Published
20 August 2020
  • Journal article

Multimorbidity, polypharmacy, and COVID-19 infection within the UK Biobank cohort

Authors
McQueenie, Ross
Foster, Hamish M.E.
Jani, Bhautesh D. 
Katikireddi, Srinivasa Vittal 
Sattar, Naveed
Pell, Jill P. 
Ho, Frederick K. 
Niedzwiedz, Claire L. 
Hastie, Claire E. 
Anderson, Jana J. 
Mark, Patrick B.
Sullivan, Michael
O'Donnell, Catherine A. 
Mair, Frances S.
Nicholl, Barbara I.
Source
PLoS One

Abstract

Background: It is now well recognised that the risk of severe COVID-19 increases with some long-term conditions (LTCs). However, prior research primarily focuses on individual LTCs and there is a lack of data on the influence of multimorbidity (≥2 LTCs) on the risk of COVID-19. Given the high prevalence of multimorbidity, more detailed understanding of the associations with multimorbidity and COVID-19 would improve risk stratification and help protect those most vulnerable to severe COVID-19. Here we examine the relationships between multimorbidity, polypharmacy (a proxy of multimorbidity), and COVID-19; and how these differ by sociodemographic, lifestyle, and physiological prognostic factors. Methods and findings: We studied data from UK Biobank (428,199 participants; aged 37–73; recruited 2006–2010) on self-reported LTCs, medications, sociodemographic, lifestyle, and physiological measures which were linked to COVID-19 test data. Poisson regression models examined risk of COVID-19 by multimorbidity/polypharmacy and effect modification by COVID-19 prognostic factors (age/sex/ethnicity/socioeconomic status/smoking/physical activity/BMI/systolic blood pressure/renal function). 4,498 (1.05%) participants were tested; 1,324 (0.31%) tested positive for COVID-19. Compared with no LTCs, relative risk (RR) of COVID-19 in those with 1 LTC was no higher (RR 1.12 (CI 0.96–1.30)), whereas those with ≥2 LTCs had 48% higher risk; RR 1.48 (1.28–1.71). Compared with no cardiometabolic LTCs, having 1 and ≥2 cardiometabolic LTCs had a higher risk of COVID-19; RR 1.28 (1.12–1.46) and 1.77 (1.46–2.15), respectively. Polypharmacy was associated with a dose response higher risk of COVID-19. All prognostic factors were associated with a higher risk of COVID-19 infection in multimorbidity; being non-white, most socioeconomically deprived, BMI ≥40 kg/m2, and reduced renal function were associated with the highest risk of COVID-19 infection: RR 2.81 (2.09–3.78); 2.79 (2.00–3.90); 2.66 (1.88–3.76); 2.13 (1.46–3.12), respectively. No multiplicative interaction between multimorbidity and prognostic factors was identified. Important limitations include the low proportion of UK Biobank participants with COVID-19 test data (1.05%) and UK Biobank participants being more affluent, healthier and less ethnically diverse than the general population. Conclusions: Increasing multimorbidity, especially cardiometabolic multimorbidity, and polypharmacy are associated with a higher risk of developing COVID-19. Those with multimorbidity and additional factors, such as non-white ethnicity, are at heightened risk of COVID-19.

Rights

Available under License Creative Commons Attribution.

Cite as

McQueenie, R., Foster, H., Jani, B., Katikireddi, S., Sattar, N., Pell, J., Ho, F., Niedzwiedz, C., Hastie, C., Anderson, J., Mark, P., Sullivan, M., O'Donnell, C., Mair, F. & Nicholl, B. 2020, 'Multimorbidity, polypharmacy, and COVID-19 infection within the UK Biobank cohort', PLoS One, 15(8), article no: e0238091. http://dx.doi.org/10.1371/journal.pone.0238091

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Topics
Coronavirus (COVID-19)
Keywords
COVID-19 Prescription medicines Long term conditions Risk factor
Publisher
Public Library of Science
Source repository
University of Glasgow
Last updated: 02 June 2023
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