Thapsigargin and Tunicamycin Block SARS-CoV-2 Entry into Host Cells via Differential Modulation of Unfolded Protein Response (UPR), AKT Signaling, and Apoptosis.
Abeer Al OtaibiSindiyan Al Shaikh MubarakFatimah Al HejjiAbdulrahman AlmasaudHaya Al JamiJahangir IqbalAli Al QarniNaif Khalaf Al HarbiAhmed BakillahPublished in: Cells (2024)
These findings suggest that short-term pre-existing ER stress prior to virus infection induces a specific UPR response in host cells capable of counteracting stress-inducible elements signaling, thereby depriving SARS-Co-V2 of essential components for entry and replication. Pharmacological manipulation of ER stress in host cells might provide new therapeutic strategies to alleviate SARS-CoV-2 infection.