The m6A methyltransferase METTL3 drives neuroinflammation and neurotoxicity through stabilizing BATF mRNA in microglia.

IF 13.7 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Cell Death and Differentiation Pub Date : 2024-06-20 DOI:10.1038/s41418-024-01329-y
Xun Wu, Haixiao Liu, Jin Wang, Shenghao Zhang, Qing Hu, Tinghao Wang, Wenxing Cui, Yingwu Shi, Hao Bai, Jinpeng Zhou, Liying Han, Leiyang Li, Tianzhi Zhao, Yang Wu, Jianing Luo, Dayun Feng, Wei Guo, Shunnan Ge, Yan Qu
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Abstract

Persistent neuroinflammation and progressive neuronal loss are defining features of acute brain injury including traumatic brain injury (TBI) and cerebral stroke. Microglia, the most abundant type of brain-resident immune cells, continuously surveil the environment and play a central role in shaping the inflammatory state of the central nervous system (CNS). In the study, we discovered that the protein expression of METTL3 (a m6A methyltransferase) was upregulated in inflammatory microglia independent of increased Mettl3 gene transcription following TBI in both human and mouse subjects. Subsequently, we identified TRIP12, a HECT-domain E3 ubiquitin ligase, as a negative regulator of METTL3 protein expression by facilitating METTL3 K48-linked polyubiquitination. Importantly, selective ablation of Mettl3 inhibited microglial pathogenic activities, diminished neutrophil infiltration, rescued neuronal loss and facilitated functional recovery post-TBI. Using MeRIP-seq and CUT&Tag sequencing, we identified that METTL3 promoted the expression of Basic Leucine Zipper Transcriptional Factor ATF-Like (BATF), which in turn directly bound to a cohort of characteristic inflammatory cytokines and chemokine genes. Enhanced activities of BATF in microglia elicited TNF-dependent neurotoxicity and can also promote neutrophil recruitment through releasing CXCL2. Pharmacological inhibition of METTL3 using a BBB-penetrating drug-loaded nano-system showed satisfactory therapeutic effects in both TBI and stroke mouse models. Collectively, our findings identified METTL3-m6A-BATF axis as a potential therapeutic target for terminating detrimental neuroinflammation and progressive neuronal loss following acute brain injury. METTL3 protein is significantly up-regulated in inflammatory microglia due to the decreased proteasomal degradation mediated by TRIP12 and ERK-USP5 pathways. METTL3 stabilized BATF mRNA stability and promoted BATF expression through the m6A-IGF2BP2-dependent mechanism. Elevated expression of BATF elicits a pro-inflammatory gene program in microglia, and aggravates neuroinflammatory response including local immune responses and peripheral immune cell infiltration. Genetic deletion or pharmaceutically targeting METTL3-BATF axis suppressed microglial pro-inflammatory activities and promoted neurological recovery following TBI and stroke.

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m6A甲基转移酶METTL3通过稳定小胶质细胞中的BATF mRNA驱动神经炎症和神经毒性。
持续的神经炎症和进行性神经元损失是包括创伤性脑损伤(TBI)和脑卒中在内的急性脑损伤的显著特征。小胶质细胞是脑驻留免疫细胞中数量最多的一种,它们不断监测周围环境,在中枢神经系统(CNS)炎症状态的形成过程中发挥着核心作用。在这项研究中,我们发现在人和小鼠受到创伤性脑损伤后,炎性小胶质细胞中 METTL3(一种 m6A 甲基转移酶)的蛋白表达上调,而与 Mettl3 基因转录增加无关。随后,我们确定了 TRIP12(一种 HECT 域 E3 泛素连接酶)通过促进 METTL3 K48 链接的多泛素化而成为 METTL3 蛋白表达的负调控因子。重要的是,选择性消减Mettl3可抑制小胶质细胞的致病活动,减少中性粒细胞浸润,挽救神经元损失并促进创伤后功能恢复。通过 MeRIP-seq 和 CUT&Tag 测序,我们发现 METTL3 促进了碱性亮氨酸拉链转录因子 ATF-Like (BATF)的表达,而 BATF 又直接与一系列特征性炎症细胞因子和趋化因子基因结合。小胶质细胞中 BATF 活性的增强会诱发 TNF 依赖性神经毒性,还能通过释放 CXCL2 促进中性粒细胞的募集。在创伤性脑损伤和脑卒中小鼠模型中,使用 BBB 穿透性药物载荷纳米系统对 METTL3 进行药理抑制显示出令人满意的治疗效果。总之,我们的研究结果发现,METTL3-m6A-BATF 轴是终止急性脑损伤后有害神经炎症和进行性神经元损失的潜在治疗靶点。由于 TRIP12 和 ERK-USP5 通路介导的蛋白酶体降解减少,METTL3 蛋白在炎性小胶质细胞中明显上调。METTL3 可稳定 BATF mRNA 的稳定性,并通过 m6A-IGF2BP2 依赖性机制促进 BATF 的表达。BATF 的表达升高会引起小胶质细胞中的促炎基因程序,并加重神经炎症反应,包括局部免疫反应和外周免疫细胞浸润。基因缺失或药物靶向 METTL3-BATF 轴可抑制小胶质细胞促炎活动,促进创伤性脑损伤和中风后的神经功能恢复。
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来源期刊
Cell Death and Differentiation
Cell Death and Differentiation 生物-生化与分子生物学
CiteScore
24.70
自引率
1.60%
发文量
181
审稿时长
3 months
期刊介绍: Mission, vision and values of Cell Death & Differentiation: To devote itself to scientific excellence in the field of cell biology, molecular biology, and biochemistry of cell death and disease. To provide a unified forum for scientists and clinical researchers It is committed to the rapid publication of high quality original papers relating to these subjects, together with topical, usually solicited, reviews, meeting reports, editorial correspondence and occasional commentaries on controversial and scientifically informative issues.
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