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SummaryStructural detailsExperimental detailsFunctional detailsSequence NeighborHistoryDownloads

3OTF

Structural basis for the cAMP-dependent gating in human HCN4 channel

Summary for 3OTF
Entry DOI10.2210/pdb3otf/pdb
DescriptorPotassium/sodium hyperpolarization-activated cyclic nucleotide-gated channel 4, ADENOSINE-3',5'-CYCLIC-MONOPHOSPHATE (3 entities in total)
Functional Keywordscyclic-nucleotide binding, transport protein
Biological sourceHomo sapiens (human)
Total number of polymer chains1
Total formula weight26217.65
Authors
Xu, X.,Vysotskaya, Z.V.,Liu, Q.,Zhou, L. (deposition date: 2010-09-11, release date: 2010-10-13, Last modification date: 2023-09-06)
Primary citationXu, X.,Vysotskaya, Z.V.,Liu, Q.,Zhou, L.
Structural basis for the cAMP-dependent gating in the human HCN4 channel.
J.Biol.Chem., 285:37082-37091, 2010
Cited by
PubMed Abstract: Hyperpolarization-activated cAMP-regulated (HCN) channels play important physiological roles in both cardiovascular and central nervous systems. Among the four HCN isoforms, HCN2 and HCN4 show high expression levels in the human heart, with HCN4 being the major cardiac isoform. The previously published crystal structure of the mouse HCN2 (mHCN2) C-terminal fragment, including the C-linker and the cyclic-nucleotide binding domain (CNBD), has provided many insights into cAMP-dependent gating in HCN channels. However, structures of other mammalian HCN channel isoforms have been lacking. Here we used a combination of approaches including structural biology, biochemistry, and electrophysiology to study cAMP-dependent gating in HCN4 channel. First we solved the crystal structure of the C-terminal fragment of human HCN4 (hHCN4) channel at 2.4 Å. Overall we observed a high similarity between mHCN2 and hHCN4 crystal structures. Functional comparison between two isoforms revealed that compared with mHCN2, the hHCN4 protein exhibited marked different contributions to channel function, such as a ∼3-fold reduction in the response to cAMP. Guided by structural differences in the loop region between β4 and β5 strands, we identified residues that could partially account for the differences in response to cAMP between mHCN2 and hHCN4 proteins. Moreover, upon cAMP binding, the hHCN4 C-terminal protein exerts a much prolonged effect in channel deactivation that could have significant physiological contributions.
PubMed: 20829353
DOI: 10.1074/jbc.M110.152033
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (2.4 Å)
Structure validation

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