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23F型肺炎球菌合成寡糖和天然多糖-蛋白结合疫苗引发的兔免疫球蛋白G(IgG)的表位特异性:与人类抗23F多糖IgG的比较

Epitope specificity of rabbit immunoglobulin G (IgG) elicited by pneumococcal type 23F synthetic oligosaccharide- and native polysaccharide-protein conjugate vaccines: comparison with human anti-polysaccharide 23F IgG.

作者信息

Alonso de Velasco E, Verheul A F, van Steijn A M, Dekker H A, Feldman R G, Fernández I M, Kamerling J P, Vliegenthart J F, Verhoef J, Snippe H

机构信息

Eijkman-Winkler Laboratory of Medical Microbiology, Utrecht University, The Netherlands.

出版信息

Infect Immun. 1994 Mar;62(3):799-808. doi: 10.1128/iai.62.3.799-808.1994.

Abstract

Streptococcus pneumoniae type 23F capsular polysaccharide (PS23F) consitss of a repeating glycerol-phosphorylated branched tetrasaccharide. The immunogenicities of the following related antigens were investigated: (i) a synthetic trisaccharide comprising the backbone of one repeating unit, (ii) a synthetic tetrasaccharide comprising the complete repeating unit, and (iii) native PS23F (all three conjugated to keyhole limpet hemocyanin [KLH]) and (iv) formalin-killed S. pneumoniae 23F. All antigens except the trisaccharide-KLH conjugate induced relatively high anti-PS23F antibody levels in rabbits. The epitope specificity of such antibodies was then studied by means of an inhibition immunoassay. The alpha(1-->2)-linked L-rhamnose branch was shown to be immunodominant for immunoglobulin G (IgG) induced by tetrasaccharide-KLH, PS23F-KLH, and killed S. pneumoniae 23F: in most sera L-rhamnose totally inhibited the binding of IgG to PS23F. Thus, there appears to be no major difference in epitope specificity between IgG induced by tetrasaccharide-KLH and that induced by antigens containing the polymeric form of PS23F. Human anti-PS23F IgG (either vaccine induced or naturally acquired) had a different epitope specificity: none of the inhibitors used, including L-rhamnose and tetrasaccharide-KLH, exhibited substantial inhibition. These observations suggest that the epitope recognized by human IgG on PS23F is larger than the epitope recognized by rabbit IgG. Both human and rabbit antisera efficiently opsonized type 23F pneumococci, as measured in a phagocytosis assay using human polymorphonuclear leukocytes.

摘要

23F型肺炎链球菌荚膜多糖(PS23F)由重复的甘油磷酸化支链四糖组成。对以下相关抗原的免疫原性进行了研究:(i)一种包含一个重复单元主链的合成三糖,(ii)一种包含完整重复单元的合成四糖,以及(iii)天然PS23F(所有三种均与钥孔戚血蓝蛋白[KLH]偶联)和(iv)经福尔马林灭活的23F型肺炎链球菌。除三糖-KLH偶联物外,所有抗原均在兔体内诱导出相对较高的抗PS23F抗体水平。然后通过抑制免疫测定法研究此类抗体的表位特异性。结果显示,α(1→2)连接的L-鼠李糖分支对于由四糖-KLH、PS23F-KLH和灭活的23F型肺炎链球菌诱导产生的免疫球蛋白G(IgG)具有免疫显性:在大多数血清中,L-鼠李糖完全抑制了IgG与PS23F的结合。因此,由四糖-KLH诱导产生的IgG与由含有PS23F聚合形式的抗原诱导产生的IgG在表位特异性上似乎没有重大差异。人抗PS23F IgG(无论是疫苗诱导的还是自然获得的)具有不同的表位特异性:所使用的抑制剂,包括L-鼠李糖和四糖-KLH,均未表现出明显的抑制作用。这些观察结果表明,人IgG在PS23F上识别的表位大于兔IgG识别的表位。在使用人多形核白细胞的吞噬试验中测定发现,人抗血清和兔抗血清均能有效地调理23F型肺炎球菌。

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