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首页> 外文期刊>Vaccine >The 13-valent pneumococcal conjugate vaccine (PCV13) elicits cross-functional opsonophagocytic killing responses in humans to Streptococcus pneumoniae serotypes 6C and 7A
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The 13-valent pneumococcal conjugate vaccine (PCV13) elicits cross-functional opsonophagocytic killing responses in humans to Streptococcus pneumoniae serotypes 6C and 7A

机译:13价肺炎球菌结合疫苗(PCV13)引发人类对肺炎链球菌血清型6C和7A的跨功能性吞噬吞噬反应

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The introduction of a 7-valent pneumococcal conjugate vaccine (PCV7) in 2000 dramatically reduced the incidence of invasive pneumococcal disease (IPD) caused by the seven serotypes covered by the vaccine. Following the introduction of PCV7, which contains a serotype 6B conjugate, some decrease in IPD due to serotype 6A was noted suggesting that the serotype 68 conjugate provided some partial cross-protection against serotype 6A. However, no effect on serotype 6C was observed. In 2010, a pneumococcal conjugate vaccine with expanded serotype coverage (PCV13) was introduced that expanded the serotype coverage to 13 serotypes including serotype 6A. To assess whether the 6A conjugate in PCV13 could potentially induce functional anti-6C antibody responses, an opsonophagocytic assay (OPA) for serotype 6C was developed. Randomly chosen subsets of immune sera collected from infants receiving three doses of PCV7 or PCV13 were tested in OPA assays for serotype 6A, 6B and 6C. PCV7 immune sera demonstrated strong OPA responses, defined as percentage of subjects having an OPA titer >= 1:8, to serotype 6B (100% responders), partial responses to serotype 6A (70% responders) but only minimal responses to serotype 6C (22% responders). In contrast. PCV13 immune sera showed strong OPA responses to serotypes 6A (100% responders), 6B (100% responders) and 6C (96% responders). Furthermore, during pre-clinical work it was observed that serotype 7F (included in PCV13) and serotype 7A (not included in PCV13) shared serogroup-specific epitopes. To determine whether such epitopes also may be eliciting cross-functional antibody, PCV13 immune sera were also tested in serotype 7A and 7F OPA assays. All PCV13 immune sera demonstrated OPA responses to both of these serotypes. Taken together these results suggest that immunization with PCV13 has the potential to induce cross-protective responses to related serotypes not directly covered by the vaccine
机译:2000年引入7价肺炎球菌结合疫苗(PCV7)大大降低了由该疫苗涵盖的7种血清型引起的侵袭性肺炎球菌疾病(IPD)的发生率。在引入含有血清型6B缀合物的PCV7之后,注意到由于血清型6A导致IPD有所降低,这表明血清型68缀合物提供了针对血清型6A的部分交叉保护。然而,未观察到对血清型6C的影响。 2010年,引入了具有扩大的血清型覆盖率的肺炎球菌结合疫苗(PCV13),将血清型覆盖率扩大到13种血清型,包括6A型血清型。为了评估PCV13中的6A偶联物是否可能潜在诱导功能性抗6C抗体反应,开发了针对血清型6C的调理吞噬试验(OPA)。从接受三剂PCV7或PCV13的婴儿中收集的随机选择的免疫血清子集在6种血清型6A,6B和6C的OPA分析中进行了测试。 PCV7免疫血清表现出强烈的OPA反应,定义为对6B血清型(100%反应者)的OPA效价> = 1:8的受试者的百分比,对6A血清型(70%反应者)的部分反应,但对6C血清型只有极小的反应22%的回应者)。相反。 PCV13免疫血清显示出对血清型6A(100%反应者),6B(100%反应者)和6C(96%反应者)的强烈OPA反应。此外,在临床前工作期间,观察到血清型7F(包括在PCV13中)和血清型7A(不包括在PCV13中)共享血清群特异性表位。为了确定这些表位是否也可能引发交叉功能抗体,还在血清型7A和7F OPA分析中测试了PCV13免疫血清。所有PCV13免疫血清均显示对这两种血清型都有OPA反应。综上所述,这些结果表明,用PCV13进行免疫接种具有诱导针对疫苗未直接覆盖的相关血清型的交叉保护反应的潜力。

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