| Literature DB >> 33469573 |
Aartik Sarma, Stephanie Christenson, Eran Mick, Thomas Deiss, Catherine DeVoe, Angela Pisco, Rajani Ghale, Alejandra Jauregui, Ashley Byrne, Farzad Moazed, Natasha Spottiswoode, Pratik Sinha, Beth Zha, Norma Neff, Michelle Tan, Paula Hayakawa Serpa, K Mark Ansel, Jennifer Wilson, Aleksandra Leligdowicz, Emily Seigel, Marina Sirota, Joseph DeRisi, Michael Matthay, Comet Consortium, Carolyn Hendrickson, Kirsten Kangelaris, Matthew Krummel, Prescott Woodruff, David Erle, Carolyn Calfee, Charles Langelier.
Abstract
We performed comparative lower respiratory tract transcriptional profiling of 52 critically ill patients with the acute respiratory distress syndrome (ARDS) from COVID-19 or from other etiologies, as well as controls without ARDS. In contrast to a cytokine storm, we observed reduced proinflammatory gene expression in COVID-19 ARDS when compared to ARDS due to other causes. COVID-19 ARDS was characterized by a dysregulated host response with increased PTEN signaling and elevated expression of genes with non-canonical roles in inflammation and immunity that were predicted to be modulated by dexamethasone and granulocyte colony stimulating factor. Compared to ARDS due to other types of viral pneumonia, COVID-19 was characterized by impaired interferon-stimulated gene expression (ISG). We found that the relationship between SARS-CoV-2 viral load and expression of ISGs was decoupled in patients with COVID-19 ARDS when compared to patients with mild COVID-19. In summary, assessment of host gene expression in the lower airways of patients with COVID-19 ARDS did not demonstrate cytokine storm but instead revealed a unique and dysregulated host response predicted to be modified by dexamethasone.Entities:
Year: 2021 PMID: 33469573 PMCID: PMC7814832 DOI: 10.21203/rs.3.rs-141578/v1
Source DB: PubMed Journal: Res Sq