Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation

In vivo GITR ligation has previously been shown to augment T-cell-mediated anti-tumor immunity, yet the underlying mechanisms of this activity, particularly its in vivo effects on CD4+ foxp3+ regulatory T cells (Tregs), have not been fully elucidated. In order to translate this immunotherapeutic app...

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Autores principales: Cohen, Adam D., Schaer, David A., Liu, Cailian, Li, Yanyun, Hirschhorn-Cymmerman, Daniel, Kim, Soo Chong, Diab, Adi, Rizzuto, Gabrielle, Duan, Fei, Perales, Miguel A., Merghoub, Taha, Houghton, Alan N., Wolchok, Jedd D.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2862699/
https://www.ncbi.nlm.nih.gov/pubmed/20454651
http://dx.doi.org/10.1371/journal.pone.0010436
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author Cohen, Adam D.
Schaer, David A.
Liu, Cailian
Li, Yanyun
Hirschhorn-Cymmerman, Daniel
Kim, Soo Chong
Diab, Adi
Rizzuto, Gabrielle
Duan, Fei
Perales, Miguel A.
Merghoub, Taha
Houghton, Alan N.
Wolchok, Jedd D.
author_facet Cohen, Adam D.
Schaer, David A.
Liu, Cailian
Li, Yanyun
Hirschhorn-Cymmerman, Daniel
Kim, Soo Chong
Diab, Adi
Rizzuto, Gabrielle
Duan, Fei
Perales, Miguel A.
Merghoub, Taha
Houghton, Alan N.
Wolchok, Jedd D.
author_sort Cohen, Adam D.
collection PubMed
description In vivo GITR ligation has previously been shown to augment T-cell-mediated anti-tumor immunity, yet the underlying mechanisms of this activity, particularly its in vivo effects on CD4+ foxp3+ regulatory T cells (Tregs), have not been fully elucidated. In order to translate this immunotherapeutic approach to the clinic it is important gain better understanding of its mechanism(s) of action. Utilizing the agonist anti-GITR monoclonal antibody DTA-1, we found that in vivo GITR ligation modulates regulatory T cells (Tregs) directly during induction of melanoma tumor immunity. As a monotherapy, DTA-1 induced regression of small established B16 melanoma tumors. Although DTA-1 did not alter systemic Treg frequencies nor abrogate the intrinsic suppressive activity of Tregs within the tumor-draining lymph node, intra-tumor Treg accumulation was significantly impaired. This resulted in a greater Teff:Treg ratio and enhanced tumor-specific CD8+ T-cell activity. The decreased intra-tumor Treg accumulation was due both to impaired infiltration, coupled with DTA-1-induced loss of foxp3 expression in intra-tumor Tregs. Histological analysis of B16 tumors grown in Foxp3-GFP mice showed that the majority of GFP+ cells had lost Foxp3 expression. These “unstable” Tregs were absent in IgG-treated tumors and in DTA-1 treated TDLN, demonstrating a tumor-specific effect. Impairment of Treg infiltration was lost if Tregs were GITR(−/−), and the protective effects of DTA-1 were reduced in reconstituted RAG1(−/−) mice if either the Treg or Teff subset were GITR-negative and absent if both were negative. Our results demonstrate that DTA-1 modulates both Teffs and Tregs during effective tumor treatment. The data suggest that DTA-1 prevents intra-tumor Treg accumulation by altering their stability, and as a result of the loss of foxp3 expression, may modify their intra-tumor suppressive capacity. These findings provide further support for the continued development of agonist anti-GITR mAbs as an immunotherapeutic strategy for cancer.
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spelling pubmed-28626992010-05-07 Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation Cohen, Adam D. Schaer, David A. Liu, Cailian Li, Yanyun Hirschhorn-Cymmerman, Daniel Kim, Soo Chong Diab, Adi Rizzuto, Gabrielle Duan, Fei Perales, Miguel A. Merghoub, Taha Houghton, Alan N. Wolchok, Jedd D. PLoS One Research Article In vivo GITR ligation has previously been shown to augment T-cell-mediated anti-tumor immunity, yet the underlying mechanisms of this activity, particularly its in vivo effects on CD4+ foxp3+ regulatory T cells (Tregs), have not been fully elucidated. In order to translate this immunotherapeutic approach to the clinic it is important gain better understanding of its mechanism(s) of action. Utilizing the agonist anti-GITR monoclonal antibody DTA-1, we found that in vivo GITR ligation modulates regulatory T cells (Tregs) directly during induction of melanoma tumor immunity. As a monotherapy, DTA-1 induced regression of small established B16 melanoma tumors. Although DTA-1 did not alter systemic Treg frequencies nor abrogate the intrinsic suppressive activity of Tregs within the tumor-draining lymph node, intra-tumor Treg accumulation was significantly impaired. This resulted in a greater Teff:Treg ratio and enhanced tumor-specific CD8+ T-cell activity. The decreased intra-tumor Treg accumulation was due both to impaired infiltration, coupled with DTA-1-induced loss of foxp3 expression in intra-tumor Tregs. Histological analysis of B16 tumors grown in Foxp3-GFP mice showed that the majority of GFP+ cells had lost Foxp3 expression. These “unstable” Tregs were absent in IgG-treated tumors and in DTA-1 treated TDLN, demonstrating a tumor-specific effect. Impairment of Treg infiltration was lost if Tregs were GITR(−/−), and the protective effects of DTA-1 were reduced in reconstituted RAG1(−/−) mice if either the Treg or Teff subset were GITR-negative and absent if both were negative. Our results demonstrate that DTA-1 modulates both Teffs and Tregs during effective tumor treatment. The data suggest that DTA-1 prevents intra-tumor Treg accumulation by altering their stability, and as a result of the loss of foxp3 expression, may modify their intra-tumor suppressive capacity. These findings provide further support for the continued development of agonist anti-GITR mAbs as an immunotherapeutic strategy for cancer. Public Library of Science 2010-05-03 /pmc/articles/PMC2862699/ /pubmed/20454651 http://dx.doi.org/10.1371/journal.pone.0010436 Text en Cohen et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Cohen, Adam D.
Schaer, David A.
Liu, Cailian
Li, Yanyun
Hirschhorn-Cymmerman, Daniel
Kim, Soo Chong
Diab, Adi
Rizzuto, Gabrielle
Duan, Fei
Perales, Miguel A.
Merghoub, Taha
Houghton, Alan N.
Wolchok, Jedd D.
Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation
title Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation
title_full Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation
title_fullStr Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation
title_full_unstemmed Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation
title_short Agonist Anti-GITR Monoclonal Antibody Induces Melanoma Tumor Immunity in Mice by Altering Regulatory T Cell Stability and Intra-Tumor Accumulation
title_sort agonist anti-gitr monoclonal antibody induces melanoma tumor immunity in mice by altering regulatory t cell stability and intra-tumor accumulation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2862699/
https://www.ncbi.nlm.nih.gov/pubmed/20454651
http://dx.doi.org/10.1371/journal.pone.0010436
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