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儿童期起病精神分裂症患者非精神病性同胞的大脑皮质发育

Cortical brain development in nonpsychotic siblings of patients with childhood-onset schizophrenia.

作者信息

Gogtay Nitin, Greenstein Deanna, Lenane Marge, Clasen Liv, Sharp Wendy, Gochman Pete, Butler Philip, Evans Alan, Rapoport Judith

机构信息

Child Psychiatry Branch, National Institute of Mental Health, National Institutes of Health, Bldg 10, Bethesda, MD 20892, USA.

出版信息

Arch Gen Psychiatry. 2007 Jul;64(7):772-80. doi: 10.1001/archpsyc.64.7.772.

Abstract

CONTEXT

Cortical gray matter (GM) loss is marked and progressive in childhood-onset schizophrenia (COS) during adolescence but becomes more circumscribed by early adulthood. Nonpsychotic siblings of COS probands could help evaluate whether the cortical GM abnormalities are familial/trait markers.

OBJECTIVE

To map cortical development in nonpsychotic siblings of COS probands.

DESIGN

Using an automated measurement and prospectively acquired anatomical brain magnetic resonance images, we mapped cortical GM thickness in healthy full siblings (n = 52, 113 scans; age 8 through 28 years) of patients with COS, contrasting them with age-, sex-, and scan interval-matched healthy controls (n = 52, 108 scans). The false-discovery rate procedure was used to control for type I errors due to multiple comparisons.

SETTING

An ongoing COS study at the National Institute of Mental Health.

PARTICIPANTS

Fifty-two healthy full siblings of patients with COS, aged 8 through 28 years, and 52 healthy controls.

MAIN OUTCOME MEASURES

Longitudinal trajectories of cortical GM development in healthy siblings of patients with COS compared with matched healthy controls and exploratory measure of the relationship between developmental GM trajectories and the overall functioning as defined by the Global Assessment Scale (GAS) score.

RESULTS

Younger, healthy siblings of patients with COS showed significant GM deficits in the left prefrontal and bilateral temporal cortices and smaller deficits in the right prefrontal and inferior parietal cortices compared with the controls. These cortical deficits in siblings disappeared by age 20 years and the process of deficit reduction correlated with overall functioning (GAS scores) at the last scan.

CONCLUSIONS

Prefrontal and temporal GM loss in COS appears to be a familial/trait marker. Amelioration of regional GM deficits in healthy siblings was associated with higher global functioning (GAS scores), suggesting a relationship between brain plasticity and functional outcome for these nonpsychotic, nonspectrum siblings.

摘要

背景

在儿童期起病的精神分裂症(COS)中,皮质灰质(GM)损失在青少年期显著且呈进行性,但到成年早期会变得更加局限。COS先证者的非精神病性同胞有助于评估皮质GM异常是否为家族性/特质性标志物。

目的

描绘COS先证者的非精神病性同胞的皮质发育情况。

设计

我们使用自动测量方法和前瞻性获取的大脑解剖磁共振图像,描绘了COS患者的健康同胞手足(n = 52,113次扫描;年龄8至28岁)的皮质GM厚度,并将他们与年龄、性别和扫描间隔匹配的健康对照者(n = 52,108次扫描)进行对比。采用错误发现率程序来控制因多次比较导致的I型错误。

地点

美国国立精神卫生研究所正在进行的一项COS研究。

参与者

52名年龄在8至28岁之间的COS患者的健康同胞手足以及52名健康对照者。

主要结局指标

与匹配的健康对照者相比,COS患者健康同胞手足的皮质GM发育的纵向轨迹,以及发育性GM轨迹与由全球评估量表(GAS)评分定义的整体功能之间关系的探索性指标。

结果

与对照组相比,COS患者较年轻的健康同胞手足在左侧前额叶和双侧颞叶皮质显示出显著的GM缺损,在右侧前额叶和顶下皮质的缺损较小。同胞手足中的这些皮质缺损在20岁时消失,缺损减少的过程与最后一次扫描时的整体功能(GAS评分)相关。

结论

COS中的前额叶和颞叶GM损失似乎是一种家族性/特质性标志物。健康同胞手足中区域GM缺损的改善与更高的整体功能(GAS评分)相关,这表明这些非精神病性、非谱系同胞的大脑可塑性与功能结局之间存在关联。

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