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综合分析确定了新冠病毒肺炎住院治疗背后的易感基因。

Integrative analyses identify susceptibility genes underlying COVID-19 hospitalization.

作者信息

Pathak Gita A, Singh Kritika, Miller-Fleming Tyne W, Wendt Frank R, Ehsan Nava, Hou Kangcheng, Johnson Ruth, Lu Zeyun, Gopalan Shyamalika, Yengo Loic, Mohammadi Pejman, Pasaniuc Bogdan, Polimanti Renato, Davis Lea K, Mancuso Nicholas

机构信息

Yale School of Medicine, Department of Psychiatry, Division of Human Genetics, New Haven, CT USA.

Veteran Affairs Connecticut Healthcare System, West Haven, CT USA.

出版信息

medRxiv. 2020 Dec 8:2020.12.07.20245308. doi: 10.1101/2020.12.07.20245308.

Abstract

Despite rapid progress in characterizing the role of host genetics in SARS-Cov-2 infection, there is limited understanding of genes and pathways that contribute to COVID-19. Here, we integrated a genome-wide association study of COVID-19 hospitalization (7,885 cases and 961,804 controls from COVID-19 Host Genetics Initiative) with mRNA expression, splicing, and protein levels (n=18,502). We identified 27 genes related to inflammation and coagulation pathways whose genetically predicted expression was associated with COVID-19 hospitalization. We functionally characterized the 27 genes using phenome- and laboratory-wide association scans in Vanderbilt Biobank (BioVU; n=85,460) and identified coagulation-related clinical symptoms, immunologic, and blood-cell-related biomarkers. We replicated these findings across trans-ethnic studies and observed consistent effects in individuals of diverse ancestral backgrounds in BioVU, pan-UK Biobank, and Biobank Japan. Our study highlights putative causal genes impacting COVID-19 severity and symptomology through the host inflammatory response.

摘要

尽管在确定宿主遗传学在SARS-CoV-2感染中的作用方面取得了快速进展,但对于导致COVID-19的基因和途径的了解仍然有限。在此,我们将一项关于COVID-19住院治疗的全基因组关联研究(来自COVID-19宿主遗传学倡议的7885例病例和961804例对照)与mRNA表达、剪接和蛋白质水平(n = 18502)进行了整合。我们鉴定出27个与炎症和凝血途径相关的基因,其遗传预测表达与COVID-19住院治疗相关。我们在范德比尔特生物银行(BioVU;n = 85460)中使用全表型和全实验室关联扫描对这27个基因进行了功能表征,并确定了与凝血相关的临床症状、免疫和血细胞相关的生物标志物。我们在跨种族研究中重复了这些发现,并在BioVU、泛英国生物银行和日本生物银行中不同祖先背景的个体中观察到了一致的效应。我们的研究突出了通过宿主炎症反应影响COVID-19严重程度和症状的假定因果基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/911d/7743085/3cd277e0bc70/nihpp-2020.12.07.20245308-f0001.jpg

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