首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Oligosaccharide conjugates of Bordetella pertussis and bronchiseptica induce bactericidal antibodies an addition to pertussis vaccine
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Oligosaccharide conjugates of Bordetella pertussis and bronchiseptica induce bactericidal antibodies an addition to pertussis vaccine

机译:百日咳博德特氏菌和支气管败血病的寡糖结合物可诱导杀菌抗体是百日咳疫苗的补充

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摘要

Pertussis is a highly contagious respiratory disease that is especially dangerous for infants and children. Despite mass vaccination, reported pertussis cases have increased in the United States and other parts of the world, probably because of increased awareness, improved diagnostic means, and waning vaccine-induced immunity among adolescents and adults. Licensed vaccines do not kill the organism directly; the addition of a component inducing bactericidal antibodies would improve vaccine efficacy. We investigated Bordetella pertussis and Bordetella bronchiseptica LPS-derived core oligosaccharide (OS) protein conjugates for their immunogenicity in mice. B. pertussis and B. bronchiseptica core OS were bound to aminooxylated BSA via their terminal Kdo residues. The two conjugates induced similar anti-B. pertussis LPS IgG levels in mice. B. bronchiseptica was investigated because it is easier to grow than B. pertussis. Using B. bronchiseptica genetically modified strains deficient in the O-specific polysaccharide, we isolated fractions of core OS with one to five repeats of the terminal trisaccharide, having at the nonreducing end a GlcNAc or GalNAc, and bound them to BSA at different densities. The highest antibody levels in mice were elicited by conjugates containing an average of 8–17 OS chains per protein and with one repeat of the terminal trisaccharide. Conjugate-induced antisera were bactericidal against B. pertussis, and the titers correlated with ELISA-measured antibody levels (r = 0.74). Such conjugates are easy to prepare and standardize; added to a recombinant pertussis toxoid, they may induce antibacterial and antitoxin immunity.
机译:百日咳是一种高度传染性的呼吸系统疾病,对婴儿和儿童特别危险。尽管进行了大规模疫苗接种,但在美国和世界其他地区,报告的百日咳病例有所增加,这可能是由于意识增强,诊断手段改善以及青少年和成人疫苗诱导的免疫力下降所致。经许可的疫苗不会直接杀死该生物。加入诱导杀菌抗体的成分将提高疫苗效力。我们调查了百日咳博德特氏菌和支气管博德特氏菌LPS衍生的核心寡糖(OS)蛋白偶联物在小鼠中的免疫原性。百日咳博德特氏菌和支气管败血性博德特氏菌核心OS通过其末端Kdo残基与氨氧基化BSA结合。两种结合物诱导相似的抗-B。百日咳小鼠LPS IgG水平。研究了支气管败血杆菌,因为它比百日咳杆菌更容易生长。使用缺乏O特异性多糖的支气管败血杆菌基因改造菌株,我们分离出具有一到五个末端三糖重复序列(在非还原端具有GlcNAc或GalNAc)的核心OS组分,并将它们以不同的密度与BSA结合。小鼠中最高的抗体水平是由每个蛋白平均包含8-17条OS链和末端三糖重复序列的缀合物引起的。共轭物诱导的抗血清对百日咳博德特氏菌具有杀菌作用,其滴度与ELISA测定的抗体水平相关(r = 0.74)。这样的结合物易于制备和标准化。如果将其添加到重组百日咳类毒素中,它们可能会诱导抗菌和抗毒素免疫。

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