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Cross-neutralizing antibodies elicited by the Cervarix® human papillomavirus vaccine display a range of Alpha-9 inter-type specificities

机译:Cervarix®人乳头瘤病毒疫苗引发的交叉中和抗体显示出多种Alpha-9类型间特异性

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摘要

The highly efficacious human papillomavirus (HPV) vaccines contain virus-like particles (VLP) representing genotypes HPV16 and HPV18, which together account for approximately 70% of cervical cancer cases. Vaccine-type protection is thought to be mediated by high titer, type-specific neutralizing antibodies. The vaccines also confer a degree of cross-protection against some genetically-related types from the Alpha-9 (HPV16-like: HPV31, HPV33, HPV35, HPV52, HPV58) and Alpha-7 (HPV18-like: HPV39, HPV45, HPV59, HPV68) species groups. Cross-protection is coincident with the detection of low titer serum responses against non-vaccine types by vaccinees. Such antibodies may be the effectors of cross-protection or their detection may be useful as a correlate or surrogate.This study evaluated whether cross-neutralization of HPV types from the Alpha-9 species group is mediated by antibodies with a predominantly type-restricted specificity for HPV16 that nevertheless exhibit low affinity interactions with non-vaccine types, or by antibody specificities that demonstrate similar recognition of vaccine and non-vaccine types but are present at very low levels.Antibodies generated following Cervarix® vaccination of 13–14 year old girls were evaluated by pseudovirus neutralization, VLP ELISA and by enrichment of target antigen specificity using VLP-immobilized beads. Two-dimensional hierarchical clustering of serology data demonstrated that the antibody specificity profile generated by VLP ELISA was both quantitatively and qualitatively different from the neutralizing antibody specificity profile. Target-specific antibody enrichment demonstrated that cross-neutralization of non-vaccine types was due to a minority of antibodies rather than by the weak interactions of a predominantly type-restricted HPV16 antibody specificity. Furthermore, cross-neutralization of non-vaccine types appeared to be mediated by multiple antibody specificities, recognizing single and multiple non-vaccine types, and whose specificities were not predictable from examination of the serum neutralizing antibody profile. These data contribute to our understanding of the antibody specificities elicited following HPV vaccination and have potential implications for vaccine-induced cross-protection.
机译:高效人乳头瘤病毒(HPV)疫苗含有代表基因型HPV16和HPV18的病毒样颗粒(VLP),它们合起来约占宫颈癌病例的70%。疫苗类型的保护被认为是由高滴度,类型特异性的中和抗体介导的。疫苗还赋予一定程度的交叉保护,以抵抗来自Alpha-9(类似于HPV16:HPV31,HPV33,HPV35,HPV52,HPV58)和Alpha-7(类似于HPV18:HPV39,HPV45,HPV59)的某些与遗传相关的类型(HPV68)物种组。交叉保护与疫苗接种者检测到针对非疫苗类型的低滴度血清反应相吻合。此类抗体可能是交叉保护的效应子,或者它们的检测可能用作相关或替代。这项研究评估了来自Alpha-9物种组的HPV类型的交叉中和作用是否是由主要具有类型限制特异性的抗体介导的对于HPV16而言,与非疫苗类型表现出低亲和力相互作用,或通过抗体特异性表现出对疫苗和非疫苗类型的相似识别,但含量却非常低.Cervarix ®疫苗接种后产生的抗体通过假病毒中和,VLP ELISA和使用固定VLP的磁珠富集靶抗原特异性,对13-14岁女孩进行了评估。血清学数据的二维分层聚类表明,VLP ELISA产生的抗体特异性谱与中和抗体特异性谱在数量和质量上都不同。靶标特异性抗体的富集证明非疫苗类型的交叉中和是由于少数抗体引起的,而不是由于主要受类型限制的HPV16抗体特异性的弱相互作用。此外,非疫苗类型的交叉中和似乎是由多种抗体特异性介导的,识别出一种和多种非疫苗类型,并且其特异性是无法通过检查血清中和抗体谱来预测的。这些数据有助于我们理解HPV疫苗接种后引起的抗体特异性,并可能对疫苗诱导的交叉保护产生潜在影响。

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