PCP4 regulates Purkinje cell excitability and cardiac rhythmicity
Eugene E. Kim, … , Mario Delmar, Glenn I. Fishman
Eugene E. Kim, … , Mario Delmar, Glenn I. Fishman
Published October 8, 2014
Citation Information: J Clin Invest. 2014;124(11):5027-5036. https://doi.org/10.1172/JCI77495.
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PCP4 regulates Purkinje cell excitability and cardiac rhythmicity

Abstract

Cardiac Purkinje cells are important triggers of ventricular arrhythmias associated with heritable and acquired syndromes; however, the mechanisms responsible for this proarrhythmic behavior are incompletely understood. Here, through transcriptional profiling of genetically labeled cardiomyocytes, we identified expression of Purkinje cell protein-4 (Pcp4), a putative regulator of calmodulin and Ca2+/calmodulin-dependent kinase II (CaMKII) signaling, exclusively within the His-Purkinje network. Using Pcp4-null mice and acquired cardiomyopathy models, we determined that reduced expression of PCP4 is associated with CaMKII activation, abnormal electrophysiology, dysregulated intracellular calcium handling, and proarrhythmic behavior in isolated Purkinje cells. Pcp4-null mice also displayed profound autonomic dysregulation and arrhythmic behavior in vivo. Together, these results demonstrate that PCP4 regulates cardiac excitability through both Purkinje cell–autonomous and central mechanisms and identify this modulator of CaMKII signaling as a potential arrhythmia-susceptibility candidate.

Authors

Eugene E. Kim, Akshay Shekhar, Jia Lu, Xianming Lin, Fang-Yu Liu, Jie Zhang, Mario Delmar, Glenn I. Fishman

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Figure 8

Pcp4-null mice are prone to ventricular arrhythmias and aberrant ventricular conduction.

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Pcp4-null mice are prone to ventricular arrhythmias and aberrant ventric...
(AE) Representative ECG tracings from anesthetized mice after administration of caffeine and epinephrine (CE). (A) Pcp4+/+ control mouse ECG demonstrates sinus tachycardia without ventricular ectopy. (BE) Pcp4–/– mutant mouse ECGs demonstrate (B) isolated PVC; (C) monomorphic ventricular tachycardia (MMVT); (D) bidirectional ventricular tachycardia (BVT); and (E) aberrant ventricular conduction (AVC). (F) Comparison of PVC frequency between Pcp4+/+ and Pcp4–/– mice after caffeine and epinephrine. (G) Proportion of Pcp4-null mice that developed ventricular arrhythmias or AVC after caffeine and epinephrine (n > 11 ). Data represent mean ± SEM. *P < 0.05.