Litcius/Paper detail

The active form of the influenza cap-snatching endonuclease inhibitor baloxavir marboxil is a tight binding inhibitor

Brendan Todd, Egor P. Tchesnokov, Matthias Götte

2021Journal of Biological Chemistry45 citationsDOIOpen Access PDF

Abstract

ions and BXA is required to observe inhibition, which is consistent with active site binding. Conversely, a preformed complex of FluB-ht and RNA substrate prevents BXA from accessing the active site. Unlike integrase inhibitors that interact with the DNA substrate, BXA behaves like RNase H inhibitors that compete with the nucleic acid at the active site. The collective data support the conclusion that BXA is a tight binding inhibitor and the I38T mutation diminishes these properties.

Topics & Concepts

RNase HChemistryMolecular biologyNucleaseIntegraseBiochemistryBinding siteEnzymeRNase PDNABiologyRNAGeneHIV Research and TreatmentRNA and protein synthesis mechanismsHIV/AIDS drug development and treatment