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健康青少年的分裂型特质相关皮质磁化与精神分裂症相关基因的表达有关。

Schizotypy-Related Magnetization of Cortex in Healthy Adolescence Is Colocated With Expression of Schizophrenia-Related Genes.

机构信息

Department of Psychiatry, University of Cambridge, Cambridge, United Kingdom.

Department of Psychiatry, University of Cambridge, Cambridge, United Kingdom.

出版信息

Biol Psychiatry. 2020 Aug 1;88(3):248-259. doi: 10.1016/j.biopsych.2019.12.005. Epub 2019 Dec 13.

Abstract

BACKGROUND

Genetic risk is thought to drive clinical variation on a spectrum of schizophrenia-like traits, but the underlying changes in brain structure that mechanistically link genomic variation to schizotypal experience and behavior are unclear.

METHODS

We assessed schizotypy using a self-reported questionnaire and measured magnetization transfer as a putative microstructural magnetic resonance imaging marker of intracortical myelination in 68 brain regions in 248 healthy young people (14-25 years of age). We used normative adult brain gene expression data and partial least squares analysis to find the weighted gene expression pattern that was most colocated with the cortical map of schizotypy-related magnetization.

RESULTS

Magnetization was significantly correlated with schizotypy in the bilateral posterior cingulate cortex and precuneus (and for disorganized schizotypy, also in medial prefrontal cortex; all false discovery rate-corrected ps < .05), which are regions of the default mode network specialized for social and memory functions. The genes most positively weighted on the whole-genome expression map colocated with schizotypy-related magnetization were enriched for genes that were significantly downregulated in two prior case-control histological studies of brain gene expression in schizophrenia. Conversely, the most negatively weighted genes were enriched for genes that were transcriptionally upregulated in schizophrenia. Positively weighted (downregulated) genes were enriched for neuronal, specifically interneuronal, affiliations and coded a network of proteins comprising a few highly interactive "hubs" such as parvalbumin and calmodulin.

CONCLUSIONS

Microstructural magnetic resonance imaging maps of intracortical magnetization can be linked to both the behavioral traits of schizotypy and prior histological data on dysregulated gene expression in schizophrenia.

摘要

背景

遗传风险被认为在精神分裂症样特征的谱系上驱动临床变异,但将基因组变异与分裂型体验和行为联系起来的大脑结构的潜在变化尚不清楚。

方法

我们使用自我报告的问卷评估分裂型特质,并在 248 名健康年轻人(14-25 岁)的 68 个大脑区域中测量磁化传递,作为皮质内髓鞘化的磁共振成像微观结构标志物。我们使用正常成人脑基因表达数据和偏最小二乘分析来找到与与分裂型特质相关的磁化皮质图最重合的加权基因表达模式。

结果

磁化与双侧后扣带回和楔前叶的分裂型特质显著相关(对于紊乱性分裂型特质,也与内侧前额叶相关;所有经假发现率校正后的 p 值均<0.05),这些区域是默认模式网络中专门用于社交和记忆功能的区域。在全基因组表达图谱上权重最高的基因与与分裂型特质相关的磁化最重合,这些基因在精神分裂症大脑基因表达的两项先前病例对照组织学研究中显著下调。相反,权重最低的基因在精神分裂症中上调。权重较高的(下调的)基因富集了神经元,特别是中间神经元,其编码由少数高度交互的“枢纽”组成的蛋白质网络,如钙调蛋白和钙调蛋白。

结论

皮质内磁化的磁共振成像微观结构图谱可以与分裂型特质的行为特征以及精神分裂症中失调基因表达的先前组织学数据联系起来。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/995c/7369635/08c3e2e65527/gr1.jpg

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