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Article: Structural basis of differences in isoform-specific gating and lidocaine block between cardiac and skeletal muscle sodium channels

TitleStructural basis of differences in isoform-specific gating and lidocaine block between cardiac and skeletal muscle sodium channels
Authors
Li, RAEnnis, ILTomaselli, GFMarbán, E
KeywordsChemicals And Cas Registry Numbers
Issue Date2002
PublisherAmerican Society for Pharmacology and Experimental Therapeutics. The Journal's web site is located at http://www.molpharm.org
Citation
Molecular Pharmacology, 2002, v. 61 n. 1, p. 136-141 How to Cite?
DOI: http://dx.doi.org/10.1124/mol.61.1.136
AbstractVoltage-gated Na+ channels underlie rapid conduction in heart and skeletal muscle. Cardiac sodium channels open and close over more negative potentials than do skeletal muscle sodium channels; heart channels are also more sensitive to lidocaine block. The structural basis of these differences is poody understood. We mutated nine isoform-specific υ1 (rat skeletal muscle) channel residues in domain IV to those at equivalent locations in hH1 (human cardiac) channels. Channel constructs were expressed in tsA-201 cells and screened for changes in gating and lidocaine sensitivity. Only L1373E, located in the linker between the S1 and S2 transmembrane segments, shifted activation gating and use-dependent block by lidocaine toward that seen in hH1. The converse mutation, hH1-E1555L, shifted the phenotype of hill to resemble that of υ1. Therefore, we identified a previously unsuspected glutamate-to-leucine isoform-specific variant site (i.e., 1555 in hH1 and 1373 in υ1) that significantly influences gating and drug block in sodium channels. The identification of the residue at this position plays a major role in shaping the responses of sodium channels to voltage and to lidocaine, helping to rationalize the distinctive behavior of cardiac sodium channels.
Persistent Identifierhttp://hdl.handle.net/10722/91487
ISSN
0026-895X
2021 Impact Factor: 4.054
2020 SCImago Journal Rankings: 1.469
ISI Accession Number ID
WOS:000173135000016
References
References in Scopus

 

DC FieldValueLanguage
dc.contributor.authorLi, RAen_HK
dc.contributor.authorEnnis, ILen_HK
dc.contributor.authorTomaselli, GFen_HK
dc.contributor.authorMarbán, Een_HK
dc.date.accessioned2010-09-17T10:20:12Z-
dc.date.available2010-09-17T10:20:12Z-
dc.date.issued2002en_HK
dc.identifier.citationMolecular Pharmacology, 2002, v. 61 n. 1, p. 136-141en_HK
dc.identifier.issn0026-895Xen_HK
dc.identifier.urihttp://hdl.handle.net/10722/91487-
dc.description.abstractVoltage-gated Na+ channels underlie rapid conduction in heart and skeletal muscle. Cardiac sodium channels open and close over more negative potentials than do skeletal muscle sodium channels; heart channels are also more sensitive to lidocaine block. The structural basis of these differences is poody understood. We mutated nine isoform-specific υ1 (rat skeletal muscle) channel residues in domain IV to those at equivalent locations in hH1 (human cardiac) channels. Channel constructs were expressed in tsA-201 cells and screened for changes in gating and lidocaine sensitivity. Only L1373E, located in the linker between the S1 and S2 transmembrane segments, shifted activation gating and use-dependent block by lidocaine toward that seen in hH1. The converse mutation, hH1-E1555L, shifted the phenotype of hill to resemble that of υ1. Therefore, we identified a previously unsuspected glutamate-to-leucine isoform-specific variant site (i.e., 1555 in hH1 and 1373 in υ1) that significantly influences gating and drug block in sodium channels. The identification of the residue at this position plays a major role in shaping the responses of sodium channels to voltage and to lidocaine, helping to rationalize the distinctive behavior of cardiac sodium channels.en_HK
dc.languageengen_HK
dc.publisherAmerican Society for Pharmacology and Experimental Therapeutics. The Journal's web site is located at http://www.molpharm.orgen_HK
dc.relation.ispartofMolecular Pharmacologyen_HK
dc.subjectChemicals And Cas Registry Numbersen_HK
dc.subject.meshAmino Acids - genetics - metabolismen_HK
dc.subject.meshAnimalsen_HK
dc.subject.meshElectrophysiologyen_HK
dc.subject.meshHeart - drug effectsen_HK
dc.subject.meshHumansen_HK
dc.subject.meshLidocaine - chemistry - pharmacologyen_HK
dc.subject.meshMuscle, Skeletal - drug effects - metabolismen_HK
dc.subject.meshMyocardium - metabolismen_HK
dc.subject.meshProtein Isoforms - metabolismen_HK
dc.subject.meshProtein Structure, Tertiaryen_HK
dc.subject.meshRatsen_HK
dc.subject.meshSodium Channel Blockersen_HK
dc.subject.meshSodium Channels - chemistry - physiologyen_HK
dc.titleStructural basis of differences in isoform-specific gating and lidocaine block between cardiac and skeletal muscle sodium channelsen_HK
dc.typeArticleen_HK
dc.identifier.emailLi, RA:ronaldli@hkucc.hku.hken_HK
dc.identifier.authorityLi, RA=rp01352en_HK
dc.description.naturelink_to_subscribed_fulltext-
dc.identifier.doi10.1124/mol.61.1.136en_HK
dc.identifier.pmid11752214-
dc.identifier.scopuseid_2-s2.0-0036144123en_HK
dc.relation.referenceshttp://www.scopus.com/mlt/select.url?eid=2-s2.0-0036144123&selection=ref&src=s&origin=recordpageen_HK
dc.identifier.volume61en_HK
dc.identifier.issue1en_HK
dc.identifier.spage136en_HK
dc.identifier.epage141en_HK
dc.identifier.isiWOS:000173135000016-
dc.publisher.placeUnited Statesen_HK
dc.identifier.scopusauthoridLi, RA=7404724466en_HK
dc.identifier.scopusauthoridEnnis, IL=6604033332en_HK
dc.identifier.scopusauthoridTomaselli, GF=7005223451en_HK
dc.identifier.scopusauthoridMarbán, E=8075977300en_HK
dc.identifier.issnl0026-895X-

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