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齐拉西酮对糖尿病合并慢性精神分裂症患者代谢指标的影响。

Ziprasidone's effect on metabolic markers in patients with diabetes and chronic schizophrenia.

作者信息

Lindenmayer Jean Pierre, Tedeschi Frank, Yusim Anna, Khan Anzalee, Kaushik Saurabh, Smith Robert C, Parakadavil Mohan

机构信息

Department of Psychiatry, New York University School of Medicine, New York, NY, USA.

出版信息

Clin Schizophr Relat Psychoses. 2012 Jan;5(4):185-92. doi: 10.3371/CSRP.5.4.2.

Abstract

BACKGROUND

Despite numerous studies of diabetes mellitus type II (DM-II) in schizophrenia and schizoaffective disorder, there have been no studies on the glycemic effects of switching patients with long-standing symptomatic DM-II from their current antipsychotic regimen to ziprasidone.

METHODS

An open-label, prospective inpatient study was conducted with 26 suboptimally responding inpatients with DSM-IV diagnoses of schizophrenia or schizoaffective disorder and comorbid DM-II who were switched to ziprasidone monotherapy and followed for 8 weeks. Outcome measures were fasting glucose, triglycerides, cholesterol, insulin levels, capillary blood glucose levels and weight. After a 3-week cross-titration period, patients were treated with ziprasidone up to a dose of 320 mg daily.

RESULTS

Of the 26 study participants, 16 completed the entire study period of 63 days and 10 (38.46%) discontinued participation, primarily due to psychotic relapse. There was a statistically significant reduction in fasting glucose (F=4.43, p=0.05; 14.68 mg/dL mean reduction), capillary blood glucose levels (F=8.90, p=0.01; 25.36 mg/dL mean reduction), weight (F=4.46, p=0.05; 4.68 lb mean weight loss) and Body Mass Index (F=4.40, p=0.05; 3.62 kg/m(2) mean reduction). There was also a reduction in the use of antidiabetic medications after the switch to ziprasidone. Nine (34.62%) patients met criteria for metabolic syndrome (MetS) at baseline, as compared to 4 (15.38%) at endpoint. No change was observed in positive symptoms (F=0.62, p=0.44), negative symptoms (F=1.47, p=0.24) and in total PANSS score (F=0.12, p=0.74).

CONCLUSIONS

This study suggests significant improvement in metabolic side effects and MetS in the subset of the patients who were able to tolerate switching from a polypharmacy regimen to ziprasidone. There was a large discontinuation rate, which limited the sustained beneficial effects of ziprasidone. The decision to switch to ziprasidone in patients with prior suboptimal response has to balance the potential metabolic benefits and the potential relapse risks of the individual patient first and foremost.

摘要

背景

尽管对精神分裂症和分裂情感性障碍中的II型糖尿病(DM-II)进行了大量研究,但尚未有关于将长期有症状的DM-II患者从当前抗精神病药物治疗方案转换为齐拉西酮治疗后血糖影响的研究。

方法

对26例疗效欠佳的住院患者进行了一项开放标签的前瞻性住院研究,这些患者符合DSM-IV诊断标准,患有精神分裂症或分裂情感性障碍且合并DM-II,他们被转换为齐拉西酮单药治疗并随访8周。观察指标包括空腹血糖、甘油三酯、胆固醇、胰岛素水平、毛细血管血糖水平和体重。经过3周的交叉滴定期后,患者接受齐拉西酮治疗,剂量最高可达每日320毫克。

结果

26名研究参与者中,16人完成了为期63天的整个研究期,10人(38.46%)停止参与,主要原因是精神病性复发。空腹血糖(F = 4.43,p = 0.05;平均降低14.68毫克/分升)、毛细血管血糖水平(F = 8.90,p = 0.01;平均降低25.36毫克/分升)、体重(F = 4.46,p = 0.05;平均减重4.68磅)和体重指数(F = 4.40,p = 0.05;平均降低3.62千克/平方米)有统计学意义的降低。转换为齐拉西酮治疗后,抗糖尿病药物的使用也有所减少。9名(34.62%)患者在基线时符合代谢综合征(MetS)标准,而在终点时为4名(15.38%)。阳性症状(F = 0.62,p = 0.44)、阴性症状(F = 1.47,p = 0.24)和PANSS总分(F = 0.12,p = 0.74)均未观察到变化。

结论

本研究表明,对于能够耐受从联合用药方案转换为齐拉西酮治疗的患者亚组,代谢副作用和MetS有显著改善。停药率较高,这限制了齐拉西酮的持续有益效果。对于先前疗效欠佳的患者,决定转换为齐拉西酮治疗时,首先必须权衡个体患者潜在的代谢益处和潜在的复发风险。

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