首页> 外文期刊>journal of cardiovascular pharmacology >Antiarrhythmic Agentcomma; MShyphen;551comma; Protects Against Pinacidil plus; Hypoxiahyphen;Induced Ventricular Fibrillation in Langendorffhyphen;Perfused Rabbit Isolated Heart
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Antiarrhythmic Agentcomma; MShyphen;551comma; Protects Against Pinacidil plus; Hypoxiahyphen;Induced Ventricular Fibrillation in Langendorffhyphen;Perfused Rabbit Isolated Heart

机译:Antiarrhythmic Agentcomma; MShyphen;551comma; Protects Against Pinacidil plus; Hypoxiahyphen;Induced Ventricular Fibrillation in Langendorffhyphen;Perfused Rabbit Isolated Heart

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SummaryWe studied the electrophysiologic and anti-fibrillatory effects of the class III agent MS-551 in a rabbit isolated heart model in which ventricular fibrillation (VF) occurs reproducibly under conditions of hyp-oxia/reoxygenation in the presence of the ATP-dependent potassium channel opener, pinacidil. Ten minutes after MS-551 or vehicle administration, addition of pinacidil (1.25 μM) to the buffer was followed by a 12-min hypoxic period and 40-min reoxygenation. At a low concentration of MS-551 (1.0 μM), VF occurred in 5 of 6 hearts, the same incidence as in the control group (5 of 6). In contrast 0 of 6 hearts treated with 15 μMMS-551 developed VF (p 0.05 vs. vehicle). Ventricular effective refractory period (VERP) was determined in a separate group of isolated hearts (n = 13). Pinacidil alone, during normoxic perfusion, decreased VERP 48 ± 11% (p 0.05) 15 min after exposure. Five minutes of hypoxia alone also decreased VERP (57 ± 8%, p 0.05). Under normoxic conditions, MS-551 increased ERP 31 ± 10% (p 0.05 vs. baseline). VERP prolongation by MS-551 was reduced in the presence of pinacidil but remained 22 ± 6% (p 0.05) above baseline. The results suggest that VERP shortening owing to pinacidil mediated ATP-dependent K+channel opening is associated with development of VF in isolated heart. MS-551 attenuates the pinacidil-mediated decrease in VERP and prevents pinacidil + hypoxia-reoxygenation-induced VF. Because pinacidil and hypoxia open myocardial KATPchannels, putatively decreasing VERP, MS-551 may exert its antifibrillatory effect through partial blockade of K+ATPchannels

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