Regulatory T Cells Exhibit Distinct Features in Human Breast Cancer

Plitas, George; Konopacki, Catherine; Wu, Kenmin; Bos, Paula D.; Morrow, Monica; Putintseva, Ekaterina V.; Chudakov, Dmitriy M.; Rudensky, Alexander Y.

doi:10.1016/j.immuni.2016.10.032

Cited by 546 publications

(695 citation statements)

References 44 publications

(42 reference statements)

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“…Use of adjacent tumorfree tissue allows identification of tumor-specific, rather than tissue-specific, differences in Tregs and T cells, as discussed previously (34)(35)(36). In addition to showing increased numbers of Tregs in tumors compared with adjacent lung tissue, our study is the first to our knowledge to show tumor-specific increases in Treg numbers within lung LNs, even in early stages, when LNs are free of metastases.…”

Section: Discussionsupporting

confidence: 59%

“…Moreover, we found a negative correlation between Ki67 + expression in Tregs and tumor size, suggesting that along with tumor growth, factors such as hypoxia, nutrient deprivation, and tumor necrosis may impair division of immune cells, including Tregs. A recent study of Tregs in human breast cancer came to a similar conclusion by showing that the TCR repertoires between normal tissue and tumor-associated Tregs did not overlap, suggesting that Tregs are recruited (36).…”

Section: Discussionmentioning

confidence: 69%

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Human lung tumor FOXP+ Tregs upregulate four “Treg-locking” transcription factors

Akimova¹,

Zhang²,

Negorev³

et al. 2017

JCI Insight

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Section: Discussionsupporting

confidence: 59%

Section: Discussionmentioning

confidence: 69%

Human lung tumor FOXP+ Tregs upregulate four “Treg-locking” transcription factors

Akimova¹,

Zhang²,

Negorev³

et al. 2017

JCI Insight

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“…The classical ligand for CCR8 are CCL1 and CCL18, however it has been shown that CCL17 also induces migration of CCR8-expressing cells 44 , which is relevant in the cancer field as CCL17 has been strongly associated with tumour progression 27 . Same year, two independent research groups also described CCR8 as one of the main chemokine receptor in Tregs present in breast 45 , colorectal and non-small-cell lung cancer 46 . Whereas Plitas et al, mentioned that tumour environment has the ability to potentiate CCR8 expression in Tregs, De Simone et al, discussed that the presence of CCL18 in different tumours might be associated with the migration of CCR8 + cells 45,46 .…”

Section: Regulatory Cd4 + Th-like Helper Cells In Cancermentioning

confidence: 99%

“…Same year, two independent research groups also described CCR8 as one of the main chemokine receptor in Tregs present in breast 45 , colorectal and non-small-cell lung cancer 46 . Whereas Plitas et al, mentioned that tumour environment has the ability to potentiate CCR8 expression in Tregs, De Simone et al, discussed that the presence of CCL18 in different tumours might be associated with the migration of CCR8 + cells 45,46 . In 2017, our research group characterized the presence of Th1, Th2, Th17 and Th1/17 Tregs in peripheral blood and several tissues, such as skin, colon, thymus, spleen and liver perfusates 31 .…”

Section: Regulatory Cd4 + Th-like Helper Cells In Cancermentioning

confidence: 99%

“…Another possible explanation is the specific expansion of Th2-like subsets at the cancer site to reduce the antitumour immunological response. For example, the expression of TIGIT (T-Cell Immunoreceptor With Ig And ITIM Domains) has been found in tumour-infiltrating conventional CD4 + T-cells compared to circulating CD4 + Tcells 45 . It has been demonstrated that TIGIT contributes to the induction of a selective Treg-cell-mediated suppression of pro-inflammatory Th1 and Th17 cells but not Th2 cell responses 47 , thus it is possible that Th2 cells are not only recruited to the tumour site, but also promoted by evading TIGIT-mediated inhibition.…”

Section: Regulatory Cd4 + Th-like Helper Cells In Cancermentioning

confidence: 99%

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Effector and Regulatory CD4+ T helper lineages in cancer

Lombardi¹

2017

J Cancer Treat & Diagnosis

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Regulatory CD4+T-cells have been recently classified as regulatory T helper (Th)-like cells according to the expression of specific transcription factors, cytokines and chemokine receptors that mirror effector Th lineages. In our report: "An Atlas of Human Regulatory T Helper-like Cells Reveals Features of Th2-like Tregs that Support a Tumorigenic Environment" we found that Th2-like Tregs were increased in the tumour microenvironment in comparison with Th1-like, Th17-like and Th1/Th17-like Tregs. In addition, despite similar expression of CCR4 between all Tregs subtypes, Th2-like Tregs migrated more toward CCL17 and CCL22, and expressed higher levels of CCR8 than the other Th-like Tregs. Other studies have characterised human tissue-infiltrating Tregs and demonstrated that CCR8 is the main chemokine receptor differentially expressed in Tregs isolated from malignant tissues in comparison with healthy tissues. Given that CCR8 is a marker of Th2 lineages it is possible that Th2-like Tregs and CCR8+ Tregs are the same population of cells involved in tumour progression. However, whether they are recruited or differentiated in situ by the tumour microenvironment is still unknown. In this mini review, we describe the role of the different Th subsets in health and cancer and we present the different hypotheses about the presence of Th2-like Tregs in the tumorigenic environments.

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In Vitro 3D Spheroid Model Preserves Tumor Microenvironment of Hot and Cold Breast Cancer Subtypes

Dhandapani

Siddiqui

Karadkar

et al. 2023

Adv Healthcare Materials

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Dynamic interaction of cancer, immune, and stromal cells with extracellular matrix components modulates and resists the response of standard care therapies. To mimic this, an in vitro 3D spheroid model is designed using liquid overlay method to simulate hot (MDA‐MB‐231) and cold (MCF‐7) breast tumor microenvironment (TME). This study shows increased mesenchymal phenotype, stemness, and suppressive microenvironment in MDA‐MB‐231‐spheroids upon exposure to doxorubicin. Intriguingly, the presence of human dermal fibroblasts enhances cancer‐associated fibroblast phenotype in MDA‐MB‐231‐spheroids through increased expression of CXCL12 and FSP‐1, leading to higher infiltration of immune cells (THP‐1 monocytes). However, a suppressive TME is observed in both subtypes, as seen by upregulation of M2‐macrophage‐specific CD68 and CD206 markers. Specifically, increased PDL‐1 expressing tumor‐associated macrophages along with FoxP3 expressing T regulatory cells are found in MDA‐MB‐231‐spheroids when cultured with peripheral blood mononuclear cells. Further, it is found that the addition of 1‐methyl‐tryptophan, a potent indoleamine‐2,3‐dioxygenase‐1 inhibitor, subsides the suppressive phenotype by decreasing the M2 polarization via downregulation of tryptophan metabolism and IL10 expression, particularly in MCF‐7 triculture spheroids. Thus, the in vitro 3D spheroid model of TME can be utilized in therapeutics to validate immunomodulatory drugs for various breast cancer subtypes.

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Regulatory T Cells Exhibit Distinct Features in Human Breast Cancer

Cited by 546 publications

References 44 publications

Human lung tumor FOXP+ Tregs upregulate four “Treg-locking” transcription factors

Human lung tumor FOXP+ Tregs upregulate four “Treg-locking” transcription factors

Effector and Regulatory CD4+ T helper lineages in cancer

In Vitro 3D Spheroid Model Preserves Tumor Microenvironment of Hot and Cold Breast Cancer Subtypes

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