• Am. J. Respir. Crit. Care Med. · Oct 2024

    Sex-specific Genetic Determinants of Right Ventricular Structure and Function.

    • Lars Harbaum, Jan K Hennigs, Julian Pott, Jonna Ostermann, Christoph R Sinning, Arunashis Sau, Ewa Sieliwonczyk, Fu Siong Ng, Christopher J Rhodes, Khodr Tello, Hans Klose, Stefan Gräf, and Martin R Wilkins.
    • Imperial College London, London, United Kingdom of Great Britain and Northern Ireland.
    • Am. J. Respir. Crit. Care Med. 2024 Oct 7.

    RationaleWhile sex differences in right heart phenotypes have been observed, the molecular drivers remain unknown.ObjectivesTo provide biological insights into sex differences in the structure and function of the right ventricle (RV) using common genetic variation.MethodsRV phenotypes were obtained from cardiac magnetic resonance imaging in 18,156 women and 16,171 men from the UK Biobank. Observational analyses and sex-stratified genome-wide association studies were performed. Candidate female-specific loci were evaluated against invasively measured cardiac performance in 479 female patients with idiopathic or heritable pulmonary arterial hypertension (PAH), recruited to the UK NIHR BioResource Rare Diseases study.Measurements And Main ResultsSex was associated with differences in RV volumes and ejection fraction in models adjusting for left heart counterparts, blood pressure, lung function and sex hormone levels. Six genome-wide significant loci (13%) revealed heterogeneity of allelic effects between women and men, and significant sex-by-genotype interaction. These included two sex-specific candidate loci present in women only: a locus for RV ejection fraction in BMPR1A and a locus for RV end-systolic volume near DMRT2. Epigenetic data in RV tissue indicate that variation at the BMPR1A locus likely alters transcriptional regulation. In female patients with PAH, a variant located in the promoter of BMPR1A was significantly associated with cardiac index (effect size 0.16 l/min/m2), despite similar RV afterload.ConclusionsBMPR1A has emerged as a biologically plausible candidate gene for female-specific genetic determination of RV function, showing associations with cardiac performance under chronically increased afterload in female patients with PAH.

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