| Literature DB >> 31891209 |
Francesco Gentile1, Ahmed H Elmenoufy2,3, Gloria Ciniero4,5, David Jay6, Feridoun Karimi-Busheri6, Khaled H Barakat7, Michael Weinfeld6,8, Frederick G West2,8, Jack A Tuszynski1,4,6.
Abstract
The heterodimer of DNA excision repair protein ERCC-1 and DNA repair endonuclease XPF (ERCC1-XPF) is a 5'-3' structure-specific endonuclease essential for the nucleotide excision repair (NER) pathway, and it is also involved in other DNA repair pathways. In cancer cells, ERCC1-XPF plays a central role in repairing DNA damage induced by chemotherapeutics including platinum-based and cross-linking agents; thus, its inhibition is a promising strategy to enhance the effect of these therapies. In this study, we rationally modified the structure of F06, a small molecule inhibitor of the ERCC1-XPF interaction (Molecular Pharmacology, 84, 2013 and 12), to improve its binding to the target. We followed a multi-step computational approach to investigate potential modification sites of F06, rationally design and rank a library of analogues, and identify candidates for chemical synthesis and in vitro testing. Our top compound, B5, showed an improved half-maximum inhibitory concentration (IC50 ) value of 0.49 µM for the inhibition of ERCC1-XPF endonuclease activit, and lays the foundation for further testing and optimization. Also, the computational approach reported here can be used to develop DNA repair inhibitors targeting the ERCC1-XPF complex.Entities:
Keywords: DNA repair; ERCC1-XPF; chemotherapy; computer-aided drug design; molecular dynamics; protein; protein interaction; small molecules; virtual screening
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Year: 2020 PMID: 31891209 DOI: 10.1111/cbdd.13660
Source DB: PubMed Journal: Chem Biol Drug Des ISSN: 1747-0277 Impact factor: 2.817