Brodkin E S, McDougle C J, Naylor S T, Cohen D J, Price L H
Abraham Ribicoff Research Facilities, Connecticut Mental Health Center, New Haven, Connecticut, USA.
J Child Adolesc Psychopharmacol. 1997 Summer;7(2):109-21. doi: 10.1089/cap.1997.7.109.
The purpose of this investigation was to determine the short-term efficacy and tolerability of clomipramine in a consecutive series of adults with pervasive developmental disorders (PDDs). Thirty-five adults with PDDs (DSM-IV), 16 of whom were nonverbal, entered a 12-week prospective open-label trial of clomipramine. The initial sample included 18 patients with autistic disorder, 6 patients with Asperger's disorder, and 11 patients with pervasive developmental disorder not otherwise specified (PDDNOS). Behavioral ratings were obtained at baseline and after 4, 8, and 12 weeks of clomipramine. Eighteen (55%) of the 33 patients who completed the trial were categorized as treatment responders based on scores of "much improved" or "very much improved" on the Clinical Global Impression (CGI) global improvement item (p < 0.001). Ten (63%) of 16 patients with autistic disorder, 2 (33%) of 6 patients with Asperger's disorder, and 6 (55%) of 11 patients with PDDNOS were considered responders to clomipramine treatment. In those 18 patients, clomipramine significantly reduced total repetitive thoughts and behavior (p < 0.001) and also aggression (p < 0.001), and improved some aspects of social relatedness, such as eye contact and verbal responsiveness (p < 0.001). Change in these specific symptom clusters over time was not related to DSM-IV subtype of PDD. The level of autistic behavior, as measured by the Autism Behavior Checklist (ABC) score, and full-scale intelligence quotient (IQ) were not significantly associated with global treatment response. Whereas clomipramine was well tolerated by most patients, 13 had clinically significant adverse effects. Three patients had seizures during clomipramine treatment, including 2 who had prior seizure disorders and were taking anticonvulsants. Of the 32 patients who had no history of prior seizures, only 1 had a seizure during clomipramine treatment. There were no adverse cardiovascular or extrapyramidal effects. All responders continued on clomipramine after completion of the study. The results of this open-label trial suggest that clomipramine may be an effective drug for reducing repetitive thoughts and actions and aggressive behavior and for improving some elements of social behavior, such as eye contact and verbal responsivity in adults with PDDs. Careful monitoring of adverse effects, particularly seizures, is warranted. Although an electroencephalogram (EEG) is not mandatory in patients with PDD prior to clomipramine treatment, we recommend that patients with PDD and a history of seizures be treated initially with a selective serotonin uptake inhibitor rather than with clomipramine. The findings of this study require replication in a double-blind placebo-controlled investigation before definitive statements of efficacy and tolerability can be made.
本研究的目的是确定氯米帕明对一系列连续的广泛性发育障碍(PDD)成年患者的短期疗效和耐受性。35名患有PDD(DSM-IV)的成年人,其中16名无言语能力,进入了一项为期12周的氯米帕明前瞻性开放标签试验。初始样本包括18名自闭症谱系障碍患者、6名阿斯伯格综合征患者和11名未特定指明的广泛性发育障碍(PDDNOS)患者。在基线以及氯米帕明治疗4周、8周和12周后进行行为评分。在完成试验的33名患者中,18名(55%)根据临床总体印象(CGI)总体改善项目中“明显改善”或“非常明显改善”的评分被归类为治疗反应者(p < 0.001)。16名自闭症谱系障碍患者中有10名(63%)、6名阿斯伯格综合征患者中有2名(33%)以及11名PDDNOS患者中有6名(55%)被认为是氯米帕明治疗的反应者。在这18名患者中,氯米帕明显著减少了总的重复思维和行为(p < 0.001)以及攻击行为(p < 0.001),并改善了社会关系的一些方面,如眼神接触和言语反应性(p < 0.001)。这些特定症状群随时间的变化与PDD的DSM-IV亚型无关。通过自闭症行为检查表(ABC)评分衡量的自闭症行为水平和全量表智商(IQ)与总体治疗反应无显著关联。虽然大多数患者对氯米帕明耐受性良好,但有13名出现了具有临床意义的不良反应。3名患者在氯米帕明治疗期间发生癫痫,其中2名既往有癫痫病史且正在服用抗惊厥药物。在32名无既往癫痫病史的患者中,只有1名在氯米帕明治疗期间发生癫痫。未出现不良心血管或锥体外系反应。所有反应者在研究结束后继续服用氯米帕明。这项开放标签试验的结果表明,氯米帕明可能是一种有效药物,可减少PDD成年患者的重复思维和行为以及攻击行为,并改善社会行为的一些要素,如眼神接触和言语反应性。需要仔细监测不良反应,尤其是癫痫。虽然在氯米帕明治疗前对PDD患者不强制进行脑电图(EEG)检查,但我们建议有癫痫病史的PDD患者初始治疗时使用选择性5-羟色胺再摄取抑制剂而非氯米帕明。在能够做出关于疗效和耐受性的确切声明之前,本研究的结果需要在双盲安慰剂对照研究中进行重复验证。
