Selective exclusion and selective binding both contribute to ion selectivity in KcsA, a model potassium channel

Abstract

The selectivity filter in potassium channels, a main component of the ion permeation pathway, configures a stack of binding sites (sites S1-S4) to which K(+) and other cations may bind. Specific ion binding to such sites induces changes in the filter conformation, which play a key role in defining both selectivity and permeation. Here, using the potassium channel KcsA as a model, we contribute new evidence to reinforce this assertion. First, ion binding to KcsA blocked by tetrabutylammonium at the most cytoplasmic site in the selectivity filter (S4) suggests that such a site, when in the nonconductive filter conformation, has a higher affinity for cation binding than the most extracellular S1 site. This filter asymmetry, along with differences in intracellular and extracellular concentrations of K(+)versus Na(+) under physiological conditions, should strengthen selection of the permeant K(+) by the channel. Second, we used different K(+) concentrations to shift the equilibrium between nonconductive and conductive states of the selectivity filter in which to test competitive binding of Na(+) These experiments disclosed a marked decrease in the affinity of Na(+) to bind the channel when the conformational equilibrium shifts toward the conductive state. This finding suggested that in addition to the selective binding of K(+) and other permeant species over Na(+), there is a selective exclusion of nonpermeant species from binding the channel filter, once it reaches a fully conductive conformation. We conclude that selective binding and selective exclusion of permeant and nonpermeant cations, respectively, are important determinants of ion channel selectivity.