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The synergic modeling for the binding of fluoroquinolone antibiotics to the hERG potassium channel |
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| Authors: | Sunghi Ryu Yumi N Imai Shigetoshi Oiki |
| Institution: | 1. CMC Center, Takeda Pharmaceutical Company Limited, Osaka 532-8686, Japan;2. Pharmaceutical Research Division, Takeda Pharmaceutical Company Limited, Fujisawa 251-8555, Japan;3. Department of Molecular Physiology and Biophysics, University of Fukui Faculty of Medical Sciences, Fukui 910-1193, Japan |
| Abstract: | The fluoroquinolone antibiotic binding site in the hERG potassium channel was examined for the residues involved and their position in the tetrameric channel. The blocking effect of the two fluoroquinolones levofloxacin and sparfloxacin to tandem dimers of the hERG mutants were evaluated electrophysiologically. The results indicated that two Tyr652s in the neighboring subunits and one or two Phe656s in the diagonal subunits contributed to the blockade in the case of both compounds, and Ser624 was also involved. The docking studies suggested that the protonated carboxyl group in the compounds strongly interacts with Phe656 as a π acceptor. |
| Keywords: | hERG liability Tandem dimer mutant Binding mode prediction Electrophysiology Carboxyl group |
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