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Development of T-B cell collaboration in neonatal mice.

Authors :
Astori, M
Finke, D
Karapetian, O
Acha-Orbea, H
Source :
International Immunology; March 1999, Vol. 11 Issue: 3 p445-451, 7p
Publication Year :
1999

Abstract

The neonatal immune response is impaired during the first weeks after birth. To obtain a better understanding of this immaturity, we investigated the development of T cell interactions with B cells in mice. For this purpose, we analyzed the immune response to three T-dependent antigens in vivo: (i) the polyclonal antibody response induced by vaccinia virus; (ii) the production of polyclonal and specific antibodies following immunization with hapten-carrier conjugates; (iii) the mouse mammary tumor virus superantigen (sAg) response involving an increase in sAg-reactive T cells and induction of polyclonal antibody production. After vaccinia virus injection into neonates, the polyclonal antibody response was similar to that observed in adult mice. The antibody response to hapten-carrier conjugates, however, was delayed and reduced. Injection with sAg-expressing B cells from neonatal or adult mice allowed us to determine whether B cells, T cells or both were implicated in the reduced immune response. In these sAg responses, neonatal T cells were stimulated by both neonatal and adult sAg-presenting B cells but only B cells from adult mice differentiated into IgM- and IgG-secreting plasma cells in the neonatal environment in vivo. Injecting neonatal B cells into adult mice did not induce antibody production. These results demonstrate that the environment of the neonatal lymph node is able to support a T and B cell response, and that immaturity of B cells plays a key role in the reduced immune response observed in the neonate.

Details

Language :
English
ISSN :
09538178 and 14602377
Volume :
11
Issue :
3
Database :
Supplemental Index
Journal :
International Immunology
Publication Type :
Periodical
Accession number :
ejs63932159
Full Text :
https://doi.org/10.1093/intimm/11.3.445