Claims
- 1. A DNA molecule encoding an insulin precursor having the formula
- B(1-29) -X.sub.1 --X.sub.2 --Y.sub.2 --Y.sub.1 --A(1-21)
- wherein B(1-29) are the 29 first amino acid residues of the B chain of human insulin starting from the N-terminum, A(1-21) are the 21 amino acid residues of the A chain of human insulin, X.sub.1 represents a peptide bond or one naturally-occurring alpha-amino acid residue, X.sub.2 represents Glu or Asp, and Y.sub.1 and Y.sub.2 each represents Lys or Arg, the positions A6 and A11, A7 and B7 and A20 and B19, respectively, are connected through sulphur bridges, and, optionally, one or more of the glutamic acid residues in positions A4, A17, B13 and B21 are substituted by another naturally-occurring alpha-amino acid residue having an uncharged side chain.
- 2. A DNA molecule, as claimed in claim 1, wherein one or more of the glutamic acid residues in the positions A4, A17, B13 and B21 of said insulin precursor are substituted by another naturally-occurring alpha amino acid residue having an uncharged side chain.
- 3. A replicable plasmid containing the DNA molecule of claim 1.
- 4. A DNA sequence encoding an insulin precursor having the formula
- B(1-29l)-Asp-Lys-Arg-A(1-21)
- wherein B(1-29) are the 29 first amino acid residues of the B chain of human insulin starting from the N-terminus, A(1-21) are the 21 amino acid residues of the A chain of human insulin, the positions A6 and A11, A7 and B7 and A20 and B19, respectively, are connected through sulphur bridges, and, optionally, one or more of the glutamic acid residues in the positions A4, A7, B13 and B21 are substituted by another naturally-occurring alpha-amino acid residue having an uncharged side chain.
- 5. A DNA molecule of claim 4, wherein one or more of the glutamic acid residues in the positions A4, A17, B13 and B21 are substituted by another naturally-occurring alpha-amino acid residue having an uncharged side chain.
- 6. A DNA molecule encoding an insulin precursor having the formula
- B(1-29)-Glu-Lys-Arg-A(1-21)
- wherein B(1-29) are the 29 first amino acid residues of the B chain of human insulin starting from the N-terminus, A(1-21) are the 21 amino acid residues of the A chain of human insulin, the positions A6 and A11, A7 and B7 and A20 and B19, respectively, are connected through sulphur bridges, and, optionally, one or more of the glutamic acid residues in the positions A4, A7, B13 and B21 are substituted by another naturally-occurring alpha-amino acid residue having an uncharged side chain.
- 7. A DNA molecule of claim 6, wherein one or more of the glutamic acid residues in the positions A4, A17, B13 and B21 are substituted by another naturally-occurring alpha-amino acid residue having an uncharged side chain.
- 8. A process for the production of an insulin precursor having the formula
- B(1-29)-X.sub.1 --X.sub.2 --Y.sub.2 --Y.sub.1 --A(1-21)
- wherein B(1-29) are the 29 first amino acid residues of the B chain of human insulin starting from the N-terminus, A(1-21) are the 21 amino acid residues of the A chain of human insulin, X.sub.1 represents a peptide bond or one naturally-occurring alpha-amino acid residue, X.sub.2 represents Glu or Asp, and Y.sub.1 and Y.sub.2 each represents Lys or Arg, the positions A6 and A11, A7 and B7 and A20 and B19, respectively, are connected through sulphur bridges, and, optionally, one or more of the glutamic acid residues in positions A4, A17, B13 and B21 are substituted by another amino acid residue having an uncharged side chain, said process comprising culturing a yeast strain transformed with a replicable plasmid comprising a DNA sequence encoding said insulin precursor operably linked to a signal peptide, in a suitable culture medium to which said insulin precursor is secreted and isolating said insulin precursor from said culture medium.
- 9. A process as claimed in claim 8, which further comprises converting said precursor, optionally after isolation, into des(B30) insulin by tryptic digestion.
- 10. A process as claimed in claim 8, which further comprises converting said precursor into human insulin or an insulin analog by enzymatic treatment.
Priority Claims (1)
Number |
Date |
Country |
Kind |
3361/88 |
Jun 1988 |
DKX |
|
Parent Case Info
This is a division of co-pending application Ser. No. 623,739, filed as PCT/DK89/00152, Jan. 19, 1989, now U.S. Pat. No. 5,202,415.
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4916212 |
Markussen et al. |
Apr 1990 |
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Number |
Date |
Country |
0037255 |
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EPX |
195691 |
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EPX |
Divisions (1)
|
Number |
Date |
Country |
Parent |
623739 |
Dec 1990 |
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