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Literature DB >> 30009548

Molecular properties of gp100-reactive T-cell receptors drive the cytokine profile and antitumor efficacy of transgenic host T cells.

Jonathan M Eby¹, Angela R Smith², Timothy P Riley², Cormac Cosgrove³, Christian M Ankney¹, Steven W Henning³, Chrystal M Paulos⁴, Elizabeth Garrett-Mayer⁵, Rosalie M Luiten^6,7, Michael I Nishimura^1,8, Brian M Baker², I Caroline Le Poole^1,3,9.

Abstract

To study the contribution of T-cell receptors (TCR) to resulting T-cell responses, we studied three different human αβ TCRs, reactive to the same gp100-derived peptide presented in the context of HLA-A*0201. When expressed in primary CD8 T cells, all receptors elicited classic antigen-induced IFN-γ responses, which correlated with TCR affinity for peptide-MHC in the order T4H2 > R6C12 > SILv44. However, SILv44 elicited superior IL-17A release. Importantly, in vivo, SILv44-transgenic T cells mediated superior antitumor responses to 888-A2 + human melanoma tumor cells upon adoptive transfer into tumor-challenged mice while maintaining IL-17 expression. Modeling of the TCR ternary complexes suggested architectural differences between SILv44 and the other complexes, providing a potential structural basis for the observed differences. Overall, the data reveal a more prominent role for the T-cell receptor in defining host T-cell physiology than traditionally assumed, while parameters beyond IFN-γ secretion and TCR affinity ultimately determine the reactivity of tumor-reactive T cells.

Entities: CellLine Chemical Disease Gene Species

Keywords: IL-17A; T-cell receptor; melanoma; molecular modeling; transgenic T cells

Mesh：

Substances：

Year: 2018 PMID： 30009548 PMCID： PMC6309485 DOI： 10.1111/pcmr.12724

Source DB: PubMed Journal: Pigment Cell Melanoma Res ISSN： 1755-1471 Impact factor: 4.693

39 in total

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