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蛋白质异戊二烯化在健康和代谢应激状态下胰岛β细胞功能中的作用

Protein prenylation in islet β-cell function in health and metabolic stress.

作者信息

Kowluru Anjaneyulu

机构信息

Biomedical Research Service, John D. Dingell VA Medical Center and Department of Pharmaceutical Sciences, Eugene Applebaum College of Pharmacy and Health Sciences, Wayne State University, Detroit, MI 48201, United States.

出版信息

Biochem Pharmacol. 2025 Aug;238:116994. doi: 10.1016/j.bcp.2025.116994. Epub 2025 May 21.

Abstract

Protein prenylation has been implicated in a variety of cellular functions, including cytoskeletal remodeling, trafficking and fusion of secretory vesicles with the plasma membrane. It involves incorporation of either a 15-carbon farnesyl or a 20-carbon geranylgeranyl derivative of mevalonic acid into cysteines at the C-terminus of substrate proteins. At least four types of prenyltransferases, namely farnesyl transferase (FTase) and the geranylgeranyl transferases I-III (GGTase-I, II, and III) have been identified in mammalian cells. Published evidence suggests expression of functionally active forms of these prenyltransferases and their candidate substrate proteins in human islets, rodent islets, and clonal β-cells. Pharmacological and molecular biological evidence implicates requisite roles for protein prenylation in glucose-stimulated insulin secretion. Evidence is also emerging to indicate significant defects in protein prenylome in β-cell models of impaired insulin secretion and diabetes. This review will provide a status update on modulatory roles of protein prenylation, enzymes involved in this signaling pathway, their structural composition and regulation in the context of islet β-cell function in normal health. In addition, experimental evidence on the metabolic fate of protein prenylation pathway in the pancreatic β-cell following chronic exposure to diabetogenic stimuli is reviewed herein. Lastly, crucial gaps in our current understanding, and potential opportunities for future research in this area of islet biology are highlighted.

摘要

蛋白质异戊二烯化参与了多种细胞功能,包括细胞骨架重塑、分泌囊泡与质膜的运输和融合。它涉及将甲羟戊酸的15碳法尼基或20碳香叶基香叶基衍生物掺入底物蛋白C末端的半胱氨酸中。在哺乳动物细胞中已鉴定出至少四种类型的异戊二烯基转移酶,即法尼基转移酶(FTase)和香叶基香叶基转移酶I-III(GGTase-I、II和III)。已发表的证据表明,这些异戊二烯基转移酶及其候选底物蛋白的功能活性形式在人胰岛、啮齿动物胰岛和克隆β细胞中表达。药理学和分子生物学证据表明蛋白质异戊二烯化在葡萄糖刺激的胰岛素分泌中起必要作用。越来越多的证据表明胰岛素分泌受损和糖尿病的β细胞模型中蛋白质异戊二烯化组存在显著缺陷。本综述将提供关于蛋白质异戊二烯化的调节作用、参与该信号通路的酶、它们在正常健康状态下胰岛β细胞功能背景下的结构组成和调节的最新情况。此外,本文还综述了慢性暴露于致糖尿病刺激后胰腺β细胞中蛋白质异戊二烯化途径的代谢命运的实验证据。最后,强调了我们目前理解中的关键差距以及胰岛生物学这一领域未来研究的潜在机会。

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