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首页> 外文期刊>Journal of Medical Virology >Genetic variability of human coronavirus OC43-, 229E-, and NL63-like strains and their association with lower respiratory tract infections of hospitalized infants and immunocompromised patients.
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Genetic variability of human coronavirus OC43-, 229E-, and NL63-like strains and their association with lower respiratory tract infections of hospitalized infants and immunocompromised patients.

机译:人冠状病毒OC43、229E和NL63样菌株的遗传变异性及其与住院婴儿和免疫功能低下患者下呼吸道感染的关系。

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摘要

In the winter-spring seasons 2003-2004 and 2004-2005, 47 (5.7%) patients with acute respiratory infection associated with human coronavirus (hCoV) 229E-, NL63-, and OC43-like strains were identified among 823 (597 immunocompetent and 226 immunocompromised) patients admitted to hospital with acute respiratory syndromes. Viral infections were diagnosed by either immunological (monoclonal antibodies) or molecular (RT-PCR) methods. Each of two sets of primer pairs developed for detection of all CoVs (panCoV) failed to detect 15 of the 53 (28.3%) hCoV strains identified. On the other hand, all hCoV strains could be detected by using type-specific primers targeting genes 1ab and N. The HuH-7 cell line was found to be susceptible to isolation and identification of OC43- and 229E-like strains. Overall, hCoV infection was caused by OC43-like, 229E-like, and NL63-like strains in 25 (53.2%), 10 (21.3%), and 9 (19.1%) patients, respectively. In addition, three patients (6.4%) were infected by untypeable hCoV strains. NL63-like strains were not found to circulate in 2003-2004, and 229E-like strains did not circulate in 2004-2005, while OC43-like strains were detected in both seasons. The monthly distribution reached a peak during January through March. Lower predominated over upper respiratory tract infections in each age group. In addition, hCoV infections interested only immunocompetent infants and young children during the first year of life, while all adults were immunocompromised patients. Coinfections of hCoVs and other respiratory viruses (mostly interesting the first year of life) were observed in 14 of the 47 (29.8%) patients and were associated with severe respiratory syndromes more frequently than hCoV single infections (P = 0.002). In conclusion, the use of multiple primer sets targeting different genes is recommended for diagnosis of all types of hCoV infection. In addition, the detection of still untypeable hCoV strains suggests that the number of hCoVs involved in human pathology might further increase. Finally, hCoVs should be screened routinely for in both infants and immunocompromised patients with acute respiratory infection.
机译:在2003-2004年和2004-2005年冬春季节期间,在823例(597例具有免疫能力的人)中检出47例(5.7%)与人类冠状病毒(hCoV)229E-,NL63-和OC43样菌株相关的急性呼吸道感染患者。 226名免疫功能低下)患者因急性呼吸道综合症入院。通过免疫学(单克隆抗体)或分子学(RT-PCR)方法诊断出病毒感染。开发用于检测所有CoV(panCoV)的两组引物对中的每对均未能检测到所鉴定的53个(28.3%)hCoV菌株中的15个。另一方面,通过使用针对基因1ab和N的类型特异性引物可以检测到所有hCoV菌株。发现HuH-7细胞株易于分离和鉴定OC43和229E样菌株。总体而言,hCoV感染分别由25(53.2%),10(21.3%)和9(19.1%)的OC43样,229E样和NL63样菌株引起。此外,三名患者(6.4%)被无法分型的hCoV株感染。没有发现NL63样菌株在2003-2004年间流通,而229E样菌株在2004-2005年间没有流通,而在两个季节均检测到OC43样菌株。在1月到3月之间,每月的分布达到了峰值。在每个年龄段,下呼吸道感染以上呼吸道感染为主。此外,hCoV感染仅对具有免疫能力的婴儿和生命的第一年感兴趣,而所有成人均为免疫功能低下的患者。在47例患者中有14例(29.8%)观察到了hCoV和其他呼吸道病毒的合并感染(最有趣的是第一年),与hCoV单一感染相比,与严重呼吸系统综合症的发病率更高(P = 0.002)。总之,建议使用针对不同基因的多种引物对诊断所有类型的hCoV感染。此外,仍无法分型的hCoV毒株的检测表明,人类病理学中涉及的hCoV的数量可能会进一步增加。最后,应常规筛查婴儿和免疫功能低下急性呼吸道感染患者的hCoV。

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