Assessing the prediction of type 2 diabetes risk using polygenic and clinical risk scores in South Asian study populations

Background: Genome-wide polygenic risk scores (PRS) have shown high specificity and sensitivity in predicting type 2 diabetes (T2D) risk in Europeans. However, the PRS-driven information and its clinical significance in non-Europeans are underrepresented. We examined the predictive efficacy and tran...

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Veröffentlicht in:Therapeutic advances in endocrinology and metabolism 2023-01, Vol.14, p.20420188231220120-20420188231220120
Hauptverfasser: Rout, Madhusmita, Wander, Gurpreet S., Ralhan, Sarju, Singh, Jai Rup, Aston, Christopher E., Blackett, Piers R., Chernausek, Steven, Sanghera, Dharambir K.
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Sprache:eng
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Zusammenfassung:Background: Genome-wide polygenic risk scores (PRS) have shown high specificity and sensitivity in predicting type 2 diabetes (T2D) risk in Europeans. However, the PRS-driven information and its clinical significance in non-Europeans are underrepresented. We examined the predictive efficacy and transferability of PRS models using variant information derived from genome-wide studies of Asian Indians (AIs) (PRSAI) and Europeans (PRSEU) using 13,974 AI individuals. Methods: Weighted PRS models were constructed and analyzed on 4602 individuals from the Asian Indian Diabetes Heart Study/Sikh Diabetes Study (AIDHS/SDS) as discovery/training and test/validation datasets. The results were further replicated in 9372 South Asian individuals from UK Biobank (UKBB). We also assessed the performance of each PRS model by combining data of the clinical risk score (CRS). Results: Both genetic models (PRSAI and PRSEU) successfully predicted the T2D risk. However, the PRSAI revealed 13.2% odds ratio (OR) 1.80 [95% confidence interval (CI) 1.63–1.97; p = 1.6 × 10−152] and 12.2% OR 1.38 (95% CI 1.30–1.46; p = 7.1 × 10−237) superior performance in AIDHS/SDS and UKBB validation sets, respectively. Comparing individuals of extreme PRS (ninth decile) with the average PRS (fifth decile), PRSAI showed about two-fold OR 20.73 (95% CI 10.27–41.83; p = 2.7 × 10−17) and 1.4-fold OR 3.19 (95% CI 2.51–4.06; p = 4.8 × 10−21) higher predictability to identify subgroups with higher genetic risk than the PRSEU. Combining PRS and CRS improved the area under the curve from 0.74 to 0.79 in PRSAI and 0.72 to 0.75 in PRSEU. Conclusion: Our data suggest the need for extending genetic and clinical studies in varied ethnic groups to exploit the full clinical potential of PRS as a risk prediction tool in diverse study populations.
ISSN:2042-0188
2042-0196
DOI:10.1177/20420188231220120