早发性精神分裂症谱系障碍治疗中抗精神病药物相关体重增加的预测因素和调节因素研究
Predictors and Moderators of Antipsychotic-Related Weight Gain in the Treatment of Early-Onset Schizophrenia Spectrum Disorders Study.
作者信息
Taylor Jerome H, Jakubovski Ewgeni, Gabriel Daniel, Bloch Michael H
机构信息
1 Child Study Center, Yale University , New Haven, Connecticut.
2 Department of Psychiatry, Yale University , New Haven, Connecticut.
出版信息
J Child Adolesc Psychopharmacol. 2018 Sep;28(7):474-484. doi: 10.1089/cap.2017.0147. Epub 2018 Jun 19.
BACKGROUND
Antipsychotic-related weight gain is a common clinically relevant side effect when treating psychotic disorders in pediatric populations, yet few predictors and no moderators of antipsychotic-related weight gain are known.
METHODS
The Treatment of Early-Onset Schizophrenia Spectrum Disorders (TEOSS) study randomized 119 youths (age 8-19 years) with schizophrenia or schizoaffective disorder to 8 weeks of antipsychotic treatment with molindone, risperidone, or olanzapine and assessed treatment response and side effects. In this secondary analysis, we used multivariable linear regression and receiver operating characteristic analysis to investigate predictors and moderators of weight change and percent weight change from baseline to week 8.
RESULTS
Treatment assignment was the most discriminant predictor of weight change [F(2, 66) = 17.00, p < 0.001] and percent weight change [F(2, 66) = 16.85, p < 0.001]. Mean weight gain was 0.74 (standard deviation ±3.51) kg for molindone, 4.13 ± 3.79 kg for risperidone, and 7.29 ± 3.44 kg for olanzapine. After adjusting for treatment assignment, lower pretreatment hemoglobin A1C (HgbA1C) predicted more weight gain [F(1, 55) = 4.71, p = 0.03]. Diagnosis (schizoaffective vs. schizophrenia) moderated weight change [F(2, 63) = 6.02, p = 0.004] and percent weight change [F(2, 63) = 5.26, p = 0.008] such that schizoaffective diagnosis predicted larger weight gain for youths in the risperidone treatment arm. Age, sex, family income, baseline weight, and symptoms neither predicted nor moderated weight change or percent weight change.
CONCLUSION
We identified prognostic subgroups and novel risk factors for antipsychotic-related weight gain. We confirmed that antipsychotic choice is extremely important for predicting future weight gain. We also found that younger age did not predict greater weight gain, in contrast to prior studies. Our findings require replication in an independent sample because we did not adjust for multiple comparisons to minimize false negatives. ClinicalTrials.gov Identifier: NCT00053703.
背景
在儿科人群中治疗精神障碍时,抗精神病药物相关体重增加是一种常见的具有临床相关性的副作用,但已知的抗精神病药物相关体重增加的预测因素很少,且没有调节因素。
方法
早发性精神分裂症谱系障碍治疗(TEOSS)研究将119名患有精神分裂症或分裂情感性障碍的青少年(8 - 19岁)随机分为接受8周的吗茚酮、利培酮或奥氮平抗精神病药物治疗组,并评估治疗反应和副作用。在这项二次分析中,我们使用多变量线性回归和受试者工作特征分析来研究从基线到第8周体重变化和体重变化百分比的预测因素和调节因素。
结果
治疗分配是体重变化[F(2, 66) = 17.00, p < 0.001]和体重变化百分比[F(2, 66) = 16.85, p < 0.001]最具判别力的预测因素。吗茚酮组的平均体重增加为0.74(标准差±3.51)kg,利培酮组为4.13 ± 3.79 kg,奥氮平组为7.29 ± 3.44 kg。在调整治疗分配后,较低的治疗前糖化血红蛋白(HgbA1C)预测体重增加更多[F(1, 55) = 4.71, p = 0.03]。诊断(分裂情感性障碍与精神分裂症)调节体重变化[F(2, 63) = 6.02, p = 0.004]和体重变化百分比[F(2, 63) = 5.26, p = 0.008],使得分裂情感性障碍诊断预测利培酮治疗组青少年体重增加更大。年龄、性别、家庭收入、基线体重和症状既不能预测也不能调节体重变化或体重变化百分比。
结论
我们确定了抗精神病药物相关体重增加的预后亚组和新的风险因素。我们证实抗精神病药物的选择对于预测未来体重增加极其重要。我们还发现与先前研究相反,年龄较小并不能预测更大的体重增加。我们的研究结果需要在独立样本中进行重复验证,因为我们没有对多重比较进行调整以尽量减少假阴性。临床试验.gov标识符:NCT00053703。
Zotero 插件