Structural Basis of Proline-Specific Exopeptidase Activity as Observed in Human Dipeptidyl Peptidase-IV

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• 作者：Thoma ; Ralf ; Lö ; ffler ; Bernd ; Stihle ; Martine ; Huber ; Walter ; Ruf ; Armin ; Hennig ; Michael
• 刊名：Structure
• 出版年：2003
• 出版时间：August, 2003
• 年：2003
• 卷：11
• 期：8
• 页码：947-959
• 全文大小：1.69 M

文摘

Inhibition of dipeptidyl peptidase IV (DPP-IV), the main glucagon-like peptide 1 (GLP1)-degrading enzyme, has been proposed for the treatment of type II diabetes. We expressed and purified the ectodomain of human DPP-IV in Pichia pastoris and determined the X-ray structure at 2.1 Å resolution. The enzyme consists of two domains, the catalytic domain, with an α/β hydrolase fold, and a β propeller domain with an 8-fold repeat of a four-strand β sheet motif. The β propeller domain contributes two important functions to the molecule that have not been reported for such structures, an extra β sheet motif that forms part of the dimerization interface and an additional short helix with a double Glu sequence motif. The Glu motif provides recognition and a binding site for the N terminus of the substrates, as revealed by the complex structure with diprotin A, a substrate with low turnover that is trapped in the tetrahedral intermediate of the reaction in the crystal.