Institute of Molecular and Industrial Biotechnology, Faculty of Biotechnology and Food Sciences, Lodz University of Technology, Stefanowskiego Street 4/10, 90-924 Łódź, Poland.
Core Research Laboratory, Department of Endocrinology, Department of Tumor and Immunology, Precision Medical Institute, Western China Science and Technology Innovation Port, School of Medicine, the Second Affiliated Hospital of Xi'an Jiaotong University, DaMingGong, Jian Qiang Road, Wei Yang district, Xi'an 710016, China.
J Med Chem. 2021 Jul 22;64(14):9677-9710. doi: 10.1021/acs.jmedchem.1c00410. Epub 2021 Jul 8.
A fundamental role of pancreatic β-cells to maintain proper blood glucose level is controlled by the Ras superfamily of small GTPases that undergo post-translational modifications, including prenylation. This covalent attachment with either a farnesyl or a geranylgeranyl group controls their localization, activity, and protein-protein interactions. Small GTPases are critical in maintaining glucose homeostasis acting in the pancreas and metabolically active tissues such as skeletal muscles, liver, or adipocytes. Hyperglycemia-induced upregulation of small GTPases suggests that inhibition of these pathways deserves to be considered as a potential therapeutic approach in treating T2D. This Perspective presents how inhibition of various points in the mevalonate pathway might affect protein prenylation and functioning of diabetes-affected tissues and contribute to chronic inflammation involved in diabetes mellitus (T2D) development. We also demonstrate the currently available molecular tools to decipher the mechanisms linking the mevalonate pathway's enzymes and GTPases with diabetes.
胰岛β细胞的基本功能是维持血糖水平的稳定,这一功能受到 Ras 家族小 GTP 酶的调控,这些小 GTP 酶会发生翻译后修饰,包括棕榈酰化。这种与法尼基或香叶基基团的共价连接控制了它们的定位、活性和蛋白-蛋白相互作用。小 GTP 酶在维持胰腺和代谢活跃组织(如骨骼肌、肝脏或脂肪组织)中的葡萄糖稳态中起着关键作用。高血糖诱导的小 GTP 酶上调表明,抑制这些途径值得被考虑作为治疗 T2D 的一种潜在治疗方法。本文从多个角度探讨了抑制法尼醇途径的各个环节如何影响受糖尿病影响的组织中的蛋白棕榈酰化和功能,并探讨其与糖尿病慢性炎症的关系。我们还展示了目前可用的分子工具,以阐明法尼醇途径的酶和 GTP 酶与糖尿病之间的联系的机制。
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