Authors: Salman Basrai, Ido Nofech-Mozes, Rajesh Detroja, Fernando L. Scolari, Mehran Bakhtiari, Andrea Arruda, Tracy Murphy, Scott V. Bratman, Steven M. Chan, Mark D. Minden, Jae Sook Ahn, Dennis D. H. Kim, Robert Kridel, Filio Billia, Sagi Abelson
Short Description: The abundance, dynamics, and context-dependent heterogeneity of DNA methylation, where a pattern considered abnormal in one cell type may be normal in another, complicate the identification of early methylation changes that drive or signal disease development. This complexity can obscure early markers of increased disease risk, making it challenging to detect and intervene in disease processes at their inception. Here, we report 31,744 CpG loci exhibiting highly consistent methylation profiles in the blood of young, healthy individuals. We assess alterations at these epigenetically stable loci in 8,886 individuals across 29 diverse cohorts, including those with hematological cancers (n = 3159), cardiovascular complications (n = 2788), and healthy controls (n = 2939). Our findings reveal methylation pattern disruption in myeloid and lymphoid malignancies, correlating with clonal burden dynamics and mutation frequency throughout leukemia treatment. In non-cancer cohorts, we observe that methylation levels at epigenetically stable loci become increasingly variable with age, a shift linked to higher cardiovascular disease risk and lower survival rates. This study highlights DNA methylation instability as a blood-based biomarker for both hematological cancer and cardiovascular disease and uncovers a mechanistic link between methylation dynamics and the expansion of maladaptive hematopoietic clones.
Interest: Epigenetics, DNA Methylation, Cardiogenic Shock, Transcription Factors