以膳食黄酮类化合物为新型配体的游离脂肪酸受体GPCR 43的克隆与分子模拟

Arooma Ihtsham, Rida Hayat, F. Khan
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引用次数: 0

摘要

g蛋白偶联受体(gpcr)被认为是在健康和疾病中参与调节体内稳态的最大的膜蛋白家族。GPCR43或FFA2(游离脂肪酸受体2)与糖尿病有关。为了进行结构研究,需要有效的方法来表达gpcr。由1-2个跨膜结构域组成的小GPCR片段通常用于核磁共振研究。本研究克隆了GPCR43的前三个跨膜片段1-3 (GPCR43- tm1 -3),分别在C端和N端分别用表达增强标签、AT4和His标签表达为pET23b(+)。据报道,对2型糖尿病(T2DM)有益的植物化合物类黄酮与靶基因GPCR43对接。我们的研究结果表明,配体与GPCR43具有更好的结合相互作用。结果表明,与其他配体相比,地奥司明具有较好的结合亲和力,是最佳配体。因此,我们得出结论,地奥明可能通过GPCR43途径成为T2DM的潜在候选药物。然而,研究证实其在2型糖尿病动物模型中的有效性。
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Cloning and molecular modeling of free fatty acid receptor GPCR 43 with dietary flavonoids as novel ligands
G-protein couple receptors (GPCRs) are considered as the largest membrane protein family involved in the regulation of body homeostasis in health and disease. GPCR43 or FFA2 (free fatty acid receptor 2) is implicated in diabetes. Efficient methods are needed to express GPCRs for structural studies. Small GPCR fragments consisting of 1-2 transmembrane domains are routinely used in NMR studies. In the present study, the first three transmembrane segments 1-3 of GPCR43 (GPCR43-TM1-3) were cloned and expressed with expression enhancement tag, AT4 and His tag at the C and N termini respectively into pET23b(+). The plant compounds, flavonoids, with reported beneficial effects in diabetes mellitus type 2 (T2DM) were subjected to docking against the target, GPCR43. Our results revealed that the ligands exhibited better binding interaction to GPCR43. Diosmin was predicted to be the best ligand with good binding affinity than the other ligands. Hence, we concluded that Diosmin may become a potential drug candidate for T2DM via GPCR43 pathway. However, studies are warranted to confirm its efficacy in animal models of T2DM.
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来源期刊
Kuwait Journal of Science & Engineering
Kuwait Journal of Science & Engineering MULTIDISCIPLINARY SCIENCES-
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3 months
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