Biochemical and structural insights into mesotrypsin: an unusual human trypsin.

Moh'd A Salameh, Evette S Radisky
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Abstract

Thirty five years ago mesotrypsin was first isolated from the human pancreas. It was described as a minor trypsin isoform with the remarkable property of near total resistance to biological trypsin inhibitors. Another unusual feature of mesotrypsin was discovered later, when it was found that mesotrypsin has defective affinity toward many protein substrates of other trypsins. As the younger sibling of the two major trypsins secreted by the pancreas, cationic and the anionic trypsin, it has been speculated to represent an evolutionary waste with no apparent function. We know now that mesotrypsin is functionally very different from the other trypsins, with novel substrate specificity that hints at distinct physiological functions. Recently, evidence has begun to emerge implicating mesotrypsin in direct involvement in cancer progression. This review will explore the biochemical characteristics of mesotrypsin and structural insights into its specificity, function, and inhibition.

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中胰蛋白酶:一种不寻常的人类胰蛋白酶。
35年前,中胰蛋白酶首次从人类胰腺中分离出来。它被描述为一种次要的胰蛋白酶异构体,具有对生物胰蛋白酶抑制剂几乎完全耐药的显著特性。中胰蛋白酶的另一个不寻常的特征是后来发现的,当时发现中胰蛋白酶对其他胰蛋白酶的许多蛋白质底物具有缺陷的亲和力。作为胰腺分泌的两种主要胰蛋白酶(阳离子胰蛋白酶和阴离子胰蛋白酶)的弟妹,它被推测为一种没有明显功能的进化废物。我们现在知道中胰蛋白酶在功能上与其他胰蛋白酶非常不同,具有新的底物特异性,暗示着不同的生理功能。最近,有证据表明中胰蛋白酶直接参与癌症的进展。本文将探讨中胰蛋白酶的生化特性及其特异性、功能和抑制的结构见解。
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