Feasibility of multiorgan risk prediction with routinely collected diagnostics: a prospective cohort study in the UK Biobank

Author:

McCracken CelesteORCID,Raisi-Estabragh Zahra,Szabo Liliana,Veldsman Michele,Raman Betty,Topiwala Anya,Roca-Fernández Adriana,Husain Masud,Petersen Steffen E,Neubauer Stefan,Nichols Thomas E

Abstract

ObjectivesDespite rising rates of multimorbidity, existing risk assessment tools are mostly limited to a single outcome of interest. This study tests the feasibility of producing multiple disease risk estimates with at least 70% discrimination (area under the receiver operating curve, AUROC) within the time and information constraints of the existing primary care health check framework.DesignObservational prospective cohort studySettingUK Biobank.Participants228 240 adults from the UK population.InterventionsNone.Main outcome measuresMyocardial infarction, atrial fibrillation, heart failure, stroke, all-cause dementia, chronic kidney disease, fatty liver disease, alcoholic liver disease, liver cirrhosis and liver failure.ResultsUsing a set of predictors easily gathered at the standard primary care health check (such as the National Health Service Health Check), we demonstrate that it is feasible to simultaneously produce risk estimates for multiple disease outcomes with AUROC of 70% or greater. These predictors can be entered once into a single form and produce risk scores for stroke (AUROC 0.727, 95% CI 0.713 to 0.740), all-cause dementia (0.823, 95% CI 0.810 to 0.836), myocardial infarction (0.785, 95% CI 0.775 to 0.795), atrial fibrillation (0.777, 95% CI 0.768 to 0.785), heart failure (0.828, 95% CI 0.818 to 0.838), chronic kidney disease (0.774, 95% CI 0.765 to 0.783), fatty liver disease (0.766, 95% CI 0.753 to 0.779), alcoholic liver disease (0.864, 95% CI 0.835 to 0.894), liver cirrhosis (0.763, 95% CI 0.734 to 0.793) and liver failure (0.746, 95% CI 0.695 to 0.796).ConclusionsEasily collected diagnostics can be used to assess 10-year risk across multiple disease outcomes, without the need for specialist computing or invasive biomarkers. Such an approach could increase the utility of existing data and place multiorgan risk information at the fingertips of primary care providers, thus creating opportunities for longer-term multimorbidity prevention. Additional work is needed to validate whether these findings would hold in a larger, more representative cohort outside the UK Biobank.

Funder

BHF Centre of Research Excellence, Oxford

HORIZON EUROPE Reforming and enhancing the European Research and Innovation system

NIHR Integrated Academic Training

Health Data Research UK

UK Research and Innovation

Wellcome Trust

BHF Clinical Research Training Fellowship

NIHR Oxford Biomedical Research Centre

NIHR Barts Biomedical Research Centre, Queen Mary University of London

Publisher

BMJ

Reference71 articles.

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