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靶向酶原激活以控制糜蛋白酶原-前列腺蛋白酶的蛋白水解级联反应。

Targeting zymogen activation to control the matriptase-prostasin proteolytic cascade.

机构信息

School of Pharmacy, University of Maryland, Baltimore, MD 21201, USA.

出版信息

J Med Chem. 2011 Nov 10;54(21):7567-78. doi: 10.1021/jm200920s. Epub 2011 Oct 12.

Abstract

Membrane-associated serine protease matriptase has been implicated in human diseases and might be a drug target. In the present study, a novel class of matriptase inhibitors targeting zymogen activation is developed by a combination of the screening of compound library using a cell-based matriptase activation assay and a computer-aided search of commercially available analogues of a selected compound. Four structurally related compounds are identified that can inhibit matriptase activation with IC(50) at low micromolar concentration in both intact-cell and cell-free systems, suggesting that these inhibitors target the matriptase autoactivation machinery rather than the intracellular signaling pathways. These activation inhibitors can also inhibit prostasin activation, a downstream event that occurs in lockstep with matriptase activation. In contrast, the matriptase catalytic inhibitor CVS-3983 at a concentration 300-fold higher than its K(i) fails to inhibit activation of either protease. Our results suggest that inhibiting matriptase activation is an efficient way to control matriptase function.

摘要

膜相关丝氨酸蛋白酶组织蛋白酶 H 已被牵涉到人类疾病中,并且可能是一个药物靶点。在本研究中,通过使用基于细胞的组织蛋白酶 H 激活测定法对化合物文库进行筛选,以及对选定化合物的市售类似物进行计算机辅助搜索,开发了一种针对酶原激活的新型组织蛋白酶 H 抑制剂。鉴定出四种结构相关的化合物,它们能够以低微摩尔浓度在完整细胞和无细胞系统中抑制组织蛋白酶 H 的激活,这表明这些抑制剂针对的是组织蛋白酶 H 的自动激活机制,而不是细胞内信号通路。这些激活抑制剂还可以抑制前激肽释放酶的激活,这是与组织蛋白酶 H 激活同步发生的下游事件。相比之下,组织蛋白酶 H 催化抑制剂 CVS-3983 的浓度比其 K(i)高 300 倍,也不能抑制这两种蛋白酶的激活。我们的结果表明,抑制组织蛋白酶 H 的激活是控制组织蛋白酶 H 功能的有效方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d887/3214968/6c230c923437/nihms-332152-f0001.jpg

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