Rickels K, Schweizer E
Department of Psychiatry, University of Pennsylvania, Philadelphia 19104-2649, USA.
J Clin Psychopharmacol. 1998 Dec;18(6 Suppl 2):12S-18S. doi: 10.1097/00004714-199812001-00004.
This article compares panic disorder (PD) medications and discusses long-term therapy. In a review of the literature, monoamine oxidase inhibitors (MAOIs), selective serotonin reuptake inhibitors (SSRIs), and benzodiazepines prove effective in treating PD. MAOIs treat comorbid depression; frequent side effects are dizziness and orthostatic hypotension. SSRIs are better tolerated than MAOIs, producing mild anticholinergic effects, but also producing gastrointestinal side effects and sexual dysfunction. Benzodiazepines are generally well tolerated when titrated gradually; moderate sedation is the most common short-term side effect. Long-term risks are physical dependence and withdrawal reactions. One hundred six PD patients were enrolled in a double-blind, 8-month, placebo-controlled trial of alprazolam and imipramine. In the 8-week short-term phase, daily dosages were titrated up to 10 mg/day of alprazolam and 250 mg/day of imipramine. The greatest number of dropouts occurred during this phase (lack of improvement and/or side effects). Alprazolam patients had a significantly more rapid onset of improvement and lower adverse events and attrition rates. In the 6-month maintenance period, patients continued short-term treatment. Patients receiving either alprazolam or imipramine developed tolerance to some side effects. At maintenance-phase completion, 62% of the alprazolam-group patients and 26% of both the imipramine- and placebo-group patients were panic free (p<0.01). Dosages were tapered to zero over 3 weeks; one third of the alprazolam patients could not discontinue. During the unblinded, 15-month follow-up, patients received open treatment selected by personal physicians on an as-needed basis. At the end of follow-up, all patients were reassessed. Patients who had completed both short-term and maintenance phases were far more likely to be panic-free (85% vs. 55%; p<0.01). PD is chronic and recurrent, and 8 months is an effective treatment period. Maintenance treatment does not lead to tolerance, even with benzodiazepines. Dose tapering must be very gradual. Completion of a long-term maintenance program strongly predicts remission.
本文比较了惊恐障碍(PD)的药物治疗并探讨了长期治疗。在文献综述中,单胺氧化酶抑制剂(MAOIs)、选择性5-羟色胺再摄取抑制剂(SSRIs)和苯二氮䓬类药物被证明对治疗PD有效。MAOIs可治疗共病的抑郁症;常见副作用为头晕和体位性低血压。SSRIs比MAOIs耐受性更好,会产生轻度抗胆碱能作用,但也会产生胃肠道副作用和性功能障碍。苯二氮䓬类药物若逐渐滴定剂量,一般耐受性良好;中度镇静是最常见的短期副作用。长期风险是身体依赖和戒断反应。106名PD患者参与了一项为期8个月的阿普唑仑和丙咪嗪双盲、安慰剂对照试验。在8周的短期阶段,每日剂量滴定至阿普唑仑10毫克/天和丙咪嗪250毫克/天。该阶段出现的退出人数最多(无改善和/或副作用)。阿普唑仑组患者改善起效明显更快,不良事件和损耗率更低。在6个月的维持期,患者继续进行短期治疗。接受阿普唑仑或丙咪嗪治疗的患者对某些副作用产生了耐受性。维持期结束时,阿普唑仑组62%的患者以及丙咪嗪组和安慰剂组26%的患者惊恐症状消失(p<0.01)。剂量在3周内逐渐减至零;三分之一的阿普唑仑患者无法停药。在为期15个月的非盲法随访期间,患者根据需要接受个人医生选择的开放治疗。随访结束时,对所有患者进行重新评估。完成短期和维持期治疗的患者无惊恐症状的可能性要高得多(85%对55%;p<0.01)。PD是慢性复发性疾病,8个月是一个有效的治疗期。维持治疗不会导致耐受性,即使使用苯二氮䓬类药物也是如此。剂量递减必须非常缓慢。完成长期维持治疗方案可有力预测病情缓解。
