DNA甲基化
碎片(计算)
核小体
胎儿游离DNA
DNA断裂
计算生物学
生物
DNA
液体活检
基因组学
遗传学
基因
基因组
癌症
组蛋白
基因表达
细胞凋亡
胎儿
生态学
产前诊断
怀孕
程序性细胞死亡
作者
Yunyun An,Xin Zhao,Ziteng Zhang,Zhaohua Xia,Mengqi Yang,Li Ma,Yu Zhao,Gang Xu,Shunda Du,Xiang’an Wu,Shuowen Zhang,Xin Hong,Xin Jin,Kun Sun
标识
DOI:10.1038/s41467-023-35959-6
摘要
Plasma cell-free DNA (cfDNA) are small molecules generated through a non-random fragmentation procedure. Despite commendable translational values in cancer liquid biopsy, however, the biology of cfDNA, especially the principles of cfDNA fragmentation, remains largely elusive. Through orientation-aware analyses of cfDNA fragmentation patterns against the nucleosome structure and integration with multidimensional functional genomics data, here we report a DNA methylation - nuclease preference - cutting end - size distribution axis, demonstrating the role of DNA methylation as a functional molecular regulator of cfDNA fragmentation. Hence, low-level DNA methylation could increase nucleosome accessibility and alter the cutting activities of nucleases during DNA fragmentation, which further leads to variation in cutting sites and size distribution of cfDNA. We further develop a cfDNA ending preference-based metric for cancer diagnosis, whose performance has been validated by multiple pan-cancer datasets. Our work sheds light on the molecular basis of cfDNA fragmentation towards broader applications in cancer liquid biopsy.
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