社区老年人季节性人类冠状病毒OC43、HKU1、NL63和229E症状感染的临床和血清学特征

IF 2 Q4 VIROLOGY
M. Verheul, M. Hendriks, C. V. B. de Melo, Sophie van Tol, G. Godeke, R. van Binnendijk, W. Luytjes, C. Reusken, J. van Beek
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摘要

引言呼吸道感染是老年人常见的疾病原因,可能导致严重的发病率或死亡率。虽然该人群中高达10%的呼吸道感染是由四种人类冠状病毒(hCoV)之一OC43、HKU1、NL63和229E引起的,但关于hCoV流行病学和免疫反应的数据在社区感染的老年人中有限。此外,通常很难区分和识别不同的hCoV感染。因此,研究了临床特征和使用血清学来识别近期感染的可能性。方法对出现hCoV相关症状性流感样疾病(ILI)的社区老年人的临床特征和体液免疫反应进行研究。通过使用重组刺突蛋白的蛋白质微阵列鉴定每种hCoV特异性的血清抗体。结果经分子证实感染hCoV的参与者的症状很难与引起ILI的其他病毒病原体的症状区分开来。总体而言,基于累积症状评分的hCoV严重程度低于研究中存在的其他引起ILI的感染。此外,症状评分与抗体水平的变化无关。使用单一血清样本来识别最近的感染,导致受试者工作特征(ROC)曲线下面积(AUC)值在0.5和0.7之间的感染之间的区别有限,这取决于hCoV。然而,在急性和恢复时间点间隔8周收集的配对血清学样本显示,根据hCoV,ROC AUC值在0.78和0.96之间的类型特异性抗体增加。讨论尽管hCoV之间的临床特征是可比较的,但抗体动力学分析可能为识别最近的hCoV感染提供一种替代方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical and serological characteristics of symptomatic infection with seasonal human coronaviruses OC43, HKU1, NL63, and 229E in community-dwelling older adults
Introduction Respiratory infections are a common cause of illness in older adults, potentially resulting in severe morbidity or mortality. While up to 10% of respiratory infections in this population are caused by one of the four human coronaviruses (hCoVs), OC43, HKU1, NL63, and 229E, data on hCoV epidemiological and immunological responses are limited in communitydwelling older adults. In addition, it is often difficult to distinguish and identify distinct hCoV infections. Therefore, both clinical characteristics and the possibility of using serology to identify recent infections were investigated. Methods Clinical characteristics and humoral immune responses were studied in community-dwelling older adults who presented with hCoV-related symptomatic influenza-like illness (ILI). Serum antibodies specific for each hCoV were identified by protein microarray using recombinant spike proteins. Result The symptoms of participants with molecular confirmation of hCoV infection were difficult to distinguish from symptoms of other viral pathogens causing ILI. Overall, severity based on a cumulative symptom score was less for hCoV than the other ILI-causing infections present in the study. Furthermore, symptom score did not correlate with changes in antibody levels. Using single serum samples to identify recent infections resulted in limited distinction among infections with receiver operating characteristic (ROC) area under the curve (AUC) values between 0.5 and 0.7, depending on the hCoV. However, paired serology samples collected at acute and recovery timepoints with an 8-week interval show an increase in type-specific antibodies with ROC AUC values between 0.78 and 0.96, depending on the hCoV. Discussion Although clinical characteristics are comparable between hCoVs, the analysis of antibody kinetics may provide an alternative method for identifying recent hCoV infections.
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