Polygenic Scores for Obstructive Sleep Apnoea Reveal Pathways Contributing to Cardiovascular Disease

Authors

Nuzulul Kurniansyah
Satu J Strausz
Geetha Chittoor
Shreyash Gupta
Anne E Justice
Yana Hrytsenko
Brendan T Keenan
Brian E Cade
Brian W Spitzer
Heming Wang
Jennifer Huffman
Matthew R Moll
Bernhard Haring
Su Yon Jung
Laura M Raffield
Robert Kaplan
Jerome I Rotter
Stephen S Rich
Sina A Gharib
Traci M Bartz
Peter Y Liu
Han Chen
Myriam Fornage
Lifang Hou
Daniel Levy
Alanna C Morrison
Heather M Ochs-Balcom
Bruce M Psaty
Peter W F Wilson
Kelly Cho
Allan I Pack
Hanna M Ollila
Susan Redline
Daniel J Gottlieb
Tamar Sofer

Publication Date

6-4-2025

Journal

eBioMedicine

Abstract

Background: Obstructive sleep apnoea (OSA) is a common chronic condition, with obesity its strongest risk factor. Polygenic scores (PGSs) summarise the genetic liability to phenotype and can provide insights into relationships between phenotypes. Recently, large datasets that include genetic data and OSA status became available, providing an opportunity to utilise PGS approaches to study the genetic relationship between OSA and other phenotypes, while differentiating OSA-specific from obesity-specific genetic factors.

Methods: Using race/ethnic diverse samples from over 1.2 million individuals from the Million Veteran Program, FinnGen, TOPMed, All of Us (AoU), Geisinger's MyCode, MGB Biobank, and the Human Phenotype Project, we developed and assessed PGSs for OSA, both without (BMIunadjOSA-PGS) and with adjustment for the genetic contributions of BMI (BMIadjOSA-PGS).

Findings: Adjusted odds ratios (ORs) for OSA per 1 standard deviation of the PGSs ranged from 1.38 to 2.75. The associations of BMIadjOSA- and BMIunadjOSA-PGSs with CVD outcomes in AoU shared both common and distinct patterns. Only BMIunadjOSA-PGS was associated with type 2 diabetes, heart failure, and coronary artery disease, while both BMIadjOSA- and BMIunadjOSA-PGSs were associated with hypertension and stroke. Sex stratified analyses revealed that BMIadjOSA-PGS association with hypertension was driven by females (OR = 1.1, p-value = 0.002, OR = 1.01 p-value = 0.2 in males). OSA PGSs were also associated with body fat measures with some sex-specific associations.

Interpretation: Distinct components of OSA genetic risk are related and independent of obesity. Sex-specific associations with body fat distribution measures may explain differing OSA risks and associations with cardiometabolic morbidities between sexes.

Funding: R01AG080598.

Keywords

Genetically determined OSA, Sex differences, Body fat distribution, Diverse populations

DOI

10.1016/j.ebiom.2025.105790

PMID

40472801

PMCID

PMC12171572

PubMedCentral® Posted Date

6-4-2025

PubMedCentral® Full Text Version

Post-print

Published Open-Access

yes