| Literature DB >> 27315565 |
Rohit Bavi1, Raj Kumar1, Shailima Rampogu1, Minky Son1, Chanin Park1, Ayoung Baek1, Hyong-Ha Kim2, Jung-Keun Suh3, Seok Ju Park4, Keun Woo Lee5.
Abstract
Helicobacter pylori (H. pylori) persevere in the human stomach, an environment in which they encounter many DNA-damaging conditions, including gastric acidity. The pathogenicity of H. pylori is enhanced by its well-developed DNA repair mechanism, thought of as 'machinery,' such as nucleotide excision repair (NER). NER involves multi-enzymatic excinuclease proteins (UvrABC endonuclease), which repair damaged DNA in a sequential manner. UvrB is the central component in prokaryotic NER, essential for damage recognition. Therefore, molecular modeling studies of UvrB protein from H. pylori are carried out with homology modeling and molecular dynamics (MD) simulations. The results reveal that the predicted structure is bound to a DNA hairpin with 3-bp stem, an 11-nucleotide loop, and 3-nt 3' overhang. In addition, a mutation of the Y96A variant indicates reduction in the binding affinity for DNA. Free-energy calculations demonstrate the stability of the complex and help identify key residues in various interactions based on residue decomposition analysis. Stability comparative studies between wild type and mutant protein-DNA complexes indicate that the former is relatively more stable than the mutant form. This predicted model could also be useful in designing new inhibitors for UvrB protein, as well as preventing the pathogenesis of H. pylori.Entities:
Keywords: Free energy calculations; Helicobacter pylori; Homology modeling and molecular dynamics simulations; Nucleotide excision repair; UvrB
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Year: 2016 PMID: 27315565 DOI: 10.1016/j.compbiomed.2016.06.005
Source DB: PubMed Journal: Comput Biol Med ISSN: 0010-4825 Impact factor: 4.589