性别和年龄特异性小脑结构偏差及其与精神病高危个体症状维度和临床结局的关系。
Sex- and Age-Specific Deviations in Cerebellar Structure and Their Link With Symptom Dimensions and Clinical Outcome in Individuals at Clinical High Risk for Psychosis.
机构信息
Department of Psychology, Emory University, Atlanta, GA, USA.
Department of Human Genetics, Emory University, Atlanta, GA, USA.
出版信息
Schizophr Bull. 2023 Mar 15;49(2):350-363. doi: 10.1093/schbul/sbac169.
BACKGROUND
The clinical high-risk (CHR) period offers a temporal window into neurobiological deviations preceding psychosis onset, but little attention has been given to regions outside the cerebrum in large-scale studies of CHR. Recently, the North American Prodrome Longitudinal Study (NAPLS)-2 revealed altered functional connectivity of the cerebello-thalamo-cortical circuitry among individuals at CHR; however, cerebellar morphology remains underinvestigated in this at-risk population, despite growing evidence of its involvement in psychosis.
STUDY DESIGN
In this multisite study, we analyzed T1-weighted magnetic resonance imaging scans obtained from N = 469 CHR individuals (61% male, ages = 12-36 years) and N = 212 healthy controls (52% male, ages = 12-34 years) from NAPLS-2, with a focus on cerebellar cortex and white matter volumes separately. Symptoms were rated by the Structured Interview for Psychosis-Risk Syndromes (SIPS). The outcome by two-year follow-up was categorized as in-remission, symptomatic, prodromal-progression, or psychotic. General linear models were used for case-control comparisons and tests for volumetric associations with baseline SIPS ratings and clinical outcomes.
STUDY RESULTS
Cerebellar cortex and white matter volumes differed between the CHR and healthy control groups at baseline, with sex moderating the difference in cortical volumes, and both sex and age moderating the difference in white matter volumes. Baseline ratings for major psychosis-risk dimensions as well as a clinical outcome at follow-up had tissue-specific associations with cerebellar volumes.
CONCLUSIONS
These findings point to clinically relevant deviations in cerebellar cortex and white matter structures among CHR individuals and highlight the importance of considering the complex interplay between sex and age when studying the neuromaturational substrates of psychosis risk.
背景
临床高风险(CHR)时期提供了一个时间窗口,可以观察到精神病发作前的神经生物学偏差,但在对 CHR 的大规模研究中,很少关注大脑以外的区域。最近,北美前驱纵向研究(NAPLS)-2 揭示了 CHR 个体中小脑-丘脑-皮质回路的功能连接发生改变;然而,小脑形态在这一高危人群中仍未得到充分研究,尽管越来越多的证据表明其与精神病有关。
研究设计
在这项多中心研究中,我们分析了来自 NAPLS-2 的 469 名 CHR 个体(61%为男性,年龄为 12-36 岁)和 212 名健康对照者(52%为男性,年龄为 12-34 岁)的 T1 加权磁共振成像扫描,重点分别分析小脑皮质和白质体积。症状由精神病风险综合征结构化访谈(SIPS)进行评定。以两年随访为结果,分为缓解、有症状、前驱进展或精神病。使用一般线性模型进行病例对照比较,并测试与基线 SIPS 评分和临床结局的体积关联。
研究结果
CHR 组和健康对照组在基线时小脑皮质和白质体积存在差异,性别调节了皮质体积的差异,性别和年龄都调节了白质体积的差异。主要精神病风险维度的基线评分以及随访时的临床结局与小脑体积有组织特异性关联。
结论
这些发现表明 CHR 个体的小脑皮质和白质结构存在临床相关偏差,并强调在研究精神病风险的神经成熟基础时,考虑性别和年龄之间的复杂相互作用的重要性。
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