Concomitant genetic ablation of L-type Ca_v1.3 (α_1D) and T-type Ca_v3.1 (α_1G) Ca²⁺ channels disrupts heart automaticity.

Cardiac automaticity is set by pacemaker activity of the sinus node (SAN). In addition to the ubiquitously expressed cardiac voltage-gated L-type Ca_v1.2 Ca²⁺ channel isoform, pacemaker cells within the SAN and the atrioventricular node co-express voltage-gated L-type Ca_v1.3 and T-type Ca_v3.1 Ca²⁺ channels (SAN-VGCCs). The role of SAN-VGCCs in automaticity is incompletely understood. We used knockout mice carrying individual genetic ablation of Ca_v1.3 (Ca_v1.3^-/-) or Ca_v3.1 (Ca_v3.1^-/-) channels and double mutant Ca_v1.3^-/-/Ca_v3.1^-/- mice expressing only Ca_v1.2 channels. We show that concomitant loss of SAN-VGCCs prevents physiological SAN automaticity, blocks impulse conduction and compromises ventricular rhythmicity. Coexpression of SAN-VGCCs is necessary for impulse formation in the central SAN. In mice lacking SAN-VGCCs, residual pacemaker activity is predominantly generated in peripheral nodal and extranodal sites by f-channels and TTX-sensitive Na⁺ channels. In beating SAN cells, ablation of SAN-VGCCs disrupted late diastolic local intracellular Ca²⁺ release, which demonstrates an important role for these channels in supporting the sarcoplasmic reticulum based "Ca²⁺ clock" mechanism during normal pacemaking. These data implicate an underappreciated role for co-expression of SAN-VGCCs in heart automaticity and define an integral role for these channels in mechanisms that control the heartbeat.

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