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首页> 外文期刊>Clinical and vaccine immunology: CVI >Functional and Antigen-Specific Serum Antibody Levels as Correlates of Protection against Shigellosis in a Controlled Human Challenge Study
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Functional and Antigen-Specific Serum Antibody Levels as Correlates of Protection against Shigellosis in a Controlled Human Challenge Study

机译:功能和抗原特异性血清抗体水平作为对照志贺氏菌病预防性对照研究中的相关因素

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摘要

Shigella is an important cause of diarrheal disease in young children living in developing countries. No approved vaccines are available, and the development of vaccine candidates has been hindered by the lack of firm immunological correlates of protection, among other reasons. To address this gap in knowledge, we established quantitative assays to measure Shigella-specific serum bactericidal antibody (SBA) and opsonophagocytic killing antibody (OPKA) activities and investigated their potential association with protection against disease in humans. SBA, OPKA, and Ipa-, VirG (IscA)-, and Shigella flexneri 2a lipopolysaccharide-specific serum IgG titers were determined in adult volunteers who received Shigella vaccine candidate EcSf2a-2 and in unvaccinated controls, all of whom were challenged with virulent Shigella flexneri 2a. Prechallenge antibody titers were compared with disease severity after challenge. SBA and OPKA, as well as IpaB- and VirG-specific IgG, significantly correlated with reduced illness. SBA and OPKA assays were also used to evaluate the immunogenicity of leading live attenuated vaccine candidates Shigella CVD 1204 and CVD 1208S in humans. A single oral immunization with CVD 1204 or CVD 1208S resulted in SBA seroconversion rates of 71% and 47% and OPKA seroconversion rates of 57% and 35%, respectively. Higher functional antibody responses were induced by CVD 1204, which is consistent with its lower attenuation. This is the first demonstration of SBA, OPKA, and IpaB- and VirG-specific IgG levels as potential serological correlates of protection against shigellosis in humans. These results warrant further studies to establish their capacity to predict protective immunity and vaccine efficacy.
机译:志贺氏菌是生活在发展中国家幼儿中腹泻病的重要原因。没有获得批准的疫苗,除其他原因外,由于缺乏牢固的保护性免疫相关性,阻碍了候选疫苗的开发。为了解决这一知识空白,我们建立了定量检测方法,以测量志贺氏菌特异性血清杀菌抗体(SBA)和调理吞噬杀伤抗体(OPKA)的活性,并研究了它们与人类疾病防护的潜在联系。在接受志贺氏菌疫苗候选EcSf2a-2的成年志愿者和未接种疫苗的对照中确定了SBA,OPKA和Ipa-,VirG(IscA)-和弗氏志贺氏菌2a脂多糖特异性血清IgG滴度,所有受试者均接受了强力志贺氏菌攻击flexneri 2a。将激发前抗体的效价与激发后疾病的严重程度进行比较。 SBA和OPKA以及IpaB和​​VirG特异性IgG与疾病减少显着相关。 SBA和OPKA分析还用于评估人类主要减毒活疫苗候选志贺氏菌CVD 1204和CVD 1208S的免疫原性。用CVD 1204或CVD 1208S进行的单次口服免疫分别导致SBA血清转化率分别为71%和47%和OPKA血清转化率分别为57%和35%。 CVD 1204诱导了更高功能的抗体应答,这与其较低的衰减相符。这是SBA,OPKA以及IpaB和​​VirG特异性IgG水平的首次证明,它是人类抵抗志贺氏菌病的潜在潜在血清学相关因素。这些结果值得进一步研究,以建立其预测保护性免疫和疫苗功效的能力。

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