Blocking of valinomycin-mediated bilayer membrane conductance by substituted benzimidazoles.

K H Kuo, T R Fukuto, T A Miller and L J Bruner

ABSTRACT

Valinomycin selectively transports alkali cations, e.g. potassiumions, across lipid bilayer membranes. The blocking of this carrier-mediatedtransport by four substituted benzimidazoles has been investigated.The compounds are 4,5,6,7-tetrachloro-2-trifluoromethylbenzimidazole,(TTFB); 4,5,6,7,-tetrachloro-2-methylbenzimidazole, (TMB); 2-trifluoromethylbenzimidazole,(TFB); and 2-methylbenzimidazole, (MBM). Because of its lowacidic dissociation constant (pKa = 5.04), the blocking efficiencyof TTFB in both neutral and anionic forms in the aqueous phasecould be studied. The compounds exhibit the blocking efficiencysequence, TTFB- greater than TTFB0 greater than TMB0 greaterthan TFB0 greater than MBM0. The corresponding scale of decreasinglipophilicity, as determined by octanol/water partitioning,is TTFB0 greater than TMB0 greater than TTFB- greater than TFB0greater than MBM0. Comparison of neutral species establishesa positive correlation of blocking efficiency with lipophilicity,with the latter being conferred primarily by chlorination ofthe benzenoid nucleus. Anionic TTFB, on the other hand, is themost effective blocking agent studied in spite of the fact thatits dissociation in the aqueous phase markedly impedes its entry(presumably as a neutral species) into a bulk hydrocarbon phase.This observation suggests that the blocking of valinomycin-mediatedbilayer membrane conductance takes place at the membrane/solutioninterface.

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