Comprehensive human cell-type methylation atlas reveals origins of circulating cell-free DNA in health and disease

Joshua Moss(Hebrew University of Jerusalem), Judith Magenheim, Daniel Neiman, Hai Zemmour, Netanel Loyfer(Hebrew University of Jerusalem), Amit Korach(Hadassah Medical Center), Yaacov Samet(Hadassah Medical Center), Myriam Maoz(Hadassah Medical Center), Henrik Druid(Swedish National Board of Forensic Medicine), Peter Arner(Karolinska University Hospital), Keng-Yeh Fu(Karolinska Institutet), Еndre Kiss(Karolinska Institutet), Kirsty L. Spalding(Karolinska University Hospital), Giora Landesberg(Hadassah Medical Center), Aviad Zick(Hadassah Medical Center), Albert Grinshpun(Hadassah Medical Center), A. M. James Shapiro(University of Alberta), Markus Grompe(Oregon Health & Science University), Avigail Dreazan Wittenberg, Benjamin Gläser(Hadassah Medical Center), Ruth Shemer(Hebrew University of Jerusalem), Tommy Kaplan(Hebrew University of Jerusalem), Yuval Dor(Hebrew University of Jerusalem)
Nature Communications
November 23, 2018
Cited by 1,026Open Access
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Abstract

Methylation patterns of circulating cell-free DNA (cfDNA) contain rich information about recent cell death events in the body. Here, we present an approach for unbiased determination of the tissue origins of cfDNA, using a reference methylation atlas of 25 human tissues and cell types. The method is validated using in silico simulations as well as in vitro mixes of DNA from different tissue sources at known proportions. We show that plasma cfDNA of healthy donors originates from white blood cells (55%), erythrocyte progenitors (30%), vascular endothelial cells (10%) and hepatocytes (1%). Deconvolution of cfDNA from patients reveals tissue contributions that agree with clinical findings in sepsis, islet transplantation, cancer of the colon, lung, breast and prostate, and cancer of unknown primary. We propose a procedure which can be easily adapted to study the cellular contributors to cfDNA in many settings, opening a broad window into healthy and pathologic human tissue dynamics.


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