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首页> 外文期刊>Brain research >Association of the adrenergic alpha 2a receptor-1291C/G polymorphism with weight change and treatment response to mirtazapine in patients with major depressive disorder.
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Association of the adrenergic alpha 2a receptor-1291C/G polymorphism with weight change and treatment response to mirtazapine in patients with major depressive disorder.

机译:抑郁症患者肾上腺素α2a受体-1291C / G多态性与体重变化和对米氮平的治疗反应相关。

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BACKGROUND: Adrenergic alpha2a receptors (ADRA2A) are expressed in the central nervous system and peripheral tissues. The primary mechanism of action of mirtazapine is the antagonism of central presynaptic alpha2 receptors. Mirtazapine is reportedly associated with weight gain. Our objective was to determine whether the ADRA2A -1291C/G polymorphism is associated with weight gain and treatment response to mirtazapine in patients with major depressive disorder (MDD). METHODS: The ADRA2A -1291C/G polymorphism was analyzed in 314 MDD patients and 162 control subjects. All patients were evaluated using the 21-item Hamilton Depression Rating Scale at the beginning of the study and at 1, 2, 4, and 8 weeks of mirtazapine treatment. RESULTS: No relationship was observed between the ADRA2A -1291C/G polymorphism and MDD. No significant difference was found between responder and non-responder groups when comparing the ADRA2A genotype distribution with treatment response to mirtazapine. Repeated measures ANOVA withthe last observation carry-forward test indicated that after adjusting for baseline body weight, age, and gender, the subjects with the C/C genotype exhibited a greater mean body weight gain than the subjects with the C/G or G/G genotype after 8 weeks of mirtazapine treatment (p=0.052). CONCLUSIONS: The ADRA2A -1291C/G polymorphism does not appear to be a predictor of treatment response to mirtazapine. This polymorphism was weakly associated with weight change after 8 weeks of mirtazapine treatment. Further investigation is required to determine whether other polymorphisms of this gene influence treatment response and weight change in patients receiving mirtazapine.
机译:背景:肾上腺素α2a受体(ADRA2A)在中枢神经系统和周围组织中表达。米氮平的主要作用机制是中枢突触前α2受体的拮抗作用。据报道,米氮平与体重增加有关。我们的目的是确定ADRA2A -1291C / G基因多态性是否与体重增加以及对重度抑郁症(MDD)患者对米氮平的治疗反应有关。方法:分析了314名MDD患者和162名对照受试者的ADRA2A -1291C / G多态性。在研究开始以及米氮平治疗的第1、2、4和8周时,使用21项汉密尔顿抑郁量表对所有患者进行评估。结果:ADRA2A -1291C / G多态性与MDD之间没有相关性。将ADRA2A基因型分布与对米氮平的治疗反应进行比较时,反应者和非反应者组之间没有发现显着差异。重复测量方差分析与最后一次观察结转测试表明,在校正基线体重,年龄和性别后,具有C / C基因型的受试者表现出的平均体重增加量大于具有C / G或G /米氮平治疗8周后的G基因型(p = 0.052)。结论:ADRA2A -1291C / G多态性似乎不是米氮平治疗反应的预测指标。米氮平治疗8周后,这种多态性与体重变化微弱相关。需要进一步的研究以确定该基因的其他多态性是否影响接受米氮平的患者的治疗反应和体重变化。

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