首页> 外文期刊>Brain: A journal of neurology >Opening of ATP-sensitive potassium channels causes migraine attacks: a new target for the treatment of migraine
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Opening of ATP-sensitive potassium channels causes migraine attacks: a new target for the treatment of migraine

机译:ATP敏感钾通道的开放导致偏头痛攻击:一种治疗偏头痛的新目标

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摘要

Migraine is one of the most disabling and prevalent of all disorders. To improve understanding of migraine mechanisms and to suggest a new therapeutic target, we investigated whether opening of ATP-sensitive potassium channels (K-ATP) would cause migraine attacks. In this randomized, double-blind, placebo-controlled, crossover study, 16 patients aged 18-49 years with one to five migraine attacks a month were randomly allocated to receive an infusion of 0.05 mg/min K-ATP channel opener levcromakalim and placebo on two different days (ClinicalTrials.gov number, NCT03228355). The primary endpoints were the difference in incidence of migraine attacks, headaches and the difference in area under the curve (AUC) for headache intensity scores (0-12 h) and for middle cerebral artery blood flow velocity (0-2 h) between levcromakalim and placebo. Between 24 May 2017 and 23 November 2017, 16 patients randomly received levcromakalim and placebo on two different days. Sixteen patients (100%) developed migraine attacks after levcromakalim compared with one patient (6%) after placebo (P = 0.0001); the difference of incidence is 94% [95% confidence interval (CI) 78-100%]. The incidence of headache over the 12 h observation period was higher but not significant after levcromakalim (n = 16) than after placebo (n = 7) (P = 0.016) (95% CI 16-71%). The AUC for headache intensity was significantly larger after levcromakalim compared to placebo (AUC(0-12h), P50.0001). There was no change in mean middle cerebral artery blood flow velocity after levcromakalim compared to placebo (AUC(0-2h) P = 0.46). Opening of K-ATP channels caused migraine attacks in all patients. This suggests a crucial role of these channels in migraine pathophysiology and that K-ATP channel blockers could be potential targets for novel drugs for migraine.
机译:偏头痛是所有疾病最令人伤害和普遍的侵略性之一。为了提高对偏头痛机制的理解并提出新的治疗目标,我们研究了ATP敏感钾通道(K-ATP)的开放会导致偏头痛攻击。在这种随机,双盲,安慰剂控制的交叉研究中,18-49岁的16名患者随机分配了一至五个偏头痛的攻击,以接受输注0.05 mg / min K-ATP通道开启器Levcromakalim和安慰剂在两个不同的日子(ClinicalTrials.gov号,NCT03228355)。初级终点是偏头痛攻击,头痛和曲线区域下面积差异的差异(AUC)的发生率,用于头痛强度分数(0-12小时)和Levcromakalim之间的中脑动脉血流速度(0-2小时)和安慰剂。 2017年5月24日至2017年11月24日,16名患者随机接受了Levcromakalim和安慰剂两次不同的日子。 Levcromakalim在安慰剂后的一名患者(6%)比较(P = 0.0001)后,十六名患者(100%)在Levcromakalim后发育偏头痛攻击;发病率差异为94%[95%置信区间(CI)78-100%]。在Levcromakalim(n = 16)后,12小时观察时期头痛的发生率高于安慰剂(n = 7)后(n = 7)(p = 0.016)(95%CI 16-71%)。 Levcromakalim与安慰剂(AUC(0-12h),P50.0001)相比,Levcromakalim后,头痛强度的AUC显着大。 Levcromakalim与安慰剂相比,Levcromakalim后的平均中动脉血流速度没有变化(AUC(0-2H)p = 0.46)。 K-ATP通道的开放导致所有患者的偏头痛攻击。这表明这些通道在偏头痛病理生理学中的关键作用,并且K-ATP通道阻滞剂可能是偏头痛新药物的潜在目标。

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