Research Unit, Tirat Carmel Mental Health Center, POB 9, Tirat Carmel 30200, Israel.
Psychopharmacology (Berl). 2013 Apr;226(3):615-22. doi: 10.1007/s00213-012-2935-2. Epub 2012 Dec 13.
Combination treatment with reboxetine, a selective norepinephrine reuptake inhibitor, and betahistine, a histamine H1 receptor agonist/H3 antagonist, was developed to produce complementary action in CNS pathways regulating appetite and body weight. In the present placebo-controlled study, we evaluated whether a reboxetine-betahistine combination attenuates olanzapine-induced weight gain in schizophrenia patients.
Forty-three inpatients with DSM-IV schizophrenic disorder participated in a randomized double-blind study. Reboxetine (4 mg/day) with betahistine (48 mg/day) (N = 29) or placebo (N = 14) was co-administered with olanzapine (10 mg/day) for 6 weeks. Mental status was assessed at baseline and endpoint with relevant rating scales. Intention-to-treat method was used for statistical analysis.
Seven patients in the study group and four in the placebo group discontinued the trial. At the end of the trial, patients in the olanzapine/reboxetine + betahistine group gained significantly less weight than those in the olanzapine/placebo group [2.02 ± 2.37 and 4.77 ± 3.16 kg, respectively; t = 2. 89, degrees of freedom (df) = 41, p = 0.006]. The weight-attenuating effect of this combination was twofold larger than the weight-attenuating effect previously demonstrated with reboxetine alone. Significantly fewer patients in the study group than in the comparison group increased their initial weight by >7 %, the cutoff for clinically significant weight gain [3/29 (10.3 %) and 6/14 (42.9 %), respectively; χ (2) = 6.03, df = 1, p = 0.014]. The reboxetine-betahistine combination was safe and well tolerated.
Reboxetine-betahistine combination produces a clinically meaningful attenuation of olanzapine-induced weight gain. These results justify direct comparison between the reboxetine-betahistine combination and reboxetine alone.
使用选择性去甲肾上腺素再摄取抑制剂瑞波西汀和组胺 H1 受体激动剂/ H3 拮抗剂倍他司汀的联合治疗旨在产生对调节食欲和体重的中枢神经系统途径的互补作用。在本安慰剂对照研究中,我们评估了瑞波西汀-倍他司汀联合治疗是否可减轻精神分裂症患者奥氮平引起的体重增加。
43 例 DSM-IV 精神分裂症住院患者参与了这项随机双盲研究。瑞波西汀(4mg/天)联合倍他司汀(48mg/天)(N=29)或安慰剂(N=14)与奥氮平(10mg/天)联合治疗 6 周。在基线和终点使用相关评定量表评估精神状态。采用意向治疗方法进行统计分析。
研究组中有 7 例患者和安慰剂组中有 4 例患者退出试验。试验结束时,奥氮平/瑞波西汀+倍他司汀组的患者体重增加明显少于奥氮平/安慰剂组[分别为 2.02±2.37kg 和 4.77±3.16kg;t=2.89,自由度(df)=41,p=0.006]。该联合治疗的减重效果是瑞波西汀单独治疗的两倍。与安慰剂组相比,研究组中体重增加超过 7%(临床显著体重增加的截止值)的患者明显更少[分别为 3/29(10.3%)和 6/14(42.9%);χ2(2)=6.03,df=1,p=0.014]。瑞波西汀-倍他司汀联合治疗安全且耐受良好。
瑞波西汀-倍他司汀联合治疗可显著减轻奥氮平引起的体重增加。这些结果证明了瑞波西汀-倍他司汀联合治疗与瑞波西汀单独治疗之间直接比较的合理性。
