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        生物資訊

        抗糖尿病藥物目標(biāo)GPR40的結(jié)構(gòu)

        作者:admin 來源:Nature 發(fā)布時(shí)間: 2014-09-05 08:34  瀏覽次數(shù):
        購買進(jìn)口儀器、試劑和耗材——就在始于2001年的畢特博生物 effectnews.cn

         Nature:抗糖尿病藥物目標(biāo)GPR40的結(jié)構(gòu)

        “G-蛋白耦合受體”(GPCR) “人GPR40” (hGPR40,亦稱為“自由脂肪酸受體-1”)是用于2-型糖尿病治療的一個有吸引力的治療目標(biāo)。它是一種膜蛋白,主要是在胰腺 β-細(xì)胞中和小腸腸內(nèi)分泌細(xì)胞中表達(dá),充當(dāng)一個營養(yǎng)物傳感器,增強(qiáng)胰島素分泌和“胰高血糖素樣受體-1”的分泌。

        這項(xiàng)研究報(bào)告了與TAK-875 (fasiglifam,它是GPR40 的一個部分激動劑,目前正在進(jìn)行三期臨床試驗(yàn))形成復(fù)合物的hGPR40的詳細(xì)原子結(jié)構(gòu)。該結(jié)構(gòu)顯示TAK-875以一種通常的方式結(jié)合,并且表明TAK-875和天然基質(zhì)通過脂質(zhì)雙層進(jìn)入“受體結(jié)合袋”。

        原文摘要:

        High-resolution structure of the human GPR40 receptor bound to allosteric agonist TAK-875

        Ankita Srivastava, Jason Yano, Yoshihiko Hirozane, Georgia Kefala, Franz Gruswitz,Gyorgy Snell, Weston Lane, Anthony Ivetac, Kathleen Aertgeerts, Jasmine Nguyen, Andy Jennings & Kengo Okada

        Human GPR40 receptor (hGPR40), also known as free fatty-acid receptor 1 (FFAR1), is a G-protein-coupled receptor that binds long-chain free fatty acids to enhance glucose-dependent insulin secretion. Novel treatments for type-2 diabetes mellitus are therefore possible by targeting hGPR40 with partial or full agonists. TAK-875, or fasiglifam, is an orally available, potent and selecive partial agonist of hGPR40 receptor, which reached phase III clinical trials for the potential treatment of type-2 diabetes mellitus. Data from clinical studies indicate that TAK-875, which is an ago-allosteric modulator of hGPR40 (ref. 3), demonstrates improved glycaemic control and low hypoglycaemic risk in diabetic patients. Here we report the crystal structure of hGPR40 receptor bound to TAK-875 at 2.3 Å resolution. The co-complex structure reveals a unique binding mode of TAK-875 and suggests that entry to the non-canonical binding pocket most probably occurs via the lipid bilayer. The atomic details of the extensive charge network in the ligand binding pocket reveal additional interactions not identified in previous studies and contribute to a clear understanding of TAK-875 binding to the receptor. The hGPR40–TAK-875 structure also provides insights into the plausible binding of multiple ligands to the receptor, which has been observed in radioligand binding and Ca2+ influx assay studies. Comparison of the transmembrane helix architecture with other G-protein-coupled receptors suggests that the crystallized TAK-875-bound hGPR40 complex is in an inactive-like state.

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