Products/Services Used | Details | Operation |
---|---|---|
Gene Synthesis | 14-mer peptides (49) with the sequence AA(X1–X8)YAYR, with X1–X8 being the P4 – P4’ sequence of 46 3CLpro cleavage sites Genscript In this paper, Figure 2, Table 1, Figure S2 | Get A Quote |
Peptide Library Services | Get A Quote | |
ORF cDNA Clones/MolecularCloud | Get A Quote |
The main viral protease (3CLpro) is indispensable for SARS-CoV-2 replication. We delineate the human protein substrate landscape of 3CLpro by TAILS substrate-targeted N-terminomics. We identify more than 100 substrates in human lung and kidney cells supported by analyses of SARS-CoV-2-infected cells. Enzyme kinetics and molecular docking simulations of 3CLpro engaging substrates reveal how noncanonical cleavage sites, which diverge from SARS-CoV, guide substrate specificity. Cleaving the interactors of essential effector proteins, effectively stranding them from their binding partners, amplifies the consequences of proteolysis. We show that 3CLpro targets the Hippo pathway, including inactivation of MAP4K5, and... More