Author: Raghavan, Somasundaram; Kenchappa, Divya; Leo, M.
Title: SARSâ€CoVâ€2 spike protein induces degradation of junctional proteins that maintain endothelial barrier integrity Cord-id: dda8uv52 Document date: 2021_5_14
ID: dda8uv52
Snippet: BACKGROUND: SARSâ€CoVâ€2 enters cells through the Angiotensinâ€converting enzyme 2 (ACEâ€2) receptor present on the cell surface. ACEâ€2 is present in many cell types including endothelial cells, where it functions to protect against oxidative damage. Reports suggest that COVIDâ€19 patients also showed symptoms related to endothelial damage. We hypothesized that these vascular symptoms might be associated with disrupted endothelial barrier integrity. We investigated this in vitro using end
Document: BACKGROUND: SARSâ€CoVâ€2 enters cells through the Angiotensinâ€converting enzyme 2 (ACEâ€2) receptor present on the cell surface. ACEâ€2 is present in many cell types including endothelial cells, where it functions to protect against oxidative damage. Reports suggest that COVIDâ€19 patients also showed symptoms related to endothelial damage. We hypothesized that these vascular symptoms might be associated with disrupted endothelial barrier integrity. We investigated this in vitro using endothelial cell culture and recombinant SARSâ€CoVâ€2 spike protein S1 Receptorâ€Binding Domain (S1RBD). MATERIALS AND METHODS: Mouse brain microvascular endothelial cells from normal (C57BL/6 mice) and diabetic (db/db) mice were used. The expression of VEâ€Cadherin, PECAMâ€1, JAMâ€A and Connexin 43, was probed by Western blot in normal and diabetic cells, before and after treatment with S1RBD. RESULTS: The expression of VEâ€Cadherin, an endothelial adherens junction protein, was not affected by diabetes or by S1RBD treatment. PECAMâ€1 expression showed a small but significant (~15%) decrease after S1RD treatment in control cells. Junctional Adhesion Molecule (JAMâ€A), a tight junction protein, and the gap junction protein, Connexinâ€43, decreased by ~50 and 80% respectively in the presence of S1RBD when compared to untreated controls. Expression of PECAMâ€1, JAMâ€A and connexinâ€43 were significantly lower in untreated diabetic endothelial cells, compared to untreated control cells. This expression level further decreased significantly in the presence of S1RBD, with maximal effects observed with JAMâ€A and Connexinâ€43 expression (~80 and 90% decrease, respectively). These results indicate that healthy and diabetic endothelial cells respond differently when challenged with SARSâ€CoVâ€2 S1RBD. CONCLUSION: S1RBDâ€induces degradation of endothelial junctional proteins that likely affects endothelial barrier function and causes vascular damage.
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