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肽中的脯氨酸基序及其生物加工过程。

Proline motifs in peptides and their biological processing.

作者信息

Vanhoof G, Goossens F, De Meester I, Hendriks D, Scharpé S

机构信息

Department of Clinical Biochemistry, University of Antwerp, Wilrijk, Belgium.

出版信息

FASEB J. 1995 Jun;9(9):736-44.

PMID:7601338
Abstract

Many biologically important peptide sequences contain proline. It confers unique conformational constraints on the peptide chain in that the side-chain is cyclized back onto the backbone amide position. Inside an alpha-helix the possibility of making hydrogen bonds to the preceding turn is lost and a kink will be introduced. The conformational restrictions imposed by proline motifs in a peptide chain appear to imply important structural or biological functions as can be deduced from their often remarkably high degree of conservation as found in many proteins and peptides, especially cytokines, growth factors, G-protein-coupled receptors, V3 loops of the HIV envelope glycoprotein gp 120, and neuro- and vasoactive peptides. Only a limited number of peptidases are known to be able to hydrolyze proline adjacent bonds. Their activity is influenced by the isomeric state (cis-trans) as well as the position of proline in the peptide chain. The three proline specific metallo-peptidases (aminopeptidase P, carboxypeptidase P and prolidase) are activated by Mn2+, whereas the three serine type peptidases cleaving a post proline bond (prolyl oligopeptidase, dipeptidyl peptidase IV, and prolylcarboxypeptidase) share the sequential order of the catalytic Ser-Asp-His triade, which differentiates them from the chymotrypsin (His-Asp-Ser) and subtilisin (Asp-His-Ser) families. An endo or C terminal Pro-Pro bond and an endo pre-Pro peptide bond possess a high degree of resistance to any mammalian proteolytic enzyme.

摘要

许多具有生物学重要性的肽序列都含有脯氨酸。它赋予肽链独特的构象限制,因为其侧链环化回到主链酰胺位置。在α-螺旋内部,与前一圈形成氢键的可能性丧失,并且会引入一个扭结。肽链中脯氨酸基序所施加的构象限制似乎暗示着重要的结构或生物学功能,这可以从它们在许多蛋白质和肽中经常具有的高度保守性推断出来,特别是细胞因子、生长因子、G蛋白偶联受体、HIV包膜糖蛋白gp 120的V3环以及神经和血管活性肽。已知只有有限数量的肽酶能够水解脯氨酸相邻的键。它们的活性受异构体状态(顺式-反式)以及脯氨酸在肽链中的位置影响。三种脯氨酸特异性金属肽酶(氨肽酶P、羧肽酶P和脯氨酰肽酶)由Mn2+激活,而三种切割脯氨酸后键的丝氨酸型肽酶(脯氨酰寡肽酶、二肽基肽酶IV和脯氨酰羧肽酶)共享催化性丝氨酸-天冬氨酸-组氨酸三联体的顺序,这使它们与胰凝乳蛋白酶(组氨酸-天冬氨酸-丝氨酸)和枯草杆菌蛋白酶(天冬氨酸-组氨酸-丝氨酸)家族区分开来。一个内部或C末端的脯氨酸-脯氨酸键以及一个内部的脯氨酸前肽键对任何哺乳动物蛋白水解酶都具有高度抗性。

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