Renin-angiotensin system blockers and susceptibility to COVID-19: a multinational open science cohort study

  1. Daniel R. Morales
  2. Mitchell M. Conover
  3. Seng Chan You
  4. Nicole Pratt
  5. Kristin Kostka
  6. Talita Duarte-Salles
  7. Sergio Fernández-Bertolín
  8. Maria Aragón
  9. Scott L. DuVall
  10. Kristine Lynch
  11. Thomas Falconer
  12. Kees van Bochove
  13. Cynthia Sung
  14. Michael E. Matheny
  15. Christophe G. Lambert
  16. Fredrik Nyberg
  17. Thamir M. Alshammari
  18. Andrew E. Williams
  19. Rae Woong Park
  20. James Weaver
  21. Anthony G. Sena
  22. Martijn J. Schuemie
  23. Peter R. Rijnbeek
  24. Ross D. Williams
  25. Jennifer C.E. Lane
  26. Albert Prats-Uribe
  27. Lin Zhang
  28. Carlos Areia
  29. Harlan M. Krumholz
  30. Daniel Prieto-Alhambra
  31. Patrick B. Ryan
  32. George Hripcsak
  33. Marc A. Suchard
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Abstract

Introduction

Angiotensin converting enzyme inhibitors (ACEs) and angiotensin receptor blockers (ARBs) could influence infection risk of coronavirus disease (COVID-19). Observational studies to date lack pre-specification, transparency, rigorous ascertainment adjustment and international generalizability, with contradictory results.

Methods

Using electronic health records from Spain (SIDIAP) and the United States (Columbia University Irving Medical Center and Department of Veterans Affairs), we conducted a systematic cohort study with prevalent ACE, ARB, calcium channel blocker (CCB) and thiazide diuretic (THZ) users to determine relative risk of COVID-19 diagnosis and related hospitalization outcomes. The study addressed confounding through large-scale propensity score adjustment and negative control experiments.

Results

Following over 1.1 million antihypertensive users identified between November 2019 and January 2020, we observed no significant difference in relative COVID-19 diagnosis risk comparing ACE/ARB vs CCB/THZ monotherapy (hazard ratio: 0.98; 95% CI 0.84 - 1.14), nor any difference for mono/combination use (1.01; 0.90 - 1.15). ACE alone and ARB alone similarly showed no relative risk difference when compared to CCB/THZ monotherapy or mono/combination use. Directly comparing ACE vs. ARB demonstrated a moderately lower risk with ACE, non-significant for monotherapy (0.85; 0.69 - 1.05) and marginally significant for mono/combination users (0.88; 0.79 - 0.99). We observed, however, no significant difference between drug-classes for COVID-19 hospitalization or pneumonia risk across all comparisons.

Conclusion

There is no clinically significant increased risk of COVID-19 diagnosis or hospitalization with ACE or ARB use. Users should not discontinue or change their treatment to avoid COVID-19.

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