| Literature DB >> 33752803 |
Wanxia Gai1,2,3, Ze Zhou1,2, Sean Agbor-Enoh4,5,6, Xiaodan Fan7, Sheng Lian7, Peiyong Jiang1,2,3, Suk Hang Cheng1,2, John Wong8, Stephen L Chan9, Moon Kyoo Jang4,6, Yanqin Yang4,6, Raymond Hs Liang10, Wai Kong Chan11, Edmond Sk Ma11, Tak Y Leung12, Rossa Wk Chiu1,2, Hannah Valantine4,6, Kc Allen Chan1,2,3, Ym Dennis Lo1,2,3.
Abstract
We developed genetic-epigenetic tissue mapping (GETMap) to determine the tissue composition of plasma DNA carrying genetic variants not present in the constitutional genome through comparing their methylation profiles with relevant tissues. We validated this approach by showing that, in pregnant women, circulating DNA carrying fetal-specific alleles was entirely placenta-derived. In lung transplant recipients, we showed that, at 72 hr after transplantation, the lung contributed only a median of 17% to the plasma DNA carrying donor-specific alleles, and hematopoietic cells contributed a median of 78%. In hepatocellular cancer patients, the liver was identified as the predominant source of plasma DNA carrying tumor-specific mutations. In a pregnant woman with lymphoma, plasma DNA molecules carrying cancer mutations and fetal-specific alleles were accurately shown to be derived from the lymphocytes and placenta, respectively. Analysis of tissue origin for plasma DNA carrying genetic variants is potentially useful for noninvasive prenatal testing, transplantation monitoring, and cancer screening.Entities:
Keywords: GETMap; cfdna; ctdna; human; liquid biopsy; medicine; nipt; plasma DNA deconvolution
Year: 2021 PMID: 33752803 PMCID: PMC7997656 DOI: 10.7554/eLife.64356
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140