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首页> 外文期刊>Circulation: An Official Journal of the American Heart Association >Acacetin, a natural flavone, selectively inhibits human atrial repolarization potassium currents and prevents atrial fibrillation in dogs.
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Acacetin, a natural flavone, selectively inhibits human atrial repolarization potassium currents and prevents atrial fibrillation in dogs.

机译:Acacetin是一种天然的黄酮,可选择性抑制人的心房复极钾电流,并防止狗的房颤。

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BACKGROUND: The development of atrium-selective antiarrhythmic agents is a current strategy for inhibiting atrial fibrillation (AF). The present study investigated whether the natural flavone acacetin from the traditional Chinese medicine Xuelianhua would be an atrium-selective anti-AF agent. METHODS AND RESULTS: The effects of acacetin on human atrial ultrarapid delayed rectifier K(+) current (I(Kur)) and other cardiac ionic currents were studied with a whole-cell patch technique. Acacetin suppressed I(Kur) and the transient outward K(+) current (IC(50) 3.2 and 9.2 mumol/L, respectively) and prolonged action potential duration in human atrial myocytes. The compound blocked the acetylcholine-activated K(+) current; however, it had no effect on the Na(+) current, L-type Ca(2+) current, or inward-rectifier K(+) current in guinea pig cardiac myocytes. Although acacetin caused a weak reduction in the hERG and hKCNQ1/hKCNE1 channels stably expressed in HEK 293 cells, it did not prolong the corrected QT interval in rabbit hearts. In anesthetized dogs, acacetin (5 mg/kg) prolonged the atrial effective refractory period in both the right and left atria 1 to 4 hours after intraduodenal administration without prolongation of the corrected QT interval, whereas sotalol at 5 mg/kg prolonged both the atrial effective refractory period and the corrected QT interval. Acacetin prevented AF induction at doses of 2.5 mg/kg (50%), 5 mg/kg (85.7%), and 10 mg/kg (85.7%). Sotalol 5 mg/kg also prevented AF induction (60%). CONCLUSIONS: The present study demonstrates that the natural compound acacetin is an atrium-selective agent that prolongs the atrial effective refractory period without prolonging the corrected QT interval and effectively prevents AF in anesthetized dogs after intraduodenal administration. These results indicate that oral acacetin is a promising atrium-selective agent for the treatment of AF.
机译:背景:心房选择性抗心律失常药的发展是抑制心房颤动(AF)的当前策略。本研究调查了中药血联华中的天然黄酮乙酰水杨酸是否会成为一种心房选择性抗AF药物。方法和结果:采用全细胞贴片技术研究了醋氨蝶呤对人心房超快速延迟整流器K(+)电流(I(Kur))和其他心脏离子电流的影响。 Acacetin抑制人心房肌细胞中的I(Kur)和瞬时向外K(+)电流(分别为IC(50)3.2和9.2 mumol / L)并延长了动作电位的持续时间。该化合物阻断了乙酰胆碱激活的K(+)电流;但是,它对豚鼠心肌细胞中的Na(+)电流,L型Ca(2+)电流或整流器K(+)电流没有影响。尽管阿西西汀引起在HEK 293细胞中稳定表达的hERG和hKCNQ1 / hKCNE1通道的弱减弱,但它并未延长兔心脏的校正QT间隔。在麻醉的狗中,阿沙西汀(5 mg / kg)在十二指肠内给药后左右心房延长了有效心房不应期,延长了十二指肠内给药后的1至4小时,而5 mg / kg的索他洛尔延长了心房的有效不应期。有效不应期和校正的QT间隔。 Acacetin在2.5 mg / kg(50%),5 mg / kg(85.7%)和10 mg / kg(85.7%)的剂量下可预防房颤诱发。 5 mg / kg的索他洛尔还可以预防房颤诱发(60%)。结论:本研究表明,天然化合物阿沙西汀是一种中庭选择剂,可延长心房有效不应期,而不会延长校正的QT间隔,并有效预防十二指肠内给药后麻醉犬的房颤。这些结果表明,口服阿卡西汀是用于治疗房颤的有前途的心房选择剂。

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