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新鲜分离的胰岛中线粒体内膜的质子泄漏增加。

The Proton Leak of the Inner Mitochondrial Membrane Is Enlarged in Freshly Isolated Pancreatic Islets.

作者信息

Alshafei Mohammed, Morsi Mai, Reschke Julia, Rustenbeck Ingo

机构信息

Institute of Pharmacology, Toxicology and Clinical Pharmacy, Technische Universität Braunschweig, 38106 Braunschweig, Germany.

Department of Pharmacology, Faculty of Pharmacy, Assiut University, Assiut 71526, Egypt.

出版信息

Biomedicines. 2024 Aug 2;12(8):1747. doi: 10.3390/biomedicines12081747.

Abstract

In a number of investigations on the mechanism of the metabolic amplification of insulin secretion, differences between the response of freshly isolated islets and of islets cultured for one day have been observed. Since no trivial explanation like insufficient numbers of viable cells after cell culture could be found, a more thorough investigation into the mechanisms responsible for the difference was made, concentrating on the function of the mitochondria as the site where the metabolism of nutrient stimulators of secretion forms the signals impacting on the transport and fusion of insulin granules. Using combinations of inhibitors of oxidative phosphorylation, we come to the conclusion that the mitochondrial membrane potential is lower and the exchange of mitochondrial reducing equivalents is faster in freshly isolated islets than in cultured islets. The significantly higher rate of oxygen consumption in fresh islets than in cultured islets (13 vs. 8 pmol/min/islet) was not caused by a different activity of the FF-ATPase, but by a larger proton leak. These observations raise the questions as to whether the proton leak is a physiologically regulated pathway and whether its larger size in fresh islets reflects the working condition of the islets within the pancreas.

摘要

在多项关于胰岛素分泌代谢放大机制的研究中,已观察到新鲜分离的胰岛与培养一天的胰岛在反应上存在差异。由于未发现像细胞培养后活细胞数量不足这样简单的解释,因此对造成这种差异的机制进行了更深入的研究,重点关注线粒体的功能,因为分泌营养刺激物的代谢在此处形成影响胰岛素颗粒运输和融合的信号。通过使用氧化磷酸化抑制剂的组合,我们得出结论,新鲜分离的胰岛中线粒体膜电位较低,线粒体还原当量的交换比培养的胰岛更快。新鲜胰岛中氧气消耗速率显著高于培养的胰岛(13对8皮摩尔/分钟/胰岛),这并非由F₀F₁ - ATP酶的不同活性引起,而是由更大的质子泄漏导致。这些观察结果引发了关于质子泄漏是否是一种生理调节途径以及其在新鲜胰岛中更大的程度是否反映胰岛在胰腺内的工作状态的问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f7f/11351158/c829b31d014a/biomedicines-12-01747-g001.jpg

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