Ionic Mechanisms of Impulse Propagation Failure in the FHF2-Deficient Heart.

Rationale: FHFs (fibroblast growth factor homologous factors) are key regulators of sodium channel (Na) inactivation. Mutations in these critical proteins have been implicated in human diseases including Brugada syndrome, idiopathic ventricular arrhythmias, and epileptic encephalopathy. The underlying ionic mechanisms by which reduced Na availability in knockout () mice predisposes to abnormal excitability at the tissue level are not well defined.

Objective: Using animal models and theoretical multicellular linear strands, we examined how FHF2 orchestrates the interdependency of sodium, calcium, and gap junctional conductances to safeguard cardiac conduction.

Methods And Results: mice were challenged by reducing calcium conductance (gCa) using verapamil or by reducing gap junctional conductance (Gj) using carbenoxolone or by backcrossing into a cardiomyocyte-specific Cx43 (connexin 43) heterozygous background. All conditions produced conduction block in mice, with wild-type () mice showing normal impulse propagation. To explore the ionic mechanisms of block in hearts, multicellular linear strand models incorporating FHF2-deficient Na inactivation properties were constructed and faithfully recapitulated conduction abnormalities seen in mutant hearts. The mechanisms of conduction block in mutant strands with reduced gCa or diminished Gj are very different. Enhanced Na inactivation due to FHF2 deficiency shifts dependence onto calcium current (I) to sustain electrotonic driving force, axial current flow, and action potential (AP) generation from cell-to-cell. In the setting of diminished Gj, slower charging time from upstream cells conspires with accelerated Na inactivation in mutant strands to prevent sufficient downstream cell charging for AP propagation.

Conclusions: FHF2-dependent effects on Na inactivation ensure adequate sodium current (I) reserve to safeguard against numerous threats to reliable cardiac impulse propagation.