Blood-based Epigenome-wide Analyses of Chronic Low-grade Inflammation Across Diverse Population Cohorts

Overview

Journal Cell Genom

Date 2024 May 1

PMID 38692281

Authors

Robert F Hillary

Hong Kiat Ng

Daniel L McCartney

Hannah R Elliott

Rosie M Walker

Archie Campbell

Felicia Huang

Kenan Direk

Paul Welsh

Naveed Sattar

Janie Corley

Caroline Hayward

Andrew M McIntosh

Cathie Sudlow

Kathryn L Evans

Simon R Cox

John C Chambers

Marie Loh

Caroline L Relton

Riccardo E Marioni

Paul D Yousefi

Matthew Suderman

Affiliations

Soon will be listed here.

Abstract

Chronic inflammation is a hallmark of age-related disease states. The effectiveness of inflammatory proteins including C-reactive protein (CRP) in assessing long-term inflammation is hindered by their phasic nature. DNA methylation (DNAm) signatures of CRP may act as more reliable markers of chronic inflammation. We show that inter-individual differences in DNAm capture 50% of the variance in circulating CRP (N = 17,936, Generation Scotland). We develop a series of DNAm predictors of CRP using state-of-the-art algorithms. An elastic-net-regression-based predictor outperformed competing methods and explained 18% of phenotypic variance in the Lothian Birth Cohort of 1936 (LBC1936) cohort, doubling that of existing DNAm predictors. DNAm predictors performed comparably in four additional test cohorts (Avon Longitudinal Study of Parents and Children, Health for Life in Singapore, Southall and Brent Revisited, and LBC1921), including for individuals of diverse genetic ancestry and different age groups. The best-performing predictor surpassed assay-measured CRP and a genetic score in its associations with 26 health outcomes. Our findings forge new avenues for assessing chronic low-grade inflammation in diverse populations.

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