Faculty Opinions recommendation of Constitutive crosspresentation of tissue antigens by dendritic cells controls CD8+ T cell tolerance in vivo.

Author(s):  
Paul Gleeson
Immunity ◽  
2008 ◽  
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Nancy Luckashenak ◽  
Samira Schroeder ◽  
Katrin Endt ◽  
Darja Schmidt ◽  
Karsten Mahnke ◽  
...  

2009 ◽  
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S. Brauer ◽  
C. Brenner ◽  
K. Lahl ◽  
H. Schild ◽  
...  

2008 ◽  
Vol 181 (1) ◽  
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Thomas Fehr ◽  
Fabienne Haspot ◽  
Joshua Mollov ◽  
Meredith Chittenden ◽  
Timothy Hogan ◽  
...  

2008 ◽  
Vol 181 (7) ◽  
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Christiane Dresch ◽  
Stephanie L. Edelmann ◽  
Peggy Marconi ◽  
Thomas Brocker

1997 ◽  
Vol 56 ◽  
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N. Parigon ◽  
C. Cambouris ◽  
J.-P. Abastado ◽  
P. Debré ◽  
...  

2002 ◽  
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Aaron C. Shur ◽  
Doley J. Hong ◽  
...  

CD8+ T cell tolerance to self-proteins prevents autoimmunity but represents an obstacle to generating T cell responses to tumor-associated antigens. We have made a T cell receptor (TCR) transgenic mouse specific for a tumor antigen and crossed TCR-TG mice to transgenic mice expressing the tumor antigen in hepatocytes (gag-TG). TCRxgag mice showed no signs of autoimmunity despite persistence of high avidity transgenic CD8+ T cells in the periphery. Peripheral CD8+ T cells expressed phenotypic markers consistent with antigen encounter in vivo and had upregulated the antiapoptotic molecule Bcl-2. TCRxgag cells failed to proliferate in response to antigen but demonstrated cytolytic activity and the ability to produce interferon γ. This split tolerance was accompanied by inhibition of Ca2+ flux, ERK1/2, and Jun kinasephosphorylation, and a block in both interleukin 2 production and response to exogenous interleukin 2. The data suggest that proliferation and expression of specific effector functions characteristic of reactive cells are not necessarily linked in CD8+ T cell tolerance.


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