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研究来自[具体来源1]、[具体来源2]和[具体来源3]的环肽以及异叶汉防己碱B衍生肽中潜在的胰高血糖素样肽-1受体激动剂用于治疗2型糖尿病:一项计算机模拟研究。

Investigating Potential GLP-1 Receptor Agonists in Cyclopeptides from , , and , and Peptides Derived from Heterophyllin B for the Treatment of Type 2 Diabetes: An In Silico Study.

作者信息

Liao Hui-Jun, Tzen Jason T C

机构信息

Graduate Institute of Biotechnology, National Chung Hsing University, Taichung 402, Taiwan.

出版信息

Metabolites. 2022 Jun 15;12(6):549. doi: 10.3390/metabo12060549.

DOI:10.3390/metabo12060549
PMID:35736482
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9227353/
Abstract

GLP-1 receptor agonists stimulate GLP-1R to promote insulin secretion, whereas DPP4 inhibitors slow GLP-1 degradation. Both approaches are incretin-based therapies for T2D. In addition to GLP-1 analogs, small nonpeptide GLP-1RAs such as LY3502970, TT-OAD2, and PF-06882961 have been considered as possible therapeutic alternatives. , , and are plants rich in cyclopeptides with hypoglycemic effects. Our previous study demonstrated the potential of their cyclopeptides for DPP4 inhibition. Reports of cyclic setmelanotide as an MC4R (GPCR) agonist and cyclic α-conotoxin chimeras as GLP-1RAs led to docking studies of these cyclopeptides with GLP-1R. Heterophyllin B, Pseudostellarin B, Cyclolinopeptide B, Cyclolinopeptide C, Drymarin A, and Diandrine C are abundant in these plants, with binding affinities of -9.5, -10.4, -10.3, -10.6, -11.2, and -11.9 kcal/mol, respectively. The configuration they demonstrated established multiple hydrogen bonds with the transmembrane region of GLP-1R. DdC:(cyclo)-GGPYWP showed the most promising docking score. The results suggest that, in addition to DPP4, GLP-1R may be a hypoglycemic target of these cyclopeptides. This may bring about more discussion of plant cyclopeptides as GLP-1RAs. Moreover, peptides derived from the HB precursor (IFGGLPPP), including IFGGWPPP, IFPGWPPP, IFGGYWPPP, and IFGYGWPPPP, exhibited diverse interactions with GLP-1R and displayed backbones available for further research.

摘要

胰高血糖素样肽-1(GLP-1)受体激动剂刺激GLP-1受体以促进胰岛素分泌,而二肽基肽酶4(DPP4)抑制剂则减缓GLP-1的降解。这两种方法都是基于肠促胰岛素的2型糖尿病治疗方法。除了GLP-1类似物外,小分子非肽类GLP-1受体激动剂(如LY3502970、TT-OAD2和PF-06882961)也被视为可能的治疗替代方案。 、 和 是富含具有降血糖作用的环肽的植物。我们之前的研究证明了其环肽对DPP4的抑制潜力。环赛美拉诺肽作为黑皮质素4受体(MC4R,一种G蛋白偶联受体)激动剂以及环α-芋螺毒素嵌合体作为GLP-1受体激动剂的报道引发了这些环肽与GLP-1受体的对接研究。异叶林B、假参环肽B、环林肽B、环林肽C、干马林A和二安德里宁C在这些植物中含量丰富,其结合亲和力分别为-9.5、-10.4、-10.3、-10.6、-11.2和-11.9千卡/摩尔。它们展示的构型与GLP-1受体的跨膜区域形成了多个氢键。DdC:(环)-GGPYWP显示出最有前景的对接分数。结果表明,除了DPP4外,GLP-1受体可能是这些环肽的降血糖靶点。这可能会引发更多关于植物环肽作为GLP-1受体激动剂的讨论。此外,源自HB前体(IFGGLPPP)的肽,包括IFGGWPPP、IFPGWPPP、IFGGYWPPP和IFGYGWPPPP,与GLP-1受体表现出多样的相互作用,并展示出可供进一步研究的骨架。

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