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Virtual Pharmacophore Screening Identifies Small Molecule Inhibitors of the Rev1-CT/RIR Protein-Protein Interaction.

ChemMedChem. 2019; 
DashRadha C,OzenZuleyha,McCarthyKaitlyn R,ChatterjeeNimrat,HarrisCynthia A,RizzoAlessandro A,WalkerGraham C,KorzhnevDmitry M,HaddenMatthew
Products/Services Used Details Operation
Peptide Synthesis … molecules purchased from ChemBridge. The polκ-RIR peptide (560-575) incorporating an N-terminal fluorescent FAM label (FAM-Polκ-RIR) utilized in the FP assay was custom synthesized by GenScript. Recombinant Rev1-CT … Get A Quote

摘要

Translesion synthesis (TLS) has emerged as a mechanism through which several forms of cancer develop acquired resistance to first-line genotoxic chemotherapies by allowing replication to continue in the presence of damaged DNA. Small molecules that inhibit TLS hold promise as a novel class of anti-cancer agents that can serve to enhance the efficacy of these front-line therapies. We previously utilized a structure-based rational design approach to identify the phenazopyridine scaffold as an inhibitor of TLS that functions by disrupting the protein-protein interaction (PPI) between the C-terminal domain of the TLS DNA polymerase Rev1 (Rev1-CT) and the Rev1 interacting regions (RIR) of other TLS DNA polymerases. ... More

关键词

pharmacophore, virtual screening, translesion synthesis, Rev1-CT, ca