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炎症、缺氧和高糖对分离的人胰岛影响的代谢组学研究

Metabolomics Study of the Effects of Inflammation, Hypoxia, and High Glucose on Isolated Human Pancreatic Islets.

作者信息

Garcia-Contreras Marta, Tamayo-Garcia Alejandro, Pappan Kirk L, Michelotti Gregory A, Stabler Cherie L, Ricordi Camillo, Buchwald Peter

机构信息

Diabetes Research Institute, Miller School of Medicine, University of Miami , Miami, Florida 33136, United States.

Ri.MED Foundation , Palermo 90133, Italy.

出版信息

J Proteome Res. 2017 Jun 2;16(6):2294-2306. doi: 10.1021/acs.jproteome.7b00160. Epub 2017 May 9.

Abstract

The transplantation of human pancreatic islets is a therapeutic possibility for a subset of type 1 diabetic patients who experience severe hypoglycemia. Pre- and post-transplantation loss in islet viability and function, however, is a major efficacy-limiting impediment. To investigate the effects of inflammation and hypoxia, the main obstacles hampering the survival and function of isolated, cultured, and transplanted islets, we conducted a comprehensive metabolomics evaluation of human islets in parallel with dynamic glucose-stimulated insulin release (GSIR) perifusion studies for functional evaluation. Metabolomics profiling of media and cell samples identified a total of 241 and 361 biochemicals, respectively. Metabolites that were altered in highly significant manner in both included, for example, kynurenine, kynurenate, citrulline, and mannitol/sorbitol under inflammation (all elevated) plus lactate (elevated) and N-formylmethionine (depressed) for hypoxia. Dynamic GSIR experiments, which capture both first- and second-phase insulin release, found severely depressed insulin-secretion under hypoxia, whereas elevated baseline and stimulated insulin-secretion was measured for islet exposed to the inflammatory cytokine cocktail (IL-1β, IFN-γ, and TNF-α). Because of the uniquely large changes observed in kynurenine and kynurenate, they might serve as potential biomarkers of islet inflammation, and indoleamine-2,3-dioxygenase on the corresponding pathway could be a worthwhile therapeutic target to dampen inflammatory effects.

摘要

对于一部分经历严重低血糖的1型糖尿病患者而言,人胰岛移植是一种治疗选择。然而,胰岛移植前后的活性和功能丧失是限制疗效的主要障碍。为了研究炎症和缺氧(阻碍分离、培养及移植胰岛存活和功能的主要因素)的影响,我们对人胰岛进行了全面的代谢组学评估,并同时进行了动态葡萄糖刺激胰岛素释放(GSIR)灌流研究以评估功能。对培养基和细胞样本的代谢组学分析分别鉴定出了241种和361种生化物质。在炎症(均升高)和缺氧(乳酸升高、N-甲酰甲硫氨酸降低)状态下,两种情况下均有显著变化的代谢物包括犬尿氨酸、犬尿酸、瓜氨酸和甘露醇/山梨醇。动态GSIR实验可同时捕捉胰岛素释放的第一阶段和第二阶段,结果发现缺氧条件下胰岛素分泌严重受抑,而暴露于炎性细胞因子混合物(IL-1β、IFN-γ和TNF-α)的胰岛则测得基线胰岛素分泌升高和刺激后胰岛素分泌增加。由于犬尿氨酸和犬尿酸出现了特别大的变化,它们可能作为胰岛炎症的潜在生物标志物,相应途径中的吲哚胺-2,3-双加氧酶可能是减轻炎症作用的一个值得研究的治疗靶点。

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