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线粒体膜电位与缺血性神经元死亡。

Mitochondrial membrane potential and ischemic neuronal death.

作者信息

Iijima Takehiko

机构信息

Department of Anesthesiology, Kyorin University, School of Medicine, 6-20-2 Shinkawa Mitaka City, Tokyo 181-8611, Japan.

出版信息

Neurosci Res. 2006 Jul;55(3):234-43. doi: 10.1016/j.neures.2006.04.005. Epub 2006 May 22.

Abstract

Mitochondria are intracellular organelles in which high energy phosphate is produced. Ischemia causes depletion of the materials necessary to produce this phosphate and strongly affects the electron transport chain. Apoptosis commences during and after ischemia. As such, it is likely that a significant relationship exists between inactivation of electron transport and apoptosis. Mitochondrial membrane potential (MMP) reflects performance of the electron transport chain and can indicate a pathological disorder of this system. In an experimental setting, oxygen-glucose depletion (OGD) in neuronal cell culture has been employed to simulate an ischemic condition. The relationship between MMP and subsequent neuronal death during and after OGD has been examined. MMP dissipation and concomitant neuronal death have been reported, but recent studies have demonstrated mitochondrial hyperpolarization preceding neuronal death. The direction of MMP polarization depends on the extent of OGD. Long OGD results in depolarization, while shorter OGD induces hyperpolarization. Neurons are still viable during hyperpolarization, but the process may switch on the apoptotic cascade. Meanwhile, dissipation of MMP seems to be a consequence of severe energy deficit, leading to necrosis. MMP may be a marker of subsequent apoptosis, although a causal relationship remains to be determined.

摘要

线粒体是产生高能磷酸的细胞内细胞器。缺血会导致产生这种磷酸所需物质的耗尽,并强烈影响电子传递链。凋亡在缺血期间及之后开始。因此,电子传递失活与凋亡之间可能存在显著关系。线粒体膜电位(MMP)反映电子传递链的性能,并可表明该系统的病理紊乱。在实验环境中,已采用神经元细胞培养中的氧-葡萄糖剥夺(OGD)来模拟缺血状态。已研究了OGD期间及之后MMP与随后神经元死亡之间的关系。已有报道称MMP耗散及伴随的神经元死亡,但最近的研究表明在神经元死亡之前线粒体发生超极化。MMP极化的方向取决于OGD的程度。长时间的OGD导致去极化,而较短时间的OGD诱导超极化。在超极化期间神经元仍然存活,但该过程可能会开启凋亡级联反应。同时,MMP的耗散似乎是严重能量缺乏的结果,导致坏死。MMP可能是随后凋亡的标志物,尽管因果关系仍有待确定。

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