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首页> 外文期刊>Journal of Clinical Microbiology >Humoral immune responses to VP4 and its cleavage products VP5* and VP8* in infants vaccinated with rhesus rotavirus.
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Humoral immune responses to VP4 and its cleavage products VP5* and VP8* in infants vaccinated with rhesus rotavirus.

机译:接种了恒河猴轮状病毒的婴儿对VP4及其裂解产物VP5 *和VP8 *的体液免疫反应。

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The humoral immune response to rhesus rotavirus (RRV) VP4 and its cleavage products VP5* and VP8* was determined in paired serum samples from 44 infants vaccinated with RRV or human rotavirus-RRV reassortants and 5 placebo recipients. Our aim was to try to measure the response to those regions of VP4 most closely related to protection. An enzyme-linked immunosorbent assay (ELISA) was used to measure the immunoglobulin G immune response to baculovirus-expressed full-length RRV VP4, full-length VP8*, and the amino-terminal polypeptide of VP5* called VP5*(1) (amino acids 248 to 474). The two antigenic regions of VP4 selected for study, VP5*(1) and VP8*, have previously been shown to contain most of the cross-reactive and strain-specific neutralization epitopes, respectively, while the remaining carboxy-terminal half of VP5* (amino acids 475 to 776) has not been clearly associated with neutralization. All three recombinant proteins were antigenically conserved, since they reacted with a library of neutralizing monoclonal antibodies directed at VP4. There was a high percentage of seroresponders to VP4 (61%) or to VP8* (52%), but fewer infants seroresponded to VP5*(1) (11%). In addition, infants responding to VP5*(1) had considerably lower titers than to VP4 or VP8*. Immune response to VP4 correlated strongly with the responses detected by the plaque reduction neutralization assay but did not correlate with the responses detected by the ELISA to whole RRV. These data imply that the VP5*(1) region is less immunogenic than the VP8* region of VP4 in infants immunized with RRV or RRV reassortants. The low immunogenicity of VP5* might adversely affect the efficacy of RRV vaccine candidates.
机译:在从44例接受RRV或人轮状病毒-RRV重新分类接种的婴儿和5名安慰剂接受者的配对血清样本中确定了对恒河猴轮状病毒(RRV)VP4及其裂解产物VP5 *和VP8 *的体液免疫应答。我们的目的是尝试评估对VP4与保护最相关的区域的反应。酶联免疫吸附试验(ELISA)用于测量对杆状病毒表达的全长RRV VP4,全长VP8 *和VP5 *的氨基末端多肽VP5 *(1)的免疫球蛋白G免疫反应(氨基酸248至474)。先前已显示选择用于研究的VP4的两个抗原区域VP5 *(1)和VP8 *分别包含大多数交叉反应和菌株特异性中和表位,而VP5 *的其余羧基末端一半(氨基酸475至776)尚未明确与中和相关。由于这三种重组蛋白都与针对VP4的中和单克隆抗体文库反应,因此在抗原上是保守的。 VP4(61%)或VP8 *(52%)的血清反应率较高,而VP5 *(1)的血清反应的婴儿率较低(11%)。此外,对VP5 *(1)有反应的婴儿的滴度明显低于对VP4或VP8 *的滴度。对VP4的免疫应答与噬斑减少中和试验检测到的应答高度相关,但与ELISA对整个RRV的检测的应答不相关。这些数据表明,在用RRV或RRV重配子免疫的婴儿中,VP5 *(1)区的免疫原性低于VP4的VP8 *区。 VP5 *的低免疫原性可能会对RRV候选疫苗的功效产生不利影响。

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