Michael Tocco, John W Newcomer, Yongcai Mao, Andrei Pikalov
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引用次数: 0
摘要
目的:抑郁症患者代谢综合征(MetS)发病率升高与死亡率升高有关。这项事后分析评估了鲁拉西酮治疗对双相抑郁症患者代谢综合征风险的影响:本次分析使用的数据包括3项双盲(DB)、安慰剂对照、为期6周的研究,研究对象为双相抑郁症成人患者(N = 1192),其中包括1项单药治疗和2项辅助试验(锂或丙戊酸钠)。此外,还分析了一项为期 6 个月的开放标签(OL)扩展研究(单一疗法,316 人;辅助疗法,497 人);以及一项为期 5 个月的 OL 稳定期研究,随后随机进行一项为期 28 周的鲁拉西酮(DB)安慰剂对照辅助疗法研究(490 人)。MetS 的定义基于 NCEP ATP III 标准(2005 年修订版):在短期研究中,鲁拉西酮与安慰剂的新发MetS患者比例相似(单一疗法,13.9% vs 15.3%;辅助疗法,13.6% vs 11.0%);在为期6个月的延长期研究(单一疗法,15.2%;辅助疗法,16.9%)和为期5个月的稳定期研究(辅助疗法,12.2%)中,新发MetS患者比例保持稳定。经过28周的DB治疗后(稳定期研究中的5个月治疗后),在终点(OC)观察到新发MetS,鲁拉西酮组为26.2%,安慰剂组为30.8%:这项事后分析发现,鲁拉西酮的短期和长期治疗与双相情感障碍I患者相对较低的MetS发病风险有关。这些结果与精神分裂症患者的类似分析结果一致。
Lurasidone and risk of metabolic syndrome: results from short and long-term studies in patients with bipolar depression.
Objective: The elevated prevalence of metabolic syndrome (MetS) in patients with depression has been associated with increased mortality. This post hoc analysis assessed the effect of treatment with lurasidone on risk of MetS in patients with bipolar depression.
Methods: Data used in the current analyses consisted of 3 double-blind (DB), placebo-controlled, 6-week studies in adults with bipolar I depression (N = 1192), consisting of 1 monotherapy, and 2 adjunctive trials (lithium or valproate). Also analyzed was a 6-month open-label (OL) extension study (monotherapy, N = 316; adjunctive therapy, N = 497); and a 5-month, OL, stabilization phase followed by randomization to a 28-week DB, placebo-controlled, adjunctive therapy study with lurasidone (N = 490). MetS was defined based on NCEP ATP III criteria (2005 revision).
Results: The proportion of patients with new-onset MetS was similar for lurasidone vs placebo in the short-term studies (monotherapy, 13.9% vs 15.3%; adjunctive therapy, 13.6% vs 11.0%); and remained stable during both the 6-month extension phase study (monotherapy, 15.2%; adjunctive therapy, 16.9%), and the 5-month stabilization study (adjunctive therapy, 12.2%). After 28 weeks of DB treatment (following 5-month treatment in the stabilization study), new onset MetS was observed at endpoint (OC) in 26.2% of the lurasidone group, and 30.8% of the placebo group.
Conclusions: This post hoc analysis found that both short and long-term treatment with lurasidone was associated with a relatively low risk for the development of MetS in patients with bipolar I disorder. These findings are consistent with similar analyses in patients with schizophrenia.
期刊介绍:
CNS Spectrums covers all aspects of the clinical neurosciences, neurotherapeutics, and neuropsychopharmacology, particularly those pertinent to the clinician and clinical investigator. The journal features focused, in-depth reviews, perspectives, and original research articles. New therapeutics of all types in psychiatry, mental health, and neurology are emphasized, especially first in man studies, proof of concept studies, and translational basic neuroscience studies. Subject coverage spans the full spectrum of neuropsychiatry, focusing on those crossing traditional boundaries between neurology and psychiatry.