Assessing the performance of European-derived cardiometabolic polygenic risk scores in South-Asians and their interplay with family history

Emadeldin Hassanin; Carlo Maj; Hannah Klinkhammer; Peter Krawitz; Patrick May; Dheeraj Reddy Bobbili

doi:10.1186/s12920-023-01598-5

BMC Medical Genomics (Jul 2023)

Assessing the performance of European-derived cardiometabolic polygenic risk scores in South-Asians and their interplay with family history

Emadeldin Hassanin,
Carlo Maj,
Hannah Klinkhammer,
Peter Krawitz,
Patrick May,
Dheeraj Reddy Bobbili

Affiliations

Emadeldin Hassanin: Luxembourg Centre for Systems Biomedicine, University of Luxembourg
Carlo Maj: Centre for Human Genetics, University of Marburg
Hannah Klinkhammer: Institute for Genomic Statistics and Bioinformatics, University of Bonn
Peter Krawitz: Institute for Genomic Statistics and Bioinformatics, University of Bonn
Patrick May: Luxembourg Centre for Systems Biomedicine, University of Luxembourg
Dheeraj Reddy Bobbili: Luxembourg Centre for Systems Biomedicine, University of Luxembourg

DOI: https://doi.org/10.1186/s12920-023-01598-5
Journal volume & issue: Vol. 16, no. 1
pp. 1 – 11

Abstract

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Abstract Background & aims We aimed to assess the performance of European-derived polygenic risk scores (PRSs) for common metabolic diseases such as coronary artery disease (CAD), obesity, and type 2 diabetes (T2D) in the South Asian (SAS) individuals in the UK Biobank. Additionally, we studied the interaction between PRS and family history (FH) in the same population. Methods To calculate the PRS, we used a previously published model derived from the EUR population and applied it to the individuals of SAS ancestry from the UKB study. Each PRS was adjusted according to an individual’s genotype location in the principal components (PC) space to derive an ancestry adjusted PRS (aPRS). We calculated the percentiles based on aPRS and stratified individuals into three aPRS categories: low, intermediate, and high. Considering the intermediate-aPRS percentile as a reference, we compared the low and high aPRS categories and generated the odds ratio (OR) estimates. Further, we measured the combined role of aPRS and first-degree family history (FH) in the SAS population. Results The risk of developing severe obesity for SAS individuals was almost twofold higher for individuals with high aPRS than for those with intermediate aPRS, with an OR of 1.95 (95% CI = 1.71–2.23, P < 0.01). At the same time, the risk of severe obesity was lower in the low-aPRS group (OR = 0.60, CI = 0.53–0.67, P < 0.01). Results in the same direction were found in the EUR data, where the low-PRS group had an OR of 0.53 (95% CI = 0.51–0.56, P < 0.01) and the high-PRS group had an OR of 2.06 (95% CI = 2.00-2.12, P < 0.01). We observed similar results for CAD and T2D. Further, we show that SAS individuals with a familial history of CAD and T2D with high-aPRS are associated with a higher risk of these diseases, implying a greater genetic predisposition. Conclusion Our findings suggest that CAD, obesity, and T2D GWAS summary statistics generated predominantly from the EUR population can be potentially used to derive aPRS in SAS individuals for risk stratification. With future GWAS recruiting more SAS participants and tailoring the PRSs towards SAS ancestry, the predictive power of PRS is likely to improve further.

Published in BMC Medical Genomics

ISSN: 1755-8794 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine; Science: Biology (General): Genetics
Website: https://bmcmedgenomics.biomedcentral.com

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