Targeting immune checkpoints in breast cancer: an update of early results

Solinas, Cinzia; Gombos, Andrea; Latifyan, Sofiya; Piccart‐Gebhart, Martine; Kok, Marleen; Buisseret, Laurence

doi:10.1136/esmoopen-2017-000255

Cited by 128 publications

(101 citation statements)

References 121 publications

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“…Treatment of TNBC remains challenging, because the tumors are highly aggressive and lack therapeutic targets (2, 3). Among the therapeutic options for TNBC, immunotherapy is emerging as a promising approach, but clinical studies in patients with TNBC revealed unsatisfactory outcomes, which is largely attributed to the lack of TILs (36).…”

Section: Discussionmentioning

confidence: 99%

Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 ⁺ T cells

Chen

Cong

et al. 2020

Sci. Adv.

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CCR9+ T cells have an increased potential to be activated and therefore may mediate strong antitumor responses. Here, we found, however, that CCL25, the only chemokine for CCR9+ cells, is not expressed in human or murine triple-negative breast cancers (TNBCs), raising a hypothesis that intratumoral delivery of CCL25 may enhance antitumor immunotherapy in TNBCs. We first determined whether this approach can enhance CD47-targeted immunotherapy using a tumor acidity–responsive nanoparticle delivery system (NP-siCD47/CCL25) to sequentially release CCL25 protein and CD47 small interfering RNA in tumor. NP-siCD47/CCL25 significantly increased infiltration of CCR9+CD8+ T cells and down-regulated CD47 expression in tumor, resulting in inhibition of tumor growth and metastasis through a T cell–dependent immunity. Furthermore, the antitumor effect of NP-siCD47/CCL25 was synergistically enhanced when used in combination with programmed cell death protein–1/programmed death ligand-1 blockades. This study offers a strategy to enhance immunotherapy by promoting CCR9+CD8+ T cell tumor infiltration.

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Section: Discussionmentioning

confidence: 99%

Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 ⁺ T cells

Chen

Cong

et al. 2020

Sci. Adv.

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“…Reports show that, not only immune infiltrating cells, but also circulating cells can possess an immune suppressive phenotype in cancer patients. [14][15][16] We investigated a set of immune checkpoints/ ligands including PD-1, CTLA-4, TIM-3, LAG-3, TIGIT, VISTA and PD-L1 in peripheral blood mononuclear cells (PBMCs) from healthy donors (n = 32), breast cancer patients (n = 31) and colorectal cancer patients (n = 23). Results showed that the expressions of TIM-3, TIGIT and PD-L1 in PBMCs of PBC patients were significantly higher and LAG-3 was significantly lower compared with HD ( Figure 1(c-f)).…”

Section: Upregulation Of Immune Checkpoints In Circulation Of Breast mentioning

confidence: 99%

DNA methylation of immune checkpoints in the peripheral blood of breast and colorectal cancer patients

et al. 2018

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Aberrant expression of immune checkpoints (ICs) in cancer creates an immunosuppressive microenvironment, which supports immune evasion of tumor cells. We have recently reported that epigenetic modifications are critical for ICs expression in the tumor microenvironment (TME) of primary breast cancer (PBC) and colorectal cancer (CRC). Herein, we investigated transcriptomic expression of ICs (PD-1, CTLA-4, LAG-3, TIM-3, TIGIT) and PD-L1 in peripheral blood of PBC and CRC patients, compared to healthy donors (HD). We found that expressions of TIM-3, TIGIT, PD-L1 were significantly upregulated, while LAG-3 expression was downregulated in peripheral blood of PBC and CRC patients. Demethylation enzymes TET2 and TET3 were also upregulated. In addition, promoter DNA methylation status of PD-1 was significantly hypermethylated, while PD-L1 was hypomethylated in PBC and CRC patients. Furthermore, TIGIT was significantly hypomethylated only in CRC patients. Remarkably, promoter methylation status of LAG-3, TIGIT and PD-L1 was in concordance with transcriptomic expression in CRC: the more the hypomethylation, the higher the expression. In comparison, we found that CTLA-4, TIM-3, TIGIT and PD-L1 in PBC, and CTLA-4 in CRC patients were significantly upregulated in peripheral blood, compared with tumor tissues of the same patients. However, demethylation status of all ICs was higher in TT, except for TIGIT in PBC, and CTLA-4 in CRC patients. These data indicate that the underlying mechanisms behind peripheral upregulation of PD-L1 and TIGIT in cancer patients could be due to aberrant promoter methylation profile. Moreover, demethylation inhibitors together with anti-PD-L1/ anti-TIGIT could be a more efficient therapeutic strategy in cancer patients. ARTICLE HISTORY

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“…There is evidence that the low immunogenicity and the intense immunosuppressive tumor microenvironment (TME) of breast cancers (BC) limit the benefit of immunotherapies targeting the adaptive immune system, such as checkpoint inhibitors (CPI) [1,2]. Immunosuppressive mechanisms are essential for the development of normal mammary glands; these strategies are also used by BC cells to promote tumor tolerance and escape from immune surveillance in the early stages of disease, suggesting an important role of adaptive and innate immunity in BC development and progression.…”

Section: Introductionmentioning

confidence: 99%

The Role of Immune Escape and Immune Cell Infiltration in Breast Cancer

2018

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While detailed analysis of aberrant cancer cell signaling pathways and changes in cancer cell DNA has dominated the field of breast cancer biology for years, there now exists increasing evidence that the tumor microenvironment (TME) including tumor-infiltrating immune cells support the growth and development of breast cancer and further facilitate invasion and metastasis formation as well as sensitivity to drug therapy. Furthermore, breast cancer cells have developed different strategies to escape surveillance from the adaptive and innate immune system. These include loss of expression of immunostimulatory molecules, gain of expression of immunoinhibitory molecules such as PD-L1 and HLA-G, and altered expression of components involved in apoptosis. Furthermore, the composition of the TME plays a key role in breast cancer development and treatment response. In this review we will focus on i) the different immune evasion mechanisms used by breast cancer cells, ii) the role of immune cell infiltration in this disease, and (iii) implication for breast cancer-based immunotherapies.

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Targeting immune checkpoints in breast cancer: an update of early results

Cited by 128 publications

References 121 publications

Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 ⁺ T cells

Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 ⁺ T cells

DNA methylation of immune checkpoints in the peripheral blood of breast and colorectal cancer patients

The Role of Immune Escape and Immune Cell Infiltration in Breast Cancer

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Targeting immune checkpoints in breast cancer: an update of early results

Cited by 128 publications

References 121 publications

Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 + T cells

Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 + T cells

DNA methylation of immune checkpoints in the peripheral blood of breast and colorectal cancer patients

The Role of Immune Escape and Immune Cell Infiltration in Breast Cancer

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Product

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Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 ⁺ T cells

Intratumoral delivery of CCL25 enhances immunotherapy against triple-negative breast cancer by recruiting CCR9 ⁺ T cells