Single-Cell RNA Sequencing and Assay for Transposase-Accessible Chromatin Using Sequencing Reveals Cellular and Molecular Dynamics of Aortic Aging in Mice

染色质 转录组 生物 衰老 表观遗传学 细胞生物学 转座酶 转录因子 嘉雅宠物 细胞 染色质免疫沉淀 染色质重塑 遗传学 基因表达 基因 发起人 基因组 转座因子
作者
Wenhui Xie,Yilang Ke,Qinyi You,Jing Li,Lu Chen,Dang Li,Jun Fang,Xiaofeng Chen,Yuanyuan Zhou,Liangwan Chen,Huashan Hong
出处
期刊:Arteriosclerosis, Thrombosis, and Vascular Biology [Lippincott Williams & Wilkins]
卷期号:42 (2): 156-171 被引量:25
标识
DOI:10.1161/atvbaha.121.316883
摘要

The impact of vascular aging on cardiovascular diseases has been extensively studied; however, little is known regarding the cellular and molecular mechanisms underlying age-related vascular aging in aortic cellular subpopulations. Approach and Results: Transcriptomes and transposase-accessible chromatin profiles from the aortas of 4-, 26-, and 86-week-old C57/BL6J mice were analyzed using single-cell RNA sequencing and assay for transposase-accessible chromatin sequencing. By integrating the heterogeneous transcriptome and chromatin accessibility data, we identified cell-specific TF (transcription factor) regulatory networks and open chromatin states. We also determined that aortic aging affects cell interactions, inflammation, cell type composition, dysregulation of transcriptional control, and chromatin accessibility. Endothelial cells 1 have higher gene set activity related to cellular senescence and aging than do endothelial cells 2. Moreover, construction of senescence trajectories shows that endothelial cell 1 and fibroblast senescence is associated with distinct TF open chromatin states and an mRNA expression model. Our data provide a system-wide model for transcriptional and epigenetic regulation during aortic aging at single-cell resolution.
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