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Disruption of tubulin polymerization and cell proliferation by 1-naphthylarsonic acid
Authors:Mahinpour Roya  Riazi Gholamhossein  Shokrgozar Mohammad A  Sarbolouki Mohammad N  Ahmadian Shahin  Douraghi Masoumeh  Hadi Alijanvand Hamid  Azadmanesh Kayhan  Heidari Maryam  Naghdi Gheshlaghi Zahra  Moosavi-Movahedi Ali A
Institution:Department of Organic Chemistry, Faculty of Chemistry, University of Kashan, Kashan, Iran.
Abstract:Arsenical compounds exhibit a differential toxicity to cancer cells. Microtubules are a primary target of a number of anticancer drugs, such as arsenical compounds. The interaction of 1-NAA (1-naphthylarsonic acid) has been investigated on microtubule polymerization under in vitro and cellular conditions. Microtubules were extracted from sheep brain. Transmission electron microscopy was used to show microtubule structure in the presence of 1-NAA. Computational docking method was applied for the discovery of ligand-binding sites on the microtubular proteins. Proliferation of HeLa cells and HF2 (human foreskin fibroblasts) was measured by the MTT 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl-2H-tetrazolium bromide] assay method following their incubation with 1-NAA. Fluorescence microscopic labelling was done with the help of α-tubulin monoclonal antibody and Tunel kit was used to investigate the apoptotic effects of 1-NAA on the HeLa cells. 1-NAA inhibits the tubulin polymerization by the formation of abnormal polymers having high affinity to the inner cell wall.
Keywords:anti‐mitotic agent  HeLa cell  human foreskin fibroblasts (HF2)  microtubule  1‐naphthylarsonic acid (1‐NAA)
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