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Renin-Angiotensin System Inhibitor Discontinuation Does Not Modify Systemic ACE2 Levels in COVID-19: A Randomized, Open-Label, Controlled Trial (preprint)

Vincent Rathkolb; Marianna Traugott; Andreas Heinzel; Marko Poglitsch; Judith Aberle; Farsad Eskandary; Agnes Abrahamowicz; Martin Mueller; Petra Knollmueller; Tarik Shoumariyeh; Jasmin Stuflesser; Ivan Seeber; Georg Gibas; Hannah Mayfurth; Viktoria Tinhof; Lukas Schmoelz; Markus Zeitlinger; Christian Schörgenhofer; Bernd Jilma; Bernd Genser; Wolfgang Hoepler; Sara Omid; Mario Karolyi; Christoph Wenisch; Rainer Oberbauer; Alexander Zoufaly; Manfred Hecking; Roman Reindl-Schwaighofer.

ssrn; 2023.

Preprint in English | PREPRINT-SSRN | ID: ppzbmed-10.2139.ssrn.4435341

Subject(s)

COVID-19 , Hypertension

The Systemic Renin-Angiotensin System in COVID-19 (preprint)

Roman Reindl-Schwaighofer; Sebastian Hödlmoser; Oliver Domenig; Katharina Krenn; Farsad Eskandary; Simon Krenn; Christian Schörgenhofer; Benedikt Rumpf; Mario Karolyi; Marianna T. Traugott; Agnes Abrahamowicz; Viktoria Tinhof; Hannah Mayfurth; Vincent Rathkolb; Sebastian Mußnig; Lukas Schmölz; Roman Ullrich; Andreas Heinzel; Franz König; Christina Binder; Diana Bonderman; Robert Strassl; Elisabeth Puchhammer-Stöckl; Gregor Gorkiewicz; Judith H. Aberle; Bernd Jilma; Christoph Wenisch; Marko Poglitsch; Rainer Oberbauer; Alexander Zoufaly; Manfred Hecking.

researchsquare; 2022.

Preprint in English | PREPRINT-RESEARCHSQUARE | ID: ppzbmed-10.21203.rs.3.rs-1381017.v2

ABSTRACT

Introduction: SARS-CoV-2 gains cell entry via angiotensin-converting enzyme (ACE) 2, a membrane-bound enzyme of the “alternative” (alt) renin-angiotensin system (RAS). ACE2 counteracts angiotensin II by converting it to potentially protective angiotensin 1–7.Methods Using mass spectrometry, we assessed key metabolites of the classical RAS (angiotensins I–II) and alt-RAS (angiotensins 1–7 and 1–5) pathways as well as ACE and ACE2 concentrations in 159 patients hospitalized with COVID-19, stratified by disease severity (severe, n = 76; non-severe: n = 83). Plasma renin activity (PRA-S) was calculated as the sum of RAS metabolites. We estimated ACE activity using the angiotensin II:I ratio (ACE-S) and estimated systemic alt-RAS activation using the ratio of alt-RAS axis metabolites to PRA-S (ALT-S). We applied mixed linear models to assess how PRA-S and ACE/ACE2 concentrations affected ALT-S, ACE-S, and angiotensins II and 1–7.Results Median angiotensin I and II levels were higher with severe versus non-severe COVID-19 (both p < 0.05), demonstrating activation of classical RAS. The difference disappeared with analysis limited to patients not taking a RAS inhibitor. ALT-S in severe COVID-19 increased with time (days 1–6: 0.12; days 11–16: 0.22) and correlated with ACE2 concentration (r = 0.831). ACE-S was lower in severe versus non-severe COVID-19 (p < 0.001), but ACE concentrations were similar between groups and weakly correlated with ACE-S (r = 0.232). ACE2 and ACE-S trajectories in severe COVID-19, however, did not differ between survivors and non-survivors. Overall RAS alteration in severe COVID-19 resembled severity of disease-matched patients with influenza. In mixed linear models, renin activity most strongly predicted angiotensin II and 1–7 levels. ACE2 also predicted angiotensin 1–7 levels and ALT-S. No single factor or the combined model, however, could fully explain ACE-S. ACE2 and ACE-S trajectories in severe COVID-19 did not differ between survivors and non-survivors.Conclusions Angiotensin II was elevated in severe COVID-19 but markedly influenced by RAS inhibitors and driven by overall RAS activation. ACE-S was significantly lower with severe COVID-19 and did not correlate with ACE concentrations. A shift to the alt-RAS axis because of increased ACE2 could partially explain the relative reduction in angiotensin II levels.

Subject(s)

COVID-19

Subject(s)

ABSTRACT

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