METTL3以m6A-HuR依赖性方式调节GPR39的表达,从而抑制新生儿缺氧缺血性脑病中的小胶质细胞脓毒症。

IF 2.9 3区 医学 Q2 NEUROSCIENCES Neuroscience Pub Date : 2024-10-24 DOI:10.1016/j.neuroscience.2024.10.038
Xili Jiang, Wei Zhang, Shucai Xie
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引用次数: 0

摘要

背景:新生儿缺氧缺血性脑病(HIE新生儿缺氧缺血性脑病(HIE)是导致新生儿死亡和长期残疾的重要原因。我们以前曾发现,在新生儿 HIE 大鼠模型中,GPR39 激活可减轻神经炎症。本研究旨在探讨 GPR39 是否会影响 HIE 后的小胶质细胞脓毒症:方法:建立了新生大鼠 HIE 模型和氧-葡萄糖剥夺(OGD)小胶质细胞模型。通过TTC、H&E染色和Nissl染色评估神经元损失和脑梗塞。用 Western 印迹、LDH 检测试剂盒、ELISA 和流式细胞术评估了嗜热症。总 m6A 水平和 GPR39 m6A 修饰是通过 m6A dot 印迹和 MeRIP 测定的。通过分子相互作用实验分析了 METTL3/HuR/GSK3β 与 GPR39 之间的相互作用。用放线菌素 D 检验了 GPR39 mRNA 的稳定性:结果:在新生 HIE 大鼠和 OGD 处理的小胶质细胞中,GPR39 水平升高。在 HIE 模型中,当 GPR39 被敲除时,脑损伤和神经元损失显著增加。敲除 GPR39 会加重 NLRP3 炎性体介导的小胶质细胞热解。METTL3 以 m6A 依赖性方式上调 GPR39 的表达。METTL3 增强了 HuR 和 GPR39 的相互作用。在暴露于 OGD 的小胶质细胞中,METTL3 提高了 GPR39 的表达和 mRNA 稳定性,而在 HuR 消耗后,这种表达和 mRNA 稳定性下降。敲除 METTL3 可促进小胶质细胞脓毒症,而 GPR39 激动剂可逆转这种现象。此外,GPR39上调可抑制小胶质细胞的脓毒症,但GSK3β激活剂SNP可逆转这一结果:结论:METTL3通过调控m6A-HuR依赖性GPR39的稳定来抑制新生儿HIE中的小胶质细胞脓毒症,这有助于新生儿HIE治疗药物的开发。
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METTL3 inhibits microglial pyroptosis in neonatal hypoxia-ischemia encephalopathy by regulating GPR39 expression in an m6A-HuR-dependent manner.

Background: Neonatal hypoxia-ischemia encephalopathy (HIE) is a significant reason for neonatal mortality and prolonged disability. We have previously revealed that GPR39 activation attenuates neuroinflammation in a neonatal HIE rat model. This study aimed to investigate whether GPR39 affected microglial pyroptosis post-HIE.

Methods: A neonatal rat model of HIE and a microglia cell model of oxygen-glucose deprivation (OGD) were established. Neuronal loss and cerebral infarction were assessed by using TTC, H&E staining, and Nissl staining. Pyroptosis was evaluated with western blot, LDH assay kit, ELISA, and flow cytometry. Total m6A level and GPR39 m6A modification were determined using m6A dot blot and MeRIP. The interaction between METTL3/HuR/GSK3β and GPR39 was analyzed by performing molecular interaction experiments. GPR39 mRNA stability was examined with actinomycin D.

Results: The level of GPR39 was increased in neonatal HIE rats and OGD-treated microglia. Brain injury and neuronal loss were significantly increased in the HIE model when GPR39 was knocked down. GPR39 knockdown aggravated NLRP3 inflammasome-mediated microglial pyroptosis. METTL3 upregulated GPR39 expression in an m6A-dependent manner. METTL3 enhanced the interaction of HuR and GPR39. In OGD-exposed microglia, METTL3 elevated GPR39 expression and mRNA stability, which declined after HuR depletion. METTL3 knockdown promoted microglial pyroptosis, which was reversed by GPR39 agonist. Furthermore, microglial pyroptosis was inhibited by GPR39 upregulation, but the outcome was reverted by GSK3β activator SNP.

Conclusion: METTL3 inhibits microglial pyroptosis in neonatal HIE via regulating m6A-HuR dependent stabilization of GPR39, which contributes to therapeutics development for neonatal HIE.

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来源期刊
Neuroscience
Neuroscience 医学-神经科学
CiteScore
6.20
自引率
0.00%
发文量
394
审稿时长
52 days
期刊介绍: Neuroscience publishes papers describing the results of original research on any aspect of the scientific study of the nervous system. Any paper, however short, will be considered for publication provided that it reports significant, new and carefully confirmed findings with full experimental details.
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