行为障碍的皮层结构和皮层下体积:对 ENIGMA 反社会行为工作组的 15 个国际队列进行的协调分析。

IF 30.8 1区 医学 Q1 PSYCHIATRY
Yidian Gao, Marlene Staginnus
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引用次数: 0

摘要

背景:在所有儿童精神障碍中,行为障碍的发病率最高,但其神经生物学特性仍不清楚。不一致的研究结果限制了我们对大脑结构改变在品行障碍中所起作用的理解。本研究旨在确定行为障碍最稳健且可复制的大脑结构相关因素:ENIGMA-反社会行为工作组对来自15个国际队列的核磁共振成像结构数据进行了协调分析。资格标准是样本平均年龄在18岁以下,有性别、年龄和行为障碍诊断数据,至少有10名行为障碍患者和10名发育正常的患者。所有参与者的三维 T1 加权核磁共振成像脑部扫描均采用 ENIGMA 标准化方案进行预处理。我们使用一般线性模型评估了皮层厚度、表面积和皮层下体积的组间差异,并对年龄、性别和颅内总体积进行了调整。我们还研究了各组别与性别、各组别与年龄之间的交互作用,以及 DSM-亚型比较(儿童期发病与青少年期发病,胼胝-非情感特质水平低与高)。有行为障碍生活经历的人未参与本研究:我们整理了 1185 名患有行为障碍的青少年(339 名[28-6%]女性和 846 名[71-4%]男性)和 1253 名发育正常的青少年(446 名[35-6%]女性和 807 名[64-4%]男性)的个人参与者数据,他们的平均年龄为 13-5 岁(SD 3-0; 范围 7-21)。种族和民族信息不详。与发育正常的青少年相比,行为障碍组 26 个皮质区域的表面积和总表面积均较低(Cohen's d 0-09-0-26)。尾部前扣带回皮层(d 0-16)和颞上沟两侧(d -0-13)的皮层厚度不同。行为障碍组的杏仁核(0-13 d)、伏隔核(0-11 d)、丘脑(0-14 d)和海马(0-12 d)体积也较小。在对多动症合并症或智商进行调整后,大多数差异仍然显著。没有发现不同性别或不同年龄组之间的相互作用。DSM定义的行为障碍亚型之间几乎没有差异。然而,与对照组相比,高胼胝-非情感特质的个体比低胼胝-非情感特质的个体表现出更广泛的差异:我们的研究结果提供了强有力的证据,表明行为障碍患者的大脑结构发生了微妙但广泛的改变,这种改变跨越亚型和性别,主要体现在表面积上。这些发现进一步证明了大脑结构的改变可能是导致行为障碍的原因之一。在研究和临床实践中,需要更多地考虑这种认识不足的障碍:医学科学院和经济与社会研究理事会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cortical structure and subcortical volumes in conduct disorder: a coordinated analysis of 15 international cohorts from the ENIGMA-Antisocial Behavior Working Group.

Background: Conduct disorder is associated with the highest burden of any mental disorder in childhood, yet its neurobiology remains unclear. Inconsistent findings limit our understanding of the role of brain structure alterations in conduct disorder. This study aims to identify the most robust and replicable brain structural correlates of conduct disorder.

Methods: The ENIGMA-Antisocial Behavior Working Group performed a coordinated analysis of structural MRI data from 15 international cohorts. Eligibility criteria were a mean sample age of 18 years or less, with data available on sex, age, and diagnosis of conduct disorder, and at least ten participants with conduct disorder and ten typically developing participants. 3D T1-weighted MRI brain scans of all participants were pre-processed using ENIGMA-standardised protocols. We assessed group differences in cortical thickness, surface area, and subcortical volumes using general linear models, adjusting for age, sex, and total intracranial volume. Group-by-sex and group-by-age interactions, and DSM-subtype comparisons (childhood-onset vs adolescent-onset, and low vs high levels of callous-unemotional traits) were investigated. People with lived experience of conduct disorder were not involved in this study.

Findings: We collated individual participant data from 1185 young people with conduct disorder (339 [28·6%] female and 846 [71·4%] male) and 1253 typically developing young people (446 [35·6%] female and 807 [64·4%] male), with a mean age of 13·5 years (SD 3·0; range 7-21). Information on race and ethnicity was not available. Relative to typically developing young people, the conduct disorder group had lower surface area in 26 cortical regions and lower total surface area (Cohen's d 0·09-0·26). Cortical thickness differed in the caudal anterior cingulate cortex (d 0·16) and the banks of the superior temporal sulcus (d -0·13). The conduct disorder group also had smaller amygdala (d 0·13), nucleus accumbens (d 0·11), thalamus (d 0·14), and hippocampus (d 0·12) volumes. Most differences remained significant after adjusting for ADHD comorbidity or intelligence quotient. No group-by-sex or group-by-age interactions were detected. Few differences were found between DSM-defined conduct disorder subtypes. However, individuals with high callous-unemotional traits showed more widespread differences compared with controls than those with low callous-unemotional traits.

Interpretation: Our findings provide robust evidence of subtle yet widespread brain structural alterations in conduct disorder across subtypes and sexes, mostly in surface area. These findings provide further evidence that brain alterations might contribute to conduct disorder. Greater consideration of this under-recognised disorder is needed in research and clinical practice.

Funding: Academy of Medical Sciences and Economic and Social Research Council.

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来源期刊
Lancet Psychiatry
Lancet Psychiatry PSYCHIATRY-
CiteScore
58.30
自引率
0.90%
发文量
0
期刊介绍: The Lancet Psychiatry is a globally renowned and trusted resource for groundbreaking research in the field of psychiatry. We specialize in publishing original studies that contribute to transforming and shedding light on important aspects of psychiatric practice. Our comprehensive coverage extends to diverse topics including psychopharmacology, psychotherapy, and psychosocial approaches that address psychiatric disorders throughout the lifespan. We aim to channel innovative treatments and examine the biological research that forms the foundation of such advancements. Our journal also explores novel service delivery methods and promotes fresh perspectives on mental illness, emphasizing the significant contributions of social psychiatry.
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