Claims
- 1. A packaging cell line capable of complementing recombinant adenoviruses of a subgroup other than subgroup C wherein said packaging cell line expresses an E1 sequence derived from a serotype different from the serotype of said recombinant adenovirus.
- 2. The packaging cell line of claim 1 wherein said cell line expresses E1A or a fragment thereof.
- 3. The packaging cell line of claim 1 wherein said cell line expresses E1B or a fragment thereof.
- 4. A packaging cell line capable of complementing recombinant adenovirus derived from subgroup B, said cell line expressing E1A or a fragment thereof, and at least part of a serotype-specific E1B sequence derived from a different serotype than said E1A or fragment thereof.
- 5. The packaging cell line of claim 4 wherein said at least part of a serotype-specific E1B sequence is driven by a heterologous promoter.
- 6. The packaging cell line of claim 4 wherein said at least part of a serotype-specific E1B is terminated by a heterologous poly-adenylation signal.
- 7. The packaging cell line of claim 4 wherein said at least part of a serotype-specific E1B is E1B-55K.
- 8. The packaging cell line of claim 4 wherein said at least part of a serotype-specific E1B is E1B-21K.
- 9. The packaging cell line of claim 1 wherein said cell line is derived from primary, diploid human cells, said primary diploid human cells being transformed by adenovirus E1 sequences either operatively linked on one DNA molecule or located on two separate DNA molecules, said sequences being operatively linked to regulatory sequences enabling transcription and translation of encoded proteins.
- 10. The packaging cell line of claim 9 wherein the primary, diploid human cells are selected from the group consisting of primary human retinoblasts, primary human embryonic kidney cells and primary human amniocytes.
- 11. The packaging cell line of claim 9 wherein the primary, diploid human cells are transfected with the adenovirus E1A gene to induce unlimited proliferation.
- 12. The packaging cell line of claim 11 wherein said cells co-express the E1B gene.
- 13. The packaging cell line of claim 9, wherein the primary, diploid human cells are transformed by expression of adenovirus E1 proteins of a subgroup other than subgroup C.
- 14. The packaging cell line of claim 13 wherein the subgroup is adenoviral subgroup B.
- 15. The packaging cell line of claim 9 wherein the primary diploid human cells are transformed by adenovirus E1 sequences located on two separate DNA molecules wherein one DNA molecule carries at least part of the E1 sequences of the serotype enabling efficient transformation and the second DNA molecule carries at least part of the sequences necessary for serotype-specific complementation.
- 16. A method of making a packaging cell line capable of complementing recombinant adenoviruses of a subgroup other than subgroup C, said method comprising:
expressing in a packaging cell an E1 sequence derived from a serotype other than a serotype of subgroup C.
- 17. The method according to claim 15, wherein said packaging cell expresses E1A.
- 18. The method according to claim 15, wherein said packaging cell expresses E1B.
- 19. The method according to claim 15, further comprising:
expressing E4-ORF6 of a serotype other than a serotype of subgroup C.
- 20. A process for producing a packaging cell line capable of complementing recombinant subgroup B adenovirus comprising:
transforming a cell with at least one nucleic acid molecule comprising at least a part of an E1 sequence; expressing in said transformed cell E1A sequence or a fragment thereof having E1A complementing activity; and expressing in said transformed cell at least a part of a serotype-specific E1B sequence derived from a different serotype than said E1A sequence or fragment thereof to produce a cell line capable of complementing recombinant adenovirus.
- 21. The process of claim 20, wherein expression of said at least apart of a serotype-specific E1B sequence is driven by a heterologous promoter.
- 22. The process of claim 20, wherein expression of said at least apart of a serotype-specific E1B sequence is terminated by a heterologous poly-adenylation signal.
- 23. The process of claim 20, wherein said at least a part of a serotype-specific E1B is E1B-55K.
- 24. A process of producing a packaging cell line comprising:
transforming primary, diploid human cells with an E1A sequence or a fragment thereof having E1A complementing activity and at least apart of a serotype-specific E1B sequence derived from a different serotype than said E1A sequence or fragment thereof having E1B complementing activity; enabling transcription of said E1A sequence or fragment thereof and said at least a part of a serotype-specific E1B; and enabling translation of the E1A transcription product or fragment thereof and said at least a part of a serotype-specific E1B transcription product of the previous step thus, producing a packaging cell line.
- 25. The process of claim 24, wherein the primary, diploid human cells are selected from the group consisting of primary human retinoblasts, primary human embryonic kidney cells and primary human amniocytes.
- 26. The process of claim 24, wherein at least a part of a serotype-specific E1B sequence is of a serotype of a subgroup other than subgroup C.
- 27. The process of claim 26, wherein said at least a part of a serotype-specific E1B sequence is of a serotype of subgroup B.
- 28. The process of claim 24, wherein said E1A sequence or fragment thereof and at least a part of a serotype-specific E1B sequence are located on two separate nucleic acid molecules.
- 29. A packaging cell line produced by the process of any one of claims 16-28.
- 30. A process of producing a recombinant adenovirus of a subgroup other than subgroup C, said process comprising:
expressing in a cell an E1 sequence of a serotype different from said recombinant adenovirus; introducing a genome sequence of said recombinant adenovirus into said cell, wherein said genome sequence lacks a functional E1 sequence; allowing replication of said genome sequence; allowing expression of proteins encoded by said genome sequence; and allowing packaging of the replicated genome sequences thus, producing a recombinant adenovirus.
- 31. The process of claim 30, further comprising:
harvesting said produced recombinant adenovirus.
- 32. The process of claim 30, wherein the recombinant adenovirus contains a heterologous nucleic acid sequence of interest.
- 33. The process of claim 30, wherein said E1 sequence is operably linked to a heterologous poly-adenylation signal and/or a heterologous promoter.
- 34. The process of claim 30, wherein said E1 sequence expresses E1B-21K and/or E1B-55K protein.
- 35. The process of claim 30, wherein said E1 sequence comprises an E1A sequence or a fragment thereof having E1A complementing activity, of a serotype different from said recombinant adenovirus, and at least a part of a serotype-specific E1B sequence of a different serotype than said E1A sequence.
- 36. The process of claim 35, wherein said recombinant adenovirus is Ad35 or Ad11.
- 37. The process of claim 35, wherein at least a part of a serotype-specific E1B sequence is of a serotype of a subgroup other than subgroup C
- 38. The process of claim 35, wherein said at least a part of a serotype-specific E1B sequence is of a serotype of subgroup B.
CROSS-REFERENCE TO RELATED APPLICATIONS
[0001] This application is a continuation of application Ser. No. 09/713,678, filed Nov. 15, 2000, pending (the contents of the entirety of which are incorporated by this reference), now U.S. Pat. No. ______, which is a continuation-in-part of application Ser. No. 09/573,740, filed May 18, 2000, pending, which claims benefit, under 35 U.S.C. § 119(e), of the filing date of U.S. Provisional Application Serial No. 60/134,764, filed May 18, 1999.
Provisional Applications (1)
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Number |
Date |
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|
60134764 |
May 1999 |
US |
Continuations (1)
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Number |
Date |
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Parent |
09713678 |
Nov 2000 |
US |
Child |
10272041 |
Oct 2002 |
US |
Continuation in Parts (1)
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Number |
Date |
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Parent |
09573740 |
May 2000 |
US |
Child |
09713678 |
Nov 2000 |
US |