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前额叶皮层中神经元 H3K4me3 表观基因组的发育调控和个体差异。

Developmental regulation and individual differences of neuronal H3K4me3 epigenomes in the prefrontal cortex.

机构信息

Department of Psychiatry, Brudnick Neuropsychiatric Research Institute, University of Massachusetts Medical School, Worcester, MA 01604, USA.

出版信息

Proc Natl Acad Sci U S A. 2010 May 11;107(19):8824-9. doi: 10.1073/pnas.1001702107. Epub 2010 Apr 26.

Abstract

Little is known about the regulation of neuronal and other cell-type specific epigenomes from the brain. Here, we map the genome-wide distribution of trimethylated histone H3K4 (H3K4me3), a mark associated with transcriptional regulation, in neuronal and nonneuronal nuclei collected from prefrontal cortex (PFC) of 11 individuals ranging in age from 0.5 to 69 years. Massively parallel sequencing identified 12,732-19,704 H3K4me3 enriched regions (peaks), the majority located proximal to (within 2 kb of) the transcription start site (TSS) of annotated genes. These included peaks shared by neurons in comparison with three control (lymphocyte) cell types, as well as peaks specific to individual subjects. We identified 6,213 genes that show highly enriched H3K4me3 in neurons versus control. At least 1,370 loci, including annotated genes and novel transcripts, were selectively tagged with H3K4me3 in neuronal but not in nonneuronal PFC chromatin. Our results reveal age-correlated neuronal epigenome reorganization, including decreased H3K4me3 at approximately 600 genes (many function in developmental processes) during the first year after birth. In comparison, the epigenome of aging (>60 years) PFC neurons showed less extensive changes, including increased H3K4me3 at 100 genes. These findings demonstrate that H3K4me3 in human PFC is highly regulated in a cell type- and subject-specific manner and highlight the importance of early childhood for developmentally regulated chromatin remodeling in prefrontal neurons.

摘要

目前对于大脑中神经元和其他细胞类型特异性表观基因组的调控知之甚少。在这里,我们绘制了来自 11 个人的前额叶皮层(PFC)神经元和非神经元核中小鼠组蛋白 H3K4 三甲基化(H3K4me3)的全基因组分布,年龄从 0.5 岁到 69 岁不等。大规模平行测序确定了 12732-19704 个 H3K4me3 富集区(峰),大多数位于注释基因的转录起始位点(TSS)附近(2kb 内)。这些峰包括与三种对照(淋巴细胞)细胞类型相比神经元中共享的峰,以及个体特异性的峰。我们确定了 6213 个在神经元中与对照相比高度富集 H3K4me3 的基因。至少有 1370 个基因,包括注释基因和新转录本,在神经元而非非神经元 PFC 染色质中被 H3K4me3 选择性标记。我们的结果揭示了与年龄相关的神经元表观基因组重排,包括出生后第一年约 600 个基因(许多在发育过程中起作用)的 H3K4me3 减少。相比之下,>60 岁 PFC 神经元的表观基因组变化不那么广泛,包括 100 个基因的 H3K4me3 增加。这些发现表明,人类 PFC 中的 H3K4me3 以细胞类型和个体特异性的方式受到高度调控,并强调了儿童早期对前额叶神经元发育调控染色质重塑的重要性。

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