维洛嗪与阿米替林的临床特征和血清浓度比较。

B Müller-Oerlinghausen, E Rüther
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引用次数: 23

摘要

采用对照双盲设计,对41例需要阿米替林(150 mg/d)药物治疗的抑郁综合征患者进行了为期3周的维洛嗪(300 mg/d)抗抑郁效果研究。维洛嗪与阿米替林的不同之处在于选择性抑制去甲肾上腺素的再摄取,而阿米替林也对血清素的再摄取起作用。通过汉密尔顿抑郁评定量表、Bf-S (v. Zerssen)、amdp系统和录像记录精神病理变化。除常规临床化学检查外,测定了维洛嗪和部分阿米替林的血药浓度。重复的脑电图记录通过频谱分析进行评估。根据最终hdrs评分定义的全球反应者和无反应者的数量在两个药物组之间均匀分布。amdp评估表明,维洛沙辛对发育迟缓的症状有更显著和更迅速的作用,而阿米替林主要作用于抑郁情绪、睡眠障碍和重要感觉。两种药物的脑电图谱变化与三环类抗抑郁药相似,但只有维洛嗪引起的变化在第10天和第20天达到统计学意义,阿米替林组脑电图记录的变异性更大。维洛嗪血药浓度在个体间和个体内的差异都很低。最迟在第5天达到稳态。第10 ~ 21天阿米替林血药浓度继续升高。有反应组的维洛嗪平均血药浓度高于无反应组。
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Clinical profile and serum concentration of viloxazine as compared to amitriptyline.

The antidepressive effect of viloxazine (300 mg/d) was investigated during three weeks in 41 patients with depressive syndromes requiring drug-treatment against amitriptyline (150 mg/d), using a controlled double-blind design. Viloxazine differs from amitriptyline by selective inhibition of norepinephrine re-uptake, whereas amitriptyline acts also on serotonin re-uptake. Psychopathological changes were documented by means of the Hamilton Depression Rating Scale, the Bf-S (v. Zerssen), the AMDP-System, and videotaped recordings. Besides routine clinical-chemical tests, the serum concentrations of viloxazine and partly of amitriptyline were determined. Repeated EEG-recordings were evaluated by spectral analysis. The number of global responders and non-responders -- defined according to the final HDRS-scores -- was equally distributed between the two drug-groups. The AMDP-evaluation suggests that viloxazin has a somewhat more marked and more rapid effect on symptoms of retardation, whereas amitriptyline acts predominantly on depressive mood, disturbances of sleep and vital feelings. The EEG-profile of both drugs was similar to the spectral changes seen under tricyclic antidepressants, through only the viloxazine-induced changes reached statistical significance on the 10th and 20th day, the variability of the EEG-recordings being greater in the amitriptyline group. The viloxazine blood levels showed a remarkably low inter- and intraindividual variance. Steady state was reached at day 5 at the latest. Amitriptyline serum concentrations still increased between the 10th and the 21st day. The average blood concentration of viloxazine was higher in the responder- than in the non-responder-group.

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