Synthesis of Structural ADP-Ribose Analogues as Inhibitors for SARS-CoV-2 Macrodomain 1.

Koen J RijpkemaMarion SchullerMiriam S van der VeerSjoerd RiekenDiego L R ChangPascal BalićAlex TodorovHugo MinneeSven WijngaardenIsaac A MatosNicolas C HochJeroen D C CodéeIvan AhelDmitri V Filippov

Published in: Organic letters (2024)

Protein adenosine diphosphate (ADP)-ribosylation is crucial for a proper immune response. Accordingly, viruses have evolved ADP-ribosyl hydrolases to remove these modifications, a prominent example being the SARS-CoV-2 NSP3 macrodomain, "Mac1". Consequently, inhibitors are developed by testing large libraries of small molecule candidates, with considerable success. However, a relatively underexplored angle in design pertains to the synthesis of structural substrate mimics. Here, we present the synthesis and biophysical activity of novel adenosine diphosphate ribose (ADPr) analogues as SARS-CoV-2 NSP3 Mac1 inhibitors.

Keyphrases

sars cov
small molecule
respiratory syndrome coronavirus
immune response
protein protein
molecular docking
high resolution
protein kinase
amino acid
dendritic cells
toll like receptor
binding protein
inflammatory response