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Circulating cell-free methylated DNA reveals tissue-specific, cellular damage from radiation treatment

Authors :
Megan E. McNamara
Netanel Loyfer
Amber J. Kiliti
Marcel O. Schmidt
Sapir Shabi-Porat
Sidharth S. Jain
Sarah Martinez Roth
A. Patrick McDeed IV
Nesreen Shahrour
Elizabeth Ballew
Yun-Tien Lin
Heng-Hong Li
Anne Deslattes Mays
Sonali Rudra
Anna T. Riegel
Keith Unger
Tommy Kaplan
Anton Wellstein
Source :
JCI Insight, Vol 8, Iss 14 (2023)
Publication Year :
2023
Publisher :
American Society for Clinical investigation, 2023.

Abstract

Radiation therapy is an effective cancer treatment, although damage to healthy tissues is common. Here we analyzed cell-free, methylated DNA released from dying cells into the circulation to evaluate radiation-induced cellular damage in different tissues. To map the circulating DNA fragments to human and mouse tissues, we established sequencing-based, cell-type-specific reference DNA methylation atlases. We found that cell-type-specific DNA blocks were mostly hypomethylated and located within signature genes of cellular identity. Cell-free DNA fragments were captured from serum samples by hybridization to CpG-rich DNA panels and mapped to the DNA methylation atlases. In a mouse model, thoracic radiation-induced tissue damage was reflected by dose-dependent increases in lung endothelial and cardiomyocyte methylated DNA in serum. The analysis of serum samples from patients with breast cancer undergoing radiation treatment revealed distinct dose-dependent and tissue-specific epithelial and endothelial responses to radiation across multiple organs. Strikingly, patients treated for right-sided breast cancers also showed increased hepatocyte and liver endothelial DNA in the circulation, indicating the impact on liver tissues. Thus, changes in cell-free methylated DNA can uncover cell-type-specific effects of radiation and provide a readout of the biologically effective radiation dose received by healthy tissues.

Subjects

Subjects :
Genetics
Oncology
Medicine

Details

Language :
English
ISSN :
23793708
Volume :
8
Issue :
14
Database :
Directory of Open Access Journals
Journal :
JCI Insight
Publication Type :
Academic Journal
Accession number :
edsdoj.0eb9bcb8aa8b40a4ba4c47c4e39aa949
Document Type :
article
Full Text :
https://doi.org/10.1172/jci.insight.156529