Phenotyping the virulence of SARS-CoV-2 variants in hamsters by digital pathology and machine learning

Meehan, Gavin R; Herder, Vanessa; Allan, Jay; Huang, Xinyi; Kerr, Karen; Mendonca, Diogo Correa; Ilia, Georgios; Wright, Derek W; Nomikou, Kyriaki; Gu, Quan; Arias, Sergi Molina; De Lorenzo, Giuditta; Cowton, Vanessa; Upfold, Nicole; Palmalux, Natasha; Brown, Jonathan; Barclay, Wendy; Filipe, Ana Da Silva; Furnon, Wilhelm; Patel, Arvind H; Palmarini, Massimo

doi:10.1101/2023.08.01.551417

2023

DOI: 10.1101/2023.08.01.551417

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Phenotyping the virulence of SARS-CoV-2 variants in hamsters by digital pathology and machine learning

Gavin R Meehan,

Vanessa Herder,

Jay Allan

et al.

Abstract: SARS-CoV-2 has continued to evolve throughout the COVID-19 pandemic, giving rise to multiple variants of concern (VOCs) with different biological properties. As the pandemic progresses, it will be essential to test in near real time the potential of any new emerging variant to cause severe disease. BA.1 (Omicron) was shown to be attenuated compared to the previous VOCs like Delta, but it is possible that newly emerging variants may regain a virulent phenotype. Hamsters have been proven to be an exceedingly goo… Show more

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Disease trajectories in hospitalized COVID-19 patients are predicted by clinical and peripheral blood signatures representing distinct lung pathologies

Da Silva Filho,

Herder,

Gibbins

et al. 2023

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SummaryLinking clinical biomarkers and lung pathology still is necessary to understand COVID-19 pathogenesis and the basis of progression to lethal outcomes. Resolving these knowledge gaps enables optimal treatment approaches of severe COVID-19. We present an integrated analysis of longitudinal clinical parameters, blood biomarkers and lung pathology in COVID-19 patients from the Brazilian Amazon. We identified core signatures differentiating severe recovered patients and fatal cases with distinct disease trajectories. Progression to early death was characterized by rapid and intense endothelial and myeloid activation, presence of thrombi, mostly driven by SARS-CoV-2+macrophages. Progression to late death was associated with systemic cytotoxicity, interferon and Th17 signatures and fibrosis, apoptosis, and abundant SARS-CoV-2+epithelial cells in the lung. Progression to recovery was associated with pro-lymphogenic and Th2-mediated responses. Integration of ante-mortem clinical and blood biomarkers with post-mortem lung-specific signatures defined predictors of disease progression, identifying potential targets for more precise and effective treatments.

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Disease trajectories in hospitalized COVID-19 patients are predicted by clinical and peripheral blood signatures representing distinct lung pathologies

Da Silva Filho,

Herder,

Gibbins

et al. 2023

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

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Phenotyping the virulence of SARS-CoV-2 variants in hamsters by digital pathology and machine learning

Cited by 1 publication

References 66 publications

Disease trajectories in hospitalized COVID-19 patients are predicted by clinical and peripheral blood signatures representing distinct lung pathologies

Disease trajectories in hospitalized COVID-19 patients are predicted by clinical and peripheral blood signatures representing distinct lung pathologies

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