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精神病临床高危人群中的抗精神病药物暴露:来自一项大型队列研究的实证见解

Antipsychotic Exposure in Clinical High Risk of Psychosis: Empirical Insights From a Large Cohort Study.

作者信息

Zeng JiaHui, Raballo Andrea, Gan RanPiao, Wu GuiSen, Wei YanYan, Xu LiHua, Tang XiaoChen, Hu YeGang, Tang YingYing, Chen Tao, Li ChunBo, Wang JiJun, Zhang TianHong

机构信息

Shanghai Mental Health Center, Shanghai Jiaotong University School of Medicine, Shanghai Intelligent Psychological Evaluation and Engineering Technology Research Center (20DZ2253800), Shanghai Key Laboratory of Psychotic Disorders, Shanghai, PR China.

Department of Medicine, Section of Psychiatry, Clinical Psychology and Rehabilitation, University of Perugia, Perugia, Italy.

出版信息

J Clin Psychiatry. 2022 Mar 21;83(3):21m14092. doi: 10.4088/JCP.21m14092.

Abstract

Current treatment guidelines for individuals at clinical high risk (CHR) for psychosis do not recommend the prescription of antipsychotics (not even second-generation ones) as the first treatment option for preventing psychosis. Yet, recent meta-analytic evidence indicates that antipsychotic exposure in CHR is relatively widespread and associated with a higher imminent risk of transition to psychosis. Therefore, we undertook this study to better delineate which clinical characteristics of CHR individuals may lead to the choice of antipsychotic prescription and whether it identifies a subgroup at higher risk for conversion to psychosis. Consecutively referred CHR individuals (N = 717) were assessed for demographic and clinical characteristics and followed up for 3 years (200 did not reach the end of the follow-up time) from 2016 to 2021. The sample was then dichotomized, on the basis of antipsychotic prescription, to prescribed (CHRAP+, n = 492) or not-prescribed (CHRAP-, n = 225) groups, which were subsequently compared for sociodemographic and clinical characteristics. The risks of conversion to psychosis in CHRAP+ versus CHRAP- groups were tested via survival analysis. Of the 717 CHR individuals, 492 (68.62%) were prescribed antipsychotics; among these antipsychotics, the highest proportion used was for aripiprazole (n = 152), followed by olanzapine (n = 106), amisulpride (n = 76), and risperidone (n = 64). The CHRAP+ group had younger age ( = 2.138,  = .033), higher proportion of female individuals ( = 5.084,  = .024), psychotic symptoms of greater severity ( = 7.910,  < .001), and more impaired general function ( = 5.846,  < .001) than the CHRAP- group. The CHRAP+ group had greater risk for conversion to psychosis (27.0% in the CHRAP+ group vs 10.9% in the CHRAP- group,  < .001). Factors related to positive symptoms were the most likely to influence doctors' decision-making regarding prescripton of antipsychotics, without influence of age, sex, and education levels. Clinicians may prescribe antipsychotics mainly based on the severity of positive and disorganization symptoms of CHR individuals. The CHRAP+ group was associated with a higher risk of conversion to psychosis. In pragmatic terms, this finding indicates that baseline antipsychotic prescription in CHR cohorts is a warning flag for higher incipient risk of psychosis and designates as hyper-CHR subgroup as compared to antipsychotic-naive CHR. ClinicalTrials.gov identifier: NCT04010864.

摘要

目前针对临床高危(CHR)精神病患者的治疗指南不建议将抗精神病药物(甚至不包括第二代抗精神病药物)作为预防精神病的首选治疗方案。然而,最近的荟萃分析证据表明,CHR患者中抗精神病药物的使用较为普遍,且与向精神病转变的更高近期风险相关。因此,我们开展了这项研究,以更好地描述CHR个体的哪些临床特征可能导致抗精神病药物处方的选择,以及这是否能识别出转化为精神病风险更高的亚组。对连续转诊的CHR个体(N = 717)进行人口统计学和临床特征评估,并在2016年至2021年期间进行了3年的随访(200人未达到随访结束时间)。然后根据抗精神病药物处方情况将样本分为用药组(CHRAP +,n = 492)和未用药组(CHRAP -,n = 225),随后比较两组的社会人口统计学和临床特征。通过生存分析测试CHRAP +组与CHRAP -组转化为精神病的风险。在717名CHR个体中,492人(68.62%)被开具了抗精神病药物;在这些抗精神病药物中,使用比例最高的是阿立哌唑(n = 152),其次是奥氮平(n = 106)、氨磺必利(n = 76)和利培酮(n = 64)。CHRAP +组的年龄更小(= 2.138,= 0.033),女性个体比例更高(= 5.084,= 0.024),精神病症状更严重(= 7.910,< 0.001),总体功能受损更严重(= 5.846,< 0.001)。CHRAP +组转化为精神病的风险更高(CHRAP +组为27.0%,CHRAP -组为10.9%,< 0.001)。与阳性症状相关的因素最有可能影响医生关于抗精神病药物处方的决策,不受年龄、性别和教育水平的影响。临床医生可能主要根据CHR个体阳性和紊乱症状的严重程度开具抗精神病药物。CHRAP +组转化为精神病的风险更高。实际上,这一发现表明CHR队列中的基线抗精神病药物处方是精神病初始风险较高的一个警示信号,与未使用过抗精神病药物的CHR相比,可将其指定为高CHR亚组。ClinicalTrials.gov标识符:NCT04010864。

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