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临床高危精神病性青年人群中抗精神病药物的基线暴露情况:一项为期2年的意大利随访研究

Baseline Exposure to Antipsychotic Medication in Young People at Clinical High Risk for Psychosis: A 2-Year Italian Follow-Up Study.

作者信息

Pelizza Lorenzo, Di Lisi Alessandro, Leuci Emanuela, Quattrone Emanuela, Palmisano Derna, Pupo Simona, Pellegrini Pietro, Menchetti Marco

机构信息

Department of Biomedical and Neuromotor Sciences, Alma Mater Studiorum - Università di Bologna, Bologna, Italy.

Department of Mental Health and Pathological Addiction, Azienda USL di Parma, Parma, Italy.

出版信息

Hum Psychopharmacol. 2025 Mar;40(2):e70003. doi: 10.1002/hup.70003.

Abstract

OBJECTIVE

Despite various models examining baseline factors, predicting outcomes in individuals at clinical high risk for psychosis (CHR-P) remains challenging. Specifically, neglecting factors like ongoing antipsychotic (AP) medications introduce bias and reduce method precision. The main aim of this research was to determine if the presence of AP prescription at baseline identifies a CHR-P subgroup with worse prognostic outcomes over a 2-year period.

METHODS

A group of 180 FEP individuals (92 CHR-P/AP+, 88 CHR-P/AP-) were evaluated at baseline and after 24 months using the PANSS and GAF scales. Individuals with baseline AP prescription were included in the CHR-P/AP+ subgroup; those not taking APs were grouped as CHR-P/AP-. Univariate Cox regression analysis and mixed-design ANOVA were performed.

RESULTS

After 2 years, CHR-P/AP+ had a higher rate of new hospitalization but lower rate of service disengagement. No significant inter-group difference in psychosis transition rate was found. A "time-×-group" interaction effect on longitudinal improvement in PANSS total score was observed in CHR-P/AP+ subjects.

CONCLUSIONS

It is advisable to conduct a more extensive outcome evaluation beyond the psychometric criteria for CHR-P and the mere consideration of psychosis transition. Such an approach would facilitate the identification of specific CHR-P subgroups with divergent prognoses and different AP response.

摘要

目的

尽管有各种模型研究基线因素,但预测临床高危精神病个体(CHR-P)的预后仍然具有挑战性。具体而言,忽视正在使用抗精神病药物(AP)等因素会引入偏差并降低方法的精确性。本研究的主要目的是确定基线时是否存在AP处方能识别出在2年期间预后较差的CHR-P亚组。

方法

一组180名首次发作精神病(FEP)个体(92名CHR-P/AP+,88名CHR-P/AP-)在基线和24个月后使用阳性和阴性症状量表(PANSS)及大体功能评定量表(GAF)进行评估。基线时使用AP处方的个体被纳入CHR-P/AP+亚组;未服用AP的个体被归为CHR-P/AP-组。进行单变量Cox回归分析和混合设计方差分析。

结果

2年后,CHR-P/AP+组有更高的新住院率,但服务脱离率较低。未发现组间精神病转化率有显著差异。在CHR-P/AP+受试者中观察到“时间×组”对PANSS总分纵向改善的交互作用。

结论

除了CHR-P的心理测量标准和仅考虑精神病转化之外,进行更广泛的预后评估是可取的。这种方法将有助于识别具有不同预后和不同AP反应的特定CHR-P亚组。

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