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首页> 外文期刊>Clinical and vaccine immunology: CVI >CD46 Measles Virus Receptor Polymorphisms Influence Receptor Protein Expression and Primary Measles Vaccine Responses in Naive Australian Children
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CD46 Measles Virus Receptor Polymorphisms Influence Receptor Protein Expression and Primary Measles Vaccine Responses in Naive Australian Children

机译:CD46麻疹病毒受体多态性影响幼稚的澳大利亚儿童中的受体蛋白表达和初级麻疹疫苗反应。

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Despite the availability of measles vaccines, infants continue to die from measles. Measles vaccine responses vary between individuals, and poor immunogenicity is likely to preclude protection against measles. CD46 is a ubiquitously expressed specific receptor for vaccine strains of measles virus. CD46 polymorphisms have not been functionally investigated but may affect CD46 protein expression, which in turn may mediate primary measles antibody responses in infants. In a cohort of children aged 12 to 14 months from Perth, Australia (n = 137), after their first dose of measles-mumps-rubella (MMR) vaccine, CD46 polymorphisms were genotyped, and postvaccination measles IgG and CD46 protein expression before and after measles lysate stimulation of cells were measured. Three CD46 variants (rs7144, rs11118580, and rs2724384) were significantly associated with measles virus-specific IgG levels (P = 0.008, P = 0.026, and P = 0.018, respectively). There were significant differences between CD46 rs7144 genotypes and CD46 protein expression on T cells, as well as the downregulation of CD46 and T-cell frequency after measles lysate stimulation. We show that CD46 polymorphisms were associated with primary measles antibody responses in naive infants. We also report the first association of a measles virus receptor polymorphism with functional effects on the receptor, suggesting a possible mechanism through which antibody responses are altered. Elucidating all of the interconnecting genetic factors that alter primary measles vaccine responses may be important for identifying children at risk of poor immunogenicity or vaccine failure and for the future design of vaccine strategies to help these children.
机译:尽管有麻疹疫苗可用,婴儿仍死于麻疹。麻疹疫苗的反应因人而异,且免疫原性差可能会阻止针对麻疹的保护。 CD46是麻疹病毒疫苗株普遍表达的特异性受体。 CD46 多态性尚未经过功能研究,但可能影响CD46蛋白表达,进而可能介导婴儿的麻疹原发性抗体应答。在一群来自澳大利亚珀斯的12至14个月大的儿童中( n = 137),他们首次接种了麻疹,腮腺炎,风疹(MMR)疫苗后,即为 CD46 对基因多态性进行基因分型,并测量疫苗接种后麻疹裂解液刺激细胞前后麻疹IgG和CD46蛋白的表达。三种 CD46 变体(rs7144,rs11118580和rs2724384)与麻疹病毒特异性IgG水平显着相关( P = 0.008, P = 0.026 ,并且 P 分别为0.018)。麻疹溶胞产物刺激后, CD46 rs7144基因型和CD46蛋白在T细胞上的表达,CD46和T细胞频率的下调之间存在显着差异。我们显示 CD46 多态性与幼稚婴儿的初级麻疹抗体反应有关。我们还报告了麻疹病毒受体多态性与对该受体的功能作用的首次关联,表明抗体反应通过其改变的可能机制。阐明所有改变主要麻疹疫苗反应的相互关联的遗传因素,对于鉴定具有低免疫原性或疫苗失败风险的儿童以及未来设计帮助这些儿童的疫苗策略可能是重要的。

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