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解码早期精神病:揭示跨独立队列与精神病理学相关的稳定微观结构特征。

Decoding Early Psychoses: Unraveling Stable Microstructural Features Associated with Psychopathology Across Independent Cohorts.

作者信息

Wang Haley R, Liu Zhen-Qi, Nakua Hajer, Hegarty Catherine E, Thies Melanie Blair, Patel Pooja K, Schleifer Charles H, Boeck Thomas P, McKinney Rachel A, Currin Danielle, Leathem Logan, DeRosse Pamela, Bearden Carrie E, Misic Bratislav, Karlsgodt Katherine H

出版信息

bioRxiv. 2024 May 12:2024.05.10.593636. doi: 10.1101/2024.05.10.593636.

Abstract

BACKGROUND

Early Psychosis patients (EP, within 3 years after psychosis onset) show significant variability, making outcome predictions challenging. Currently, little evidence exists for stable relationships between neural microstructural properties and symptom profiles across EP diagnoses, limiting the development of early interventions.

METHODS

A data-driven approach, Partial Least Squares (PLS) correlation, was used across two independent datasets to examine multivariate relationships between white matter (WM) properties and symptomatology, to identify stable and generalizable signatures in EP. The primary cohort included EP patients from the Human Connectome Project-Early Psychosis (n=124). The replication cohort included EP patients from the Feinstein Institute for Medical Research (n=78). Both samples included individuals with schizophrenia, schizoaffective disorder, and psychotic mood disorders.

RESULTS

In both cohorts, a significant latent component (LC) corresponded to a symptom profile combining negative symptoms, primarily diminished expression, with specific somatic symptoms. Both LCs captured comprehensive features of WM disruption, primarily a combination of subcortical and frontal association fibers. Strikingly, the PLS model trained on the primary cohort accurately predicted microstructural features and symptoms in the replication cohort. Findings were not driven by diagnosis, medication, or substance use.

CONCLUSIONS

This data-driven transdiagnostic approach revealed a stable and replicable neurobiological signature of microstructural WM alterations in EP, across diagnoses and datasets, showing a strong covariance of these alterations with a unique profile of negative and somatic symptoms. This finding suggests the clinical utility of applying data-driven approaches to reveal symptom domains that share neurobiological underpinnings.

摘要

背景

早期精神病患者(EP,精神病发作后3年内)表现出显著的变异性,这使得结果预测具有挑战性。目前,关于EP诊断中神经微观结构特性与症状特征之间稳定关系的证据很少,限制了早期干预措施的发展。

方法

采用数据驱动方法——偏最小二乘(PLS)相关性分析,对两个独立数据集进行分析,以研究白质(WM)特性与症状学之间的多变量关系,从而确定EP中稳定且可推广的特征。主要队列包括来自人类连接组计划-早期精神病项目的EP患者(n = 124)。复制队列包括来自费恩斯坦医学研究所的EP患者(n = 78)。两个样本均包括精神分裂症、分裂情感性障碍和伴有精神病性症状的心境障碍患者。

结果

在两个队列中,一个显著的潜在成分(LC)对应于一种症状特征,该特征将阴性症状(主要是表达减少)与特定躯体症状相结合。两个LC均捕捉到了WM破坏的综合特征,主要是皮质下和额叶联合纤维的组合。引人注目的是,在主要队列上训练的PLS模型准确地预测了复制队列中的微观结构特征和症状。研究结果不受诊断、药物治疗或物质使用的影响。

结论

这种数据驱动的跨诊断方法揭示了EP中WM微观结构改变的一种稳定且可重复的神经生物学特征,跨越诊断和数据集,显示出这些改变与阴性和躯体症状的独特特征之间存在很强的协方差。这一发现表明应用数据驱动方法揭示具有神经生物学基础的症状领域具有临床实用性。

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