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用于纯化类胰蛋白酶的新型亲和吸附剂的设计

Design of novel affinity adsorbents for the purification of trypsin-like proteases.

作者信息

Burton N P, Lowe C R

机构信息

Institute of Biotechnology, University of Cambridge, UK.

出版信息

J Mol Recognit. 1992 Jun;5(2):55-68. doi: 10.1002/jmr.300050203.

Abstract

A number of ligands for the selective purification by affinity chromatography of the trypsin-like protease, porcine pancreatic kallikrein, were designed de novo by computer-aided molecular design. The ligands were designed to mimic the side-chains of a number of arginyl dipeptides and included a benzamidine moiety substituted on a triazine ring. The ligands displayed inhibitory activities against pancreatic kallikrein which mirrored the specificity constants of the dipeptides they were designed to mimic. The ligand with the highest affinity for the enzyme, an analogue of a Phe-Arg dipeptide, when immobilized to Sepharose CL-4B via a hexamethylene spacer arm, purified pancreatic kallikrein 110-fold in one step from a crude pancreatic acetone extract.

摘要

通过计算机辅助分子设计从头设计了多种用于亲和色谱法选择性纯化类胰蛋白酶——猪胰激肽释放酶的配体。这些配体被设计成模拟多种精氨酰二肽的侧链,并包含一个在三嗪环上取代的苯甲脒部分。这些配体对胰激肽释放酶表现出抑制活性,反映了它们被设计模拟的二肽的特异性常数。对该酶具有最高亲和力的配体,即苯丙氨酸 - 精氨酸二肽的类似物,当通过六亚甲基间隔臂固定到琼脂糖凝胶CL - 4B上时,可从粗制的胰腺丙酮提取物中一步将胰激肽释放酶纯化110倍。

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