DNMT3A dysfunction promotes neuroinflammation and exacerbates acute ischemic stroke

IF 10.7 Q1 MEDICINE, RESEARCH & EXPERIMENTAL MedComm Pub Date : 2024-07-14 DOI:10.1002/mco2.652
Tian-Jie Lyu, Xin Qiu, Yubo Wang, Ling Zhang, Yalun Dai, Xuechun Wang, Shunying Zhao, Meilin Xiang, Lu Cui, Si Cheng, Yang Liu, Hongqiu Gu, Yong Jiang, Xia Meng, Yilong Wang, Xingquan Zhao, Xianwei Wang, Qian Li, Meng Wang, Yingyu Jiang, Zhe Xu, Xinying Huang, Hao Li, Yongjun Wang, Zixiao Li
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Abstract

Somatic mutations related to clonal hematopoiesis of indeterminate potential (CHIP) are risk factors for stroke. The impact of DNMT3A, the most mutated gene in CHIP, on clinical functional outcomes of acute ischemic stroke (AIS) remains unclear. In a well-characterized cohort of 8524 ischemic stroke patients, we demonstrated that DNMT3A-driven CHIP was significantly associated with neurological disability in these patients. With a stroke mouse model of transient middle cerebral artery occlusion (tMCAO), we demonstrated that DNMT3A protein levels in the brain penumbra increased. The DNMT3A inhibitor RG108 administration amplified neutrophil proliferation in the blood, promoted neutrophil infiltration into the brain penumbra, and exaggerated proinflammatory activation in tMCAO male mice. DNMT3A inhibition also significantly increased infarct volume and worsened neurobehavioral function in tMCAO male mice. In conclusion, DNMT3A somatic mutations are associated with worsened neurological disability in some patients with AIS, potentially through increased neutrophil proliferation and infiltration in the ischemic brain region. These findings suggest a possible mechanism for proinflammatory activation and tissue damage in the affected brain tissue, highlighting the need for further research in this area.

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DNMT3A 功能障碍会促进神经炎症并加剧急性缺血性中风。
与不确定潜能克隆造血(CHIP)相关的体细胞突变是中风的危险因素。CHIP中突变最多的基因DNMT3A对急性缺血性中风(AIS)临床功能预后的影响仍不清楚。在一组特征明确的 8524 名缺血性中风患者中,我们证实 DNMT3A 驱动的 CHIP 与这些患者的神经残疾显著相关。我们利用一过性大脑中动脉闭塞(tMCAO)的中风小鼠模型证明,大脑半影中的 DNMT3A 蛋白水平升高。服用 DNMT3A 抑制剂 RG108 会扩大血液中中性粒细胞的增殖,促进中性粒细胞向脑半影浸润,并加剧 tMCAO 雄性小鼠的促炎激活。抑制 DNMT3A 还会显著增加 tMCAO 雄性小鼠的梗死体积,恶化其神经行为功能。总之,DNMT3A 体细胞突变与一些 AIS 患者的神经残疾恶化有关,这可能是通过中性粒细胞在缺血脑区的增殖和浸润增加所致。这些发现提示了受影响脑组织中促炎激活和组织损伤的可能机制,强调了在这一领域开展进一步研究的必要性。
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6.70
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审稿时长
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