AI Article Synopsis

  • The potassium channel's selectivity filter and activation gate are interconnected in both structure and function, meaning that when the gate opens, it can cause changes in the filter.
  • A specific Threonine residue in the channel's signature sequence is essential for this communication, as a mutation here disrupts normal gating behavior, leading to a lack of proper inactivation.
  • Crystallographic studies show that activating the channel causes the filter to change from a nonconductive to a conductive state, and that closing the gate can also lead to the collapse of the selectivity filter.

Article Abstract

The selectivity filter and the activation gate in potassium channels are functionally and structurally coupled. An allosteric coupling underlies C-type inactivation coupled to activation gating in this ion-channel family (i.e., opening of the activation gate triggers the collapse of the channel's selectivity filter). We have identified the second Threonine residue within the TTVGYGD signature sequence of K channels as a crucial residue for this allosteric communication. A Threonine to Alanine substitution at this position was studied in three representative members of the K-channel family. Interestingly, all of the mutant channels exhibited lack of C-type inactivation gating and an inversion of their allosteric coupling (i.e., closing of the activation gate collapses the channel's selectivity filter). A state-dependent crystallographic study of KcsA-T75A proves that, on activation, the selectivity filter transitions from a nonconductive and deep C-type inactivated conformation to a conductive one. Finally, we provide a crystallographic demonstration that closed-state inactivation can be achieved by the structural collapse of the channel's selectivity filter.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6003467PMC
http://dx.doi.org/10.1073/pnas.1800559115DOI Listing

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