| Literature DB >> 28913709 |
Paul T Wilder1, David J Weber1, Angela Winstead2, Sabreea Parnell2, Tiara V Hinton2, Monet Stevenson2, Dipak Giri2, Samira Azemati2, Pola Olczak2, Brent V Powell2, Tijesunimi Odebode2, Solomon Tadesse2, Yongchao Zhang2, Saroj K Pramanik3, James M Wachira3, Sujan Ghimire2, Pumtiwitt McCarthy2, Alexis Barfield4, Hirendra N Banerjee4, Chao Chen5, James A Golen5, Arnold L Rheingold5, Jeanette A Krause6, Douglas M Ho7, Peter Y Zavalij8, Roosevelt Shaw2, Santosh K Mandal9.
Abstract
Cisplatin and other metal-based drugs often display side effects and tumor resistance after prolonged use. Because rhenium-based anticancer complexes are often less toxic, a novel series of organorhenium complexes were synthesized of the types: XRe(CO)3Z (X = α-diimines and Z = p-toluenesulfonate, 1-naphthalenesulfonate, 2-naphthalenesulfonate, picolinate, nicotinate, aspirinate, naproxenate, flufenamate, ibuprofenate, mefenamate, tolfenamate, N-acetyl-tryptophanate), and their biological properties were examined. Specifically, in hormone-dependent MCF-7 and hormone-independent triple-negative MDA-MB-231 breast cancer cells, the p-toluenesulfonato, 1-naphthalenesulfonato, 2-naphthalenesulfonato, picolinato, nicotinato, acetylsalicylato, flufenamato, ibuprofenato, mefenamato, and N-acetyl-tryptophanato complexes were found to be far more potent than conventional drug cisplatin. DNA-binding studies were performed in each case via UV-Vis titrations, cyclic voltammetry, gel electrophoresis, and viscosity, which suggest DNA partial intercalation interaction, and the structure-activity relationship studies suggest that the anticancer activities increase with the increasing lipophilicities of the compounds, roughly consistent with their DNA-binding activities.Entities:
Keywords: Breast cancers; Carboxylate; MCF-7; MDA-MB-231; Organorhenium; Sulfonate
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Year: 2017 PMID: 28913709 PMCID: PMC7191999 DOI: 10.1007/s11010-017-3181-z
Source DB: PubMed Journal: Mol Cell Biochem ISSN: 0300-8177 Impact factor: 3.396