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首页> 外文OA文献 >A Single 17D Yellow Fever Vaccination Provides Lifelong Immunity; Characterization of Yellow-Fever-Specific Neutralizing Antibody and T-Cell Responses after Vaccination
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A Single 17D Yellow Fever Vaccination Provides Lifelong Immunity; Characterization of Yellow-Fever-Specific Neutralizing Antibody and T-Cell Responses after Vaccination

机译:一次17D黄热病疫苗可终生免疫;疫苗接种后黄热病特异性中和抗体和T细胞反应的表征

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Prompted by recent amendments of Yellow Fever (YF) vaccination guidelines from boost to single vaccination strategy and the paucity of clinical data to support this adjustment, we used the profile of the YF-specific CD8+ T-cell subset profiles after primary vaccination and neutralizing antibodies as a proxy for potentially longer lasting immunity. PBMCs and serum were collected in six individuals on days 0, 3, 5, 12, 28 and 180, and in 99 individuals >10 years after YF-vaccination. Phenotypic characteristics of YF- tetramer+ CD8+ T-cells were determined using class I tetramers. Antibody responses were measured using a standardized plaque reduction neutralization test (PRNT). Also, characteristics of YF-tetramer positive CD8+ T-cells were compared between individuals who had received a primary- and a booster vaccination. YF-tetramer+ CD8+ T-cells were detectable on day 12 (median tetramer+ cells as percentage of CD8+ T-cells 0.2%, range 0.07-3.1%). On day 180, these cells were still present (median 0.06%, range 0.02-0.78%). The phenotype of YF-tetramer positive CD8+ T-cells shifted from acute phase effector cells on day 12, to late differentiated or effector memory phenotype (CD45RA-/+CD27-) on day 28. Two subsets of YF-tetramer positive T-cells (CD45RA+CD27- and CD45RA+CD27+) persisted until day 180. Within all phenotypic subsets, the T-bet: Eomes ratio tended to be high on day 28 after vaccination and shifted towards predominant Eomes expression on day 180 (median 6.0 (day 28) vs. 2.2 (day 180) p = 0.0625), suggestive of imprinting compatible with long-lived memory properties. YF-tetramer positive CD8+ T-cells were detectable up to 18 years post vaccination, YF-specific antibodies were detectable up to 40 years after single vaccination. Booster vaccination did not increase titers of YF-specific antibodies (mean 12.5 vs. 13.1, p = 0.583), nor induce frequencies or alter phenotypes of YF-tetramer+ CD8+ T-cells. The presence of a functionally competent YF-specific memory T-cell pool 18 years and sufficient titers of neutralizing antibodies 35-40 years after first vaccination suggest that single vaccination may be sufficient to provide long-term immunity
机译:根据最近对黄热病(YF)疫苗接种指南从加强疫苗接种策略到单次接种策略的修订以及缺乏临床数据来支持这种调整的提示,我们使用了初次接种疫苗和中和抗体后YF特异性CD8 + T细胞亚群的概况作为潜在的更长久的免疫的代理。在接种YF疫苗后的第0、3、5、12、28和180天,有6个人收集了PBMC和血清,并在10年以上的99个人中收集了PBMC和血清。使用I类四聚体测定YF-四聚体+ CD8 + T细胞的表型特征。使用标准化噬斑减少中和测试(PRNT)测量抗体反应。而且,在接受初次和加强免疫的个体之间比较了YF-四聚体阳性CD8 + T细胞的特征。在第12天可检测到YF-四聚体+ CD8 + T细胞(中四聚体+细胞占CD8 + T细胞的百分比为0.2%,范围为0.07-3.1%)。在第180天,这些细胞仍然存在(中位数为0.06%,范围为0.02-0.78%)。 YF-四聚体阳性CD8 + T细胞的表型从第12天的急性期效应细胞转变为第28天的晚期分化或效应记忆表型(CD45RA-/ + CD27-)。YF-四聚体阳性T细胞的两个子集。 (CD45RA + CD27-和CD45RA + CD27 +)一直持续到第180天。在所有表型亚组中,疫苗接种后第28天的T-bet:Eomes比值趋于高,并在第180天转向主要Eomes表达(中位数6.0(第64天) 28)vs.2.2(180天)p = 0.0625),表明印记与长寿命的内存属性兼容。在接种疫苗后长达18年可检测到YF-四聚体阳性CD8 + T细胞,在接种疫苗后40年内可检测到YF特异性抗体。加强疫苗接种不会增加YF特异性抗体的滴度(平均12.5对13.1,p = 0.583),也不会诱导YF-tetramer + CD8 + T细胞的频率或改变其表型。首次疫苗接种后18年内,功能上有效的YF特异性记忆T细胞库的存在和中和抗体的足够滴度表明,单次疫苗接种可能足以提供长期免疫力

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