Claims
- 1. A chimeric immunoglobulin (Ig) chain comprising an Ig heavy chain and a cytokine.
- 2. The chimeric Ig chain of claim 1, wherein the Ig heavy chain is joined at its carboxy-terminus by a peptide bond to the amino terminal amino acid of the cytokine.
- 3. The chimeric Ig chain of claim 1, wherein the Ig heavy chain comprises CH1, CH2, and CH3 domains.
- 4. The chimeric Ig chain of claim 1, wherein a proteolytic cleavage site is located between the Ig heavy chain and the cytokine.
- 5. The chimeric Ig chain of claim 1, wherein the variable region is derived from a mouse and the constant region is derived from a human antibody.
- 6. The chimeric Ig chain of claim 1, wherein the variable region of the Ig heavy chain is derived from an Ig specific for a cancer cell or a virus-infected cell.
- 7. The conjugate of claim 6, wherein the variable region is derived from an Ig specific for a tumor-associated antigen or a viral antigen.
- 8. The chimeric Ig chain of claim 1, wherein the cytokine is tumor necrosis factor alpha.
- 9. The chimeric Ig chain of claim 1, wherein the cytokine is interleukin-2.
- 10. The chimeric Ig chain of claim 1, wherein the cytokine is a lymphokine.
- 11. The chimeric Ig chain of claim 10, wherein the lymphokine is a lymphotoxin.
- 12. The chimeric Ig chain of claim 10, wherein the lymphokine is granulocyte-macrophage colony stimulating factor.
- 13. The chimeric Ig chain of claim 10, wherein the lymphokine is a protein which forms a dimeric or multimeric structure.
- 14. A chimeric immunoglobulin (Ig) chain comprising an Ig heavy chain having a variable region specific for a target cell antigen and a heavy chain including CH1, CH2, and CH3 domains, joined, through a peptide bond, to the amino terminus amino acid of a cytokine.
- 15. The chimeric Ig chain of claim 14, wherein the cytokine is selected from the group consisting of lymphotoxin, interleukin-2, tumor necrosis factor, and granulocyte-macrophage colony stimulating factor.
- 16. A cytokine immunoconjugate comprising:
(a) a chimeric immunoglobulin (Ig) chain including an Ig heavy chain having a variable region specific for a cancer cell or virus-infected cell, joined at the carboxy-terminus of its constant region by a peptide bond to a cytokine; and (b) an Ig light chain having a variable region specific for the cancer or virus-infected cell, said heavy and light chains forming a functional antigen-binding site.
- 17. The immunoconjugate of claim 16, wherein the chimeric heavy chain has a constant region comprising CH1, CH2, and CH3 domains.
- 18. The immunoconjugate of claim 16, wherein the cytokine is interleukin-2.
- 19. The immunoconjugate of claim 16, wherein the cytokine is tumor necrosis factor alpha.
- 20. The immunoconjugate of claim 16, wherein the cytokine is a lymphokine.
- 21. The immunoconjugate of claim 20, wherein the lymphokine is lymphotoxin.
- 22. The immunoconjugate of claim 20, wherein the lymphokine is granulocyte-macrophage stimulating factor.
- 23. A nucleic acid encoding a chimeric immunoglobulin (Ig) chain comprising an Ig heavy chain and a cytokine.
- 24. The nucleic acid of claim 23 which is DNA.
- 25. The nucleic acid of claim 23, wherein the Ig heavy chain comprises CH1, CH2, and CH3 domains.
- 26. The nucleic acid of claim 23, wherein the variable region is derived from an Ig specific for a cancer cell or a virus-infected cell.
- 27. The nucleic acid of claim 26, wherein the variable region is derived from an Ig specific for a tumor-associated antigen or a viral antigen.
- 28. The nucleic acid of claim 23, wherein a proteolytic cleavage site is located between the Ig heavy chain and the cytokine.
- 29. The nucleic acid of claim 23, wherein the variable region is derived from a mouse antibody and the constant region is derived from a human antibody.
- 30. The nucleic acid of claim 23, wherein the cytokine is interleukin-2.
- 31. The nucleic acid of claim 23, wherein the cytokine is tumor necrosis factor alpha.
- 32. The nucleic acid of claim 23, wherein the cytokine is a lymphokine.
- 33. The nucleic acid of claim 32, wherein the lymphokine is a protein which forms a dimeric or multimeric structure.
- 34. The nucleic acid of claim 32, wherein the lymphokine is a lymphotoxin.
- 35. The nucleic acid of chain 32, wherein the lymphokine is granulocyte-macrophage colony stimulating factor.
- 36. A recombinant DNA encoding a chimeric immunoglobulin (Ig) chain, comprising an Ig heavy chain having a variable region specific for a target cell antigen and heavy chain having CH1, CH2 and CH3 domain, joined, through a peptide bond, to the amino terminal amino acid of a cytokine.
- 37. The DNA construct of claim 35, wherein the cytokine is selected from the group consisting of tumor necrosis factor alpha, interleukin-2, lymphotoxin, and granulocyte-macrophage colony stimulating factor.
- 38. A cell line transfected with the nucleic acid of claim 23.
- 39. A cell line transfected with the nucleic acid of claim 36.
- 40. A cell line of claim 23 which is a myeloma cell line.
- 41. A cell line of claim 36 which is a myeloma cell line.
- 42. A method of selectively delivering a cytokine to a target cell, comprising:
(a) providing a cytokine immunoconjugate including:
a chimeric immunoglobulin (Ig) chain comprising an Ig heavy chain having a variable region specific for the target cell joined at the carboxy terminus of its constant region by a peptide bond to a cytokine, and an Ig light chain combined with the chimeric Ig heavy chain, forming a functional antigen-binding site; and (b) administering to a subject harboring the target cell an amount of the immunoconjugate sufficient to reach the target cell.
- 43. The method of claim 42 wherein said target cell is a cancer cell or a virus-infected cell.
- 44. The method of claim 42, wherein the chimeric heavy chain has a constant region comprising CH1, CH2, and CH3 domains.
- 45. The method of claim 42, wherein the cytokine is selected from the group consisting of lymphotoxin, interleukin-2, tumor necrosis factor alpha, and granulocyte-macrophage colony stimulating factor.
Parent Case Info
[0001] This application is a continuation-in-part of copending application Ser. No. 612,099, filed Nov. 9, 1990, the disclosure of which is incorporated herein by reference.
Continuations (4)
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Continuation in Parts (1)
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