儿童期精神分裂症患者的年轻非精神病兄弟姐妹的白质生长轨迹延迟。

Nitin Gogtay, Xue Hua, Reva Stidd, Christina P Boyle, Suh Lee, Brian Weisinger, Alex Chavez, Jay N Giedd, Liv Clasen, Arthur W Toga, Judith L Rapoport, Paul M Thompson
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引用次数: 30

摘要

背景:儿童期精神分裂症(COS)患者的非精神病性兄弟姐妹在早期与其先证者共享皮质灰质异常;这些在兄弟姐妹18岁时正常化,这表明精神分裂症的灰质异常可能是一种年龄特异性的内表型。COS患者还表现出明显的白质(WM)生长缺陷,这在非精神病性兄弟姐妹中尚未发现。目的研究非精神病性COS患者兄弟姐妹WM生长差异。设计纵向(5年)解剖磁共振成像研究使用一种新的基于张量的形态分析来绘制WM的生长。国家卫生研究院临床中心,贝塞斯达,马里兰州。参与者49例COS患者的健康兄弟姐妹(平均[SD]年龄,16.1[5.3]岁;男性19例,女性30例),健康人群57例作为对照(年龄16.9[5.3]岁;男性29人,女性28人)。介入磁共振成像。主要结果测量白质生长速率。结果我们比较了3个年龄段WM的生长速率。在最年轻的年龄组(7岁至6岁)
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Delayed white matter growth trajectory in young nonpsychotic siblings of patients with childhood-onset schizophrenia.

CONTEXT Nonpsychotic siblings of patients with childhood-onset schizophrenia (COS) share cortical gray matter abnormalities with their probands at an early age; these normalize by the time the siblings are aged 18 years, suggesting that the gray matter abnormalities in schizophrenia could be an age-specific endophenotype. Patients with COS also show significant white matter (WM) growth deficits, which have not yet been explored in nonpsychotic siblings. OBJECTIVE To study WM growth differences in nonpsychotic siblings of patients with COS. DESIGN Longitudinal (5-year) anatomic magnetic resonance imaging study mapping WM growth using a novel tensor-based morphometry analysis. SETTING National Institutes of Health Clinical Center, Bethesda, Maryland. PARTICIPANTS Forty-nine healthy siblings of patients with COS (mean [SD] age, 16.1 [5.3] years; 19 male, 30 female) and 57 healthy persons serving as controls (age, 16.9 [5.3] years; 29 male, 28 female). INTERVENTION Magnetic resonance imaging. MAIN OUTCOME MEASURE White matter growth rates. RESULTS We compared the WM growth rates in 3 age ranges. In the youngest age group (7 to <14 years), we found a significant difference in growth rates, with siblings of patients with COS showing slower WM growth rates in the parietal lobes of the brain than age-matched healthy controls (false discovery rate, q = 0.05; critical P = .001 in the bilateral parietal WM; a post hoc analysis identified growth rate differences only on the left side, critical P = .004). A growth rate difference was not detectable at older ages. In 3-dimensional maps, growth rates in the siblings even appeared to surpass those of healthy individuals at later ages, at least locally in the brain, but this effect did not survive a multiple comparisons correction. CONCLUSIONS In this first longitudinal study of nonpsychotic siblings of patients with COS, the siblings showed early WM growth deficits, which normalized with age. As reported before for gray matter, WM growth may also be an age-specific endophenotype that shows compensatory normalization with age.

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来源期刊
Archives of general psychiatry
Archives of general psychiatry 医学-精神病学
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4-8 weeks
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