Catecholaminergic polymorphic ventricular tachycardia (CPVT) is a familial arrhythmogenic syndrome characterized by sudden death. There are several genetic forms of CPVT associated with mutations in genes encoding the cardiac ryanodine receptor (RyR2) and its auxiliary proteins including calsequestrin (CASQ2) and calmodulin (CaM). It has been suggested that impairment of the ability of RyR2 to stay closed (ie, refractory) during diastole may be a common mechanism for these diseases. Here, we explore the possibility of engineering CaM variants that normalize abbreviated RyR2 refractoriness for subsequent viral-mediated delivery to alleviate arrhythmias in non-CaM-related CPVT

Belevych, Andriy E

Bonilla, Ingrid

Davis, Jonathan P

Gy\uf6rke, S\ue1ndor

Ho, Hsiang-Ting

Knollmann, Bjorn C

Liu, Bin

Priori, Silvia G

Radwa\u144ski, Przemys\u142aw B

Shettigar, Vikram

Tikunova, Svetlana B

Volpe, Pompeo

Walton, Shane D

Journal of the American Heart Association : Cardiovascular and Cerebrovascular Disease

English

Radwański, Przemysław B

Györke, Sándor

Archivio istituzionale della ricerca - Università di Padova

Gene Transfer of Engineered Calmodulin Alleviates Ventricular Arrhythmias in a Calsequestrin-Associated Mouse Model of Catecholaminergic Polymorphic Ventricular Tachycardia


            Background
            
              Catecholaminergic polymorphic ventricular tachycardia (
              CPVT
              ) is a familial arrhythmogenic syndrome characterized by sudden death. There are several genetic forms of
              CPVT
              associated with mutations in genes encoding the cardiac ryanodine receptor (RyR2) and its auxiliary proteins including calsequestrin (
              CASQ
              2) and calmodulin (CaM). It has been suggested that impairment of the ability of RyR2 to stay closed (ie, refractory) during diastole may be a common mechanism for these diseases. Here, we explore the possibility of engineering CaM variants that normalize abbreviated RyR2 refractoriness for subsequent viral‐mediated delivery to alleviate arrhythmias in non–CaM‐related
              CPVT
              .
            
          
          
            Methods and Results
            
              To that end, we have designed a CaM protein (
              GSH
              ‐M37Q; dubbed as therapeutic CaM or T‐CaM) that exhibited a slowed N‐terminal Ca dissociation rate and prolonged RyR2 refractoriness in permeabilized myocytes derived from
              CPVT
              mice carrying the
              CASQ
              2 mutation R33Q. This T‐CaM was introduced to the heart of R33Q mice through recombinant adeno‐associated viral vector serotype 9. Eight weeks postinfection, we performed confocal microscopy to assess Ca handling and recorded surface ECGs to assess susceptibility to arrhythmias in vivo. During catecholamine stimulation with isoproterenol, T‐CaM reduced isoproterenol‐promoted diastolic Ca waves in isolated
              CPVT
              cardiomyocytes. Importantly, T‐CaM exposure abolished ventricular tachycardia in
              CPVT
              mice challenged with catecholamines.
            
          
          
            Conclusions
            
              Our results suggest that gene transfer of T‐CaM by adeno‐associated viral vector serotype 9 improves myocyte Ca handling and alleviates arrhythmias in a calsequestrin‐associated
              CPVT
              model, thus supporting the potential of a CaM‐based antiarrhythmic approach as a therapeutic avenue for genetically distinct forms of
              CPVT
              .
            
          </jats:sec

Bin Liu

Shane D. Walton

Hsiang‐Ting Ho

Andriy E. Belevych

Svetlana B. Tikunova

Ingrid Bonilla

Vikram Shettigar

Bjorn C. Knollmann

Silvia G. Priori

Pompeo Volpe

Przemysław B. Radwański

Jonathan P. Davis

Sándor Györke

Crossref

Journal of the American Heart Association

Gene Transfer of Engineered Calmodulin Alleviates Ventricular Arrhythmias in a Calsequestrin‐Associated Mouse Model of Catecholaminergic Polymorphic Ventricular Tachycardia

Hsiang-Ting, Ho

Radwa&#324

Gy&#246

Padua Research Archive

BackgroundCatecholaminergic polymorphic ventricular tachycardia (CPVT) is a familial arrhythmogenic syndrome characterized by sudden death. There are several genetic forms of CPVT associated with mutations in genes encoding the cardiac ryanodine receptor (RyR2) and its auxiliary proteins including calsequestrin (CASQ2) and calmodulin (CaM). It has been suggested that impairment of the ability of RyR2 to stay closed (ie, refractory) during diastole may be a common mechanism for these diseases. Here, we explore the possibility of engineering CaM variants that normalize abbreviated RyR2 refractoriness for subsequent viral‐mediated delivery to alleviate arrhythmias in non–CaM‐related CPVT. Methods and ResultsTo that end, we have designed a CaM protein (GSH‐M37Q; dubbed as therapeutic CaM or T‐CaM) that exhibited a slowed N‐terminal Ca dissociation rate and prolonged RyR2 refractoriness in permeabilized myocytes derived from CPVT mice carrying the CASQ2 mutation R33Q. This T‐CaM was introduced to the heart of R33Q mice through recombinant adeno‐associated viral vector serotype 9. Eight weeks postinfection, we performed confocal microscopy to assess Ca handling and recorded surface ECGs to assess susceptibility to arrhythmias in vivo. During catecholamine stimulation with isoproterenol, T‐CaM reduced isoproterenol‐promoted diastolic Ca waves in isolated CPVT cardiomyocytes. Importantly, T‐CaM exposure abolished ventricular tachycardia in CPVT mice challenged with catecholamines. ConclusionsOur results suggest that gene transfer of T‐CaM by adeno‐associated viral vector serotype 9 improves myocyte Ca handling and alleviates arrhythmias in a calsequestrin‐associated CPVT model, thus supporting the potential of a CaM‐based antiarrhythmic approach as a therapeutic avenue for genetically distinct forms of CPVT

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https://www.research.unipd.it/bitstream/11577/3270238/1/JAHA%202018.pdf

Gene Transfer of Engineered Calmodulin Alleviates Ventricular Arrhythmias in a Calsequestrin-Associated Mouse Model of Catecholaminergic Polymorphic Ventricular Tachycardia

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Archivio istituzionale della ricerca - Università di Padova

Crossref

Padua Research Archive

Directory of Open Access Journals