Cluster organization of ion channels formed by the antibiotic syringomycin E in bilayer lipid membranes. |
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| Authors: | Y A Kaulin L V Schagina S M Bezrukov V V Malev A M Feigin J Y Takemoto J H Teeter J G Brand |
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| Affiliation: | *Monell Chemical Senses Center, Philadelphia, Pennsylvania 19104-3308 USA;#Institute of Cytology of the Russian Academy of Sciences, St. Petersburg 194064, Russia;§National Institutes of Health, NICHD, Laboratory of Physical and Structural Biology, 5/405, Bethesda, Maryland 20892 USA;¶St. Petersburg Nuclear Physics Institute of the Russian Academy of Sciences, Gatchina 188350, Russia;||Utah State University, Logan, Utah 84322-5305 USA;**University of Pennsylvania, Philadelphia, Pennsylvania 19104 USA;##Veterans Affairs Medical Center, Philadelphia, Pennsylvania 19104 USA |
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| Abstract: | The cyclic lipodepsipeptide, syringomycin E, when incorporated into planar lipid bilayer membranes, forms two types of channels (small and large) that are different in conductance by a factor of sixfold. To discriminate between a cluster organization-type channel structure and other possible different structures for the two channel types, their ionic selectivity and pore size were determined. Pore size was assessed using water-soluble polymers. Ion selectivity was found to be essentially the same for both the small and large channels. Their reversal (zero current) potentials with the sign corresponding to anionic selectivity did not differ by more than 3 mV at a twofold electrolyte gradient across the bilayer. Reduction in the single-channel conductance induced by poly(ethylene glycol)s of different molecular weights demonstrated that the aqueous pore sizes of the small and large channels did not differ by more than 2% and were close to 1 nm. Based on their virtually identical selectivity and size, we conclude that large syringomycin E channels are clusters of small ones exhibiting synchronous opening and closing. |
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