Neonatal Exposure to Antigen Primes the Immune System to Develop Responses in Various Lymphoid Organs and Promotes Bystander Regulation of Diverse T Cell Specificities

Christopher D Pack; Aimee E Cestra; Booki Min; Kevin L Legge; Lequn Li; Jacque C Caprio-Young; J. Jeremiah Bell; Randal K Gregg; Habib Zaghouani

doi:10.4049/jimmunol.167.8.4187

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Neonatal Exposure to Antigen Primes the Immune System to Develop Responses in Various Lymphoid Organs and Promotes Bystander Regulation of Diverse T Cell Specificities

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Neonatal Exposure to Antigen Primes the Immune System to Develop Responses in Various Lymphoid Organs and Promotes Bystander Regulation of Diverse T Cell Specificities

Christopher D Pack, Aimee E Cestra, Booki Min, Kevin L Legge, Lequn Li, Jacque C Caprio-Young, J. Jeremiah Bell, Randal K Gregg and Habib Zaghouani

The Journal of immunology (1950), Vol.167(8), pp.4187-4195

10/15/2001

DOI: 10.4049/jimmunol.167.8.4187

PMID: 11591739

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Abstract

Neonatal exposure to Ag has always been considered suppressive for immunity. Recent investigations, however, indicated that the neonatal immune system could be guided to develop immunity. For instance, delivery of a proteolipid protein (PLP) peptide on Ig boosts the neonatal immune system to develop responses upon challenge with the PLP peptide later. Accordingly, mice given Ig-PLP at birth and challenged with the PLP peptide as adults developed proliferative T cells in the lymph node that produced IL-4 instead of the usual Th1 cytokines. However, the spleen was unresponsive unless IL-12 was provided. Herein, we wished to determine whether such a neonatal response is intrinsic to the PLP peptide or could develop with an unrelated myelin peptide as well as whether the T cell deviation is able to confer resistance to autoimmunity involving diverse T cell specificities. Accordingly, the amino acid sequence 87–99 of myelin basic protein was expressed on the same Ig backbone, and the resulting Ig-myelin basic protein chimera was tested for induction of neonatal immunity and protection against experimental allergic encephalomyelitis. Surprisingly, the results indicated that immunity developed in the lymph node and spleen, with deviation of T cells occurring in both organs. More striking, the splenic T cells produced IL-10 in addition to IL-4, providing an environment that facilitated bystander deviation of responses to unrelated epitopes and promoted protection against experimental allergic encephalomyelitis involving diverse T cell specificities. Thus, neonatal exposure to Ag can prime responses in various organs and sustain regulatory functions effective against diverse autoreactive T cells.

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Title: Subtitle: Neonatal Exposure to Antigen Primes the Immune System to Develop Responses in Various Lymphoid Organs and Promotes Bystander Regulation of Diverse T Cell Specificities
Creators: Christopher D Pack
Aimee E Cestra
Booki Min
Kevin L Legge
Lequn Li
Jacque C Caprio-Young
J. Jeremiah Bell
Randal K Gregg
Habib Zaghouani
Resource Type: Journal article
Publication Details: The Journal of immunology (1950), Vol.167(8), pp.4187-4195
DOI: 10.4049/jimmunol.167.8.4187
PMID: 11591739
NLM abbreviation: J Immunol
ISSN: 0022-1767
eISSN: 1550-6606
Language: English
Date published: 10/15/2001
Academic Unit: Microbiology and Immunology; Pathology
Record Identifier: 9984047885702771

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