膜蛋白MCHR1拮抗剂ALB-127158和KRX-104130的类似化合物的计算预测。

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2023-12-01 Epub Date: 2023-11-09 DOI:10.1007/s10863-023-09993-4
Emrah Sariyer, Ayşegül Saral Sariyer
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引用次数: 0

摘要

肥胖已经在世界各地普遍存在,它增加了代谢紊乱的患病率,使其治疗更加困难,从而危及公众健康。开发治疗肥胖的药物是努力的重点。黑色素浓缩激素受体1(MCHR1)是其中一些治疗可能性的靶点,因为在肥胖模型中发现了黑色素浓缩荷尔蒙水平的增加。已知的MCHR1拮抗剂包括BMS-830216、GW-856464、NGD-4715、ALB-127158和AMG 076,但许多都未能通过I期临床研究。作为一种潜在的心脏毒性治疗方法,KRX-104130最近才被发现。由于MCH系统是治疗肥胖的潜在有效靶点,因此在分子水平上对MCHR1及其拮抗剂之间的相互作用进行计算机研究是本研究的主要目标。在RealEnamine文库中筛选类似物ALB-121758和KRX-104130。将通过分子对接获得的复合物嵌入模拟脑细胞膜中并模拟540ns,然后用MMPBSA.py计算MM-GBSA。通过所有这些计算研究,研究了所选类似化合物与ALB-127158和KRX-104130的相似或不同方面。本研究的特异性是分析MCHR1蛋白包埋在膜中。得出的结论是,KRX-104130的类似物Z1922310273和ALB-127158的类似物PV-002757495233在磷脂膜性质方面没有引起差异。此外,所有配体在假定的结合位点保持稳定。已经提出,当在熔炉中考虑所有这些输出时,PV-002757495233和Z1922310273化合物可以被评估为MCHR1拮抗剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Computational prediction of analog compounds of the membrane protein MCHR1 antagonists ALB-127158 and KRX-104130.

Obesity, which is already pervasive throughout the world, endangers public health by raising the prevalence of metabolic disorders and making their treatment more difficult. The development of drugs to treat obesity is a focus of effort. Melanin concentrated hormone receptor 1 (MCHR1) is the target of some of these therapeutic possibilities since as increased levels of melanin concentrated hormone have been found in obesity models. Known MCHR1 antagonists include BMS-830216, GW-856464, NGD-4715, ALB-127158, and AMG 076, but many have failed phase-I clinical studies. As a potential treatment for cardiotoxicity, KRX-104130 has only recently been identified. As MCH system is potentially effective target for treatment of obesity, in silico research into interaction between MCHR1 and its antagonists at molecular level was the primary goal of this study. Analogues ALB-127158 and KRX-104130 were screened among the RealEnamine library. The complexes obtained by molecular docking were embedded in mimics brain-cell membrane and simulated for 540 ns, and then MM-GBSA were calculated with MMPBSA.py. With all these computational studies, similar or different aspects of selected analogous compounds to ALB-127158 and KRX-104130 were investigated. The specificity of this study was that it analyzed MCHR1 protein as embedded in membrane. It was concluded that KRX-104130's analogue Z1922310273 and ALB-127158's analogue PV-002757495233 did not cause a difference in terms of phospholipid membrane properties. In addition, all ligands remained stable in putative binding site. It has been suggested that PV-002757495233 and Z1922310273 compounds can be evaluated as MCHR1 antagonists when all these outputs are considered in melting pots.

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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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