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米氮平可急性抑制抑郁症患者唾液中的皮质醇浓度。

Mirtazapine acutely inhibits salivary cortisol concentrations in depressed patients.

作者信息

Laakmann Gregor, Hennig Jürgen, Baghai Thomas, Schüle Cornelius

机构信息

Department of Psychiatry, University of Munich, Nussbaumstr. 7, 80336 Munich, Germany.

出版信息

Ann N Y Acad Sci. 2004 Dec;1032:279-82. doi: 10.1196/annals.1314.038.

Abstract

Mirtazapine has been shown to acutely inhibit cortisol secretion in healthy subjects. In the current study, the impact of mirtazapine treatment on salivary cortisol secretion was investigated in 12 patients with major depression (DSM-IV criteria). Patients were treated with mirtazapine for 3 weeks, receiving 15 mg of mirtazapine on day 0, 30 mg on day 1, and 45 mg per day from day 2 to the end of the study (day 21). Response to mirtazapine treatment was defined by a reduction of at least 50% in the Hamilton Rating Scale for Depression after 3 weeks of therapy. Salivary cortisol concentrations were measured before treatment (day -1), at the beginning of treatment (day 0), after 1 week (day 7), and after 3 weeks (day 21) of treatment with mirtazapine. Saliva samples were collected hourly from 8 am to 8 pm. A significant reduction in cortisol concentrations was already noted after 1 day of mirtazapine treatment which was comparable in responders and in nonresponders. Mirtazapine therefore appears to be an effective in decreasing hypercortisolism in depression. However, the importance of the acute inhibitory effects of mirtazapine on cortisol secretion for its antidepressant efficacy has to be further clarified.

摘要

米氮平已被证明可在健康受试者中急性抑制皮质醇分泌。在本研究中,对12例重度抑郁症患者(符合DSM-IV标准)进行了米氮平治疗对唾液皮质醇分泌影响的研究。患者接受米氮平治疗3周,第0天服用15mg米氮平,第1天服用30mg,从第2天至研究结束(第21天)每天服用45mg。米氮平治疗反应的定义为治疗3周后汉密尔顿抑郁量表评分至少降低50%。在米氮平治疗前(第-1天)、治疗开始时(第0天)、治疗1周后(第7天)和治疗3周后(第21天)测量唾液皮质醇浓度。从上午8点到晚上8点每小时收集一次唾液样本。米氮平治疗1天后皮质醇浓度即出现显著降低,反应者和无反应者的情况相当。因此,米氮平似乎对降低抑郁症患者的皮质醇增多症有效。然而,米氮平对皮质醇分泌的急性抑制作用对其抗抑郁疗效的重要性还有待进一步阐明。

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