重性抑郁障碍
灰质
神经影像学
部分各向异性
神经科学
心理学
自闭症谱系障碍
大脑结构与功能
萧条(经济学)
认知
临床心理学
医学
精神科
磁共振成像
磁共振弥散成像
白质
自闭症
宏观经济学
经济
放射科
作者
Shile Qi,Xiao Yang,Liansheng Zhao,Vince D. Calhoun,Nora I. Perrone‐Bizzozero,Shengfeng Liu,Rongtao Jiang,Tianzi Jiang,Jing Sui,Xiaohong Ma
出处
期刊:Brain
[Oxford University Press]
日期:2017-12-20
卷期号:141 (3): 916-926
被引量:85
摘要
There is compelling evidence that epigenetic factors contribute to the manifestation of depression, in which microRNA132 (miR-132) is suggested to play a pivotal role in the pathogenesis and neuronal mechanisms underlying the symptoms of depression. Additionally, several depression-associated genes [MECP2, ARHGAP32 (p250GAP), CREB, and period genes] were experimentally validated as miR-132 targets. However, most studies regarding miR-132 in major depressive disorder are based on post-mortem, animal models or genetic comparisons. This work will be the first attempt to investigate how miR-132 dysregulation may impact covariation of multimodal brain imaging data in 81 unmedicated major depressive patients and 123 demographically-matched healthy controls, as well as in a medication-naïve subset of major depressive patients. MiR-132 values in blood (patients > controls) was used as a prior reference to guide fusion of three MRI features: fractional amplitude of low frequency fluctuations, grey matter volume, and fractional anisotropy. The multimodal components correlated with miR-132 also show significant group difference in loadings. Results indicate that (i) higher miR-132 levels in major depressive disorder are associated with both lower fractional amplitude of low frequency fluctuations and lower grey matter volume in fronto-limbic network; and (ii) the identified brain regions linked with increased miR-132 levels were also associated with poorer cognitive performance in attention and executive function. Using a data-driven, supervised-learning method, we determined that miR-132 dysregulation in major depressive disorder is associated with multi-facets of brain function and structure in fronto-limbic network (the key network for emotional regulation and memory), which deepens our understanding of how miR-132 dysregulation in major depressive disorders contribute to the loss of specific brain areas and is linked to relevant cognitive impairments.
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