Pgc-1β deficiency in murine hearts caused an age-dependent pro-arrhythmic phenotype with slowed action potential conduction and accelerated fibrotic changes compared to wild type.
Mitochondrial dysfunction modeled by Pgc-1β deficiency in murine hearts creates an age-dependent arrhythmic substrate through slowed action potential conduction and accelerated fibrosis, providing a mechanistic link to atrial fibrillation.
• Ageing and several chronic conditions are associated with mitochondrial dysfunction. • We investigated atrial arrhythmia in energetically deficient Pgc-1β-/- murine hearts. • Pgc-1β-/- hearts showed increased age-dependent arrhythmic and fibrotic changes. • These were attributed to slowed action potential depolarization and conduction. • The latter offer mechanisms for the atrial arrhythmia observed in these conditions. Ageing and several age-related chronic conditions including obesity, insulin resistance and hypertension are associated with mitochondrial dysfunction and represent independent risk factors for atrial fibrillation (AF). Atrial arrhythmogenesis was investigated in Langendorff-perfused young (3–4 month) and aged (>12 month), wild type (WT) and peroxisome proliferator activated receptor-γ coactivator-1 β deficient ( Pgc-1β −/− ) murine hearts modeling age-dependent chronic mitochondrial dysfunction during regular pacing and programmed electrical stimulation (PES). The Pgc-1β −/− genotype was associated with a pro-arrhythmic phenotype progressing with age. Young and aged Pgc-1β −/− hearts showed compromised maximum action potential (AP) depolarization rates, (d V /d t ) max , prolonged AP latencies reflecting slowed action potential (AP) conduction, similar effective refractory periods and baseline action potential durations (APD 90 ) but shortened APD 90 in APs in response to extrasystolic stimuli at short stimulation intervals. Electrical properties of APs triggering arrhythmia were similar in WT and Pgc-1β −/− hearts. Pgc-1β −/− hearts showed accelerated age-dependent fibrotic change relative to WT, with young Pgc-1β −/− hearts displaying similar fibrotic change as aged WT, and aged Pgc-1β −/− hearts the greatest fibrotic change. Mitochondrial deficits thus result in an arrhythmic substrate, through slowed AP conduction and altered repolarisation characteristics, arising from alterations in electrophysiological properties and accelerated structural change.
Valli et al. (Thu,) conducted a other in Atrial arrhythmia and mitochondrial dysfunction. Pgc-1β deficiency (Pgc-1β-/- genotype) vs. Wild type (WT) genotype was evaluated on Atrial arrhythmogenesis, action potential characteristics, and fibrotic changes. Pgc-1β deficiency in murine hearts caused an age-dependent pro-arrhythmic phenotype with slowed action potential conduction and accelerated fibrotic changes compared to wild type.