Department of Psychiatry, Kyungpook National University School of Medicine, Daegu, Korea.
Clin Drug Investig. 2012 Nov;32(11):735-45. doi: 10.1007/s40261-012-0002-8.
It has been suggested that neither dose titration nor the use of a loading dose was required for amisulpride and that 800 mg/day could be given from the first day with a low risk of extrapyramidal symptoms (EPS). However, no direct study of the need for dose titration has been conducted.
This study aimed to compare the efficacy, tolerability and subjective experience of amisulpride between a group receiving an initial dose of 800 mg/day (AMI-800 group) and a group titrating up from an initial dose of 400 mg/day (AMI-400 group) over a period of 6 weeks.
A total of 68 patients with acute exacerbations of schizophrenia participated in this 6-week randomized, multicentre, open-label study of amisulpride. Thirty patients were randomly assigned to the group that received an initial dose of 400 mg/day, which was then titrated up during the first 4 weeks following a fixed schedule. Thirty-eight patients were randomly assigned to the group receiving an initial dose of amisulpride 800 mg/day, which they took until the end of the fourth week. During the fifth and sixth weeks, the doses were adjusted flexibly in both groups. Our primary outcome measures were the Clinical Global Impression (CGI) scale and the changes over time in the total and subscale scores of the Positive and Negative Syndrome Scale (PANSS).
We found no significant between-group differences in clinical improvement on the CGI and the PANSS. However, when responders were defined as those patients who experienced at least a 30 % reduction in the PANSS total scores obtained at baseline, a higher proportion of those in the AMI-800 group met the criterion for responsiveness from week 4 (week 4: 68.4 % vs 40.0 %, p = 0.02; week 6: 71.1 % vs 43.3 %, p = 0.02). Irrespective of treatment group, significant proportions of patients developed hyperprolactinaemia (86 %) and EPS (35 %). However, no statistically significant differences in the overall incidence of adverse events were observed between the two treatment groups. There were also no group differences in subjective quality of life and attitudes toward antipsychotic medication.
These results suggest that it may be useful to begin therapy, especially for acute exacerbations of schizophrenia, with an initial dose of amisulpride 800 mg/day to obtain maximal efficacy without any significant side effects.
有研究表明,氨磺必利既不需要滴定剂量,也不需要使用负荷剂量,起始剂量 800mg/d 即可,且发生锥体外系症状(EPS)的风险较低。但是,尚无关于是否需要滴定剂量的直接研究。
本研究旨在比较起始剂量 800mg/d(AMl-800 组)与起始剂量 400mg/d 滴定剂量(AMl-400 组)治疗 6 周后,氨磺必利的疗效、耐受性和主观体验。
共 68 例精神分裂症急性加重患者参与了这项为期 6 周的氨磺必利随机、多中心、开放标签研究。30 例患者被随机分配至起始剂量 400mg/d 的治疗组,随后根据固定方案在第 1 至 4 周进行滴定。38 例患者被随机分配至起始剂量 800mg/d 的治疗组,该剂量持续至第 4 周结束。在第 5 和第 6 周,两组的剂量均可灵活调整。主要结局指标为临床总体印象量表(CGI)和阳性与阴性症状量表(PANSS)总分和各分量表评分的时间变化。
我们发现两组在 CGI 和 PANSS 上的临床改善均无显著差异。但是,将 PANSS 总分较基线至少降低 30%的患者定义为应答者时,第 4 周时 AMl-800 组的应答率更高(第 4 周:68.4%比 40.0%,p=0.02;第 6 周:71.1%比 43.3%,p=0.02)。无论治疗组如何,均有相当比例的患者发生高催乳素血症(86%)和 EPS(35%)。但是,两组的不良反应总发生率无统计学差异。两组的主观生活质量和对抗精神病药物的态度也无组间差异。
这些结果表明,对于精神分裂症的急性加重,起始剂量 800mg/d 进行治疗可能有助于获得最大疗效而无明显副作用。
