Remodeling of repolarization and arrhythmia susceptibility in a myosin-binding protein C knockout mouse model | Zendy

Amir Toib | Zendy; Chen Zhang | Zendy; Giulia Borghetti | Zendy; Xiaoxiao Zhang | Zendy; Markus Wallner | Zendy; Yijun Yang | Zendy; Constantine D. Troupes | Zendy; Hajime Kubo | Zendy; Thomas E. Sharp | Zendy; Eric Feldsott | Zendy; Remus M. Berretta | Zendy; Neil Zalavadia | Zendy; Danielle M. Trappanese | Zendy; Shavonn C. Harper | Zendy; Polina Gross | Zendy; Xiongwen Chen | Zendy; Sadia Mohsin | Zendy; Steven R. Houser | Zendy

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Remodeling of repolarization and arrhythmia susceptibility in a myosin-binding protein C knockout mouse model

Author(s) -

Amir Toib,

Chen Zhang,

Giulia Borghetti,

Xiaoxiao Zhang,

Markus Wallner,

Yijun Yang,

Constantine D. Troupes,

Hajime Kubo,

Thomas E. Sharp,

Eric Feldsott,

Remus M. Berretta,

Neil Zalavadia,

Danielle M. Trappanese,

Shavonn C. Harper,

Polina Gross,

Xiongwen Chen,

Sadia Mohsin,

Steven R. Houser

Publication year - 2017

Publication title -

ajp heart and circulatory physiology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.524

H-Index - 197

eISSN - 1522-1539

pISSN - 0363-6135

DOI - 10.1152/ajpheart.00167.2017

Subject(s) - medicine , qt interval , hypertrophic cardiomyopathy , myocyte , repolarization , knockout mouse , patch clamp , muscle hypertrophy , sudden death , endocrinology , potassium channel , cardiology , long qt syndrome , electrophysiology , receptor

Hypertrophic cardiomyopathy (HCM) is one of the most common genetic cardiac diseases and among the leading causes of sudden cardiac death (SCD) in the young. The cellular mechanisms leading to SCD in HCM are not well known. Prolongation of the action potential (AP) duration (APD) is a common feature predisposing hypertrophied hearts to SCD. Previous studies have explored the roles of inward Na + and Ca 2+ in the development of HCM, but the role of repolarizing K + currents has not been defined. The objective of this study was to characterize the arrhythmogenic phenotype and cellular electrophysiological properties of mice with HCM, induced by myosin-binding protein C (MyBPC) knockout (KO), and to test the hypothesis that remodeling of repolarizing K + currents causes APD prolongation in MyBPC KO myocytes. We demonstrated that MyBPC KO mice developed severe hypertrophy and cardiac dysfunction compared with wild-type (WT) control mice. Telemetric electrocardiographic recordings of awake mice revealed prolongation of the corrected QT interval in the KO compared with WT control mice, with overt ventricular arrhythmias. Whole cell current- and voltage-clamp experiments comparing KO with WT mice demonstrated ventricular myocyte hypertrophy, AP prolongation, and decreased repolarizing K + currents. Quantitative RT-PCR analysis revealed decreased mRNA levels of several key K + channel subunits. In conclusion, decrease in repolarizing K + currents in MyBPC KO ventricular myocytes contributes to AP and corrected QT interval prolongation and could account for the arrhythmia susceptibility. NEW & NOTEWORTHY Ventricular myocytes isolated from the myosin-binding protein C knockout hypertrophic cardiomyopathy mouse model demonstrate decreased repolarizing K + currents and action potential and QT interval prolongation, linking cellular repolarization abnormalities with arrhythmia susceptibility and the risk for sudden cardiac death in hypertrophic cardiomyopathy.

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