Src抑制挽救缺血性中风中FUNDC1介导的神经元线粒体自噬。

IF 2.6 1区 医学
Tianchi Tang, Li-Bin Hu, Chao Ding, Zhihua Zhang, Ning Wang, Tingting Wang, Hang Zhou, Siqi Xia, Linfeng Fan, Xiong-Jie Fu, Feng Yan, Xiangnan Zhang, Gao Chen, Jianru Li
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引用次数: 0

摘要

背景:缺血性脑卒中触发神经元线粒体自噬,而线粒体自噬受体在缺血/再灌注(I/R)损伤诱导的神经元线粒体自吞噬中的作用尚未完全阐明。在这里,我们旨在研究线粒体自噬受体FUN14结构域包含1(FUNDC1)的参与及其在I/R损伤诱导的神经元线粒体自噬中的调节。方法:建立野生型和FUNDC1敲除小鼠的神经元I/R损伤模型,包括体内短暂性大脑中动脉闭塞(tMCAO)和体外缺氧/再灌注。评估了具有两种基因型的小鼠的卒中结果。对神经元线粒体自噬进行了体内和体外分析。对FUNDC1及其监管机构Src的活动进行了评估。通过给予Src拮抗剂PP1来评估Src对FUNDC1介导的线粒体自噬的影响。结果:令我们惊讶的是,接受tMCAO的FUNDC1敲除小鼠显示出与野生型同窝小鼠相当的卒中结果。尽管I/R损伤可以激活神经元线粒体自噬,但FUNDC1缺失并没有破坏神经元线粒体自吞噬。在早期阶段检测到FUNDC1的瞬时激活,表现为Tyr18的去磷酸化(在3 小时)的神经元I/R损伤;然而,磷酸化的Tyr18再次出现,甚至在后期(6 小时),同时FUNDC1轻链3相互作用减少。FUNDC1的自发失活与Src激活有关,以Tyr416的磷酸化为代表,在神经元I/R损伤期间,其与磷酸化FUNDC1(Tyr18)的水平平行变化。最后,在I/R条件下,FUNDC1介导的神经元线粒体自噬可以通过Src的药理学抑制来挽救。结论:FUNDC1在后期被Src灭活(6 小时)的神经元I/R损伤以及FUNDC1介导的线粒体自噬的挽救可以作为治疗缺血性中风的潜在治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Src inhibition rescues FUNDC1-mediated neuronal mitophagy in ischaemic stroke.

Background: Ischaemic stroke triggers neuronal mitophagy, while the involvement of mitophagy receptors in ischaemia/reperfusion (I/R) injury-induced neuronal mitophagy remain not fully elucidated. Here, we aimed to investigate the involvement of mitophagy receptor FUN14 domain-containing 1 (FUNDC1) and its modulation in neuronal mitophagy induced by I/R injury.

Methods: Wild-type and FUNDC1 knockout mice were generated to establish models of neuronal I/R injury, including transient middle cerebral artery occlusion (tMCAO) in vivo and oxygen glucose deprivation/reperfusion in vitro. Stroke outcomes of mice with two genotypes were assessed. Neuronal mitophagy was analysed both in vivo and in vitro. Activities of FUNDC1 and its regulator Src were evaluated. The impact of Src on FUNDC1-mediated mitophagy was assessed through administration of Src antagonist PP1.

Results: To our surprise, FUNDC1 knockout mice subjected to tMCAO showed stroke outcomes comparable to those of their wild-type littermates. Although neuronal mitophagy could be activated by I/R injury, FUNDC1 deletion did not disrupt neuronal mitophagy. Transient activation of FUNDC1, represented by dephosphorylation of Tyr18, was detected in the early stages (within 3 hours) of neuronal I/R injury; however, phosphorylated Tyr18 reappeared and even surpassed baseline levels in later stages (after 6 hours), accompanied by a decrease in FUNDC1-light chain 3 interactions. Spontaneous inactivation of FUNDC1 was associated with Src activation, represented by phosphorylation of Tyr416, which changed in parallel with the level of phosphorylated FUNDC1 (Tyr18) during neuronal I/R injury. Finally, FUNDC1-mediated mitophagy in neurons under I/R conditions can be rescued by pharmacological inhibition of Src.

Conclusions: FUNDC1 is inactivated by Src during the later stage (after 6 hours) of neuronal I/R injury, and rescue of FUNDC1-mediated mitophagy may serve as a potential therapeutic strategy for treating ischaemic stroke.

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来源期刊
Journal of Investigative Medicine
Journal of Investigative Medicine MEDICINE, GENERAL & INTERNALMEDICINE, RESE-MEDICINE, RESEARCH & EXPERIMENTAL
自引率
0.00%
发文量
111
期刊介绍: Journal of Investigative Medicine (JIM) is the official publication of the American Federation for Medical Research. The journal is peer-reviewed and publishes high-quality original articles and reviews in the areas of basic, clinical, and translational medical research. JIM publishes on all topics and specialty areas that are critical to the conduct of the entire spectrum of biomedical research: from the translation of clinical observations at the bedside, to basic and animal research to clinical research and the implementation of innovative medical care.
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