Tumor cells convert immature myeloid dendritic cells into TGF-β–secreting cells inducing CD4+CD25+ regulatory T cell proliferation

Author:

Ghiringhelli François1,Puig Pierre E.1,Roux Stephan2,Parcellier Arnaud1,Schmitt Elise1,Solary Eric1,Kroemer Guido3,Martin François1,Chauffert Bruno1,Zitvogel Laurence2

Affiliation:

1. Institut National de la Santé et de la Recherche Médicale, U517, University of Burgundy, 21079 Dijon, France

2. ERM 0208, Institut National de la Santé et de la Recherche Médicale

3. UMR 8125, Centre National de la Recherche Scientifique, Institut Gustave Roussy, 94805 Villejuif, France

Abstract

The mechanisms through which regulatory T cells accumulate in lymphoid organs of tumor-bearing hosts remain elusive. Our experiments indicate that the accumulation of CD4+CD25+ regulatory T cells (T reg cells) expressing FoxP3 and exhibiting immunosuppressive function originates from the proliferation of naturally occurring CD25+ T cells and requires signaling through transforming growth factor (TGF)–β receptor II. During tumor progression, a subset of dendritic cells (DCs) exhibiting a myeloid immature phenotype is recruited to draining lymph nodes. This DC subset selectively promotes the proliferation of T reg cells in a TGF-β–dependent manner in mice and rats. Tumor cells are necessary and sufficient to convert DCs into regulatory cells that secrete bioactive TGF-β and stimulate T reg cell proliferation. In conclusion, tumor expansion can stimulate T reg cells via a specific DC subset.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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