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Mitochondrial membrane potential regulates matrix configuration and cytochrome c release during apoptosis.

机译:线粒体膜电位调节细胞凋亡过程中的基质构型和细胞色素c的释放。

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During apoptosis, the mitochondrial membrane potential (MMP) decreases, but it is not known how this relates to the apoptotic process. It was recently suggested that cytochrome c is compartmentalized in closed cristal regions and therefore, matrix remodeling is required to attain complete cytochrome c release from the mitochondria. In this work we show that, at the onset of apoptosis, changes in MMP control matrix remodeling prior to cytochrome c release. Early after growth factor withdrawal the MMP declines and the matrix condenses. Both phenomena are reversed by adding oxidizable substrates. In mitochondria isolated from healthy cells, matrix condensation can be induced by either denying oxidizable substrates or by protonophores that dissipate the membrane potential. Matrix remodeling to the condensed state results in cristal unfolding and exposes cytochrome c to the intermembrane space facilitating its release from the mitochondria during apoptosis. In contrast, when a transmembrane potential is generated due to either electron transport or a pH gradient formed by acidifying the medium, mitochondria maintain an orthodox configuration in which most cytochrome c is sequestered in the cristae and is resistant to release by agents that disrupt the mitochondrial outer membrane.Cell Death and Differentiation (2003) 10, 709-717. doi:10.1038/sj.cdd.4401231
机译:在凋亡过程中,线粒体膜电位(MMP)降低,但尚不知道这与凋亡过程有何关系。最近有人提出,细胞色素c在封闭的晶体区域内是分隔的,因此,需要进行基质重塑才能从线粒体中完全释放出细胞色素c。在这项工作中,我们表明,在细胞凋亡开始时,细胞色素c释放之前MMP控制基质重塑的变化。生长因子撤药后早期,MMP下降,基质凝结。通过添加可氧化的底物可以逆转这两种现象。在从健康细胞中分离出的线粒体中,可以通过否定可氧化的底物或通过耗散膜电位的质子体来诱导基质凝聚。基质重塑至凝聚态会导致结晶展开,并使细胞色素c暴露于膜间空间,从而促进其在凋亡过程中从线粒体中释放出来。相反,当由于电子迁移或通过酸化介质形成的pH梯度而产生跨膜电位时,线粒体保持正统构型,其中大多数细胞色素c被螯合在cr中,并且耐破坏线粒体的物质释放。细胞死亡和分化(2003)10,709-717。 doi:10.1038 / sj.cdd.4401231

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