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基线抗精神病药物暴露对精神病临床高风险(CHR-P)的负面预后影响:是事前风险富集的“隐形”罪魁祸首吗?

Negative Prognostic Effect of Baseline Antipsychotic Exposure in Clinical High Risk for Psychosis (CHR-P): Is Pre-Test Risk Enrichment the Hidden Culprit?

机构信息

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

Center for Translational, Phenomenological and Developmental Psychopathology (CTPDP), Perugia University Hospital, Perugia, Italy.

出版信息

Int J Neuropsychopharmacol. 2021 Sep 21;24(9):710-720. doi: 10.1093/ijnp/pyab030.

DOI:10.1093/ijnp/pyab030
PMID:34036323
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8453273/
Abstract

INTRODUCTION

Sample enrichment is a key factor in contemporary early-detection strategies aimed at the identification of help-seekers at increased risk of imminent transition to psychosis. We undertook a meta-analytic investigation to ascertain the role of sample enrichment in the recently highlighted negative prognostic effect of baseline antipsychotic (AP) exposure in clinical high-risk (CHR-P) of psychosis individuals.

METHODS

Systematic review and meta-analysis of all published studies on CHR-P were identified according to a validated diagnostic procedure. The outcome was the proportion of transition to psychosis, which was calculated according to the Freeman-Tukey double arcsine transformation.

RESULTS

Thirty-three eligible studies were identified, including 16 samples with details on AP exposure at baseline and 17 samples with baseline AP exposure as exclusion criterion for enrollment. Those with baseline exposure to AP (n = 395) had higher transition rates (29.9%; 95% CI: 25.1%-34.8%) than those without baseline exposure to AP in the same study (n = 1289; 17.2%; 15.1%-19.4%) and those coming from samples that did not include people who were exposed to AP at baseline (n = 2073; 16.2%; 14.6%-17.8%; P < .05 in both the fixed-effects and the random-effects models). Heterogeneity within studies was substantial, with values above 75% in all comparisons.

CONCLUSIONS

Sample enrichment is not a plausible explanation for the higher risk of transition to psychosis of CHR-P individuals who were already exposed to AP at the enrollment in specialized early-detection programs. Baseline exposure to AP at CHR-P assessment is a major index of enhanced, imminent risk of psychosis.

摘要

简介

样本富集是当代早期检测策略的关键因素,旨在识别有即将向精神病转化风险的寻求帮助者。我们进行了一项荟萃分析,以确定样本富集在最近强调的基线抗精神病药物(AP)暴露对精神病临床高风险(CHR-P)个体的负面预后影响中的作用。

方法

根据经过验证的诊断程序,对所有关于 CHR-P 的已发表研究进行系统回顾和荟萃分析。结果是精神病转化的比例,根据 Freeman-Tukey 双反正弦变换计算。

结果

确定了 33 项符合条件的研究,其中 16 项样本有基线时 AP 暴露的详细信息,17 项样本将基线 AP 暴露作为入组的排除标准。那些基线时暴露于 AP(n=395)的人比在同一研究中没有基线时暴露于 AP 的人(n=1289)和那些来自基线时没有暴露于 AP 的样本的人(n=2073)的转化率更高(29.9%;95%CI:25.1%-34.8%),(17.2%;15.1%-19.4%)和(16.2%;14.6%-17.8%;在固定效应和随机效应模型中 P<0.05)。研究内的异质性很大,所有比较的数值均高于 75%。

结论

在专门的早期检测计划中入组时已经暴露于 AP 的 CHR-P 个体向精神病转化的风险增加,样本富集不是其风险增加的合理解释。CHR-P 评估时的基线 AP 暴露是精神病即将发生的高风险的主要指标。

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