IL-1β-driven NF-κB Transcription of ACE2 As a Mechanism of Macrophage Infection by SARS-CoV-2

Overview

Journal bioRxiv

Date 2025 Jan 7

PMID 39763770

Authors

Cadence Lee

Rachel Khan

Chris S Mantsounga

Sheila Sharma

Julia Pierce

Elizabeth Amelotte

Celia A Butler

Andrew Farinha

Crystal Parry

Olivya Caballero

Jeremi A Morrison

Saketh Uppuluri

Jeffrey J Whyte

Joshua L Kennedy

Xuming Zhang

Gaurav Choudhary

Rachel M Olson

Alan R Morrison

Affiliations

Soon will be listed here.

Abstract

Coronavirus disease 2019 (COVID-19), caused by infection with the enveloped RNA betacoronavirus, SARS-CoV-2, led to a global pandemic involving over 7 million deaths. Macrophage inflammatory responses impact COVID-19 severity; however, it is unclear whether macrophages are infected by SARS-CoV-2. We sought to identify mechanisms regulating macrophage expression of ACE2, the primary receptor for SARS-CoV-2, and to determine if macrophages are susceptible to productive infection. We developed a humanized () mouse whereby cDNA was cloned into the mouse locus under control of the native promoter. We validated the susceptibility of mice to SARS-CoV-2 infection relative to wild-type mice and an established model of acute fulminating disease. Intranasal exposure to SARS-CoV-2 led to pulmonary consolidations with cellular infiltrate, edema, and hemorrhage, consistent with pneumonia, yet unlike the model, mice survived and maintained stable weight. Infected mice also exhibited a unique plasma chemokine, cytokine, and growth factor inflammatory signature relative to mice. Infected mice demonstrated evidence of viral replication in infiltrating lung macrophages, and infection of macrophages in vitro revealed a transcriptional profile indicative of altered RNA and ribosomal processing machinery as well as activated cellular antiviral defense. Macrophage IL-1β-driven NF-κB transcription of ACE2 was an important mechanism of dynamic ACE2 upregulation, promoting macrophage susceptibility to infection. Experimental models of COVID-19 that make use of native hACE2 expression will allow for mechanistic insight into factors that can either promote host resilience or increase susceptibility to worsening severity of infection.

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