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Relationship between CD8-dependent antigen recognition,T cell functional avidity,and tumor cell recognition
Authors:Tamson V. Moore  Gretchen E. Lyons  Natasha Brasic  Jeffrey J. Roszkowski  Simon Voelkl  Andreas Mackensen  W. Martin Kast  I. Caroline Le Poole  Michael I. Nishimura
Affiliation:(1) Department of Surgery, The University of Chicago, Chicago, IL 60637, USA;(2) Department of Internal Medicine 5, Hematology/Oncology, University of Erlangen, 91054 Erlangen, Germany;(3) Norris Comprehensive Cancer Center, University of Southern California, Los Angeles, CA 90033, USA;(4) Departments of Molecular Microbiology &; Immunology and Obstetrics &; Gynecology, University of Southern California, Los Angeles, CA 90033, USA;(5) Departments of Pathology and Microbiology &; Immunology, Loyola University Medical Center, Maywood, IL 60153, USA;(6) Department of Surgery, Medical University of South Carolina, 86 Jonathan Lucas Street, Suite 512H, P.O. Box 250613, Charleston, USA;
Abstract:Effective immunotherapy using T cell receptor (TCR) gene-modified T cells requires an understanding of the relationship between TCR affinity and functional avidity of T cells. In this study, we evaluate the relative affinity of two TCRs isolated from HLA-A2-restricted, gp100-reactive T cell clones with extremely high functional avidity. Furthermore, one of these T cell clones, was CD4CD8 indicating that antigen recognition by this clone was CD8 independent. However, when these TCRs were expressed in CD8 Jurkat cells, the resulting Jurkat cells recognized gp100:209–217 peptide loaded T2 cells and had high functional avidity, but could not recognize HLA-A2+ melanoma cells expressing gp100. Tumor cell recognition by Jurkat cells expressing these TCRs could not be induced by exogenously loading the tumor cells with the native gp100:209–217 peptide. These results indicate that functional avidity of a T cell does not necessarily correlate with TCR affinity and CD8-independent antigen recognition by a T cell does not always mean its TCR will transfer CD8-independence to other effector cells. The implications of these findings are that T cells can modulate their functional avidity independent of the affinity of their TCRs. Companion Paper: “Characterization of MHC class-I restricted TCRαβ+ CD4 CD8 double negative T cells recognizing the gp100 antigen from a melanoma patient after gp100 vaccination” by Simon Voelkl, Tamson V. Moore, Michael Rehli, Michael I. Nishimura, Andreas Mackensen, and Karin Fischer. doi:.
Keywords:T cells  TCR  Melanoma  Affinity
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