系统综述:青少年抑郁症的白质微观结构组织

Petya D. Radoeva MD, PhD , Victor T. Milev BS , Jeffrey I. Hunt MD , Christopher H. Legere AB , Sean C.L. Deoni PhD , Stephen J. Sheinkopf PhD , Carla A. Mazefsky PhD , Noah S. Philip MD , Daniel P. Dickstein MD
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引用次数: 0

摘要

目的越来越多的文献关注抑郁症的神经机制。我们的目的是对有抑郁症的青少年与无抑郁症的青少年的白质微结构差异进行系统的回顾。方法我们检索PubMed和PsycINFO于2022年8月3日发表的论文(原始检索于2021年7月进行)。该综述已在PROSPERO上注册(注册号:CRD42021268200),并遵循了系统评价和荟萃分析的首选报告项目(PRISMA)指南。符合条件的研究是比较有和无抑郁症青少年(最初年龄为12-19岁,后来扩大到11-21岁)弥散张量/光谱成像结果的原始研究论文。如果研究只关注另一种情况下的抑郁症,仅使用维度抑郁症状评估,或使用与其他纳入的出版物相同的数据集,则排除研究。结果共检索到575条独特记录,其中收录全文论文14篇,其中青少年抑郁症824篇,非抑郁症686篇。至少在3项研究中,以下白质区域在分数各向异性方面表现出显著差异:钩扣束、扣带、前辐射冠、额枕下束和胼胝体(膝和体)。大多数研究报告,抑郁症青少年的分数各向异性减少,而不是增加。局限性包括选择性报告偏倚的可能性和不精确的风险,考虑到一些研究的小样本量。结论我们的系统综述表明,青少年抑郁症患者的边缘-皮质-纹状体-丘脑回路和胼胝体中存在异常的白质结构。未来的研究应关注抑郁症的发展轨迹,确定异质性的来源,并整合各种成像方式的发现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Systematic Review: White Matter Microstructural Organization in Adolescents With Depression

Objective

A growing body of literature has focused on the neural mechanisms of depression. Our goal was to conduct a systematic review on the white matter microstructural differences in adolescents with depressive disorders vs adolescents without depressive disorders.

Method

We searched PubMed and PsycINFO for publications on August 3, 2022 (original search conducted in July 2021). The review was registered on PROSPERO (registration number: CRD42021268200), and the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines were followed. Eligible studies were original research papers comparing diffusion tensor/spectrum imaging findings in adolescents with vs without depression (originally ages 12-19 years, later expanded to 11-21 years). Studies were excluded if they focused on depression exclusively in the context of another condition, used only dimensional depressive symptom assessment(s), or used the same dataset as another included publication.

Results

The search yielded 575 unique records, of which 14 full-text papers were included (824 adolescents with depression and 686 without depression). The following white matter regions showed significant differences in fractional anisotropy in at least 3 studies: uncinate fasciculus, cingulum, anterior corona radiata, inferior fronto-occipital fasciculus, and corpus callosum (genu and body). Most studies reported decreased, rather than increased, fractional anisotropy in adolescents with depression. Limitations include the possibility for selective reporting bias and risk of imprecision, given the small sample sizes in some studies.

Conclusion

Our systematic review suggests aberrant white matter microstructure in limbic-cortical-striatal-thalamic circuits, and the corpus callosum, in adolescents with depression. Future research should focus on developmental trajectories in depression, identifying sources of heterogeneity and integrating findings across imaging modalities.

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JAACAP open
JAACAP open Psychiatry and Mental Health
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