)
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Number |
Date |
Country |
Parent |
08812994 |
Mar 1997 |
US |
Child |
09990747 |
Nov 2001 |
US |