Therapeutic depletion of CCR8<sup>+</sup>tumor-infiltrating regulatory T cells elicits antitumor immunity and synergizes with anti-PD-1 therapy

Damme, Helena Van; Dombrecht, Bruno; Kiss, Máté; Roose, Heleen; Allen, Elizabeth; Overmeire, Eva Van; Kancheva, Daliya; Martens, Liesbet; Murgaski, Aleksandar; Bardet, Pauline M. R.; Blancke, Gillian; Jans, Maude; Bolli, Evangelia; Martins, Maria Solange; Elkrim, Yvon; Dooley, James; Boon, Louis; Schwarze, Julia Katharina; Tacke, Frank; Movahedi, Kiavash; Vandamme, Niels; Neyns, Bart; Ocak, Sebahat; Scheyltjens, Isabelle; Vereecke, Lars; Nana, Frank Aboubakar; Merchiers, Pascal; Laoui, Damya; Ginderachter, Jo A. Van

doi:10.1136/jitc-2020-001749

Cited by 112 publications

(91 citation statements)

References 59 publications

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“…Whether the anti-CCR8 antibodies used functioned in part through induction of Treg cell depletion has yet to be formally tested. The hypothesis that therapeutic depletion of CCR8 + cells rather than blockade of CCR8 function leads to induction of anti-tumour immunity is indeed consistent with recently reported findings that administration of anti-CCR8 nanobodies with blocking function does not augment tumour immunity, but does so when provided the capability for ADCC [40].…”

Section: Discussionsupporting

confidence: 89%

CCR8 marks highly suppressive Treg cells within tumours but is dispensable for their accumulation and suppressive function

et al. 2021

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Section: Discussionsupporting

confidence: 89%

CCR8 marks highly suppressive Treg cells within tumours but is dispensable for their accumulation and suppressive function

et al. 2021

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“… 75 Two recent preclinical studies demonstrated that anti-CCR8 antibodies with Fc-dependent ADCC activity selectively deplete tumor-infiltrating Tregs due to prominent CCR8 expression by the activated Tregs in the TME, leading to long-lasting antitumor immune responses and synergistic antitumor effects with PD-1 blockade. 130 131 …”

Section: Targeting Chemokine Receptors and Immune Checkpoint Molecules On Tregsmentioning

confidence: 99%

Mechanisms of regulatory T cell infiltration in tumors: implications for innovative immune precision therapies

Nishikawa

Koyama

2021

J Immunother Cancer

150

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With the broad application of cancer immunotherapies such as immune checkpoint inhibitors in multiple cancer types, the immunological landscape in the tumor microenvironment (TME) has become enormously important for determining the optimal cancer treatment. Tumors can be immunologically divided into two categories: inflamed and non-inflamed based on the extent of immune cell infiltration and their activation status. In general, immunotherapies are preferable for the inflamed tumors than for non-inflamed tumors. Regulatory T cells (Tregs), an immunosuppressive subset of CD4+ T cells, play an essential role in maintaining self-tolerance and immunological homeostasis. In tumor immunity, Tregs compromise immune surveillance against cancer in healthy individuals and impair the antitumor immune response in tumor-bearing hosts. Tregs, therefore, accelerate immune evasion by tumor cells, leading to tumor development and progression in various types of cancer. Therefore, Tregs are considered to be a crucial therapeutic target for cancer immunotherapy. Abundant Tregs are observed in the TME in many types of cancer, both in inflamed and non-inflamed tumors. Diverse mechanisms of Treg accumulation, activation, and survival in the TME have been uncovered for different tumor types, indicating the importance of understanding the mechanism of Treg infiltration in each patient when selecting the optimal Treg-targeted therapy. Here, we review recent advances in the understanding of mechanisms leading to Treg abundance in the TME to optimize Treg-targeted therapy. Furthermore, in addition to the conventional strategies targeting cell surface molecules predominantly expressed by Tregs, reagents targeting molecules and signaling pathways specifically employed by Tregs for infiltration, activation, and survival in each tumor type are illustrated as novel Treg-targeted therapies. The effectiveness of immune precision therapy depends on conditions in the TME of each cancer patient.

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“…The elevated abundance of activated CD8 + T cells, was accompanied by both a decreased infiltration of FoxP3 + regulatory T cells (Tregs), as well as a reduced expression of CCR8 on the Tregs (Fig. 1t, u), indicative for reduced suppressive phenotype of these cells [33].…”

Section: Cd40 Agonist Therapy Repolarises B16f10 Tumours Resulting In Reduced Tumour Growthmentioning

confidence: 99%

“…6g). Both Tregs and neutrophils were shown to suppress CD8 + T cells in LLC tumours [33,42], which could be responsible for the lower initial abundance of CD8 + T cells in LLC tumours and their inability to expand upon αCD40 + αCSF1R treatment (Fig. 6h).…”

Section: Llc Tumours Do Not Respond To αCd40 Therapy When Combined With Tam/neutrophil Depleting Therapies Nor Therapies Boosting Cd8 + Tmentioning

confidence: 99%

Distinct cDC subsets co-operate in CD40 agonist response while suppressive microenvironments and lack of antigens subvert efficacy

Murgaski

Kiss

Damme

et al. 2021

Preprint

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Agonistic αCD40 therapy has shown to inhibit cancer progression, but only in a fraction of patients. Hence, understanding the cancer cell-intrinsic and microenvironmental determinants of αCD40 therapy response is crucial to identify responsive patient populations and design efficient combination treatments. Here, we showed that the therapeutic efficacy of αCD40 in responder melanoma tumours, relied on pre-existing cDC1-primed CD8+ T cells, however cDC1s were dispensable after αCD40 administration. Surprisingly, in response to αCD40 the abundance of activated cDCs, potentially derived from cDC2s increased, thereby further activating antitumour CD8+ T cells. Hence, distinct cDC subsets are required to induce αCD40 responses. By contrast, lung tumours, characterised by a high abundance of macrophages, were resistant to αCD40 therapy. Combining αCD40 therapy with macrophage depletion led to tumour growth inhibition only in the presence of strong neoantigens. Accordingly, treatment with immunogenic cell-death inducing chemotherapy sensitised non-immunogenic tumours to αCD40 therapy.

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Therapeutic depletion of CCR8⁺tumor-infiltrating regulatory T cells elicits antitumor immunity and synergizes with anti-PD-1 therapy

Cited by 112 publications

References 59 publications

CCR8 marks highly suppressive Treg cells within tumours but is dispensable for their accumulation and suppressive function

CCR8 marks highly suppressive Treg cells within tumours but is dispensable for their accumulation and suppressive function

Mechanisms of regulatory T cell infiltration in tumors: implications for innovative immune precision therapies

Distinct cDC subsets co-operate in CD40 agonist response while suppressive microenvironments and lack of antigens subvert efficacy

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Therapeutic depletion of CCR8+tumor-infiltrating regulatory T cells elicits antitumor immunity and synergizes with anti-PD-1 therapy

Cited by 112 publications

References 59 publications

CCR8 marks highly suppressive Treg cells within tumours but is dispensable for their accumulation and suppressive function

CCR8 marks highly suppressive Treg cells within tumours but is dispensable for their accumulation and suppressive function

Mechanisms of regulatory T cell infiltration in tumors: implications for innovative immune precision therapies

Distinct cDC subsets co-operate in CD40 agonist response while suppressive microenvironments and lack of antigens subvert efficacy

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Therapeutic depletion of CCR8⁺tumor-infiltrating regulatory T cells elicits antitumor immunity and synergizes with anti-PD-1 therapy