新型GPR40激动剂CNX-011-67可增强链脲佐菌素诱导的糖尿病大鼠及2型糖尿病患者胰岛的葡萄糖反应性、胰岛素分泌及胰岛胰岛素含量。
CNX-011-67, a novel GPR40 agonist, enhances glucose responsiveness, insulin secretion and islet insulin content in n-STZ rats and in islets from type 2 diabetic patients.
作者信息
Sunil Venkategowda, Verma Mahesh Kumar, Oommen Anup M, Sadasivuni Manojkumar, Singh Jaideep, Vijayraghav Dasarahalli N, Chandravanshi Bhawna, Shetty Jayalaxmi, Biswas Sanghamitra, Dandu Anilkumar, Moolemath Yoganand, Venkataranganna Marikunte V, Somesh Baggavalli P, Jagannath Madanahalli R
机构信息
Connexios Life Sciences Pvt Ltd, #49, "SHILPA VIDYA" 1st Main, 3rd Phase, JP Nagar, Bangalore 560078, India.
出版信息
BMC Pharmacol Toxicol. 2014 Mar 25;15:19. doi: 10.1186/2050-6511-15-19.
BACKGROUND
GPR40 is a G-protein coupled receptor regulating free fatty acid induced and also glucose induced insulin secretion. We generated neonatally-streptozotocin-treated female rats (n-STZ) and treated them with CNX-011-67, a GPR40 agonist to examine the role of GPR40 in modulation of glucose metabolism, insulin secretion and content.
METHODS
Female n-STZ animals were orally administered with CNX-011-67 (15 mg/kg body weight, twice daily) or with vehicle for 8 weeks (n = 8 per group). Glucose tolerance in treated animals and insulin secretion, islet insulin content and gene expression in isolated islets were determined. Islets from type 2 diabetic mellitus (T2DM) patients were treated with different concentrations of glucose in presence or absence of CNX-011-67 and insulin secretion was measured.
RESULTS
Treatment of n-STZ rats with GPR40 agonist CNX-011-67 enhanced insulin secretion in response to oral glucose load on day 0 and this response persisted during the treatment period. The treatment also produced a 'memory effect' during which insulin secretion in response to oral glucose load remained enhanced, for a week, even in absence of the agonist. Activation of GPR40 enhanced responsiveness of islets to glucose and increased glucose induced insulin secretion and islet insulin content. An increase in islet mRNA expression of GCK, PDX1, insulin and PC was also observed. Acute treatment of islets from n-STZ rats with GPR40 agonist enhanced cellular ATP content. Activation of GPR40 enhanced mitochondrial calcium level in NIT-1 insulinoma cells. CNX-011-67 increased insulin secretion in islets from T2DM patients which were non-responsive to increased glucose concentration
CONCLUSIONS
Our data provide evidence that activation of GPR40 with CNX-011-67 stimulates glucose metabolism, enhances glucose responsiveness, increases insulin secretion and content and that pharmacological activation of GPR40 will prove beneficial for treatment of T2DM.
背景
GPR40是一种G蛋白偶联受体,可调节游离脂肪酸诱导的以及葡萄糖诱导的胰岛素分泌。我们构建了新生期经链脲佐菌素处理的雌性大鼠(n-STZ),并用GPR40激动剂CNX-011-67对其进行处理,以研究GPR40在调节葡萄糖代谢、胰岛素分泌及含量方面的作用。
方法
雌性n-STZ动物口服CNX-011-67(15mg/kg体重,每日两次)或赋形剂,持续8周(每组n = 8)。测定处理动物的葡萄糖耐量以及分离胰岛中的胰岛素分泌、胰岛胰岛素含量和基因表达。在有或无CNX-011-67的情况下,用不同浓度的葡萄糖处理2型糖尿病(T2DM)患者的胰岛,并测量胰岛素分泌。
结果
用GPR40激动剂CNX-011-67处理n-STZ大鼠可增强第0天口服葡萄糖负荷后的胰岛素分泌,且该反应在治疗期间持续存在。该处理还产生了一种“记忆效应”,在此期间,即使在没有激动剂的情况下,口服葡萄糖负荷后的胰岛素分泌在一周内仍保持增强。GPR40的激活增强了胰岛对葡萄糖的反应性,并增加了葡萄糖诱导的胰岛素分泌和胰岛胰岛素含量。还观察到胰岛中GCK、PDX1、胰岛素和PC的mRNA表达增加。用GPR40激动剂对n-STZ大鼠的胰岛进行急性处理可提高细胞ATP含量。GPR40的激活增强了NIT-1胰岛素瘤细胞中的线粒体钙水平。CNX-011-67增加了对葡萄糖浓度升高无反应的T2DM患者胰岛中的胰岛素分泌。
结论
我们的数据提供了证据,表明用CNX-011-67激活GPR40可刺激葡萄糖代谢,增强葡萄糖反应性,增加胰岛素分泌和含量,并且GPR40的药理激活将被证明对T2DM的治疗有益。
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