Targeting antigen to CD19 on B cells efficiently activates T cells

Jun Yan; Martin J. Wolff; Julia Unternaehrer; Ira Mellman; Mark J. Mamula

doi:10.1093/intimm/dxh266

Targeting antigen to CD19 on B cells efficiently activates T cells

Jun Yan, Martin J. Wolff, Julia Unternaehrer, Ira Mellman, Mark J. Mamula

Research output: Contribution to journal › Article › peer-review

Abstract

CD19 is a B cell-surface molecule that participates as an important regulatory signaling complex for antigen bound at the surface by Ig. Triggering of CD19 through its linkage with CD21 amplifies signals transduced through the Src family kinases and modulates B cell differentiation in response to antigen. This study examines the kinetics of antigen uptake and processing of antigen directly targeted to the CD19 protein on purified B cells. We have demonstrated that the antigen internalized within minutes through CD19 forms a cap at the B cell surface and can be found within lysosomes in the cytoplasm in 90 min. B cells acquiring antigen via CD19 express elevated levels of B7-1 and B7-2 co-stimulatory molecules. Moreover, antigen-anti-CD19 complexes administered intravenously bind B cells in vivo and activate antigen-specific T cells more efficiently than non-specific uptake and in a manner similar to antigen taken up through surface IgM on B cells. This work illustrates an important and previously unrecognized mechanism for targeting proteins to B lymphocytes for antigen presentation and activation of CD4 T cells.

Original language	English
Pages (from-to)	869-877
Number of pages	9
Journal	International Immunology
Volume	17
Issue number	7
DOIs	https://doi.org/10.1093/intimm/dxh266
State	Published - Jul 2005

ASJC Scopus Subject Areas

Immunology and Allergy
Immunology

Keywords

Antigen presentation
CD19
T cell activation

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title = "Targeting antigen to CD19 on B cells efficiently activates T cells",

abstract = "CD19 is a B cell-surface molecule that participates as an important regulatory signaling complex for antigen bound at the surface by Ig. Triggering of CD19 through its linkage with CD21 amplifies signals transduced through the Src family kinases and modulates B cell differentiation in response to antigen. This study examines the kinetics of antigen uptake and processing of antigen directly targeted to the CD19 protein on purified B cells. We have demonstrated that the antigen internalized within minutes through CD19 forms a cap at the B cell surface and can be found within lysosomes in the cytoplasm in 90 min. B cells acquiring antigen via CD19 express elevated levels of B7-1 and B7-2 co-stimulatory molecules. Moreover, antigen-anti-CD19 complexes administered intravenously bind B cells in vivo and activate antigen-specific T cells more efficiently than non-specific uptake and in a manner similar to antigen taken up through surface IgM on B cells. This work illustrates an important and previously unrecognized mechanism for targeting proteins to B lymphocytes for antigen presentation and activation of CD4 T cells.",

keywords = "Antigen presentation, CD19, T cell activation",

author = "Jun Yan and Wolff, {Martin J.} and Julia Unternaehrer and Ira Mellman and Mamula, {Mark J.}",

note = "Funding Information: This study was supported by grants from the SLE Foundation to J.Y., the Ethel F. Donaghue Women{\textquoteright}s Investigator Program at Yale University and the National Institutes of Health (NIH) (AR41032, AI-36529 and AI-48120) to M.J.M. The work was also supported by NIH grant AI-34098 and the Ludwig Institute for Cancer Research to I.M. We would like to thank Renelle Gee for her outstanding technical assistance and Mark Shlomchik for his important scientific discussion and reviewing the manuscript.",

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AU - Wolff, Martin J.

AU - Unternaehrer, Julia

AU - Mellman, Ira

AU - Mamula, Mark J.

N1 - Funding Information: This study was supported by grants from the SLE Foundation to J.Y., the Ethel F. Donaghue Women’s Investigator Program at Yale University and the National Institutes of Health (NIH) (AR41032, AI-36529 and AI-48120) to M.J.M. The work was also supported by NIH grant AI-34098 and the Ludwig Institute for Cancer Research to I.M. We would like to thank Renelle Gee for her outstanding technical assistance and Mark Shlomchik for his important scientific discussion and reviewing the manuscript.

PY - 2005/7

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N2 - CD19 is a B cell-surface molecule that participates as an important regulatory signaling complex for antigen bound at the surface by Ig. Triggering of CD19 through its linkage with CD21 amplifies signals transduced through the Src family kinases and modulates B cell differentiation in response to antigen. This study examines the kinetics of antigen uptake and processing of antigen directly targeted to the CD19 protein on purified B cells. We have demonstrated that the antigen internalized within minutes through CD19 forms a cap at the B cell surface and can be found within lysosomes in the cytoplasm in 90 min. B cells acquiring antigen via CD19 express elevated levels of B7-1 and B7-2 co-stimulatory molecules. Moreover, antigen-anti-CD19 complexes administered intravenously bind B cells in vivo and activate antigen-specific T cells more efficiently than non-specific uptake and in a manner similar to antigen taken up through surface IgM on B cells. This work illustrates an important and previously unrecognized mechanism for targeting proteins to B lymphocytes for antigen presentation and activation of CD4 T cells.

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Targeting antigen to CD19 on B cells efficiently activates T cells

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ASJC Scopus Subject Areas

Keywords

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