Transcriptomics Curation of SARS-CoV-2 Related Host Genes in Mice With COVID-19 Comorbidity: A Pilot Study.

IF 2 Q3 INFECTIOUS DISEASES Infectious microbes & diseases Pub Date : 2020-05-06 eCollection Date: 2020-06-01 DOI:10.1097/IM9.0000000000000025
Kunkai Su, Xin Huang, Kaijin Xu, Weibo Du, Danhua Zhu, Meifang Yang, Wenji Yuan, Lanjuan Li
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Abstract

The pandemic of coronavirus disease 2019 (COVID-19), a respiratory disease caused by a novel severe acute respiratory syndrome coronavirus-2, is causing substantial morbidity and mortality. Along with the respiratory symptoms, underlying diseases in senior patients, such as diabetes, hypertension, and coronary heart disease, are the most common comorbidities, which cause more severe outcomes and even death. During cellular attachment and entry of severe acute respiratory syndrome coronavirus-2, the key protein involved is the angiotensin I converting enzyme 2 (ACE2), which is located on the membrane of host cells. Here, we aim to curate an expression profile of Ace2 and other COVID-19 related genes across the available diabetes murine strains. Based on strictly manual curation and bioinformatics analysis of the publicly deposited expression datasets, Ace2 and other potentially involved genes such as Furin, Tmprss2, Ang, and Ang2 were examined. We found that Ace2 expression is rather ubiquitous in three selected diabetes prone strains (db/db, ob/ob and diet-induced obese). With the most abundant datasets present, the liver shows a medium Ace2 expression level compared with the lungs, pancreatic islets, brain and even T cells. Age is a more critical factor for Ace2 expression in db/db compared with the other two strains. Besides Ace2, the other four host genes showed varied levels of correlation to each other. To accelerate research on the interaction between COVID-19 and underlying diseases, the Murine4Covid transcriptomics database (www.geneureka.org/Murine4Covid) will facilitate the design of research on COVID-19 and comorbidities.

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COVID-19合并症小鼠中SARS-CoV-2相关宿主基因的转录组学调控:一项初步研究
2019冠状病毒病(COVID-19)是一种由新型严重急性呼吸综合征冠状病毒-2引起的呼吸道疾病,其发病率和死亡率都很高。除了呼吸道症状外,糖尿病、高血压、冠心病等老年患者的潜在疾病是最常见的合并症,这些合并症会导致更严重的后果,甚至死亡。在严重急性呼吸综合征冠状病毒-2的细胞附着和进入过程中,参与的关键蛋白是位于宿主细胞膜上的血管紧张素I转换酶2 (ACE2)。在这里,我们的目标是在可用的糖尿病小鼠品系中整理Ace2和其他COVID-19相关基因的表达谱。基于对公开保存的表达数据集的严格手工整理和生物信息学分析,Ace2和其他可能涉及的基因如Furin、Tmprss2、Ang和Ang2进行了检测。我们发现Ace2在三种糖尿病易感菌株(db/db, ob/ob和饮食诱导的肥胖)中普遍表达。根据目前最丰富的数据集,与肺、胰岛、脑甚至T细胞相比,肝脏显示出中等水平的Ace2表达。与其他菌株相比,年龄是影响Ace2表达(db/db)的关键因素。除Ace2外,其余4个宿主基因均表现出不同程度的相关性。为了加速研究COVID-19与基础疾病之间的相互作用,Murine4Covid转录组学数据库(www.geneureka.org/Murine4Covid)将促进COVID-19及其合并症的研究设计。
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