4.8 Article

Effect of SARS-CoV-2 proteins on vascular permeability

ELIFE (2021)

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Journal

ELIFE
Volume 10, Issue -, Pages -

Publisher

eLIFE SCIENCES PUBL LTD
DOI: 10.7554/eLife.69314

Keywords

SARS-COV-2; vasculature; endothelium; protein interactions; Human

Categories

Biology

Funding

  1. Azrieli Foundation
  2. Israel Science Foundation [2248/19, 953/16]
  3. ERC SweetBrain [851765]
  4. TEVA
  5. Aufzien Family Center for the Prevention and Treatment of Parkinson's Disease at Tel Aviv University, Zimin
  6. TCCP
  7. Israel Science Foundation (ISF) [953/16, 2417/20]
  8. German Research Foundation (DFG) [NA: 207/10-1]
  9. Taube/Koret Global Collaboration in Neurodegenerative Diseases
  10. European Research Council Consolidator Grant OCLD [681870]
  11. Israel Ministry of Science and Technology [3-17351]
  12. Aufzien Family Center for the Prevention and Treatment of Parkinson's Disease at Tel Aviv University
  13. European Research Council (ERC) [681870, 851765] Funding Source: European Research Council (ERC)

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This study examined the effects of different SARS-CoV-2 proteins on endothelial cells, finding that most of them induced significant changes in endothelial permeability and dysfunction. By analyzing protein-protein interactions, the study predicted the endothelial proteins affected by viral proteins, shedding light on the vascular aspects of COVID-19. Through validation of the protein-protein interaction network model, specific SARS-CoV-2 proteins impacting endothelial function were identified.
Severe acute respiratory syndrome (SARS)-CoV-2 infection leads to severe disease associated with cytokine storm, vascular dysfunction, coagulation, and progressive lung damage. It affects several vital organs, seemingly through a pathological effect on endothelial cells. The SARS-CoV-2 genome encodes 29 proteins, whose contribution to the disease manifestations, and especially endothelial complications, is unknown. We cloned and expressed 26 of these proteins in human cells and characterized the endothelial response to overexpression of each, individually. Whereas most proteins induced significant changes in endothelial permeability, nsp2, nsp5_c145a (catalytic dead mutant of nsp5), and nsp7 also reduced CD31, and increased von Willebrand factor expression and IL-6, suggesting endothelial dysfunction. Using propagation-based analysis of a protein-protein interaction (PPI) network, we predicted the endothelial proteins affected by the viral proteins that potentially mediate these effects. We further applied our PPI model to identify the role of each SARS-CoV-2 protein in other tissues affected by coronavirus disease (COVID-19). While validating the PPI network model, we found that the tight junction (TJ) proteins cadherin-5, ZO-1, and beta-catenin are affected by nsp2, nsp5_c145a, and nsp7 consistent with the model prediction. Overall, this work identifies the SARS-CoV-2 proteins that might be most detrimental in terms of endothelial dysfunction, thereby shedding light on vascular aspects of COVID-19.

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