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原发性到跨模态的压缩梯度伴随着皮质下改变,并与重性抑郁障碍中的神经递质和细胞特征相关。

Compressed primary-to-transmodal gradient is accompanied with subcortical alterations and linked to neurotransmitters and cellular signatures in major depressive disorder.

机构信息

Center for Cognition and Brain Disorders, The Affiliated Hospital of Hangzhou Normal University, Hangzhou, Zhejiang Province, PR China.

Institute of Psychological Science, Hangzhou Normal University, Hangzhou, Zhejiang Province, PR China.

出版信息

Hum Brain Mapp. 2023 Dec 1;44(17):5919-5935. doi: 10.1002/hbm.26485. Epub 2023 Sep 9.

Abstract

Major depressive disorder (MDD) has been shown to involve widespread changes in low-level sensorimotor and higher-level cognitive functions. Recent research found that a primary-to-transmodal gradient could capture a cortical hierarchical organization ranging from perception and action to cognition in healthy subjects, but a prominent gradient dysfunction in MDD patients. However, whether and how this cortical gradient is linked to subcortical impairments and whether it is reflected in the microscale neurotransmitter systems and cell type-specific transcriptional signatures remain largely unknown. Data were acquired from 323 MDD patients and 328 sex- and age-matched healthy controls derived from the REST-meta-MDD project, and the human brain neurotransmitter systems density maps and gene expression data were drawn from two publicly available datasets. We investigated alterations of the primary-to-transmodal gradient in MDD patients and their correlations with clinical symptoms of depression and anxiety, as well as  their paralleled subcortical impairments. The correlations between MDD-related gradient alterations and densities of the neurotransmitter systems and gene expression information were assessed, respectively. The results demonstrated that MDD patients had a compressed primary-to-transmodal gradient accompanied by paralleled alterations in subcortical regions including the caudate, amygdala, and thalamus. The case-control gradient differences were spatially correlated with the densities of the neurotransmitter systems including the serotonin and dopamine receptors, and meanwhile with gene expression enriched in astrocytes, excitatory and inhibitory neuronal cells. These findings mapped the paralleled subcortical impairments in cortical hierarchical organization and also helped us understand the possible molecular and cellular substrates of the co-occurrence of high-level cognitive impairments with low-level sensorimotor abnormalities in MDD.

摘要

重度抑郁症(MDD)已被证明涉及低级感觉运动和高级认知功能的广泛变化。最近的研究发现,从感知和行动到认知,一种主要到跨模态的梯度可以捕捉到健康受试者的皮质分层组织,但 MDD 患者的梯度功能明显异常。然而,这种皮质梯度是否以及如何与皮质下损伤相关,以及它是否反映在微观神经递质系统和细胞类型特异性转录特征中,仍然知之甚少。数据来自 REST-meta-MDD 项目的 323 名 MDD 患者和 328 名性别和年龄匹配的健康对照者,人类大脑神经递质系统密度图和基因表达数据来自两个公开数据集。我们研究了 MDD 患者中主要到跨模态梯度的变化及其与抑郁和焦虑症状的相关性,以及与皮质下损伤的相关性。分别评估了 MDD 相关梯度变化与神经递质系统密度和基因表达信息之间的相关性。结果表明,MDD 患者的主要到跨模态梯度被压缩,同时伴有皮质下区域包括尾状核、杏仁核和丘脑的平行变化。病例对照梯度差异与包括 5-羟色胺和多巴胺受体在内的神经递质系统的密度在空间上相关,同时与星形胶质细胞、兴奋性和抑制性神经元细胞中富集的基因表达相关。这些发现描绘了皮质分层组织中平行的皮质下损伤,也帮助我们理解 MDD 中高级认知损伤与低级感觉运动异常共存的可能分子和细胞基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/da24/10619397/894d82053750/HBM-44-5919-g005.jpg

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