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The DNA methylome of human vascular endothelium and its use in liquid biopsies

DNA甲基化 表观遗传学 生物 肺癌 病理 甲基化 疾病 生物标志物 基因 免疫学 生物信息学 癌症研究 基因表达 医学 遗传学 内科学
作者
Ayelet Peretz,Netanel Loyfer,Sheina Piyanzin,Bracha Lea Ochana,Daniel Neiman,Judith Magenheim,Agnes Klochendler,Zeina Drawshy,Ilana Fox-Fisher,Ori Fridlich,Joshua Moss,Daniel Cohen,Hai Zemmour,Gordon Cann,Joerg Bredno,Oliver Venn,Batia Avni,Tural Alekberli,Yaacov Samet,Amit Korach,Ori Wald,Vladimir Yutkin,Uzi Izhar,Nir Pillar,Markus Grompe,Zvi G. Fridlender,Ariel Rokach,David Planer,Giora Landesberg,Benjamin Gläser,Ruth Shemer,Tommy Kaplan,Yuval Dor
出处
期刊:Med [Elsevier]
卷期号:4 (4): 263-281.e4 被引量:2
标识
DOI:10.1016/j.medj.2023.03.006
摘要

Background: Vascular endothelial cells (VECs) are an essential component of each tissue, contribute to multiple pathologies, and are targeted by important drugs. Yet, there is a shortage of biomarkers to assess VEC turnover. Methods: To develop DNA methylation-based liquid biopsies for VECs, we determined the methylome of VECs isolated from freshly dissociated human tissues. Findings: A comparison with a human cell-type methylome atlas yielded thousands of loci that are uniquely unmethylated in VECs. These sites are typically gene enhancers, often residing adjacent to VEC-specific genes. We also identified hundreds of genomic loci that are differentially methylated in organotypic VECs, indicating that VECs feeding specific organs are distinct cell types with a stable epigenetic identity. We established universal and lung-specific VEC markers and evaluated their presence in circulating cell-free DNA (cfDNA). Nearly 2.5% of cfDNA in the plasma of healthy individuals originates from VECs. Sepsis, graft versus host disease, and cardiac catheterization are associated with elevated levels of VEC-derived cfDNA, indicative of vascular damage. Lung-specific VEC cfDNA is selectively elevated in patients with chronic obstructive pulmonary disease (COPD) or lung cancer, revealing tissue-specific vascular turnover. Conclusions: VEC cfDNA biomarkers inform vascular dynamics in health and disease, potentially contributing to early diagnosis and monitoring of pathologies, and assessment of drug activity. Funding: This work was supported by the Beutler Research Program, Helmsley Charitable Trust, JDRF, Grail and the DON Foundation (to Y.D.). Y.D holds the Walter & Greta Stiel Chair in heart studies. B.G., R.S., J.M., D.N., T.K., and Y.D. filed patents on cfDNA analysis.
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