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Calpain chronicle—an enzyme family under multidisciplinary characterization

机译:钙蛋白酶编年史—多学科表征下的酶家族

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摘要

Calpain is an intracellular Ca2+-dependent cysteine protease (EC 3.4.22.17; Clan CA, family C02) discovered in 1964. It was also called CANP (Ca2+-activated neutral protease) as well as CASF, CDP, KAF, etc. until 1990. Calpains are found in almost all eukaryotes and a few bacteria, but not in archaebacteria. Calpains have a limited proteolytic activity, and function to transform or modulate their substrates’ structures and activities; they are therefore called, “modulator proteases.” In the human genome, 15 genes—CAPN1, CAPN2, etc.—encode a calpain-like protease domain. Their products are calpain homologs with divergent structures and various combinations of functional domains, including Ca2+-binding and microtubule-interaction domains. Genetic studies have linked calpain deficiencies to a variety of defects in many different organisms, including lethality, muscular dystrophies, gastropathy, and diabetes. This review of the study of calpains focuses especially on recent findings about their structure–function relationships. These discoveries have been greatly aided by the development of 3D structural studies and genetic models.
机译:钙蛋白酶是一种细胞内Ca 2 + 依赖性半胱氨酸蛋白酶(EC 3.4.22.17; Clan CA,家族C02),于1964年发现。它也称为CANP(Ca 2 + )活化的中性蛋白酶)以及CASF,CDP,KAF等,直到1990年。钙蛋白酶几乎存在于所有真核生物和一些细菌中,而古细菌中则没有。钙蛋白酶的蛋白水解活性有限,其功能是改变或调节其底物的结构和活性。因此,它们被称为“调节蛋白酶”。在人类基因组中,CAPN1,CAPN2等15个基因编码钙蛋白酶样蛋白酶结构域。它们的产物是钙蛋白酶同系物,具有不同的结构和功能域的各种组合,包括Ca 2 + -结合域和微管相互作用域。遗传研究已将钙蛋白酶缺乏与许多不同生物体的多种缺陷相关联,包括致死性,肌肉营养不良,胃病和糖尿病。本文对钙蛋白酶的研究重点是关于其结构-功能关系的最新发现。 3D结构研究和遗传模型的发展极大地帮助了这些发现。

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