Yves Montier scite author profile

Regulatory T cells (Tregs) may impede cancer vaccine efficacy in hematologic malignancies and cancer. CCR4 antagonists, an emergent class of Treg inhibitor, have been shown to block recruitment of Tregs mediated by CCL22 and CCL17. Our aim was to demonstrate the ability of a CCR4 antagonist (a small chemical molecule identified in silico) when combined with vaccines to break peripheral tolerance controlled by Tregs, a prerequisite for the induction of CD8(+) T cells against self Ags. Immunization of transgenic or normal mice expressing tumor-associated self Ags (Her2/neu, OVA, gp100) with a CCR4 antagonist combined with various vaccines led to the induction of effector CD8(+) T cells and partial inhibition of tumor growth expressing self Ags in both prophylactic and therapeutic settings. The CCR4 antagonist was more efficient than cyclophosphamide to elicit anti-self CD8(+) T cells. We also showed that the population of Tregs expressing CCR4 corresponded to memory (CD44(high)) and activated (ICOS(+)) Tregs, an important population to be targeted to modulate Treg activity. CCR4 antagonist represents a competitive class of Treg inhibitor able to induce functional anti-self CD8(+) T cells and tumor growth inhibition when combined with vaccines. High expression of CCR4 on human Tregs also supports the clinical development of this strategy.

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Central role of IL-6 and MMP-1 for cross talk between human intestinal mast cells and human intestinal fibroblasts

Montier¹,

Lorentz²,

Krämer³

et al. 2012

Immunobiology

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Immunothérapie des cancers

Quintin-Colonna¹,

Montier²,

Péré³

et al. 2009

bavf

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Des cellules tumorales peuvent être reconnues par le système immunitaire qui contrôle le développement de certaines tumeurs. L’immunothérapie anti-tumorale consiste à stimuler cette immunité naturelle contre les cancers. L’emploi de cytokines recombinantes (IL-2, IFNα …) et surtout d’anticorps a permis de démontrer l’efficacité clinique de cette approche. De nouvelles stratégies d’immunothérapie reposant sur l’induction de lymphocytes T anti-tumoraux par des vaccins sont en cours de développement. L’optimisation de ces vaccins repose sur leur validation dans des modèles cliniques pertinents (tumeurs spontanées des rongeurs et des carnivores), sur leur association à des molécules permettant de lever des mécanismes de résistance de la tumeur à l’immunothérapie et sur des indications cliniques mieux définies de ces vaccins.

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Yves Montier

A CCR4 antagonist combined with vaccines induces antigen-specific CD8+ T cells and tumor immunity against self antigens

Central role of IL-6 and MMP-1 for cross talk between human intestinal mast cells and human intestinal fibroblasts

Immunothérapie des cancers

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