A mechanistic model and therapeutic interventions for COVID-19 involving a RAS-mediated bradykinin storm
Michael R Garvin,
Christiane Alvarez,
J Izaak Miller,
Erica T Prates,
Angelica M Walker,
B Kirtley Amos,
Alan E Mast,
Amy Justice,
Bruce Aronow,
Daniel Jacobson
Affiliations
Michael R Garvin
Oak Ridge National Laboratory, Biosciences Division, Oak Ridge, United States
Christiane Alvarez
Oak Ridge National Laboratory, Biosciences Division, Oak Ridge, United States
J Izaak Miller
Oak Ridge National Laboratory, Biosciences Division, Oak Ridge, United States
Erica T Prates
Oak Ridge National Laboratory, Biosciences Division, Oak Ridge, United States
Angelica M Walker
Oak Ridge National Laboratory, Biosciences Division, Oak Ridge, United States; University of Tennessee Knoxville, The Bredesen Center for Interdisciplinary Research and Graduate Education, Knoxville, United States
B Kirtley Amos
University of Kentucky, Department of Horticulture, Lexington, United States
Alan E Mast
Versiti Blood Research Institute, Medical College of Wisconsin, Milwaukee, United States
Amy Justice
VA Connecticut Healthcare/General Internal Medicine, Yale University School of Medicine, West Haven, United States
Bruce Aronow
University of Cincinnati, Cincinnati, United States; Biomedical Informatics, Cincinnati Children’s Hospital Research Foundation, Cincinnati, United States
Oak Ridge National Laboratory, Biosciences Division, Oak Ridge, United States; University of Tennessee Knoxville, The Bredesen Center for Interdisciplinary Research and Graduate Education, Knoxville, United States; University of Tennessee Knoxville, Department of Psychology, Austin Peay Building, Knoxville, United States
Neither the disease mechanism nor treatments for COVID-19 are currently known. Here, we present a novel molecular mechanism for COVID-19 that provides therapeutic intervention points that can be addressed with existing FDA-approved pharmaceuticals. The entry point for the virus is ACE2, which is a component of the counteracting hypotensive axis of RAS. Bradykinin is a potent part of the vasopressor system that induces hypotension and vasodilation and is degraded by ACE and enhanced by the angiotensin1-9 produced by ACE2. Here, we perform a new analysis on gene expression data from cells in bronchoalveolar lavage fluid (BALF) from COVID-19 patients that were used to sequence the virus. Comparison with BALF from controls identifies a critical imbalance in RAS represented by decreased expression of ACE in combination with increases in ACE2, renin, angiotensin, key RAS receptors, kinogen and many kallikrein enzymes that activate it, and both bradykinin receptors. This very atypical pattern of the RAS is predicted to elevate bradykinin levels in multiple tissues and systems that will likely cause increases in vascular dilation, vascular permeability and hypotension. These bradykinin-driven outcomes explain many of the symptoms being observed in COVID-19.
