Department of Theoretical and Clinical Pharmacology, Kaunas University of Medicine, A. Mickeviciaus 9, 44307 Kaunas, Lithuania.
Medicina (Kaunas). 2009;45(10):778-84.
Mirtazapine is an established antidepressant with well-documented efficacy demonstrated in controlled clinical trials. However, the gap between the results obtained in controlled clinical trials and everyday clinical practice exists. Therefore, the importance of naturalistic studies in psychiatry is becoming recognized. The aim of present naturalistic study was to acquire data on efficacy, safety, and preference of mirtazapine orally disintegrating tablets during a 17-week treatment of depression. This prospective, open-label, multicenter study in patients with mild to severe depression was conducted at 47 mental health centers of Lithuania by 78 psychiatrists. Patients were initially given 15 mg or 30 mg of mirtazapine orally disintegrating tablets; the maximum allowed dose was 45 mg per day. The primary efficacy measure was the total score on the Hamilton Depression Rating Scale-17 (HAMD-17), the Clinical Global Impression-Severity (CGI-S), and Clinical Global Impression-Improvement (CGI-I) scales. Tolerability was primarily measured by assessing the incidence of treatment-emergent adverse events. Patients were evaluated at baseline, at weeks 1, 5, 9, 13, and 17. A total of 779 patients (595 women [76.4%] with a mean [SD] age of 50.2 [13.65] and 184 men [23.6%] with a mean [SD] age of 52.4 [14.6] years) were enrolled into the study; 687 (88.2%) patients completed the study. The mean (SD) daily dose of mirtazapine orally disintegrating tablets was 29.0 (3.8) mg. The mean total (SD) HAMD-17 score improved significantly from 25.7 (4.6) to 7.3 (4.3) (P<0.005). At each visit, the mean HAMD-17 score was significantly lower than that at the preceding visit. At week 17, remission (HAMD-17 score < or =7) was observed in 436 (56%) patients. The mean (SD) CGI-S score improved significantly from 4.9 (1.0) at baseline to 1.5 (0.6) at endpoint (P<0.001). According to the CGI-I assessments, 621 patients (89.4%) improved and improved very much. The vast majority of patients (80%) preferred the new formulation of mirtazapine - mirtazapine orally disintegrating tablet. Treatment-emergent adverse events occurred in 106 patients (13.6%). The most frequent adverse events were weight gain, sedation, dizziness, and dry mouth. In this study conducted in Lithuania with depressed patients, a significant improvement was shown in all efficacy measures. In addition, mirtazapine orally disintegrating tablet was a well-tolerated and preferable formulation for the treatment of depressed patients.
米氮平是一种已被证实的抗抑郁药,在对照临床试验中具有良好的疗效。然而,对照临床试验和日常临床实践之间存在差距。因此,精神病学中的自然主义研究的重要性正在得到认可。本自然研究的目的是在 17 周的抑郁症治疗期间获得米氮平口腔崩解片的疗效、安全性和偏好数据。这项前瞻性、开放性、多中心研究在立陶宛的 47 家心理健康中心由 78 名精神科医生进行,纳入了轻度至重度抑郁症患者。患者最初给予米氮平口腔崩解片 15 毫克或 30 毫克;每天最大允许剂量为 45 毫克。主要疗效测量指标是汉密尔顿抑郁量表-17(HAMD-17)总分、临床总体印象严重程度(CGI-S)和临床总体印象改善(CGI-I)量表。耐受性主要通过评估治疗中出现的不良事件发生率来衡量。患者在基线、第 1、5、9、13 和 17 周进行评估。共有 779 名患者(595 名女性[76.4%],平均[SD]年龄为 50.2[13.65],184 名男性[23.6%],平均[SD]年龄为 52.4[14.6]岁)入组研究;687 名(88.2%)患者完成了研究。米氮平口腔崩解片的平均(SD)日剂量为 29.0(3.8)毫克。HAMD-17 总分显著从 25.7(4.6)改善至 7.3(4.3)(P<0.005)。在每次就诊时,HAMD-17 评分均显著低于前一次就诊。第 17 周时,436 名(56%)患者达到缓解(HAMD-17 评分≤7)。CGI-S 评分显著从基线时的 4.9(1.0)改善至终点时的 1.5(0.6)(P<0.001)。根据 CGI-I 评估,621 名患者(89.4%)有改善且改善很大。绝大多数患者(80%)更喜欢米氮平的新剂型-米氮平口腔崩解片。106 名患者(13.6%)发生治疗中出现的不良事件。最常见的不良事件是体重增加、镇静、头晕和口干。在立陶宛进行的这项针对抑郁症患者的研究显示,所有疗效指标均有显著改善。此外,米氮平口腔崩解片是治疗抑郁症患者耐受性良好且优选的剂型。
Zotero 插件