Nestlé Institute of Health Sciences, Nestlé Research, EPFL Innovation Park, Lausanne, Switzerland.
Ecole Polytechnique Fédérale de Lausanne, Lausanne, Switzerland.
Diabetologia. 2020 Dec;63(12):2628-2640. doi: 10.1007/s00125-020-05275-5. Epub 2020 Sep 22.
AIMS/HYPOTHESIS: In islets from individuals with type 2 diabetes and in islets exposed to chronic elevated glucose, mitochondrial energy metabolism is impaired. Here, we studied early metabolic changes and mitochondrial adaptations in human beta cells during chronic glucose stress.
Respiration and cytosolic ATP changes were measured in human islet cell clusters after culture for 4 days in 11.1 mmol/l glucose. Metabolomics was applied to analyse intracellular metabolite changes as a result of glucose stress conditions. Alterations in beta cell function were followed using insulin secretion assays or cytosolic calcium signalling after expression of the calcium probe YC3.6 specifically in beta cells of islet clusters.
At early stages of glucose stress, mitochondrial energy metabolism was augmented in contrast to the previously described mitochondrial dysfunction in beta cells from islets of diabetic donors. Following chronic glucose stress, mitochondrial respiration increased (by 52.4%, p < 0.001) and, as a consequence, the cytosolic ATP/ADP ratio in resting human pancreatic islet cells was elevated (by 27.8%, p < 0.05). Because of mitochondrial overactivation in the resting state, nutrient-induced beta cell activation was reduced. In addition, chronic glucose stress caused metabolic adaptations that resulted in the accumulation of intermediates of the glycolytic pathway, the pentose phosphate pathway and the TCA cycle; the most strongly augmented metabolite was glycerol 3-phosphate. The changes in metabolites observed are likely to be due to the inability of mitochondria to cope with continuous nutrient oversupply. To protect beta cells from chronic glucose stress, we inhibited mitochondrial pyruvate transport. Metabolite concentrations were partially normalised and the mitochondrial respiratory response to nutrients was markedly improved. Furthermore, stimulus-secretion coupling as assessed by cytosolic calcium signalling, was restored.
CONCLUSION/INTERPRETATION: We propose that metabolic changes and associated mitochondrial overactivation are early adaptations to glucose stress, and may reflect what happens as a result of poor blood glucose control. Inhibition of mitochondrial pyruvate transport reduces mitochondrial nutrient overload and allows beta cells to recover from chronic glucose stress. Graphical abstract.
目的/假设:在 2 型糖尿病患者的胰岛中和暴露于慢性高葡萄糖的胰岛中,线粒体能量代谢受损。在这里,我们研究了慢性葡萄糖应激过程中人类β细胞的早期代谢变化和线粒体适应性。
在 11.1mmol/l 葡萄糖中培养 4 天后,测量人胰岛细胞簇中的呼吸和胞质 ATP 变化。应用代谢组学分析葡萄糖应激条件下细胞内代谢物变化。通过胰岛素分泌测定或 YC3.6 钙探针在胰岛簇中β细胞特异性表达后的胞质钙信号来跟踪β细胞功能的变化。
在葡萄糖应激的早期阶段,与先前描述的糖尿病供体胰岛β细胞中线粒体功能障碍相反,线粒体能量代谢增强。在慢性葡萄糖应激后,线粒体呼吸增加(增加 52.4%,p<0.001),因此静息人胰腺胰岛细胞中的胞质 ATP/ADP 比值升高(增加 27.8%,p<0.05)。由于静息状态下线粒体过度激活,营养诱导的β细胞激活减少。此外,慢性葡萄糖应激导致代谢适应,导致糖酵解途径、磷酸戊糖途径和 TCA 循环的中间产物积累;增加最明显的代谢物是甘油 3-磷酸。观察到的代谢物变化可能是由于线粒体无法应对持续的营养供应过剩。为了保护β细胞免受慢性葡萄糖应激,我们抑制了线粒体丙酮酸转运。代谢物浓度部分正常化,营养物质对线粒体呼吸的反应明显改善。此外,通过胞质钙信号评估的刺激-分泌偶联得到恢复。
结论/解释:我们提出代谢变化和相关的线粒体过度激活是葡萄糖应激的早期适应,可能反映了血糖控制不佳的结果。抑制线粒体丙酮酸转运可减少线粒体营养物过载,使β细胞从慢性葡萄糖应激中恢复。图表抽象。
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