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Genomic Characterization of a Newly Discovered Coronavirus Associated with Acute Respiratory Distress Syndrome in Humans

机译:新发现的冠状病毒与人类急性呼吸窘迫综合征相关的基因组特征。

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A novel human coronavirus (HCoV-EMC/2012) was isolated from a man with acute pneumonia and renal failure in June 2012. This report describes the complete genome sequence, genome organization, and expression strategy of HCoV-EMC/2012 and its relation with known coronaviruses. The genome contains 30,119 nucleotides and contains at least 10 predicted open reading frames, 9 of which are predicted to be expressed from a nested set of seven subgenomic mRNAs. Phylogenetic analysis of the replicase gene of coronaviruses with completely sequenced genomes showed that HCoV-EMC/2012 is most closely related to Tylonycteris bat coronavirus HKU4 (BtCoV-HKU4) and Pipistrellus bat coronavirus HKU5 (BtCoV-HKU5), which prototype two species in lineage C of the genus Betacoronavirus. In accordance with the guidelines of the International Committee on Taxonomy of Viruses, and in view of the 75% and 77% amino acid sequence identity in 7 conserved replicase domains with BtCoV-HKU4 and BtCoV-HKU5, respectively, we propose that HCoV-EMC/2012 prototypes a novel species in the genus Betacoronavirus. HCoV-EMC/2012 may be most closely related to a coronavirus detected in Pipistrellus pipistrellus in The Netherlands, but because only a short sequence from the most conserved part of the RNA-dependent RNA polymerase-encoding region of the genome was reported for this bat virus, its genetic distance from HCoV-EMC remains uncertain. HCoV-EMC/2012 is the sixth coronavirus known to infect humans and the first human virus within betacoronavirus lineage C. >IMPORTANCE Coronaviruses are capable of infecting humans and many animal species. Most infections caused by human coronaviruses are relatively mild. However, the outbreak of severe acute respiratory syndrome (SARS) caused by SARS-CoV in 2002 to 2003 and the fatal infection of a human by HCoV-EMC/2012 in 2012 show that coronaviruses are able to cause severe, sometimes fatal disease in humans. We have determined the complete genome of HCoV-EMC/2012 using an unbiased virus discovery approach involving next-generation sequencing techniques, which enabled subsequent state-of-the-art bioinformatics, phylogenetics, and taxonomic analyses. By establishing its complete genome sequence, HCoV-EMC/2012 was characterized as a new genotype which is closely related to bat coronaviruses that are distant from SARS-CoV. We expect that this information will be vital to rapid advancement of both clinical and vital research on this emerging pathogen.
机译:2012年6月从一名患有急性肺炎和肾功能衰竭的男子中分离出了新型人类冠状病毒(HCoV-EMC / 2012)。该报告介绍了HCoV-EMC / 2012的完整基因组序列,基因组组织和表达策略,以及与HCoV-EMC / 2012的关系。已知的冠状病毒。该基因组包含30,119个核苷酸,并包含至少10个预测的开放阅读框,其中9个被预测从七个亚基因组mRNA的嵌套集中表达。对冠状病毒复制酶基因进行了完整测序的系统进化分析表明,HCoV-EMC / 2012与 Tylonycteris 蝙蝠冠状病毒HKU4(BtCoV-HKU4)和 Pipistrellus 蝙蝠最密切相关冠状病毒HKU5(BtCoV-HKU5),它是β冠状病毒属C的两个物种的原型。根据国际病毒分类学委员会的指南,并鉴于分别具有BtCoV-HKU4和BtCoV-HKU5的7个保守复制酶结构域中75%和77%的氨基酸序列同一性,我们建议HCoV-EMC / 2012原型为一种新型细菌,称为<冠状病毒>。 HCoV-EMC / 2012可能与在荷兰的i> Pipistrellus pipistrellus 中检测到的冠状病毒最密切相关,但因为该序列仅来自RNA依赖的RNA聚合酶编码区最保守部分的短序列据报道该蝙蝠病毒的基因组,其与HCoV-EMC的遗传距离仍不确定。 HCoV-EMC / 2012是已知第六种感染人类的​​冠状病毒,也是beta冠状病毒世系C中的第一种人类病毒。>重要:冠状病毒能够感染人类和许多动物。人类冠状病毒引起的大多数感染是相对轻度的。然而,2002年至2003年由SARS-CoV引起的严重急性呼吸道综合症(SARS)的爆发以及HCoV-EMC / 2012年于2012年对人类的致命感染表明,冠状病毒能够在人类中引起严重的,有时是致命的疾病。我们已使用涉及下一代测序技术的无偏见病毒发现方法,确定了HCoV-EMC / 2012的完整基因组,该方法可进行后续的最新生物信息学,系统发育学和分类学分析。通过建立完整的基因组序列,HCoV-EMC / 2012被表征为一种新的基因型,与远离SARS-CoV的蝙蝠冠状病毒密切相关。我们希望这些信息对于这种新兴病原体的临床和重要研究的快速发展至关重要。

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