TCR Reserve: A Novel Principle of CD4 T Cell Activation by Weak Ligands | Zendy

Lisa K. McNeil | Zendy; Brian D. Evavold | Zendy

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TCR Reserve: A Novel Principle of CD4 T Cell Activation by Weak Ligands

Author(s) -

Lisa K. McNeil,

Brian D. Evavold

Publication year - 2003

Publication title -

the journal of immunology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.737

H-Index - 372

eISSN - 1550-6606

pISSN - 0022-1767

DOI - 10.4049/jimmunol.170.3.1224

Subject(s) - t cell receptor , agonist , receptor , microbiology and biotechnology , thymocyte , biology , t cell , peptide , chemistry , immunology , biochemistry , immune system

Some ligand-receptor systems have a receptor reserve where a maximal response can be achieved by occupation of a fraction of available receptors. An implication of a receptor reserve is the expansion of the number of ligands for response. To determine whether T cells follow receptor reserve, we have characterized the effect of reducing TCR levels on CD4 T cell responses elicited by altered peptide ligands that vary in potency. Agonist peptide is unaffected by a 90% reduction in TCR level while proliferation to weak agonists is significantly inhibited when TCR expression is reduced by 40%. Thymocyte-negative selection similarly demonstrates a differential requirement of TCR for response to agonist, weak agonist, and partial agonist. Therefore, our data demonstrate receptor reserve as a novel principle of T cell activation in which excess TCRs expand the antigenic repertoire to include less potent ligands.

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