口服孕酮、阿普唑仑和安慰剂治疗重度经前综合征的双盲试验。
A double-blind trial of oral progesterone, alprazolam, and placebo in treatment of severe premenstrual syndrome.
作者信息
Freeman E W, Rickels K, Sondheimer S J, Polansky M
机构信息
Department of Obstetrics and Gynecology, School of Medicine, University of Pennsylvania, Philadelphia, USA.
出版信息
JAMA. 1995 Jul 5;274(1):51-7.
OBJECTIVE
To determine the effectiveness of oral micronized progesterone, alprazolam, and placebo in premenstrual syndrome (PMS) treatment and the effect of clinical contact on treatment responses.
DESIGN
Randomized, double-blind, placebo-controlled 3-month parallel treatment arms with flexible dosage and with the length of clinical contact randomized within each treatment group.
SETTING
University hospital PMS medical treatment outpatient program in obstetrics/gynecology department.
SUBJECTS
Among volunteers for PMS treatment, 444 were evaluated and 185 meeting defined PMS criteria were randomized to treatment; treatment data are available for 170. There were no medical withdrawals for adverse events.
INTERVENTION
A double-blinded protocol in which 300 mg of oral micronized progesterone, 0.25 mg of alprazolam, or placebo was administered four times a day from day 18 of the menstrual cycle through day 2 of the next cycle, including taper. The mean daily dose at the third treatment was 1760 mg of progesterone or 1.5 mg of alprazolam. Subjects were randomized to brief (< 20 minutes) or extended (50 minutes) visits.
MAIN OUTCOME MEASURES
Daily symptom report (DSR) scored for total DSR symptoms, four DSR factors.
RESULTS
Alprazolam was significantly better than placebo or progesterone for total premenstrual symptoms and DSR factors of mental function, pain, and mood. Thirty-seven percent of the alprazolam group experienced a 50% reduction in total DSR scores. There were no clinically significant withdrawal symptoms when alprazolam administration was restricted to the luteal phase. Oral micronized progesterone therapy was no better than placebo. Brief vs extended visits had no effect on treatment outcome. Treatment response was associated with severity of premenstrual symptoms at baseline but with no other diagnostic variables.
CONCLUSIONS
Alprazolam has a role in PMS treatment and offers a therapy limited to the luteal phase. Oral micronized progesterone is ineffective for PMS.
目的
确定口服微粉化孕酮、阿普唑仑和安慰剂治疗经前期综合征(PMS)的有效性以及临床接触对治疗反应的影响。
设计
随机、双盲、安慰剂对照的3个月平行治疗组,剂量灵活,每个治疗组内临床接触时长随机。
地点
大学医院妇产科的PMS门诊治疗项目。
研究对象
在PMS治疗志愿者中,444人接受评估,185人符合既定PMS标准并被随机分配接受治疗;170人的治疗数据可用。无因不良事件而退出治疗者。
干预措施
采用双盲方案,从月经周期第18天至下一个周期第2天,每天4次给予300毫克口服微粉化孕酮、0.25毫克阿普唑仑或安慰剂,包括逐渐减量阶段。第三次治疗时的平均日剂量为1760毫克孕酮或1.5毫克阿普唑仑。受试者被随机分配接受简短(<20分钟)或延长(50分钟)的访视。
主要观察指标
每日症状报告(DSR),根据DSR总症状、四个DSR因子评分。
结果
对于经前期总症状以及精神功能、疼痛和情绪的DSR因子,阿普唑仑显著优于安慰剂或孕酮。阿普唑仑组37%的患者DSR总分降低了50%。当阿普唑仑给药仅限于黄体期时,无临床显著的撤药症状。口服微粉化孕酮治疗并不比安慰剂更好。简短访视与延长访视对治疗结果无影响。治疗反应与基线时经前期症状的严重程度相关,但与其他诊断变量无关。
结论
阿普唑仑在PMS治疗中具有作用,且提供了仅限于黄体期的治疗方法。口服微粉化孕酮对PMS无效。
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