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An Update on the Structure of hERG
by
Butler, Andrew
, Helliwell, Matthew V.
, Zhang, Yihong
, Hancox, Jules C.
, Dempsey, Christopher E.
in
Action potential
/ C-type inactivation
/ Cardiac arrhythmia
/ Channel gating
/ cryo-EM structure
/ drug block
/ Drugs
/ EKG
/ hERG
/ KCNH
/ long QT syndrome
/ Mutation
/ Pharmacology
/ Potassium
/ Potassium channels (voltage-gated)
/ Proteins
2020
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An Update on the Structure of hERG
by
Butler, Andrew
, Helliwell, Matthew V.
, Zhang, Yihong
, Hancox, Jules C.
, Dempsey, Christopher E.
in
Action potential
/ C-type inactivation
/ Cardiac arrhythmia
/ Channel gating
/ cryo-EM structure
/ drug block
/ Drugs
/ EKG
/ hERG
/ KCNH
/ long QT syndrome
/ Mutation
/ Pharmacology
/ Potassium
/ Potassium channels (voltage-gated)
/ Proteins
2020
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
An Update on the Structure of hERG
by
Butler, Andrew
, Helliwell, Matthew V.
, Zhang, Yihong
, Hancox, Jules C.
, Dempsey, Christopher E.
in
Action potential
/ C-type inactivation
/ Cardiac arrhythmia
/ Channel gating
/ cryo-EM structure
/ drug block
/ Drugs
/ EKG
/ hERG
/ KCNH
/ long QT syndrome
/ Mutation
/ Pharmacology
/ Potassium
/ Potassium channels (voltage-gated)
/ Proteins
2020
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Journal Article
An Update on the Structure of hERG
2020
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Overview
The human voltage-sensitive K
channel hERG plays a fundamental role in cardiac action potential repolarization, effectively controlling the QT interval of the electrocardiogram. Inherited loss- or gain-of-function mutations in hERG can result in dangerous \"long\" (LQTS) or \"short\" QT syndromes (SQTS), respectively, and the anomalous susceptibility of hERG to block by a diverse range of drugs underlies an acquired LQTS. A recent open channel cryo-EM structure of hERG should greatly advance understanding of the molecular basis of hERG channelopathies and drug-induced LQTS. Here we describe an update of recent research that addresses the nature of the particular gated state of hERG captured in the new structure, and the insight afforded by the structure into the molecular basis for high affinity drug block of hERG, the binding of hERG activators and the molecular basis of hERG's peculiar gating properties. Interpretation of the pharmacology of natural SQTS mutants in the context of the structure is a promising approach to understanding the molecular basis of hERG inactivation, and the structure suggests how voltage-dependent changes in the membrane domain may be transmitted to an extracellular \"turret\" to effect inactivation through aromatic side chain motifs that are conserved throughout the KCNH family of channels.
Publisher
Frontiers Media SA,Frontiers Media S.A
Subject
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