Claims
- 1. A DNA construct which comprises a nucleotide sequence that encodes a protein complex having human Factor VIII:C activity, said complex comprising a first polypeptide homologous to the A domain of human Factor VIII:C linked to a second polypeptide homologous to the C domain of human Factor VIII:C by a polypeptide spacer, wherein the polypeptide spacer comprises a first amino acid sequence homologous to a human Ig heavy chain hinge region.
- 2. The DNA construct of claim 1, wherein the Ig heavy chain hinge region comprises an amino acid sequence Pro-Pro-Thr-Pro-Pro-Thr.
- 3. The DNA construct of claim 2, wherein said first polypeptide comprises at least about 90% of the amino acid sequence of human Factor VIII:C amino acids 1-740 and said second polypeptide comprises at least about 90% of the amino acid sequence of human Factor VIII:C amino acids 1649-2332.
- 4. The DNA construct of claim 3, further comprising control sequences capable of directing the expression of said protein complex when said DNA construct is present in a eukaryotic host cell.
- 5. A host mammalian cell containing the DNA construct of claim 4.
- 6. The DNA construct of claim 1, further comprising control sequences capable of directing the expression of said protein complex when said DNA construct is present in a eukaryotic host cell.
- 7. A host mammalian cell containing the DNA construct of claim 6.
- 8. The DNA construct of claim 1, wherein the polypeptide spacer further comprises second and third amino acid sequences, wherein the second amino acid sequence is homologous to an N-terminal region of the B domain of human Factor VIII:C and the third amino acid sequence is homologous to a C-terminal region of the B domain of human Factor VIII:C, and further wherein the second and third amino acid sequences are linked by the first amino acid sequence.
- 9. The DNA construct of claim 1, wherein the polypeptide spacer comprises second and third amino acid sequences, wherein the second amino acid sequence is homologous to an N-terminal region of the B domain of Factor VIII:C and the third amino acid sequence is homologous to a C-terminal region of the B domain of human Factor VIII:C, and wherein the second and third amino acid sequences are linked by the first amino acid sequence, wherein the first amino acid sequence is homologous to a human IgA heavy chain hinge region.
- 10. A method for producing a recombinant protein complex having human Factor VIII:C activity, said method comprising expressing in a eukaryotic transformant host cell, a DNA construct encoding said protein complex joined in reading frame with control sequences providing for the expression of said DNA construct in said host cell, wherein said DNA construct comprises a nucleotide sequence that encodes a first polypeptide homologous to the A domain of human Factor VIII:C linked to a second polypeptide homologous to the C domain of human Factor VIII:C by a polypeptide spacer, wherein the polypeptide spacer comprises an amino acid sequence homologous to a human Ig heavy chain hinge region.
- 11. A method according to claim 10, wherein not more than about 5 number % of the amino acids of said first and second polypeptides differ from the naturally occurring amino acid sequences of the Factor VIII:C A and C domains, respectively.
- 12. A method according to claim 10, wherein the amino acid sequence of the second polypeptide is the same as the amino acid sequence of amino acids 1649-2322 of human Factor VIII:C.
- 13. The method of claim 1, wherein the amino acid sequence of the first polypeptide is the same as the amino acid sequence of amino acids 1-740 of human Factor VIII:C.
- 14. The method of claim 10 wherein the Ig heavy chain hinge region comprises an amino acid sequence Pro-Pro-Thr-Pro-Pro-Thr.
CROSS-REFERENCE TO RELATED APPLICATION
This application is a continuation of application Ser. No. 07/652,099, filed on Feb. 7, 1991, now abandoned, which is a continuation-in-part of application Ser. No. 07/051,916, filed on May 19, 1987, now abandoned, which is a continuation-in-part of Ser. No. 06/822,989, filed on Jan. 27, 1986 (now abandoned).
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Continuations (1)
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Continuation in Parts (2)
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