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解析人类大脑皮层和杏仁核中心理创伤的转录组特征

Decoding the transcriptomic signatures of psychological trauma in human cortex and amygdala.

作者信息

Hicks Emily M, Seah Carina, Deans Michael, Lee Seoyeon, Johnston Keira J A, Cote Alanna, Ciarcia Julia, Chakka Akash, Collier Lily, Holtzheimer Paul E, Young Keith A, Krystal John H, Brennand Kristen J, Nestler Eric J, Girgenti Matthew J, Huckins Laura M

机构信息

Department of Psychiatry, Yale University School of Medicine, 34 Park Street, New Haven, CT 06520, USA.

Pamela Sklar Division of Psychiatric Genomics, Departments of Psychiatry and of Genetics and Genomic Sciences, Icahn School of Medicine at Mount Sinai, New York, New York, 10029 USA.

出版信息

bioRxiv. 2024 Oct 23:2024.10.23.619681. doi: 10.1101/2024.10.23.619681.

Abstract

Psychological trauma has profound effects on brain function and precipitates psychiatric disorders in vulnerable individuals, however, the molecular mechanisms linking trauma with psychiatric risk remain incompletely understood. Using RNA-seq data postmortem brain tissue of a cohort of 304 donors (N=136 with trauma exposure), we investigated transcriptional signatures of trauma exposures in two cortical regions (dorsolateral prefrontal cortex, and dorsal anterior cingulate cortex) and two amygdala regions (medial amygdala and basolateral amygdala) associated with stress processing and regulation. We focused on dissecting heterogeneity of traumatic experiences in these transcriptional signatures by investigating exposure to several trauma types (childhood, adulthood, complex, single acute, combat, and interpersonal traumas) and interactions with sex. Overall, amygdala regions were more vulnerable to childhood traumas, whereas cortical regions were more vulnerable to adulthood trauma (regardless of childhood experience). Using cell-type-specific expression imputation, we identified a strong transcriptional response of medial amygdala excitatory neurons to childhood trauma, which coincided with dysregulation observed in a human induced pluripotent stem cell (hiPSC)-derived glutamatergic neurons exposed to hydrocortisone. We resolved multiscale coexpression networks for each brain region and identified modules enriched in trauma signatures and whose connectivity was altered with trauma. Trauma-associated coexpression modules provide insight into coordinated functional dysregulation with different traumas and point to potential gene targets for further dissection. Together, these data provide a characterization of the long-lasting human encoding of traumatic experiences in corticolimbic regions of human brain.

摘要

心理创伤对大脑功能有深远影响,并在易受影响的个体中引发精神障碍,然而,将创伤与精神疾病风险联系起来的分子机制仍未完全了解。利用来自304名捐赠者(N = 136有创伤暴露经历)队列的死后脑组织的RNA测序数据,我们研究了与应激处理和调节相关的两个皮质区域(背外侧前额叶皮质和背侧前扣带回皮质)以及两个杏仁核区域(内侧杏仁核和基底外侧杏仁核)中创伤暴露的转录特征。我们通过研究几种创伤类型(童年、成年、复杂、单次急性、战斗和人际创伤)的暴露情况以及与性别的相互作用,专注于剖析这些转录特征中创伤经历的异质性。总体而言,杏仁核区域更容易受到童年创伤的影响,而皮质区域更容易受到成年创伤的影响(无论童年经历如何)。利用细胞类型特异性表达估算,我们确定内侧杏仁核兴奋性神经元对童年创伤有强烈的转录反应,这与在暴露于氢化可的松的人诱导多能干细胞(hiPSC)衍生的谷氨酸能神经元中观察到的失调一致。我们解析了每个脑区的多尺度共表达网络,并确定了富含创伤特征且其连通性随创伤而改变的模块。与创伤相关的共表达模块为不同创伤的协调功能失调提供了见解,并指出了有待进一步剖析的潜在基因靶点。总之,这些数据描绘了人类大脑皮质边缘区域中创伤经历的长期编码特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/79d3/11526900/2e6c9c2eb72f/nihpp-2024.10.23.619681v1-f0001.jpg

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