Synthesis of vasoactive intestinal peptide (VIP) via the mixed anhydride method |
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Authors: | W M Schaaper H C Beyerman |
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Affiliation: | Laboratory of Organic Chemistry, Delft University of Technology Julianalaan 136, 2628 BL Delft, The Netherlands |
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Abstract: | Porcine VIP was synthesized from three segments. The segments, VIP(1-6), VIP(7-13), and VIP(14-28), were synthesized via the Repetitive Excess Mixed Anhydride (REMA) method. The low solubility of the C-terminal segment was greatly improved by a temporary substitution of Asn28 by a beta-t-butyl aspartic acid ester. The segments VIP(1-6) and VIP(7-13) were purified by HPLC and coupled via the mixed anhydride method. The product was purified by gel filtration. VIP was synthesized from VIP(1-13) and VIP(14-28) by the same procedure. After deprotection, Met17-sulfoxide reduction, and purification by ion-exchange chromatography, the product was found to have the expected amino acid composition and biological potency. A HPLC purified sample was compared with several commercial preparations of varying purity. |
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Keywords: | Vasoactive intestinal peptide Peptide synthesis Mixed anhydride method |
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