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Subunits of IgM Reconstitute Defective Contact Sensitivity in B-1 Cell-DeficientxidMice: κ Light Chains Recruit T Cells Independent of Complement
Author(s) -
Vipin Paliwal,
Ryohei Tsuji,
Marian Szczepanik,
Ivana Kawiková,
Régis A. Campos,
Manfred Kneilling,
Martin Röcken,
Janine Schuurman,
Frank A. Redegeld,
Frans P. Nijkamp,
Philip W. Askenase
Publication year - 2002
Publication title -
the journal of immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.737
H-Index - 372
eISSN - 1550-6606
pISSN - 0022-1767
DOI - 10.4049/jimmunol.169.8.4113
Subject(s) - hapten , pentamer , immunoglobulin light chain , b cell , bruton's tyrosine kinase , chemistry , antibody , microbiology and biotechnology , immunoglobulin m , cell , biology , immunology , immunoglobulin g , signal transduction , biochemistry , tyrosine kinase
The elicitation of contact sensitivity (CS) to local skin challenge with the hapten trinitrophenyl (TNP) chloride requires an early process that is necessary for local recruitment of CS-effector T cells. This is called CS initiation and is due to the B-1 subset of B cells activated at immunization to produce circulating IgM Ab. At challenge, the IgM binds hapten Ag in a complex that locally activates C to generate C5a that aids in T cell recruitment. In this study, we present evidence that CS initiation is indeed mediated by C-activating classic IgM anti-TNP pentamer. We further demonstrate the involvement of IgM subunits derived either from hybridomas or from lymphoid cells of actively immunized mice. Thus, reduced and alkylated anti-TNP IgM also initiates CS, likely due to generated H chain-L chain dimers, as does a mixture of separated H and L chains that still could weakly bind hapten, but could not activate C. Remarkably, anti-TNP kappa L chains alone mediated CS initiation that was C-independent, but was dependent on mast cells. Thus, B-1 cell-mediated CS initiation required for T cell recruitment is due to activation of C by specific IgM pentamer, and also subunits of IgM, while kappa L chains act via another C-independent but mast cell-dependent pathway.

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