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死于新冠病毒病患者的嗅球和杏仁核基因表达变化

Olfactory Bulb and Amygdala Gene Expression Changes in Subjects Dying with COVID-19.

作者信息

Piras Ignazio S, Huentelman Matthew J, Walker Jessica E, Arce Richard, Glass Michael J, Vargas Daisy, Sue Lucia I, Intorcia Anthony J, Nelson Courtney M, Suszczewicz Katsuko E, Borja Claryssa L, Desforges Marc, Deture Michael, Dickson Dennis W, Beach Thomas G, Serrano Geidy E

机构信息

Translational Genomics Research Institute, Neurogenomics Division.

Banner Sun Health Research Institute, Sun City, AZ.

出版信息

medRxiv. 2021 Sep 15:2021.09.12.21263291. doi: 10.1101/2021.09.12.21263291.

Abstract

In this study we conducted RNA sequencing on two brain regions (olfactory bulb and amygdala) from subjects who died from COVID-19 or who died of other causes. We found several-fold more transcriptional changes in the olfactory bulb than in the amygdala, consistent with our own work and that of others indicating that the olfactory bulb may be the initial and most common brain region infected. To some extent our results converge with pseudotime analysis towards common processes shared between the brain regions, possibly induced by the systemic immune reaction following SARS-CoV-2 infection. Changes in amygdala emphasized upregulation of interferon-related neuroinflammation genes, as well as downregulation of synaptic and other neuronal genes, and may represent the substrate of reported acute and subacute COVID-19 neurological effects. Additionally, and only in olfactory bulb, we observed an increase in angiogenesis and platelet activation genes, possibly associated with microvascular damages induced by neuroinflammation. Through coexpression analysis we identified two key genes ( for the synaptic neuronal network and for the angiogenesis/platelet network) that might be interesting potential targets to reverse the effects induced by SARS-CoV-2 infection. Finally, in olfactory bulb we detected an upregulation of olfactory and taste genes, possibly as a compensatory response to functional deafferentation caused by viral entry into primary olfactory sensory neurons. In conclusion, we were able to identify transcriptional profiles and key genes involved in neuroinflammation, neuronal reaction and olfaction induced by direct CNS infection and/or the systemic immune response to SARS-CoV-2 infection.

摘要

在本研究中,我们对死于新冠病毒疾病(COVID-19)或其他原因的受试者的两个脑区(嗅球和杏仁核)进行了RNA测序。我们发现嗅球中的转录变化比杏仁核中的多几倍,这与我们自己以及其他人的研究结果一致,表明嗅球可能是最初且最常受感染的脑区。在某种程度上,我们的结果与伪时间分析在脑区之间共享的共同过程上趋同,这可能是由SARS-CoV-2感染后的全身免疫反应所诱导的。杏仁核的变化强调了干扰素相关神经炎症基因的上调,以及突触和其他神经元基因的下调,这可能代表了报告的急性和亚急性COVID-19神经学效应的基础。此外,且仅在嗅球中,我们观察到血管生成和血小板激活基因增加,这可能与神经炎症诱导的微血管损伤有关。通过共表达分析,我们确定了两个关键基因(一个用于突触神经元网络,另一个用于血管生成/血小板网络),它们可能是逆转SARS-CoV-2感染所诱导效应的有趣潜在靶点。最后,在嗅球中我们检测到嗅觉和味觉基因上调,这可能是对病毒进入初级嗅觉感觉神经元导致的功能性传入神经阻滞的一种代偿反应。总之,我们能够识别出由直接中枢神经系统感染和/或对SARS-CoV-2感染的全身免疫反应所诱导的神经炎症、神经元反应和嗅觉相关的转录谱和关键基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/74b1/8452114/ca843d8b059e/nihpp-2021.09.12.21263291v1-f0001.jpg

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