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在发育中的哺乳动物大脑中,具有独特的核区室相关的基因组结构。

Distinct nuclear compartment-associated genome architecture in the developing mammalian brain.

机构信息

Department of Neurological Surgery, University of California, San Francisco, San Francisco, CA, USA.

Eli and Edythe Broad Center of Regeneration Medicine and Stem Cell Research, University of California, San Francisco, San Francisco, CA, USA.

出版信息

Nat Neurosci. 2021 Sep;24(9):1235-1242. doi: 10.1038/s41593-021-00879-5. Epub 2021 Jul 8.

Abstract

Nuclear compartments are thought to play a role in three-dimensional genome organization and gene expression. In mammalian brain, the architecture and dynamics of nuclear compartment-associated genome organization is not known. In this study, we developed Genome Organization using CUT and RUN Technology (GO-CaRT) to map genomic interactions with two nuclear compartments-the nuclear lamina and nuclear speckles-from different regions of the developing mouse, macaque and human brain. Lamina-associated domain (LAD) architecture in cells in vivo is distinct from that of cultured cells, including major differences in LADs previously considered to be cell type invariant. In the mouse and human forebrain, dorsal and ventral neural precursor cells have differences in LAD architecture that correspond to their regional identity. LADs in the human and mouse cortex contain transcriptionally highly active sub-domains characterized by broad depletion of histone-3-lysine-9 dimethylation. Evolutionarily conserved LADs in human, macaque and mouse brain are enriched for transcriptionally active neural genes associated with synapse function. By integrating GO-CaRT maps with genome-wide association study data, we found speckle-associated domains to be enriched for schizophrenia risk loci, indicating a physical relationship between these disease-associated genetic variants and a specific nuclear structure. Our work provides a framework for understanding the relationship between distinct nuclear compartments and genome function in brain development and disease.

摘要

核区室被认为在三维基因组组织和基因表达中发挥作用。在哺乳动物大脑中,与核区室相关的基因组组织的结构和动态尚不清楚。在这项研究中,我们开发了使用 CUT 和 RUN 技术(GO-CaRT)来绘制基因组与两个核区室(核纤层和核斑点)相互作用的图谱的方法,这些相互作用来自发育中的小鼠、猕猴和人类大脑的不同区域。体内细胞的核纤层相关结构域(LAD)结构与培养细胞中的结构域不同,包括先前被认为是细胞类型不变的 LAD 中的主要差异。在小鼠和人类前脑中,背侧和腹侧神经前体细胞的 LAD 结构存在差异,这与其区域特征相对应。人类和小鼠皮质中的 LAD 包含转录活性高的亚结构域,其特征是组蛋白-3-赖氨酸-9 二甲基化广泛缺失。人类、猕猴和小鼠大脑中进化保守的 LAD 富含与突触功能相关的转录活跃的神经基因。通过将 GO-CaRT 图谱与全基因组关联研究数据整合,我们发现斑点相关结构域富含精神分裂症风险位点,表明这些与疾病相关的遗传变异与特定核结构之间存在物理关系。我们的工作为理解大脑发育和疾病中不同核区室与基因组功能之间的关系提供了框架。

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