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首页> 外文期刊>Journal of Clinical Microbiology >Sensitivity and Specificity of Serologic Assays for Detection of Human Infection with 2009 Pandemic H1N1 Virus in U.S. Populations
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Sensitivity and Specificity of Serologic Assays for Detection of Human Infection with 2009 Pandemic H1N1 Virus in U.S. Populations

机译:在美国人群中检测2009年大流行H1N1病毒人类感染的血清学检测方法的敏感性和特异性

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Swine origin 2009 H1N1 influenza virus has spread globally to cause the first influenza pandemic of the 21st century. Serological studies can improve our understanding of the extent of human infection and risk factors associated with the transmission of this pandemic virus. The “gold standard” for serodiagnosis of human influenza virus infection is the detection of seroconversion between acute- and convalescent-stage samples. However, the timing of seroepidemiological investigations often precludes the collection of truly acute-phase sera, requiring development of serological criteria for evaluating convalescent-phase sera that optimize detection of true positives and true negatives. To guide seroepidemiological investigations into the spread of the novel 2009 pandemic H1N1 virus, we characterized serum antibody responses to 2009 H1N1 virus in 87 individuals with confirmed viral infection and 227 nonexposed U.S. individuals using microneutralization (MN) and hemagglutination inhibition (HI) assays. Sensitivity and specificity were determined for each assay alone and in combination for detection of 2009 H1N1 virus-specific antibodies in convalescent-phase sera. Although the HI assay was more specific for detecting antibody to 2009 H1N1, the MN assay was more sensitive, particularly for detecting low-titer seroconversions. A combination of titers (MN ≥ 40 and HI ≥ 20) provided the highest sensitivity (90%) and specificity (96%) for individuals aged <60 years and 92% specificity for adults aged ≥60 years for detection of serologically confirmed 2009 H1N1 infections in U.S. populations during the first pandemic waves. These studies provide an approach to optimize timely serological investigations for future pandemics or outbreaks of novel influenza viruses among humans.
机译:猪源2009 H1N1流感病毒已在​​全球传播,引起21世纪的第一场流感大流行。血清学研究可以增进我们对人类感染程度和与这种大流行病毒传播有关的危险因素的了解。对人类流感病毒感染进行血清诊断的“金标准”是检测急性和恢复期样品之间的血清转化。然而,血清流行病学调查的时间通常排除了收集真正急性期血清的能力,这需要制定血清学标准来评估恢复期血清,以优化对阳性和阴性的检测。为了指导血清流行病学研究新型2009大流行H1N1病毒的传播,我们使用微中和(MN)和血凝抑制(HI)分析对87例确诊病毒感染的个体和227例未暴露的美国个体的2009 H1N1病毒的血清抗体反应进行了特征分析。分别针对每个测定以及结合测定在恢复期血清中检测2009 H1N1病毒特异性抗体的敏感性和特异性。尽管HI检测对于检测2009 H1N1抗体更具特异性,但MN检测更灵敏,尤其是检测低滴度血清转化。滴度的组合(MN≥40和HI≥20)对检测血清学确认的2009 H1N1病毒具有最高的灵敏度(90%)和特异性(96%),对于60岁以下的个体和92%的特异性对于≥60岁的成年人在第一波大流行浪潮中,美国人群感染了艾滋病。这些研究提供了一种方法,可以优化及时的血清学调查,以应对人类之间未来的大流行或新型流感病毒的爆发。

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