KDM2A和H3K36me2去甲基化在神经发育过程中调节MAPK信号传导中的作用

IF 5.9 2区 医学 Q1 NEUROSCIENCES Neuroscience bulletin Pub Date : 2024-08-01 Epub Date: 2023-12-07 DOI:10.1007/s12264-023-01161-3
Zongyao Ren, Haiyan Tang, Wendiao Zhang, Minghui Guo, Jingjie Cui, Hua Wang, Bin Xie, Jing Yu, Yonghao Chen, Ming Zhang, Cong Han, Tianyao Chu, Qiuman Liang, Shunan Zhao, Yingjie Huang, Xuelian He, Kefu Liu, Chunyu Liu, Chao Chen
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引用次数: 0

摘要

智力残疾是一种以认知障碍和适应功能困难为特征的疾病。在我们的研究中,我们在不同程度ID的个体中发现了KDM2A位点的两个新生突变(c.955C>T和c.732C>A)。此外,通过Gene4Denovo数据库,我们发现了另外5例KDM2A从头突变。我们发现的突变显著降低了KDM2A蛋白的表达。为了研究KDM2A在神经发育中的作用,我们使用了2D神经干细胞模型和3D脑类器官。我们的研究结果表明,KDM2A的表达减少会损害神经祖细胞(npc)的增殖,增加细胞凋亡,诱导神经元过早分化,并影响突触成熟。通过ChIP-Seq分析,我们发现KDM2A与神经发生相关基因的转录起始位点区域结合。此外,KDM2A的敲低阻碍了H3K36me2与下游基因调控元件的结合。通过整合ChIP-Seq和RNA-Seq数据,我们发现了MAPK信号通路中核心基因的显著富集。重要的是,这种富集与p38 MAPK通路特异性相关。此外,疾病富集分析将npc和脑类器官的RNA-Seq鉴定的差异表达基因与神经发育障碍(如ID、自闭症谱系障碍和精神分裂症)联系起来。总的来说,我们的研究结果表明,KDM2A在调节下游基因H3K36me2修饰中起着至关重要的作用,从而调节MAPK信号通路,并可能影响早期大脑发育。
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The Role of KDM2A and H3K36me2 Demethylation in Modulating MAPK Signaling During Neurodevelopment.

Intellectual disability (ID) is a condition characterized by cognitive impairment and difficulties in adaptive functioning. In our research, we identified two de novo mutations (c.955C>T and c.732C>A) at the KDM2A locus in individuals with varying degrees of ID. In addition, by using the Gene4Denovo database, we discovered five additional cases of de novo mutations in KDM2A. The mutations we identified significantly decreased the expression of the KDM2A protein. To investigate the role of KDM2A in neural development, we used both 2D neural stem cell models and 3D cerebral organoids. Our findings demonstrated that the reduced expression of KDM2A impairs the proliferation of neural progenitor cells (NPCs), increases apoptosis, induces premature neuronal differentiation, and affects synapse maturation. Through ChIP-Seq analysis, we found that KDM2A exhibited binding to the transcription start site regions of genes involved in neurogenesis. In addition, the knockdown of KDM2A hindered H3K36me2 binding to the downstream regulatory elements of genes. By integrating ChIP-Seq and RNA-Seq data, we made a significant discovery of the core genes' remarkable enrichment in the MAPK signaling pathway. Importantly, this enrichment was specifically linked to the p38 MAPK pathway. Furthermore, disease enrichment analysis linked the differentially-expressed genes identified from RNA-Seq of NPCs and cerebral organoids to neurodevelopmental disorders such as ID, autism spectrum disorder, and schizophrenia. Overall, our findings suggest that KDM2A plays a crucial role in regulating the H3K36me2 modification of downstream genes, thereby modulating the MAPK signaling pathway and potentially impacting early brain development.

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来源期刊
Neuroscience bulletin
Neuroscience bulletin NEUROSCIENCES-
CiteScore
7.20
自引率
16.10%
发文量
163
审稿时长
6-12 weeks
期刊介绍: Neuroscience Bulletin (NB), the official journal of the Chinese Neuroscience Society, is published monthly by Shanghai Institutes for Biological Sciences (SIBS), Chinese Academy of Sciences (CAS) and Springer. NB aims to publish research advances in the field of neuroscience and promote exchange of scientific ideas within the community. The journal publishes original papers on various topics in neuroscience and focuses on potential disease implications on the nervous system. NB welcomes research contributions on molecular, cellular, or developmental neuroscience using multidisciplinary approaches and functional strategies. We feature full-length original articles, reviews, methods, letters to the editor, insights, and research highlights. As the official journal of the Chinese Neuroscience Society, which currently has more than 12,000 members in China, NB is devoted to facilitating communications between Chinese neuroscientists and their international colleagues. The journal is recognized as the most influential publication in neuroscience research in China.
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