Gelpin E, Bonne O, Peri T, Brandes D, Shalev A Y
The Center for Traumatic Stress, Department of Psychiatry, Hadassah University Hospital, Jerusalem, Israel.
J Clin Psychiatry. 1996 Sep;57(9):390-4.
Most types of psychotropic drugs have been tried in the treatment of chronic posttraumatic stress disorder (PTSD), but have yielded limited results. Theory and retrospective research predict that early treatment may be more efficacious. Specifically, high-potency benzodiazepines have been recommended for the treatment of acute responses to trauma and for prevention of PTSD. This study prospectively evaluates the effect of early administration of benzodiazepines on the course of PTSD and PTSD symptoms.
Thirteen trauma survivors (the benzodiazepine group) were treated within 6.7 +/- 5.8 days after the trauma (range, 2-18) with either clonazepam (N = 10, 2.7 +/- 0.8 mg/day) or alprazolam (N = 3, 2.5 mg/day). Thirteen other trauma survivors, pair-matched with subjects in the active treatment group for gender and symptom severity in the first week after the trauma, constitute the control group. Both groups were reevaluated 1 and 6 months after the trauma for PTSD symptoms (Horowitz Impact of Event Scale; Mississippi Rating Scale for Combat-Related PTSD-civilian trauma version), PTSD status (Clinician Administered PTSD Scale), state anxiety, depression, and resting heart rate.
Subjects in the benzodiazepine group did not differ from controls in 1-month and 6-month PTSD and anxiety scores. Repeated measures ANOVA showed no group or group-by-time effect on psychometric measures. A trend toward group-by-time interaction in resting heart rate was noted (progressive decrease in the benzodiazepine group). Nine benzodiazepine subjects and 3 controls met PTSD diagnostic criteria 6 months after the trauma.
Contrary to expectations, the early administration of benzodiazepines to trauma survivors with high levels of initial distress did not have a salient beneficial effect on the course of their illness, while reducing physiologic expression of arousal.
大多数类型的精神药物都曾用于治疗慢性创伤后应激障碍(PTSD),但效果有限。理论和回顾性研究预测早期治疗可能更有效。具体而言,高效苯二氮䓬类药物已被推荐用于治疗创伤后的急性反应以及预防PTSD。本研究前瞻性评估早期给予苯二氮䓬类药物对PTSD病程及PTSD症状的影响。
13名创伤幸存者(苯二氮䓬类药物组)在创伤后6.7±5.8天(范围2 - 18天)内接受治疗,其中10人服用氯硝西泮(2.7±0.8毫克/天),3人服用阿普唑仑(2.5毫克/天)。另外13名创伤幸存者作为对照组,他们在创伤后第一周与积极治疗组的受试者按性别和症状严重程度进行配对。两组在创伤后1个月和6个月时重新评估PTSD症状(霍洛维茨事件影响量表;与战斗相关的PTSD - 平民创伤版密西西比评定量表)、PTSD状态(临床医生实施的PTSD量表)、状态焦虑、抑郁和静息心率。
苯二氮䓬类药物组受试者在1个月和6个月时的PTSD及焦虑评分与对照组无差异。重复测量方差分析显示,在心理测量指标上没有组间或组×时间效应。静息心率存在组×时间交互作用趋势(苯二氮䓬类药物组逐渐下降)。创伤后6个月,9名苯二氮䓬类药物组受试者和3名对照组受试者符合PTSD诊断标准。
与预期相反,对初始痛苦程度较高的创伤幸存者早期给予苯二氮䓬类药物,对其病程没有显著的有益影响,尽管能降低觉醒的生理表现。
