Risk of Type 2 Diabetes, MASLD and Cardiovascular Disease in People Living With Polycystic Ovary Syndrome

Author:

Henney Alex E123ORCID,Gillespiec Conor S4,Lai Jonathan Y M2,Schofield Pieta5,Riley David R12,Caleyachetty Rishi6,Barber Thomas M6,Miras Alexander D7,Dobbie Laurence J8,Hughes David M9,Alam Uazman123,Hydes Theresa J1210,Cuthbertson Daniel J123

Affiliation:

1. Department of Cardiovascular & Metabolic Medicine, University of Liverpool , Liverpool L69 7ZX , UK

2. Metabolism & Nutrition Research Group, Liverpool University Hospitals NHS Foundation Trust , Liverpool, Merseyside L9 7AL , UK

3. Liverpool Centre for Cardiovascular Sciences, University of Liverpool and Liverpool University Hospitals NHS Foundation Trust , Liverpool, Merseyside L69 7ZX , UK

4. Department of Clinical Neurosciences, University of Cambridge , Cambridge CB2 3PT , UK

5. Department of Public Health, Policy & Systems, University of Liverpool , Liverpool, Merseyside L69 7ZX , UK

6. Warwick Medical School, University of Warwick , Coventry CV4 7AL , UK

7. Department of Metabolism, Digestion and Reproduction, Imperial College London, Hammersmith Hospital , London SW7 2AZ , UK

8. Department of Diabetes and Endocrinology, Guy's and St Thomas’ NHS Foundation Trust , London SE1 7EH , UK

9. Institute of Population Health, University of Liverpool , Liverpool L69 7ZX , UK

10. Department of Gastroenterology and Hepatology, Liverpool University Hospitals NHS Foundation Trust , Liverpool, Merseyside L9 7AL , UK

Abstract

Abstract Background Polycystic ovary syndrome (PCOS) is associated with adverse clinical outcomes that may differ according to PCOS phenotype. Methods Using UK Biobank data, we compared the incidence of type 2 diabetes (T2D), metabolic dysfunction associated steatotic liver disease, cardiovascular disease (CVD), hormone-dependent cancers, and dementia between PCOS participants and age- and body mass index-matched controls. We also compared multiorgan (liver, cardiac, and brain) magnetic resonance imaging (MRI) data and examined the impact of PCOS phenotype (hyperandrogenic and normoandrogenic) on these outcomes. Results We included 1008 women with PCOS (defined by diagnostic codes, self-reported diagnoses, or clinical/biochemical features of hyperandrogenism and a/oligoCmenorrhoea) and 5017 matched controls (5:1 ratio); median age, 61 years, body mass index, 28.4 kg/m². Adjusted Cox proportional hazard modeling demonstrated PCOS participants had greater incident T2D [hazard ratio (HR) 1.47; 95% confidence interval (CI), 1.11-1.95] and all-cause CVD (1.76; 1.35-2.30). No between-group differences existed for cancers or dementia. Liver MRI confirmed more PCOS participants had hepatic steatosis (proton density fat fraction >5.5%: 35.9 vs 23.9%; P = .02) and higher fibroinflammation (corrected T1 721.4 vs 701.5 ms; P = <.01) vs controls. No between-group difference existed for cardiac (biventricular/atrial structure and function) or brain (grey and white matter volumes) imaging. Normoandrogenic (but not hyperandrogenic) PCOS participants had greater incident all-cause CVD (1.82; 1.29-2.56) while hyperandrogenic (but not normoandrogenic) PCOS participants were more likely to have hepatic steatosis (8.96 vs 6.04 vs 5.23%; P = .03) with greater fibroinflammation (776.3 vs 707.7 vs 701.9 ms; P=<.01). Conclusion Cardiometabolic disease may be increased in PCOS patients with a disease phenotype-specific pattern.

Publisher

The Endocrine Society

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