4.8 Article

CryoEM structure of a prokaryotic cyclic nucleotide-gated ion channel

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1700248114

Keywords

cryoEM; ion channel; cyclic nucleotide; conformational changes; allostery

Funding

  1. National Eye Institute [R01EY010329]
  2. National Institute of Mental Health [R01MH102378]
  3. National Institute of General Medical Sciences [T32GM008268]
  4. American Heart Association [14CSA20380095]
  5. Raymond and Beverly Sackler Scholars Program in Integrative Biophysics
  6. NIH National Institute of General Medical Sciences [GM103310]
  7. Simons Foundation [349247]

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Cyclic nucleotide-gated (CNG) and hyperpolarization-activated cyclic nucleotide-regulated (HCN) ion channels play crucial physiological roles in phototransduction, olfaction, and cardiac pace making. These channels are characterized by the presence of a carboxylterminal cyclic nucleotide-binding domain (CNBD) that connects to the channel pore via a C-linker domain. Although cyclic nucleotide binding has been shown to promote CNG and HCN channel opening, the precise mechanism underlying gating remains poorly understood. Here we used cryoEM to determine the structure of the intact LliK CNG channel isolated from Leptospira licerasiae-which shares sequence similarity to eukaryotic CNG and HCN channels-in the presence of a saturating concentration of cAMP. A short S4-S5 linker connects nearby voltage-sensing and pore domains to produce a non-domain-swapped transmembrane architecture, which appears to be a hallmark of this channel family. We also observe major conformational changes of the LliK C-linkers and CNBDs relative to the crystal structures of isolated C-linker/CNBD fragments and the cryoEM structures of related CNG, HCN, and KCNH channels. The conformation of our LliK structure may represent a functional state of this channel family not captured in previous studies.

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