Epigenetic mechanism of activity-dependent neuroprotective protein in the pathogenesis of autism spectrum disorders
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摘要
Autism spectrum disorder (ASD) is a widespread neurodevelopmental disorder with a high degree of genetic heterogeneity, but the etiology remains unknown. In recent years, hundreds of autism-related risk genes have been identified, many of which are directly linked to epigenetic mechanisms. Activity-dependent neuroprotective protein (ADNP) is one of the highest-risk genes for ASD, whose mutations cause ADNP syndrome with an ASD-like phenotype (also known as Helsmoortel-VanDerAa syndrome, HVDAS). In our collection of the largest ADNP mutation cohort in China, we found that a missense mutation close to the zinc finger leads to abnormal ADNP localization and neuronal morphology. In addition, 3D protein structure prediction showed that the structure of the zinc fingers of the mutant was altered. By chromatin immunoprecipitation, we confirmed that the mutant has an altered genome-wide distribution and leads to abnormal GABAergic neuron development by mediating the formation of the H3K27me3/H3K4me3 bivalent domain of NKX2-1, an important regulator of GABAergic neuron development, which may be associated with the development of ASD. Since ADNP is also one of the critical members of the SWI/SNF complex, it may be closely related to chromatin remodeling. We have obtained a full set of epigenetic modifications and Hi-C data from mouse brain, and in the future, we will continue to explore how ADNP regulates the formation of bivalent domains of significant neurodevelopmental genes through the 3D genome and how its abnormalities lead to the development of disease.
关键词
ADNP; ASD; Epigenetic; Neuronal development; Bivalent domain
报告人
陈颀
博士在读 复旦大学脑科学研究院

稿件作者
陈颀 复旦大学脑科学研究院
孙戴静 复旦大学脑科学研究院
熊曼 复旦大学脑科学研究院
徐琼 复旦大学附属儿科医院
江燕 复旦大学脑科学研究院
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    2024

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    2024

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崖州湾国家实验室
华中农业大学
浙江大学
中国遗传学会
中国遗传学会三维基因组学专委会
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中国生物信息学基因组信息学专委会
中国遗传学会表观遗传分会
中国细胞生物学学会染色质生物学分会
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