ABSTRACT
Cardiotonic drugs and exercise training promote cardiac inotropic effects, which may affect training-induced cardiac adaptations. This study investigated the effects of long-term administration of digoxin on heart structure and function, and physical performance of rats submitted to high-intensity interval training (HIIT). Male Wistar rats, 60 days old, were divided into control (C), digoxin (DIGO), trained (T), and trained with digoxin (TDIGO). Digoxin was administered by gavage (30 µg/kg/day) for 75 days. The HIIT program consisted of treadmill running 60 min/day (8 min at 80% of the maximum speed (MS) and 2 min at 20% of the MS), 5 days per week during 60 days. The main cardiac parameters were evaluated by echocardiograph and cardiomyocyte area was determined by histology. There were no group x time effects of digoxin, HIIT or interactions (digoxin and HIIT) on functional echocardiographic parameters (heart rate; ejection fraction) or in the maximum exercise test. There was a group x time interaction, as evidenced by observed cardiac hypertrophy in the TDIGO group evaluated by ratio of left ventricle weight to body weight (p<0.002) and cardiomyocyte area (p<0.000002). Long-term administration of digoxin promoted cardiac hypertrophy without affecting cardiac function and physical performance in rats submitted to HIIT.
Subject(s)
Cardiomegaly/chemically induced , Digoxin/adverse effects , Heart/drug effects , Physical Conditioning, Animal , Animals , Echocardiography , Exercise Test , Heart Rate , High-Intensity Interval Training , Male , Random Allocation , Rats , Rats, WistarABSTRACT
RESUMO Introdução: Cardiotônicos e bloqueadores de canais de cálcio são fármacos que alteram o Ca2+ intracelular e afetam o coração. Objetivo: Avaliar os efeitos da administração de verapamil e digoxina sobre a morfologia cardíaca de ratos submetidos ao treinamento intervalado (TAI). Métodos: Ratos Wistar machos divididos em seis grupos (N = 8): Controle, Digoxina (30,0 µg.kg-1/dia), Verapamil (5,0 mg.kg-1/dia), Treinado, Treinado+digoxina e Treinado+verapamil. O TAI foi realizado em esteira rolante (60 min/dia/60 dias) concomitantemente com a administração dos fármacos. Fragmentos do ventrículo esquerdo (VE) foram coletados para análise histológica. Resultados: A digoxina e o verapamil aumentaram a área total do VE (p < 0,002), capilares/área VE (p < 0,01) e área de cardiomiócitos (p < 2,8e-10), sendo que, nesta última variável, o verapamil promoveu efeito ainda maior que a digoxina. O TAI aumentou VE/PC (p < 4e-05), o diâmetro interno do VE (p < 2,7e-6), a área de cardiomiócitos (p < 1,8e-6) e reduziu o [Lac] (p < 2,6e-5). Houve interação entre TAI e fármacos na área total (p < 9,8e-5), capilares (p < 0,04), células/área (p < 0,004) e área de cardiomiócitos (p < 2e-16). Conclusão: A digoxina promoveu hipertrofia de cardiomiócitos e, quando associada ao TAI, potencializou a hipertrofia. O verapamil foi mais eficiente em aumentar a área de cardiomiócitos em comparação com a digoxina, porém somente de forma isolada.
ABSTRACT Introduction: Cardiotonics and calcium channel blockers are drugs that alter intracellular Ca2+ and can affect the heart. Objective: To evaluate the effects of administration of verapamil and digoxin on heart morphology of rats subjected to interval training (IT). Methods: Male Wistar rats were divided into groups (n = 8): Control, Digoxin (30.0µg.kg-1/day), Verapamil (5.0 mg.kg-1/day), Trained, Trained+digoxin and Trained+verapamil. The IT was performed on a treadmill (60 min/day/60 days) concurrently with the drugs administration. Fragments of the left ventricle (LV) were collected for histological analysis. Results: Digoxin and verapamil increased the total area of the LV (p<0.002), capillary/LV area (p<0.01) and cardiomyocytes area (p<2.8e-10), and in the latter variable, verapamil promoted even greater effect than digoxin. The IT increased LV/BW (p<4e-05), the inner diameter of the LV (p<2.7e-6), the area of cardiomyocytes (p<1.8e-6), and reduced the [Lac] (p<2.6e-5). There was interaction between IT and drugs in the total area (p<9.8e-5), capillaries (p<0.04), cell/area (p<0.004) and cardiomyocytes area (p <2.0e-16). Conclusions: Digoxin promoted cardiomyocyte hypertrophy and when associated with IT, potentiated the hypertrophy. Verapamil was more efficient in increasing the cardiomyocytes area compared with digoxin, but only when isolated.
RESUMEN Introducción: Cardiotónicos y bloqueadores de los canales de calcio son fármacos que alteran el Ca2+ intracelular y afectan al corazón. Objetivo: Evaluar los efectos de la administración de verapamilo y digoxina sobre la morfología del corazón de ratas sometidas a entrenamiento a intervalos (EI). Métodos: Ratas Wistar macho, divididas en seis grupos (N = 8): Control, Digoxina (30,0 µg.kg-1/día), Verapamilo (5,0 mg.kg-1/día), Entrenado, Entrenado+digoxina y Entrenado+verapamilo. El entrenamiento a intervalos se realizó en una cinta de correr (60 min/día/60 días), con la administración concomitante de fármacos. Se recogieron fragmentos del ventrículo izquierdo (VI) para el análisis histológico. Resultados: La digoxina y el verapamilo aumentaron el área total del VI (p < 0,002), capilares/área VI (p < 0,01) y el área de los cardiomiocitos (p < 2,8e-10) y, en esta última variable, el verapamilo promovió un efecto aún mayor que la digoxina. EI entrenamiento a intervalos aumentó VI/PC (p < 4e-05), el diámetro interior del VI (p < 2,7e-6), el área de los cardiomiocitos (p < 1,8e-6) y redujo el [Lac] (p < 2,6e-5). Hubo una interacción entre fármacos y el EI en el área total (p < 9,8e-5), capilares (p<0,04), células/área (p < 0,004) y el área de los cardiomiocitos (p < 2e-16). Conclusión: La digoxina promovió la hipertrofia de los cardiomiocitos y, cuando al asociarse con el EI, potenció la hipertrofia. El verapamilo fue más eficiente en el aumento de la zona de los cardiomiocitos en comparación con la digoxina, pero sólo de forma aislada.
