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A comprehensive investigation of the mRNA and protein level of ACE2, the putative receptor of SARS-CoV-2, in human tissues and blood cells

机译:综合调查ACE2,SARS-COV-2的推定受体,在人组织和血细胞中

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The outbreak of pneumonia caused by SARS-CoV-2 posed a great threat to global human health, which urgently requires us to understand comprehensively the mechanism of SARS-CoV-2 infection. Angiotensin-converting enzyme 2 (ACE2) was identified as a functional receptor for SARS-CoV-2, distribution of which may indicate the risk of different human organs vulnerable to SARS-CoV-2 infection. Previous studies investigating the distribution of ACE2 mRNA in human tissues only involved a limited size of the samples and a lack of determination for ACE2 protein. Given the heterogeneity among humans, the datasets covering more tissues with a larger size of samples should be analyzed. Indeed, ACE2 is a membrane and secreted protein, while the expression of ACE2 in blood and common blood cells remains unknown. Herein, the proteomic data in HIPED and the antibody-based immunochemistry result in HPA were collected to analyze the distribution of ACE2 protein in human tissues. The bulk RNA-seq profiles from three separate public datasets including HPA tissue Atlas, GTEx, and FANTOM5 CAGE were also obtained to determine the expression of ACE2 in human tissues. Moreover, the abundance of ACE2 in human blood and blood cells was determined by analyzing the data in the PeptideAtlas and the HPA Blood Atlas. We found that the mRNA expression cannot reflect the abundance of ACE2 factor due to the strong differences between mRNA and protein quantities of ACE2 within and across tissues. Our results suggested that ACE2 protein is mainly expressed in the small intestine, kidney, gallbladder, and testis, while the abundance of which in brain-associated tissues and blood common cells is low. HIPED revealed enrichment of ACE2 protein in the placenta and ovary despite a low mRNA level. Further, human secretome shows that the average concentration of ACE2 protein in the plasma of males is higher than those in females. Our research will be beneficial for understanding the transmission routes and sex-based differences in susceptibility of SARS-CoV-2 infection.? The author(s).
机译:SARS-COV-2引起的肺炎爆发对全球人类健康构成了巨大威胁,这迫切需要我们全面理解SARS-COV-2感染的机制。血管紧张素转化酶2(ACE2)被鉴定为SARS-COV-2的官能受体,其分布可能表明不同人体器官容易受到SARS-COV-2感染的风险。以前研究人体组织中ACE2 mRNA分布的研究仅涉及样品的有限尺寸和缺乏ACE2蛋白的测定。鉴于人类之间的异质性,应分析覆盖更多组织的数据集,应分析具有较大尺寸的样品。实际上,ACE2是膜和分泌蛋白质,而血液和常见血细胞中ACE2的表达仍然未知。这里,收集备受阶下的蛋白质组学数据和基于抗体的免疫化学导致HPA的结果,分析人组织中ACE2蛋白的分布。还获得了来自三个单独的公共数据集的批量RNA-SEQ型材,包括HPA组织Atlas,GTEX和Fantom5笼,以确定人体组织中ACE2的表达。此外,通过分析PeptiDAlas和HPA血液地图集的数据来确定人血液和血细胞中的ACE2的丰度。我们发现mRNA表达不能反映ace2因素的丰富因子,因为MRNA和蛋白质数量在组织内部和跨组织中的敏感性。我们的研究结果表明ACE2蛋白主要在小肠,肾,胆囊和睾丸中表达,而脑相关组织和血液常见细胞中的丰度低。尽管MRNA水平低,所以在胎盘和卵巢中揭示了胎盘和卵巢中的富集。此外,人沉淀表明,雄性血浆中ACE2蛋白的平均浓度高于女性。我们的研究将有利于了解SARS-COV-2感染易感性的传输路线和性别差异。作者。

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