| dc.description.abstract | The systematic entry of SARS-CoV-2 into host cells, as mediated by its Spike (S) protein, is
highly essential for pathogenicity in humans. Hence, targeting the viral entry mechanisms
remains a major strategy for COVID-19 treatment. Although recent efforts have focused on the
direct inhibition of S-protein receptor-binding domain (RBD) interactions with human
angiotensin-converting enzyme 2 (hACE2), allosteric targeting remains an unexplored
possibility. Therefore, in this study, for the first time, we employed an integrative metaanalytical approach to investigate the allosteric inhibitory mechanisms of SARS-CoV-2 Sprotein and its association with hACE2. Findings revealed two druggable sites (Sites 1 and 2)
located at the N-terminal domain (NTD) and S2 regions of the protein. Two high-affinity
binders; ZINC3939013 (Fosaprepitant – Site 1) and ZINC27990463 (Lomitapide – Site 2) were
discovered via site-directed high-throughput screening against a library of ~1500 FDA approved
drugs. Interestingly, we observed that allosteric binding of both compounds perturbed the
prefusion S-protein conformations, which in turn, resulted in unprecedented hACE2
displacement from the RBD. Estimated ΔGbinds for both compounds were highly favorable due to
high-affinity interactions at the target sites. In addition, Site 1 residues; R190, H207, K206 and
K187, I101, R102, I119, F192, L226, V126 and W104 were identified for their crucial
involvement in the binding and stability of ZINC3939013. Likewise, energy contributions of
Q957, N953, Q954, L303, Y313, Q314, L858, V952, N953, and A956 corroborated their
importance to ZINC27990463 binding at the predicted Site 2. We believe these findings would
pave way for the structure-based discovery of allosteric SARS-CoV-2 S-protein inhibitors for
COVID-19 treatment. | |
