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Discovery of a subgenotype of human coronavirus NL63 associated with severe lower respiratory tract infection in China, 2018

机译:中国,2018年中国严重下呼吸道感染的人冠状病毒NL63亚型型的发现

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Human coronavirus NL63 (HCoV-NL63) is primarily associated with common cold in children, elderly and immunocompromised individuals. Outbreaks caused by HCoV-NL63 are rare. Here we report a cluster of HCoV-NL63 cases with severe lower respiratory tract infection that arose in Guangzhou, China, in 2018. Twenty-three hospitalized children were confirmed to be HCoV-NL63 positive, and most of whom were hospitalized with severe pneumonia or acute bronchitis. Whole genomes of HCoV-NL63 were obtained using next-generation sequencing. Phylogenetic and single amino acid polymorphism analyses showed that this outbreak was associated with two subgenotypes (C3 and B) of HCoV-NL63. Half of patients were identified to be related to a new subgenotype C3. One unique amino acid mutation at I507 L in spike protein receptor binding domain (RBD) was detected, which segregated this subgenotype C3 from other known subgenotypes. Pseudotyped virus bearing the I507 L mutation in RBD showed enhanced entry into host cells as compared to the prototype virus. This study proved that HCoV-NL63 was undergoing continuous mutation and has the potential to cause severe lower respiratory disease in humans.
机译:人冠状病毒NL63(HCOV-NL63)主要与儿童,老年人和免疫表现的常见感冒相关。 HCOV-NL63引起的爆发是罕见的。在这里,我们报告了一系列HCOV-NL63患者,具有严重的下呼吸道感染,在中国广州,2018年出现了。二十三名住院儿童被证实为HCOV-NL63阳性,其中大部分是患有严重肺炎或急性支气管炎。使用下一代测序获得HCOV-N163的全基因组。系统发育和单氨基酸多态性分析表明,该爆发与HCOV-N163的两个亚底型(C3和B)相关。鉴定了一半的患者与新的亚型C3有关。检测到尖峰蛋白受体结合结构域(RBD)中I507 L的一种独特的氨基酸突变,其从其他已知的亚阈值中分离了该亚蛋白型C3。载有原型病毒的RBD中的伪型病毒在RBD中突变显示到宿主细胞中的增强进入。本研究证明,HCoV-N163正在进行连续突变,并且有可能导致人类严重的呼吸道疾病。

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