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源自蛇毒蛋白黏附结构域的合成RGD肽:作为血小板聚集抑制剂的评估

Synthetic RGD peptides derived from the adhesive domains of snake-venom proteins: evaluation as inhibitors of platelet aggregation.

作者信息

Lu X, Deadman J J, Williams J A, Kakkar V V, Rahman S

机构信息

Protein Biochemistry Section, Thrombosis Research Institute, London, U.K.

出版信息

Biochem J. 1993 Nov 15;296 ( Pt 1)(Pt 1):21-4. doi: 10.1042/bj2960021.

Abstract

Synthetic peptides based on the RGD domains of the potent platelet aggregation inhibitors kistrin and dendroaspin were generated. The 13-amino-acid peptides were synthesized as dicysteinyl linear and disulphide cyclic forms. In platelet-aggregation studies, the cyclic peptides showed 3-fold better inhibition than their linear equivalents and approx. 100-fold greater potency than synthetic linear RGDS peptides derived from fibronectin. An amino acid substitution, Asp10-->Ala, in the kistrin-based peptide gave a 4-fold decrease in potency in the linear peptide, but produced a 2-fold elevation in the inhibitory activity of the cyclic form, generating a peptide of potency comparable with that of the parent protein.

摘要

基于强效血小板聚集抑制剂水蛭素和树眼镜蛇毒素的RGD结构域合成了合成肽。这些13个氨基酸的肽被合成为双半胱氨酰线性和二硫键环化形式。在血小板聚集研究中,环化肽的抑制作用比其线性对应物强3倍,并且比源自纤连蛋白的合成线性RGDS肽的效力大约高100倍。基于水蛭素的肽中一个氨基酸取代,即Asp10→Ala,使线性肽的效力降低了4倍,但使环化形式的抑制活性提高了2倍,产生了一种效力与亲本蛋白相当的肽。

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