Antigen-specific Tregs control T cell responses against a limited repertoire of tumor antigens in patients with colorectal carcinoma
Andreas Bonertz, … , Moritz Koch, Philipp Beckhove
Andreas Bonertz, … , Moritz Koch, Philipp Beckhove
Published October 5, 2009
Citation Information: J Clin Invest. 2009;119(11):3311-3321. https://doi.org/10.1172/JCI39608.
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Research Article

Antigen-specific Tregs control T cell responses against a limited repertoire of tumor antigens in patients with colorectal carcinoma

Abstract

Spontaneous antitumor T cell responses in cancer patients are strongly controlled by Tregs, and increased numbers of tumor-infiltrating Tregs correlate with reduced survival. However, the tumor antigens recognized by Tregs in cancer patients and the impact of these cells on tumor-specific T cell responses have not been systematically characterized. Here we used a broad panel of long synthetic peptides of defined tumor antigens and normal tissue antigens to exploit a newly developed method to identify and compare ex vivo the antigen specificities of Tregs with those of effector/memory T cells in peripheral blood of colorectal cancer patients and healthy subjects. Tregs in tumor patients were highly specific for a distinct set of only a few tumor antigens, suggesting that Tregs exert T cell suppression in an antigen-selective manner. Tumor-specific effector T cells were detectable in the majority of colorectal cancer patients but not in healthy individuals. We detected differences in the repertoires of antigens recognized by Tregs and effector/memory T cells in the majority of colorectal cancer patients. In addition, only effector/memory T cell responses against antigens recognized by Tregs strongly increased after Treg depletion. The selection of antigens according to preexisting T cell responses may improve the efficacy of future immunotherapies for cancer and autoimmune disease.

Authors

Andreas Bonertz, Jürgen Weitz, Dong-Ho Kim Pietsch, Nuh N. Rahbari, Christoph Schlude, Yingzi Ge, Simone Juenger, Israel Vlodavsky, Khashayarsha Khazaie, Dirk Jaeger, Christoph Reissfelder, Dalibor Antolovic, Maximilian Aigner, Moritz Koch, Philipp Beckhove

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Figure 5

Specificity of Tregs for TAAs in CRC patients and healthy donors.

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Specificity of Tregs for TAAs in CRC patients and healthy donors. (A) Sc...
(A) Scheme for determination of Treg specificity. DCs were pulsed with TAA polypeptide or control antigen. Autologous Tregs were added. Tregs specific for an antigen presented by the DCs were selectively activated. Polyclonally activated Teffs were added to the DCs and Tregs. Tregs activated by their respective antigen then suppressed the proliferation of the Teffs, which was measured by [3H]thymidine incorporation. (B and C) Primary data of 2 representative Treg specificity experiments displaying selective suppression of proliferation in wells where DCs were pulsed with HER2/neu and CEA (B) or telomerase (C). DC, no antigen added. Data represent mean counts per minute of 3 wells per antigen ± SEM; *P < 0.05, counts in test wells compared with pooled counts of negative control antigen (2-tailed Student’s t test). (D) CRC patients and healthy donors were tested for the presence of TAA-specific Tregs. Data represent the percentage of individuals with Tregs specific for the respective antigen; CRC patients, n = 14–56; HD, n = 10–14.