Abstract

The T cell compartment of adaptive immunity provides vertebrates with the potential to survey for and respond specifically to an incredible diversity of antigens. The T cell repertoire must be carefully regulated to prevent unwanted responses to self. In the periphery, one important level of regulation is the action of costimulatory signals in concert with T cell antigen-receptor (TCR) signals to promote full T cell activation. The past few years have revealed that costimulation is quite complex, involving an integration of activating signals and inhibitory signals from CD28 and CTLA-4 molecules, respectively, with TCR signals to determine the outcome of a T cell's encounter with antigen. Newly emerging data suggest that inhibitory signals mediated by CTLA-4 not only can determine whether T cells become activated, but also can play a role in regulating the clonal representation in a polyclonal response. This review primarily focuses on the cellular and molecular mechanisms of regulation by CTLA-4 and its manipulation as a strategy for tumor immunotherapy.

Keywords

BiologyCD28T-cell receptorT cellImmunotherapyAntigenCTLA-4Cell biologyImmunologyImmune system

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Publication Info

Year
2001
Type
review
Volume
19
Issue
1
Pages
565-594
Citations
977
Access
Closed

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Cynthia A. Chambers, Michael S. Kuhns, Jackson G. Egen et al. (2001). CTLA-4-Mediated Inhibition in Regulation of T Cell Responses: Mechanisms and Manipulation in Tumor Immunotherapy. Annual Review of Immunology , 19 (1) , 565-594. https://doi.org/10.1146/annurev.immunol.19.1.565

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DOI
10.1146/annurev.immunol.19.1.565