Literature DB >> 23807091

Cholesterol sensitivity of KIR2.1 depends on functional inter-links between the N and C termini.

Avia Rosenhouse-Dantsker1, Sergei Noskov, Diomedes E Logothetis, Irena Levitan.   

Abstract

In recent years, cholesterol has been emerging as a major regulator of ion channel function. We have previously shown that cholesterol suppresses Kir2 channels, a subfamily of constitutively active strongly rectifying K (+) channels. Furthermore, our earlier studies have shown that cholesterol sensitivity of Kir2 channels depends on a group of residues that form a belt-like structure around the cytosolic pore of the channel in proximity to the transmembrane domain. In this study, we focus on the contributions of different structural domains of Kir2 channels in the regulation of their cholesterol sensitivity. Focusing on the mildest mutation in the sensitivity belt, L222I, we show that the sensitivity of the channel to cholesterol can be restored by crosstalk between three distinct cytosolic regions: the C-terminal CD loop, the EF and GA loops of the C-terminus, and the βA sheet of the N-terminus. Thus, in addition to the importance of residues that affect the cytosolic G-loop gate in the sensitivity of Kir2 channels to cholesterol, our data suggest an important role to the interactions at the interface between the channel's N- and C- termini that couple the intracellular domains of its four subunits during gating.

Entities:  

Keywords:  IRK1; Kir2.1; cholesterol; inwardly rectifying potassium channels; lipids

Mesh:

Substances:

Year:  2013        PMID: 23807091      PMCID: PMC3989358          DOI: 10.4161/chan.25437

Source DB:  PubMed          Journal:  Channels (Austin)        ISSN: 1933-6950            Impact factor:   2.581


  47 in total

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6.  A molecular switch controls the impact of cholesterol on a Kir channel.

Authors:  Valentina Corradi; Anna N Bukiya; Williams E Miranda; Meng Cui; Leigh D Plant; Diomedes E Logothetis; D Peter Tieleman; Sergei Y Noskov; Avia Rosenhouse-Dantsker
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7.  Defining how multiple lipid species interact with inward rectifier potassium (Kir2) channels.

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  7 in total

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