Microglial mitochondrial DNA release contributes to neuroinflammation after intracerebral hemorrhage through activating AIM2 inflammasome

IF 4.6 2区 医学 Q1 NEUROSCIENCES Experimental Neurology Pub Date : 2024-09-13 DOI:10.1016/j.expneurol.2024.114950
Feng Gu , Zongqi Wang , Haojie Ding , Xinyu Tao , Juyi Zhang , Kun Dai , Xiang Li , Haitao Shen , Haiying Li , Zhouqing Chen , Zhong Wang
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Abstract

Intracerebral hemorrhage (ICH) is a severe disease that often leads to disability and death. Neuroinflammatory response is a key causative factor of early secondary brain injury after ICH. AIM2 is a DNA-sensing protein that recognizes cytosolic double-stranded DNA and take a significant part in neuroinflammation. Mitochondrial DNA participates in the translation of proteins such as the respiratory chain in the mitochondria. Whether mtDNA is involved in forming AIM2 inflammasome after ICH remains unclear. We used mice to construct ICH model in vivo and we used BV2 microglial cells treated with oxyhemoglobin to simulate ICH in vitro. Following lentiviral transfection to overexpress AIM2 antagonist P202, a notable decrease was observed in the levels of AIM2 inflammasome-associated proteins, leading to a reduction in dead neurons surrounding the hematoma and an enhancement in long-term and short-term behavior of neurological deficits. We further explored whether mtDNA took part in the AIM2 activation after ICH. The cytosolic mtDNA level was down-regulated by the mitochondrial division protector Mdivi-1 and up-regulated by transfection of mtDNA into cytoplasm. We found the expression level of AIM2 inflammasome-related proteins and inflammatory cytokines release were regulated by the cytosolic mtDNA level. In conclusion, after ICH, the mtDNA content in the cytoplasm of microglia around the hematoma rises, causing AIM2 inflammation leading to neuronal apoptosis, which leads to neurological deficits in mice. On the other hand, P202 was able to block inflammatory vesicle activation and improve neurological function by preventing the interaction between AIM2 protein and mitochondrial DNA.

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小胶质细胞线粒体 DNA 的释放通过激活 AIM2 炎症小体促进脑出血后的神经炎症
脑内出血(ICH)是一种严重疾病,常常导致残疾和死亡。神经炎症反应是 ICH 后早期继发性脑损伤的关键致病因素。AIM2 是一种 DNA 传感蛋白,能识别细胞膜双链 DNA,在神经炎症中起着重要作用。线粒体 DNA 参与线粒体呼吸链等蛋白质的翻译。mtDNA 是否参与了 ICH 后 AIM2 炎症小体的形成仍不清楚。我们用小鼠构建了体内 ICH 模型,并用氧合血红蛋白处理的 BV2 小神经胶质细胞模拟体外 ICH。慢病毒转染过表达 AIM2 拮抗剂 P202 后,观察到 AIM2 炎性体相关蛋白水平明显下降,导致血肿周围死亡神经元减少,神经功能缺损的长期和短期表现均有所改善。我们进一步探讨了 mtDNA 是否参与了 ICH 后 AIM2 的激活。线粒体分裂保护剂 Mdivi-1 下调了细胞膜 mtDNA 水平,而将 mtDNA 转染到细胞质中则上调了 mtDNA 水平。我们发现 AIM2 炎性体相关蛋白的表达水平和炎性细胞因子的释放受细胞质 mtDNA 水平的调控。总之,ICH后,血肿周围小胶质细胞胞浆中的mtDNA含量升高,引起AIM2炎症,导致神经细胞凋亡,从而导致小鼠神经功能缺损。另一方面,P202 能够阻止炎性囊泡的激活,并通过阻止 AIM2 蛋白和线粒体 DNA 之间的相互作用来改善神经功能。
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来源期刊
Experimental Neurology
Experimental Neurology 医学-神经科学
CiteScore
10.10
自引率
3.80%
发文量
258
审稿时长
42 days
期刊介绍: Experimental Neurology, a Journal of Neuroscience Research, publishes original research in neuroscience with a particular emphasis on novel findings in neural development, regeneration, plasticity and transplantation. The journal has focused on research concerning basic mechanisms underlying neurological disorders.
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