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TREM2+ and interstitial macrophages orchestrate airway inflammation in SARS-CoV-2 infection in rhesus macaques
Amit A. Upadhyay; Timothy N. Hoang; Maria Pino; Arun K. Boddapati; Elise G. Viox; Michelle Y.H. Lee; Jacqueline Corry; Zachary Strongin; David A. Cowan; Elizabeth N. Beagle; Tristan R. Horton; Sydney Hamilton; Hadj Aoued; Justin L. Harper; Kevin Nguyen; Kathryn L. Pellegrini; Gregory K. Tharp; Anne Piantadosi; Rebecca D. Levit; Rama R. Amara; Simon M. Barratt-Boyes; Susan P. Ribeiro; Rafick P. Sekaly; Thomas H. Vanderford; Raymond F. Schinazi; Mirko Paiardini; Steven E. Bosinger.
Affiliation
  • Amit A. Upadhyay; Emory University
  • Timothy N. Hoang; Emory University
  • Maria Pino; Emory University
  • Arun K. Boddapati; Emory University
  • Elise G. Viox; Emory University
  • Michelle Y.H. Lee; Emory University
  • Jacqueline Corry; University of Pittsburgh
  • Zachary Strongin; Emory University
  • David A. Cowan; Emory University
  • Elizabeth N. Beagle; Emory University
  • Tristan R. Horton; Emory University
  • Sydney Hamilton; Emory University
  • Hadj Aoued; Emory University
  • Justin L. Harper; Emory University
  • Kevin Nguyen; Emory University
  • Kathryn L. Pellegrini; Emory University
  • Gregory K. Tharp; Emory University
  • Anne Piantadosi; Emory University
  • Rebecca D. Levit; Emory University
  • Rama R. Amara; Emory University
  • Simon M. Barratt-Boyes; University of Pittsburgh
  • Susan P. Ribeiro; Emory University
  • Rafick P. Sekaly; Emory University
  • Thomas H. Vanderford; Emory University
  • Raymond F. Schinazi; Emory University
  • Mirko Paiardini; Emory University
  • Steven E. Bosinger; Emory University
Preprint in English | bioRxiv | ID: ppbiorxiv-463212
ABSTRACT
The COVID-19 pandemic remains a global health crisis, yet, the immunopathological mechanisms driving the development of severe disease remain poorly defined. Here, we utilize a rhesus macaque (RM) model of SARS-CoV-2 infection to delineate perturbations in the innate immune system during acute infection using an integrated systems analysis. We found that SARS-CoV-2 initiated a rapid infiltration (two days post infection) of plasmacytoid dendritic cells into the lower airway, commensurate with IFNA production, natural killer cell activation, and induction of interferon-stimulated genes. At this early interval, we also observed a significant increase of blood CD14-CD16+ monocytes. To dissect the contribution of lung myeloid subsets to airway inflammation, we generated a novel compendium of RM-specific lung macrophage gene expression using a combination of sc-RNA-Seq data and bulk RNA-Seq of purified populations under steady state conditions. Using these tools, we generated a longitudinal sc-RNA-seq dataset of airway cells in SARS-CoV-2-infected RMs. We identified that SARS-CoV-2 infection elicited a rapid recruitment of two subsets of macrophages into the airway a C206+MRC1-population resembling murine interstitial macrophages, and a TREM2+ population consistent with CCR2+ infiltrating monocytes, into the alveolar space. These subsets were the predominant source of inflammatory cytokines, accounting for ~75% of IL6 and TNF production, and >90% of IL10 production, whereas the contribution of CD206+MRC+ alveolar macrophages was significantly lower. Treatment of SARS-CoV-2 infected RMs with baricitinib (Olumiant(R)), a novel JAK1/2 inhibitor that recently received Emergency Use Authorization for the treatment of hospitalized COVID-19 patients, was remarkably effective in eliminating the influx of infiltrating, non-alveolar macrophages in the alveolar space, with a concomitant reduction of inflammatory cytokines. This study has delineated the major subsets of lung macrophages driving inflammatory and anti-inflammatory cytokine production within the alveolar space during SARS-CoV-2 infection. One sentence summaryMulti-omic analyses of hyperacute SARS-CoV-2 infection in rhesus macaques identified two population of infiltrating macrophages, as the primary orchestrators of inflammation in the lower airway that can be successfully treated with baricitinib
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Full text: Available Collection: Preprints Database: bioRxiv Type of study: Prognostic study Language: English Year: 2021 Document type: Preprint
Full text: Available Collection: Preprints Database: bioRxiv Type of study: Prognostic study Language: English Year: 2021 Document type: Preprint
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