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基于微孔板的完整和透化神经元顺序呼吸测量研究线粒体功能障碍。

Investigation of mitochondrial dysfunction by sequential microplate-based respiration measurements from intact and permeabilized neurons.

机构信息

Department of Anesthesiology and Center for Shock, Trauma and Anesthesiology Research, University of Maryland School of Medicine, Baltimore, Maryland, United States of America.

出版信息

PLoS One. 2012;7(4):e34465. doi: 10.1371/journal.pone.0034465. Epub 2012 Apr 4.

Abstract

Mitochondrial dysfunction is a component of many neurodegenerative conditions. Measurement of oxygen consumption from intact neurons enables evaluation of mitochondrial bioenergetics under conditions that are more physiologically realistic compared to isolated mitochondria. However, mechanistic analysis of mitochondrial function in cells is complicated by changing energy demands and lack of substrate control. Here we describe a technique for sequentially measuring respiration from intact and saponin-permeabilized cortical neurons on single microplates. This technique allows control of substrates to individual electron transport chain complexes following permeabilization, as well as side-by-side comparisons to intact cells. To illustrate the utility of the technique, we demonstrate that inhibition of respiration by the drug KB-R7943 in intact neurons is relieved by delivery of the complex II substrate succinate, but not by complex I substrates, via acute saponin permeabilization. In contrast, methyl succinate, a putative cell permeable complex II substrate, failed to rescue respiration in intact neurons and was a poor complex II substrate in permeabilized cells. Sequential measurements of intact and permeabilized cell respiration should be particularly useful for evaluating indirect mitochondrial toxicity due to drugs or cellular signaling events which cannot be readily studied using isolated mitochondria.

摘要

线粒体功能障碍是许多神经退行性疾病的组成部分。与分离的线粒体相比,完整神经元的耗氧量测量能够在更接近生理实际的条件下评估线粒体生物能量学。然而,细胞中线粒体功能的机制分析受到能量需求变化和缺乏底物控制的影响而变得复杂。这里我们描述了一种在单个微孔板上对完整和皂素通透的皮质神经元进行顺序呼吸测量的技术。该技术允许在通透后对单个电子传递链复合物进行底物控制,并且可以与完整细胞进行并排比较。为了说明该技术的实用性,我们证明了药物 KB-R7943 在完整神经元中对呼吸的抑制作用可通过急性皂素通透来传递复合物 II 底物琥珀酸而缓解,但不能通过复合物 I 底物缓解。相比之下,甲基琥珀酸,一种假定的细胞通透的复合物 II 底物,不能挽救完整神经元中的呼吸,并且在通透细胞中是一种较差的复合物 II 底物。完整和通透细胞呼吸的顺序测量对于评估由于药物或细胞信号事件引起的间接线粒体毒性特别有用,因为这些毒性事件使用分离的线粒体难以研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b83c/3319583/f28945260ef7/pone.0034465.g001.jpg

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