Li Jun, Wu Jiaying, Zhou Xinyu, Lu Yangyang, Ge Yuyang, Zhang Xiangnan
Department of Clinical Pharmacy, the First Affiliated Hospital, Zhejiang University School of Medicine, Qingchun Road 79, Xiacheng District, Hangzhou, China.
Institute of Pharmacology & Toxicology, College of Pharmaceutical Sciences, Zhejiang University, Yuhangtang Road 866, Xihu District, Hangzhou, China.
Burns Trauma. 2023 May 31;11:tkad018. doi: 10.1093/burnst/tkad018. eCollection 2023.
Cerebral ischemia is a neurological disorder associated with complex pathological mechanisms, including autophagic degradation of neuronal mitochondria, or termed mitophagy, following ischemic events. Despite being well-documented, the cellular and molecular mechanisms underlying the regulation of neuronal mitophagy remain unknown. So far, the evidence suggests neuronal autophagy and mitophagy are separately regulated in ischemic neurons, the latter being more likely activated by reperfusional injury. Specifically, given the polarized morphology of neurons, mitophagy is regulated by different neuronal compartments, with axonal mitochondria being degraded by autophagy in the cell body following ischemia-reperfusion insult. A variety of molecules have been associated with neuronal adaptation to ischemia, including PTEN-induced kinase 1, Parkin, BCL2 and adenovirus E1B 19-kDa-interacting protein 3 (Bnip3), Bnip3-like (Bnip3l) and FUN14 domain-containing 1. Moreover, it is still controversial whether mitophagy protects against or instead aggravates ischemic brain injury. Here, we review recent studies on this topic and provide an updated overview of the role and regulation of mitophagy during ischemic events.
脑缺血是一种与复杂病理机制相关的神经疾病,包括缺血事件后神经元线粒体的自噬降解,即线粒体自噬。尽管已有充分记录,但神经元线粒体自噬调节的细胞和分子机制仍不清楚。到目前为止,有证据表明,缺血神经元中神经元自噬和线粒体自噬是分别调节的,后者更可能由再灌注损伤激活。具体而言,鉴于神经元的极化形态,线粒体自噬由不同的神经元区室调节,缺血再灌注损伤后,轴突线粒体在细胞体内通过自噬降解。多种分子与神经元对缺血的适应有关,包括PTEN诱导激酶1、帕金蛋白、BCL2和腺病毒E1B 19 kDa相互作用蛋白3(Bnip3)、Bnip3样蛋白(Bnip3l)和含FUN14结构域蛋白1。此外,线粒体自噬是保护还是加重缺血性脑损伤仍存在争议。在此,我们综述了关于该主题的最新研究,并提供了缺血事件中线粒体自噬的作用和调节的最新概述。
