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氯硝西泮治疗难治性神经介导性晕厥的疗效与安全性。

Efficacy and safety of clonazepam in refractory neurally mediated syncope.

作者信息

Kadri N N, Hee T T, Rovang K S, Mohiuddin S M, Ryan T, Ashraf R, Huebert V, Hilleman D E

机构信息

Creighton University Cardiac Center, Department of Medicine, Creighton University School of Medicine, Nebraska.

出版信息

Pacing Clin Electrophysiol. 1999 Feb;22(2):307-14. doi: 10.1111/j.1540-8159.1999.tb00443.x.

Abstract

Neurally mediated syncope is a complex syndrome that is often difficult to manage using currently available treatment strategies. The efficacy and safety of clonazepam was evaluated in 35 patients with refractory neurally mediated syncope. All patients had syncope (n = 33) or disabling presyncope (n = 2) and a positive head-up tilt table test (HUTT) despite treatment with one or more of the following therapies: beta-blocker, high-salt diet, fludrocortisone, elastic compression stockings, and disopyramide. Clonazepam was initiated at 0.5 mg/day and titrated in 0.25-0.5 mg/day increments for symptom control. Early (first 8 weeks) symptomatic response was achieved in 31 of 35 (89%) patients. Early HUTT reverted to negative in 29 of 35 (83%) patients. Two patients discontinued clonazepam during early follow-up due to side effects. Thirty-three patients received long-term clonazepam therapy. Twenty-five patients had late HUTT with 21 remaining negative. Of the eight patients who did not have late HUTT, one patient discontinued clonazepam prior to HUTT due to side effects. Seven patients refused late HUTT. All seven patients achieved symptomatic control on clonazepam with two requiring dose titration. Of the 21 patients with a negative late HUTT, 18 achieved symptomatic control with two of these patients requiring dose titration. Two patients who had only partial symptom control despite dose titration achieved total symptomatic control with the addition of disopyramide and beta-blockers. Two patients with a negative late HUTT discontinued clonazepam due to side effects. One patient had been symptomatically controlled while the other had recurrent symptoms with dose limiting side effects occurring after clonazepam dose titration. In the 4 patients with a positive late HUTT, 2 patients were symptomatically controlled, 1 patients required combination therapy with a beta-blocker to achieve symptomatic control, and 1 patient discontinued therapy due to side effects. Overall, 29 of 35 (83%) patients continue to receive clonazepam with symptom control. Based on intention-to-treat HUTT results, 21 of 35 (60%) patients were responders. Four patients required clonazepam dose titration and three required combination therapy with clonazepam plus disopyramide and/or a beta-blocker to achieve control. Clonazepam was discontinued in 6 patients, 5 for side effects and 1 following a transient ischemic attack. Clonazepam appears to be an effective therapeutic alternative in patients with refractory neurally mediated syncope. Based on our preliminary findings, a placebo controlled evaluation of clonazepam in neurally mediated syncope is warranted.

摘要

神经介导性晕厥是一种复杂的综合征,使用目前可用的治疗策略往往难以处理。对35例难治性神经介导性晕厥患者评估了氯硝西泮的疗效和安全性。所有患者均有晕厥(n = 33)或致残性前驱晕厥(n = 2),且尽管接受了以下一种或多种治疗:β受体阻滞剂、高盐饮食、氟氢可的松、弹力袜和丙吡胺,但直立倾斜试验(HUTT)仍为阳性。氯硝西泮起始剂量为0.5mg/天,并以0.25 - 0.5mg/天的增量滴定以控制症状。35例患者中有31例(89%)在早期(前8周)出现症状缓解。35例患者中有29例(83%)早期HUTT转为阴性。2例患者在早期随访期间因副作用停用氯硝西泮。33例患者接受了氯硝西泮长期治疗。25例患者进行了晚期HUTT,其中21例仍为阴性。在8例未进行晚期HUTT的患者中,1例患者因副作用在HUTT前停用氯硝西泮。7例患者拒绝进行晚期HUTT。所有7例患者使用氯硝西泮后症状得到控制,其中2例需要调整剂量。在21例晚期HUTT为阴性的患者中,18例症状得到控制,其中2例需要调整剂量。2例尽管调整剂量但症状仅部分得到控制的患者,加用丙吡胺和β受体阻滞剂后症状完全得到控制。2例晚期HUTT为阴性的患者因副作用停用氯硝西泮。1例患者症状得到控制,而另1例患者症状复发,在氯硝西泮剂量滴定后出现剂量限制性副作用。在4例晚期HUTT为阳性的患者中,2例症状得到控制,1例需要联合使用β受体阻滞剂以控制症状,1例因副作用停药。总体而言,35例患者中有29例(83%)继续接受氯硝西泮治疗且症状得到控制。根据意向性治疗的HUTT结果,35例患者中有21例(60%)为反应者。4例患者需要调整氯硝西泮剂量,3例需要氯硝西泮联合丙吡胺和/或β受体阻滞剂进行联合治疗以实现控制。6例患者停用氯硝西泮,5例因副作用,1例在短暂性脑缺血发作后停药。氯硝西泮似乎是难治性神经介导性晕厥患者的一种有效治疗选择。基于我们的初步研究结果,有必要对氯硝西泮在神经介导性晕厥中的疗效进行安慰剂对照评估。

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