Literature DB >> 31664867

Investigating the utility of adult zebrafish ex vivo whole hearts to pharmacologically screen hERG channel activator compounds.

Christina M Hull1, Christine E Genge1, Yuki Hobbs1, Kaveh Rayani1, Eric Lin1, Marvin Gunawan1, Sanam Shafaattalab1, Glen F Tibbits1, Tom W Claydon1.   

Abstract

There is significant interest in the potential utility of small-molecule activator compounds to mitigate cardiac arrhythmia caused by loss of function of hERG1a voltage-gated potassium channels. Zebrafish (Danio rerio) have been proposed as a cost-effective, high-throughput drug-screening model to identify compounds that cause hERG1a dysfunction. However, there are no reports on the effects of hERG1a activator compounds in zebrafish and consequently on the utility of the model to screen for potential gain-of-function therapeutics. Here, we examined the effects of hERG1a blocker and types 1 and 2 activator compounds on isolated zkcnh6a (zERG3) channels in the Xenopus oocyte expression system as well as action potentials recorded from ex vivo adult zebrafish whole hearts using optical mapping. Our functional data from isolated zkcnh6a channels show that under the conditions tested, these channels are blocked by hERG1a channel blockers (dofetilide and terfenadine), and activated by type 1 (RPR260243) and type 2 (NS1643, PD-118057) hERG1a activators with higher affinity than hKCNH2a channels (except NS1643), with differences accounted for by different biophysical properties in the two channels. In ex vivo zebrafish whole hearts, two of the three hERG1a activators examined caused abbreviation of the action potential duration (APD), whereas hERG1a blockers caused APD prolongation. These data represent, to our knowledge, the first pharmacological characterization of isolated zkcnh6a channels and the first assessment of hERG enhancing therapeutics in zebrafish. Our findings lead us to suggest that the zebrafish ex vivo whole heart model serves as a valuable tool in the screening of hKCNH2a blocker and activator compounds.

Entities:  

Keywords:  activators; hERG; optical mapping; zERG; zebrafish; zkcnh6

Mesh:

Substances:

Year:  2019        PMID: 31664867      PMCID: PMC6962622          DOI: 10.1152/ajpregu.00190.2019

Source DB:  PubMed          Journal:  Am J Physiol Regul Integr Comp Physiol        ISSN: 0363-6119            Impact factor:   3.619


  57 in total

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2.  Frequency-dependent modulation of KCNQ1 and HERG1 potassium channels.

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4.  Concatenated hERG1 tetramers reveal stoichiometry of altered channel gating by RPR-260243.

Authors:  Wei Wu; Alison Gardner; Michael C Sanguinetti
Journal:  Mol Pharmacol       Date:  2014-12-17       Impact factor: 4.436

5.  Construction and use of a zebrafish heart voltage and calcium optical mapping system, with integrated electrocardiogram and programmable electrical stimulation.

Authors:  Eric Lin; Calvin Craig; Marcel Lamothe; Marinko V Sarunic; Mirza Faisal Beg; Glen F Tibbits
Journal:  Am J Physiol Regul Integr Comp Physiol       Date:  2015-03-04       Impact factor: 3.619

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Authors:  Peter F Aziz; Ronn E Tanel; Ilana J Zelster; Robert H Pass; Tammy S Wieand; Victoria L Vetter; R Lee Vogel; Maully J Shah
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Authors:  Thomas G Diness; Yung-Hsin Yeh; Xiao Yan Qi; Denis Chartier; Yukiomi Tsuji; Rie S Hansen; Soren-Peter Olesen; Morten Grunnet; Stanley Nattel
Journal:  Cardiovasc Res       Date:  2008-03-26       Impact factor: 10.787

Review 9.  HERG1 channel agonists and cardiac arrhythmia.

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Journal:  Curr Opin Pharmacol       Date:  2013-11-27       Impact factor: 5.547

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Journal:  PLoS One       Date:  2013-06-19       Impact factor: 3.240

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Review 3.  Zebrafish, an In Vivo Platform to Screen Drugs and Proteins for Biomedical Use.

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