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引用次数: 0
摘要
线粒体不仅能产生三磷酸腺苷(ATP),充当细胞的动力源,还能通过产生活性氧促进宿主防御。因此,败血症中的线粒体损伤直接导致能量货币短缺和免疫系统失调。除此之外,线粒体损伤还会导致释放高度危险的线粒体 DNA,通过调节新陈代谢和诱导程序性细胞死亡来促进酸中毒,从而促进败血症的病情发展。线粒体损伤会诱发各种形式的细胞死亡。细胞坏死是从凋亡向坏死的二次转化。虽然凋亡是最初的意图,但由于线粒体损伤导致 ATP 耗竭,凋亡无法完成,最终导致炎症性坏死。除了这种意外的细胞死亡外,败血症中的线粒体损伤还会诱发坏死、铁坏死和热坏死等程序性炎症诱导细胞死亡。基于这些发现,线粒体损伤的调控有望开发出治疗败血症的新方法。
Mitochondria not only generate adenosine triphosphate (ATP) and act as the powerhouse of the cell but also contribute to host defense by producing reactive oxygen species. Therefore, mitochondrial damage in sepsis directly results in a shortage of energy currency and dysregulation of the immune system. Other than those, mitochondrial damage results in the release of highly dangerous mitochondrial DNA, facilitating acidosis by modulating the metabolism and inducing programmed cell death, thereby facilitating disease progression in sepsis. Various forms of cell death are induced by mitochondrial damage. Aponecrosis is a secondary conversion from apoptosis to necrosis. Although apoptosis is initially intended, it cannot be completed due to ATP depletion from mitochondrial damage, ultimately leading to inflammatory necrosis. Besides such accidental cell death, programmed inflammation-inducing cell deaths such as necroptosis, ferroptosis, and pyroptosis are induced by mitochondrial damage in sepsis. Based on these findings, the regulation of mitochondrial damage holds promise for the development of new therapeutic approaches for sepsis.
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