Prolonged activation of human islet cannabinoid receptors in vitro induces adaptation but not dysfunction

Alonso Vilches-Flores , Zara Franklin , Astrid C. Hauge-Evans , Bo Liu , Guo C. Huang , Pratik Choudhary , Peter M. Jones , Shanta J. Persaud
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引用次数: 9

Abstract

Background

Although in vivo studies have implicated endocannabinoids in metabolic dysfunction, little is known about direct, chronic activation of the endocannabinoid system (ECS) in human islets. Therefore, this study investigated the effects of prolonged exposure to cannabinoid agonists on human islet gene expression and function.

Methods

Human islets were maintained for 2 and 5 days in the absence or presence of CB1r (ACEA) or CB2r (JWH015) agonists. Gene expression was quantified by RT-PCR, hormone levels by radioimmunoassay and apoptosis by caspase activities.

Results

Human islets express an ECS, with mRNAs encoding the biosynthetic and degrading enzymes NAPE-PLD, FAAH and MAGL being considerably more abundant than DAGLα, an enzyme involved in 2-AG synthesis, or CB1 and CB2 receptor mRNAs. Prolonged activation of CB1r and CB2r altered expression of mRNAs encoding ECS components, but did not have major effects on islet hormone secretion. JWH015 enhanced insulin and glucagon content at 2 days, but had no effect after 5 days. Treatment with ACEA or JWH015 for up to 5 days did not have marked effects on islet viability, as assessed by morphology and caspase activities.

Conclusions

Maintenance of human islets for up to 5 days in the presence of CB1 and CB2 receptor agonists causes modifications in ECS element gene expression, but does not have any major impact on islet function or viability.

General Significance

These data suggest that the metabolic dysfunction associated with over-activation of the ECS in obesity and diabetes in humans is unlikely to be secondary to impaired islet function.

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人类胰岛大麻素受体在体外的长期激活诱导适应,但不功能障碍
虽然体内研究表明内源性大麻素与代谢功能障碍有关,但对人类胰岛内源性大麻素系统(ECS)的直接、慢性激活知之甚少。因此,本研究探讨了长期暴露于大麻素激动剂对人类胰岛基因表达和功能的影响。方法在CB1r (ACEA)或CB2r (JWH015)激动剂不存在或不存在的情况下,分别维持人胰岛2天和5天。RT-PCR检测基因表达,放射免疫法检测激素水平,caspase活性检测细胞凋亡。结果人类胰岛表达ECS,编码生物合成和降解酶NAPE-PLD、FAAH和MAGL的mrna比参与2-AG合成的酶DAGLα或CB1和CB2受体mrna丰富得多。CB1r和CB2r的长期激活改变了编码ECS成分的mrna的表达,但对胰岛激素分泌没有主要影响。JWH015在第2天提高胰岛素和胰高血糖素含量,但在第5天没有影响。通过形态学和半胱天酶活性评估,用ACEA或JWH015治疗5天对胰岛活力没有显著影响。结论人胰岛在CB1和CB2受体激动剂存在下维持5天可引起ECS元件基因表达的改变,但对胰岛功能或活力没有任何重大影响。这些数据表明,人类肥胖和糖尿病患者中与ECS过度激活相关的代谢功能障碍不太可能继发于胰岛功能受损。
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