Tracking single-cell evolution using clock-like chromatin accessibility loci

Author:

Xiao YuORCID,Jin Wan,Ju LingaoORCID,Fu JieORCID,Wang GangORCID,Yu Mengxue,Chen Fangjin,Qian KaiyuORCID,Wang XinghuanORCID,Zhang YiORCID

Abstract

AbstractSingle-cell chromatin accessibility sequencing (scATAC-seq) reconstructs developmental trajectory by phenotypic similarity. However, inferring the exact developmental trajectory is challenging. Previous studies showed age-associated DNA methylation (DNAm) changes in specific genomic regions, termed clock-like differential methylation loci (ClockDML). Age-associated DNAm could either result from or result in chromatin accessibility changes at ClockDML. As cells undergo mitosis, the heterogeneity of chromatin accessibility on clock-like loci is reduced, providing a measure of mitotic age. In this study, we developed a method, called EpiTrace, that counts the fraction of opened clock-like loci from scATAC-seq data to determine cell age and perform lineage tracing in various cell lineages and animal species. It shows concordance with known developmental hierarchies, correlates well with DNAm-based clocks and is complementary with mutation-based lineage tracing, RNA velocity and stemness predictions. Applying EpiTrace to scATAC-seq data reveals biological insights with clinically relevant implications, ranging from hematopoiesis, organ development, tumor biology and immunity to cortical gyrification.

Funder

Fundamental Research Funds for the Central Universities

National Natural Science Foundation of China

Research Fund of Zhongnan Hospital of Wuhan University

Publisher

Springer Science and Business Media LLC

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