Induction of dominant transplantation tolerance by an altered peptide ligand of the male antigen Dby
Tse-Ching Chen, … , Herman Waldmann, Paul J. Fairchild
Tse-Ching Chen, … , Herman Waldmann, Paul J. Fairchild
Published June 15, 2004
Citation Information: J Clin Invest. 2004;113(12):1754-1762. https://doi.org/10.1172/JCI20569.
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Article Immunology

Induction of dominant transplantation tolerance by an altered peptide ligand of the male antigen Dby

Abstract

T cell reactivity to minor histocompatibility (mH) antigens is responsible for rejection of HLA-matched allografts, limiting the effectiveness of transplantation for the treatment of end-stage organ failure. The deadbox gene Dby is located on the Y chromosome and encodes an mH antigen that prompts rejection of male tissues by female mice. Establishing a network of regulatory T (Treg) cells that is capable of coercing naive cells to adopt a tolerant phenotype offers an attractive strategy for immune intervention in such deleterious immune responses. While various approaches have successfully induced a dominant form of transplantation tolerance, they share the propensity to provoke chronic, incomplete activation of T cells. By identifying the T cell receptor (TCR) contact sites of the dominant epitope of the Dby gene product, we have designed an altered peptide ligand (APL) that delivers incomplete signals to naive T cells from A1 ∞ RAG1–/– mice that are transgenic for a complementary TCR. Administration of this APL to female transgenic mice polarizes T cells toward a regulatory phenotype, securing a form of dominant tolerance to male skin grafts that is capable of resisting rejection by naive lymphocytes. Our results demonstrate that incomplete signaling through the TCR may establish a network of Treg cells that may be harnessed in the service of transplantation tolerance.

Authors

Tse-Ching Chen, Herman Waldmann, Paul J. Fairchild

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Characterization of APLs bearing substitutions at critical TCR contact r...
Characterization of APLs bearing substitutions at critical TCR contact residues. (A) IL-2 release by 2G7.1 cultured in the presence of 0.5 ∝M HEL1–18 and a 100 ∝M excess of APLs. All APLs competed as efficiently as the cognate peptide for binding to H-2Ek with the exception of 484H Ø R, which bound with similar affinity to the control peptide, Dbx. (B) Proliferative responses of naive female A1 ∞ RAG1–/– T cells to APLs bearing conservative substitutions at critical TCR contact sites. All experiments were repeated at least twice and yielded similar results on each occasion.