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骨骼肌线粒体闪烁、pH 值及解偶联蛋白 3 的作用。

Skeletal muscle mitoflashes, pH, and the role of uncoupling protein-3.

机构信息

Department of Biochemistry, Microbiology and Immunology, Faculty of Medicine, University of Ottawa, 451 Smyth Rd., Ottawa, ON, K1H 8M5, Canada.

Department of Pharmacology and Physiology, University of Rochester School of Medicine and Dentistry, 601 Elmwood Avenue, Rochester, NY, 14642-8711, USA.

出版信息

Arch Biochem Biophys. 2019 Mar 15;663:239-248. doi: 10.1016/j.abb.2019.01.018. Epub 2019 Jan 16.

Abstract

Mitochondrial reactive oxygen species (ROS) are important cellular signaling molecules, but can cause oxidative damage if not kept within tolerable limits. An important proximal form of ROS in mitochondria is superoxide. Its production is thought to occur in regulated stochastic bursts, but current methods using mitochondrial targeted cpYFP to assess superoxide flashes are confounded by changes in pH. Accordingly, these flashes are generally referred to as 'mitoflashes'. Here we provide regulatory insights into mitoflashes and pH fluctuations in skeletal muscle, and the role of uncoupling protein-3 (UCP3). Using quantitative confocal microscopy of mitoflashes in intact muscle fibers, we show that the mitoflash magnitude significantly correlates with the degree of mitochondrial inner membrane depolarization and ablation of UCP3 did not affect this correlation. We assessed the effects of the absence of UCP3 on mitoflash activity in intact skeletal muscle fibers, and found no effects on mitoflash frequency, amplitude or duration, with a slight reduction in the average size of mitoflashes. We further investigated the regulation of pH flashes (pHlashes, presumably a component of mitoflash) by UCP3 using mitochondrial targeted SypHer (mt-SypHer) in skeletal muscle fibers. The frequency of pHlashes was significantly reduced in the absence of UCP3, without changes in other flash properties. ROS scavenger, tiron, did not alter pHlash frequency in either WT or UCP3KO mice. High resolution respirometry revealed that in the absence of UCP3 there is impaired proton leak and Complex I-driven respiration and maximal coupled respiration. Total cellular production of hydrogen peroxide (HO) as detected by Amplex-UltraRed was unaffected. Altogether, we demonstrate a correlation between mitochondrial membrane potential and mitoflash magnitude in skeletal muscle fibers that is independent of UCP3, and a role for UCP3 in the control of pHlash frequency and of proton leak- and Complex I coupled-respiration in skeletal muscle fibers. The differential regulation of mitoflashes and pHlashes by UCP3 and tiron also indicate that the two events, though may be related, are not identical events.

摘要

线粒体活性氧(ROS)是重要的细胞信号分子,但如果不控制在可容忍的范围内,就会造成氧化损伤。线粒体中一种重要的ROS 形式是超氧自由基。其产生被认为是在有调节的随机爆发中发生的,但目前使用线粒体靶向 cpYFP 来评估超氧自由基闪烁的方法受到 pH 变化的干扰。因此,这些闪烁通常被称为“mitoflashes”。在这里,我们提供了关于骨骼肌中线粒体闪烁和 pH 波动的调节见解,以及解偶联蛋白 3(UCP3)的作用。我们使用定量共焦显微镜观察完整肌肉纤维中的 mitoflashes,结果表明,mitoflash 的幅度与线粒体内膜去极化的程度显著相关,并且 UCP3 的缺失并不影响这种相关性。我们评估了 UCP3 缺失对完整骨骼肌纤维中线粒体闪烁活动的影响,发现 mitoflash 的频率、幅度或持续时间没有影响,mitoflash 的平均大小略有减小。我们进一步使用线粒体靶向 SypHer(mt-SypHer)在骨骼肌纤维中研究了 UCP3 对 pH 闪烁(pHlashes,可能是 mitoflash 的一个组成部分)的调节作用。在 UCP3 缺失的情况下,pHlashes 的频率显著降低,而其他闪烁特性没有变化。ROS 清除剂 Tiron 在 WT 或 UCP3KO 小鼠中均未改变 pHlash 频率。高分辨率呼吸测定法显示,在 UCP3 缺失的情况下,质子泄漏和复合物 I 驱动的呼吸以及最大偶联呼吸受损。通过 Amplex-UltraRed 检测到的总细胞过氧化氢(HO)产生不受影响。总的来说,我们证明了骨骼肌纤维中线粒体膜电位与 mitoflash 幅度之间存在相关性,这种相关性独立于 UCP3,并且 UCP3 在线粒体闪烁和 pH 闪烁的频率以及质子泄漏和复合物 I 偶联呼吸的控制中发挥作用。UCP3 和 Tiron 对 mitoflashes 和 pHlashes 的不同调节也表明,这两个事件虽然可能相关,但不是相同的事件。

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Skeletal muscle mitoflashes, pH, and the role of uncoupling protein-3.骨骼肌线粒体闪烁、pH 值及解偶联蛋白 3 的作用。
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