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激素原转化酶在胰岛素生物合成中的作用:人类和实验动物中其作用存在遗传性缺陷的证据。

The role of prohormone convertases in insulin biosynthesis: evidence for inherited defects in their action in man and experimental animals.

作者信息

Steiner D F, Rouillé Y, Gong Q, Martin S, Carroll R, Chan S J

机构信息

Howard Hughes Medical Institute, Chicago, Illinois 60637, USA.

出版信息

Diabetes Metab. 1996 Apr;22(2):94-104.

PMID:8792089
Abstract

The hormone insulin remains the cornerstone of diabetic therapy since it is required for almost all cases of Type 1 and many cases of Type 2 diabetes. Since the discovery of insulin in 1921, much has been learned about its chemistry, structure and action as well as its production in the beta cell. Insulin is formed through a series of precursors, beginning with preproinsulin, the protein encoded in the insulin gene. These precursors direct the prohormone into the secretory pathway and ultimately into the secretory granules where it is converted into insulin and C-peptide. These products are stored and secreted together in a highly regulated manner in response to glucose and other stimuli. This review focuses on the recently discovered prohormone convertases, PC2 and PC3 (PC1), the enzymes responsible for the endoproteolytic processing of proinsulin to insulin and C-peptide in the beta cell as well as for the selective processing of proglucagon to glucagon in the alpha cell or GLP1 in intestinal L-cells. PC2 and PC3 are calcium-dependent serine proteases related to the bacterial enzyme subtilisin. They cleave selectively at Lys-Arg or Arg-Arg sites in precursors, generating products with C-terminal basic residues that are then removed by carboxypeptidase E, an exopeptidase. All 3 enzymes are expressed mainly in secretory granules of neuroendocrine cells throughout the body and in the brain. Inherited defects affecting the prohormone-processing enzymes have recently been found in association with unusual syndromes of obesity and other metabolic disorders.

摘要

激素胰岛素仍然是糖尿病治疗的基石,因为几乎所有1型糖尿病病例以及许多2型糖尿病病例都需要胰岛素。自1921年发现胰岛素以来,人们对其化学、结构和作用以及在β细胞中的产生有了很多了解。胰岛素是通过一系列前体形成的,始于胰岛素基因编码的蛋白质前胰岛素原。这些前体将激素原引导至分泌途径,最终进入分泌颗粒,在那里它被转化为胰岛素和C肽。这些产物在对葡萄糖和其他刺激的反应中以高度调节的方式一起储存和分泌。本综述重点关注最近发现的激素原转化酶PC2和PC3(PC1),这两种酶负责在β细胞中将胰岛素原内蛋白水解加工为胰岛素和C肽,以及在α细胞中将胰高血糖素原选择性加工为胰高血糖素或在肠L细胞中将其加工为胰高血糖素样肽1。PC2和PC3是与细菌酶枯草杆菌蛋白酶相关的钙依赖性丝氨酸蛋白酶。它们在前体中的赖氨酸-精氨酸或精氨酸-精氨酸位点选择性切割,产生具有C末端碱性残基的产物,然后被外肽酶羧肽酶E去除。这三种酶主要在全身神经内分泌细胞的分泌颗粒以及大脑中表达。最近发现,影响激素原加工酶的遗传缺陷与肥胖和其他代谢紊乱的异常综合征有关。

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