Prognostic validation of a non-laboratory and a laboratory based cardiovascular disease risk score in multiple regions of the world

Author:

Joseph Philip,Yusuf Salim,Lee Shun Fu,Ibrahim Quazi,Teo Koon,Rangarajan Sumathy,Gupta Rajeev,Rosengren Annika,Lear Scott A,Avezum Alvaro,Lopez-Jaramillo Patricio,Gulec Sadi,Yusufali Afzalhussein,Chifamba Jephat,Lanas Fernando,Kumar Rajesh,Mohammadifard Noushin,Mohan Viswanathan,Mony Prem,Kruger Annamarie,Liu Xu,Guo Baoxia,Zhao Wenqi,Yang Youzhu,Pillai Rajamohanan,Diaz Rafael,Krishnapillai Ambigga,Iqbal Romaina,Yusuf Rita,Szuba Andrzej,Anand Sonia S

Abstract

ObjectiveTo evaluate the performance of the non-laboratory INTERHEART risk score (NL-IHRS) to predict incident cardiovascular disease (CVD) across seven major geographic regions of the world. The secondary objective was to evaluate the performance of the fasting cholesterol-based IHRS (FC-IHRS).MethodsUsing measures of discrimination and calibration, we tested the performance of the NL-IHRS (n=100 475) and FC-IHRS (n=107 863) for predicting incident CVD in a community-based, prospective study across seven geographic regions: South Asia, China, Southeast Asia, Middle East, Europe/North America, South America and Africa. CVD was defined as the composite of cardiovascular death, myocardial infarction, stroke, heart failure or coronary revascularisation.ResultsMean age of the study population was 50.53 (SD 9.79) years and mean follow-up was 4.89 (SD 2.24) years. The NL-IHRS had moderate to good discrimination for incident CVD across geographic regions (concordance statistic (C-statistic) ranging from 0.64 to 0.74), although recalibration was necessary in all regions, which improved its performance in the overall cohort (increase in C-statistic from 0.69 to 0.72, p<0.001). Regional recalibration was also necessary for the FC-IHRS, which also improved its overall discrimination (increase in C-statistic from 0.71 to 0.74, p<0.001). In 85 078 participants with complete data for both scores, discrimination was only modestly better with the FC-IHRS compared with the NL-IHRS (0.74 vs 0.73, p<0.001).ConclusionsExternal validations of the NL-IHRS and FC-IHRS suggest that regionally recalibrated versions of both can be useful for estimating CVD risk across a diverse range of community-based populations. CVD prediction using a non-laboratory score can provide similar accuracy to laboratory-based methods.

Funder

Servier

Heart and Stroke Foundation of Canada

Canadian Institutes of Health Research

AstraZeneca Canada

GlaxoSmithKline

Sanofi-Aventis

Boehringer Ingelheim

Population Health Research Institute

Publisher

BMJ

Subject

Cardiology and Cardiovascular Medicine

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