| Literature DB >> 27718573 |
Ahmed Taha Ayoub1,2, Rabab M Abou El-Magd3,4, Jack Xiao5, Cody Wayne Lewis3,6, Tatiana Martins Tilli7, Kenji Arakawa8, Yosi Nindita8, Gordon Chan3,6, Luxin Sun9, Mark Glover9, Mariusz Klobukowski1, Jack Tuszynski3.
Abstract
Lankacidin group antibiotics show strong antimicrobial activity against various Gram-positive bacteria. In addition, they were shown to have considerable antitumor activity against certain cell line models. For decades, the antitumor activity of lankacidin was associated with the mechanism of its antimicrobial action, which is interference with peptide bond formation during protein synthesis. This, however, was never confirmed experimentally. Due to significant similarity to paclitaxel-like hits in a previous computational virtual screening study, we suggested that the cytotoxic effect of lankacidin is due to a paclitaxel-like action. In this study, we tested this hypothesis computationally and experimentally and confirmed that lankacidin is a microtubule stabilizer that enhances tubulin assembly and displaces taxoids from their binding site. This study serves as a starting point for optimization of lankacidin derivatives for better antitumor activities. It also highlights the power of computational predictions and their aid in guiding experiments and formulating rigorous hypotheses.Entities:
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Year: 2016 PMID: 27718573 DOI: 10.1021/acs.jmedchem.6b01264
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446