The active form of the influenza cap-snatching endonuclease inhibitor baloxavir marboxil is a tight binding inhibitor
Brendan Todd, Egor P. Tchesnokov, Matthias Götte
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