The carboxyl-terminal domains of IgA and IgM direct Isotype-specific polymerization and interaction with the polymeric immunoglobulin receptor

被引:37
作者
Braathen, R [1 ]
Sorensen, V
Brandtzaeg, P
Sandlie, I
Johansen, FE
机构
[1] Univ Oslo, Inst Pathol, Rikshosp, Lab Immunohistochem & Immunopathol, N-0027 Oslo, Norway
[2] Univ Oslo, Inst Biol, Dept Mol Cell Biol, N-0316 Oslo, Norway
关键词
D O I
10.1074/jbc.M205502200
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Mucosal surfaces are protected by polymeric immunoglobulins that are transported across the epithelium by the polymeric immunoglobulin receptor (pIgR). Only polymeric IgA and IgM containing a small polypeptide called the "joining" (J) chain can bind to the pIgR. J chain-positive IgA consists of dimers, and some larger polymers, whereas only IgM pentamers incorporate the J chain. We made domain swap chimeras between human IgA1 and IgM and found that the COOH-terminal domains of the heavy chains (Calpha3 and Cmu4, respectively) dictated the size of the polymers formed and also which polymers incorporated the J chain. We also showed that chimeric IgM molecules engineered to contain Calpha3 were able to bind the rabbit pIgR. Since the rabbit pIgR normally does not bind IgM, these results suggest that the COOH-terminal domain of the polymeric immunoglobulins is primarily responsible for interaction with the pIgR. Finally, we made a novel chimeric IgA immunoglobulin, containing the terminal domain from IgM. This recombinant molecule formed J chain-containing pentamers that could, like IgA, efficiently form covalent complexes with the human pIgR ectodomain, known as secretory component.
引用
收藏
页码:42755 / 42762
页数:8
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