Silver A A, Shytle R D, Philipp M K, Wilkinson B J, McConville B, Sanberg P R
Center for Infant and Child Development, Department of Psychiatry and Behavioral Medicine, University of South Florida College of Medicine, Tampa 33613, USA.
J Clin Psychiatry. 2001 Sep;62(9):707-14. doi: 10.4088/jcp.v62n0908.
Preclinical animal and open-trial clinical trials using nicotine gum and the transdermal nicotine patch found that treatment with nicotine potentiates the effects of neuroleptics in reducing the dyskinetic symptoms of Tourette's disorder. We sought to verify and expand these findings in a prospective double-blind placebo-controlled trial.
Seventy patients with DSM-IV Tourette's disorder were treated with either transdermal nicotine (7 mg/24 hours) or placebo patches in a 33-day, randomized, double-blind study. Each patient received an individually based optimal dose of haloperidol for at least 2 weeks prior to random assignment to nicotine or placebo treatment. A new patch was worn each day for the first 5 days. On the sixth day, the dose of haloperidol was reduced by 50%. Daily patch applications were then continued for an additional 2 weeks (through day 19), at which time the patch was discontinued, but the 50% dose of haloperidol was continued for an additional 2 weeks (through day 33). Clinical and safety assessments were made at each visit.
Patients who completed all 19 days of nicotine (N = 27) or placebo (N = 29) patch treatment were used in efficacy analyses. As documented by the Clinician- and Parent-rated Global Improvement scales, transdermal nicotine was superior to placebo in reducing the symptoms of Tourette's disorder. The Yale Global Tic Severity Scale was less sensitive in detecting a placebo/drug difference than were the global improvement scores, suggesting that some of the improvement may not have been related to treatment-related changes in tic severity, but to the emotional and behavioral symptoms. The side effects of nausea and vomiting were significantly more common in the nicotine group (71% [N = 25] and 40% [N = 14]) than in the placebo group (17% [N = 6] and 9% [N = 3]) (nausea, p = .0001; vomiting, p = .004).
Transdermal nicotine was superior to placebo in reducing behavioral symptoms when patients were receiving an optimal dose of haloperidol, when the dose of haloperidol was reduced by 50%, and when the patch had been discontinued for 2 weeks. These findings confirm earlier open-label findings and suggest that combining nicotinic receptor modulation and neuroleptics could be a therapeutic option for the treatment of Tourette's disorder. While side effects limit chronic use of nicotine, it may be useful on a p.r.n. basis. Further clinical research is warranted to investigate the use of novel nicotinic receptor modulating agents with improved safety profiles over nicotine.
临床前动物实验以及使用尼古丁口香糖和尼古丁透皮贴剂的开放试验临床试验发现,尼古丁治疗可增强抗精神病药物在减轻图雷特氏症运动障碍症状方面的效果。我们试图在前瞻性双盲安慰剂对照试验中验证并扩展这些发现。
在一项为期33天的随机双盲研究中,70名符合《精神疾病诊断与统计手册》第四版(DSM-IV)标准的图雷特氏症患者接受了尼古丁透皮贴剂(7毫克/24小时)或安慰剂贴剂治疗。在随机分配接受尼古丁或安慰剂治疗之前,每位患者均接受基于个体情况的最佳剂量氟哌啶醇治疗至少2周。头5天每天更换一片新贴剂。在第6天,将氟哌啶醇剂量减少50%。然后继续每天使用贴剂2周(至第19天),之后停止使用贴剂,但继续使用50%剂量的氟哌啶醇2周(至第33天)。每次就诊时进行临床和安全性评估。
疗效分析采用完成了全部19天尼古丁(N = 27)或安慰剂(N = 29)贴剂治疗的患者。根据临床医生和家长评定的总体改善量表记录,尼古丁透皮贴剂在减轻图雷特氏症症状方面优于安慰剂。耶鲁综合抽动严重程度量表在检测安慰剂/药物差异方面不如总体改善评分敏感,这表明部分改善可能与抽动严重程度的治疗相关变化无关,而是与情绪和行为症状有关。尼古丁组恶心和呕吐的副作用明显比安慰剂组更常见(恶心:71% [N = 25]和40% [N = 14];安慰剂组:17% [N = 6]和9% [N = 3])(恶心,p = .0001;呕吐,p = .004)。
当患者接受最佳剂量氟哌啶醇治疗时、当氟哌啶醇剂量减少50%时以及当停止使用贴剂2周后,尼古丁透皮贴剂在减轻行为症状方面优于安慰剂。这些发现证实了早期开放标签研究的结果,并表明联合烟碱受体调节和抗精神病药物可能是治疗图雷特氏症的一种治疗选择。虽然副作用限制了尼古丁的长期使用,但按需使用可能有用。有必要进行进一步的临床研究,以调查使用安全性优于尼古丁的新型烟碱受体调节剂。
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