Decitabine Treatment of Glioma-Initiating Cells Enhances Immune Recognition and Killing

Riccadonna, Cristina; Maroun, Céline Yacoub; Silly, Romain Vuillefroy de; Boehler, Margaux; Tardón, Marta Calvo; Jueliger, Simone; Taverna, Pietro; Barba, Leticia; Marinari, Eliana; Pellegatta, Serena; Bassoy, Esen Yonca; Martinvalet, Denis; Dietrich, Pierre Yves; Walker, Paul R

doi:10.1371/journal.pone.0162105

Cited by 16 publications

(17 citation statements)

References 57 publications

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“…In cases where metastatic cells transition to active growth, their apparent dependence on αB-crystallin decreases. Thus, in addition to the possibility of blood-brain barrier-permeable decitabine for the treatment of growing brain metastasis ( Chabot et al., 1983 ; Riccadonna et al., 2016 ; Tawbi et al., 2013 ), targeting αB-crystallin and other pro-survival factors expressed in dormant cells may represent an attractive strategy for eliminating indolent single cells and micro-clusters. Furthermore, we can also hypothesize from our results that only the cells that undergo reprograming for cell survival and also circumvent anti-proliferative effects might progress to macrometastasis.…”

Section: Discussionmentioning

confidence: 99%

The Brain Microenvironment Induces DNMT1 Suppression and Indolence of Metastatic Cancer Cells

et al. 2020

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Brain metastasis is an ineffective process, and many cancer cells enter into an indolent state following extravasation in the brain. Single cell RNA sequencing of melanoma brain metastases reveals that non-proliferating brain metastatic melanoma cells exhibit a pattern of gene expression associated with inhibition of DNA methyltransferase 1 (DNMT1). The brain microenvironment, specifically the combination of reactive astrocytes and mechanically soft surroundings, suppressed DNMT1 expression in various cancer types and caused cell cycle delay. Somewhat unexpectedly, we find that DNMT1 suppression not only induces cell cycle delay but also activates pro-survival signals in brain metastatic cancer cells, including L1CAM and CRYAB. Our results demonstrate that transcriptional changes triggered by DNMT1 suppression is a key step for cancer cells to survive in the brain microenvironment and that they also restrict cancer cell proliferation. The dual consequences of DNMT1 suppression can explain the persistence of indolent cancer cells in the brain microenvironment.

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Section: Discussionmentioning

confidence: 99%

The Brain Microenvironment Induces DNMT1 Suppression and Indolence of Metastatic Cancer Cells

et al. 2020

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“…This is consistent with several publications in which TP53 mutations conferred a poor prognosis but were not predictive of the response to therapy, 6,38,39 while IPSS-R, Consequently, the T cell-mediated elimination of tumour cells is enhanced due to T cell recruitment and proliferation after reactivation. 40,41 IDO-1 expression correlated inversely with the CD8/CD3 ratio in our bone marrow samples; therefore, it might well be that IDO-1 counteracts the immune cell activation of AZA and thereby promotes resistance to therapy. The level of CD8 + T cells clearly increased after/under AZA treatment and remained constantly high.…”

Section: Discussionmentioning

confidence: 82%

“…HMAs can potentiate antitumour immunity by inducing the expression of critical molecules involved in cognate recognition by cytotoxic T cells, such as MHC I and ICAM‐1. Consequently, the T cell‐mediated elimination of tumour cells is enhanced due to T cell recruitment and proliferation after reactivation 40,41 . IDO‐1 expression correlated inversely with the CD8/CD3 ratio in our bone marrow samples; therefore, it might well be that IDO‐1 counteracts the immune cell activation of AZA and thereby promotes resistance to therapy.…”

Section: Discussionmentioning

confidence: 83%

Prognostic value of indoleamine 2,3 dioxygenase in patients with higher‐risk myelodysplastic syndromes treated with azacytidine

et al. 2020

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Hypomethylating agents (HMAs) are widely used in patients with higher‐risk myelodysplastic syndromes (MDS) not eligible for stem cell transplantation; however, the response rate is <50%. Reliable predictors of response are still missing, and it is a major challenge to develop new treatment strategies. One current approach is the combination of azacytidine (AZA) with checkpoint inhibitors; however, the potential benefit of targeting the immunomodulator indoleamine‐2,3‐dioxygenase (IDO‐1) has not yet been evaluated. We observed moderate to strong IDO‐1 expression in 37% of patients with high‐risk MDS. IDO‐1 positivity was predictive of treatment failure and shorter overall survival. Moreover, IDO‐1 positivity correlated inversely with the number of infiltrating CD8+ T cells, and IDO‐1+ patients failed to show an increase in CD8+ T cells under AZA treatment. In vitro experiments confirmed tryptophan catabolism and depletion of CD8+ T cells in IDO‐1+ MDS, suggesting that IDO‐1 expression induces an immunosuppressive microenvironment in MDS, thereby leading to treatment failure under AZA treatment. In conclusion, IDO‐1 is expressed in more than one‐third of patients with higher‐risk MDS, and is predictive of treatment failure and shorter overall survival. Therefore, IDO‐1 is emerging as a promising predictor and therapeutic target, especially for combination therapies with HMAs or checkpoint inhibitors.

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“…Because HIF-1α is critical for GSC maintenance [37, 43], STAT6 downregulation may favor HIF-1α accumulation in GSCs under hypoxic conditions, thereby contributing to GSC maintenance and GBM progression. Furthermore, 5-Aza is capable of targeting GSCs [40]; thus, restoration of STAT6 may be another mechanism underlying the actions of 5-Aza against GSCs.…”

Section: Discussionmentioning

confidence: 99%

Epigenetic downregulation of STAT6 increases HIF-1α expression via mTOR/S6K/S6, leading to enhanced hypoxic viability of glioma cells

Park

Kim

et al. 2019

acta neuropathol commun

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Multifunctional signal transducer and activator of transcription (STAT) proteins play important roles in cancer. Here, we have shown that STAT6 is epigenetically silenced in some cases of malignant glioblastoma, which facilitates cancer cell survival in a hypoxic microenvironment. This downregulation results from hypermethylation of CpG islands within the STAT6 promoter by DNA methyltransferases. STAT6 interacts with Rheb under hypoxia and inhibits mTOR/S6K/S6 signaling, in turn, inducing increased HIF-1α translation. STAT6 silencing and consequent tumor-promoting effects are additionally observed in glioma stem-like cells (GSC). Despite recent advances in cancer treatment, survival rates have shown little improvement. This is particularly true in the case of glioma, where multimodal treatment and precision medicine is needed. Our study supports the application of epigenetic restoration of STAT6 with the aid of DNA methyltransferase inhibitors, such as 5-aza-2-deoxycytidine, for treatment of STAT6-silenced gliomas.

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Decitabine Treatment of Glioma-Initiating Cells Enhances Immune Recognition and Killing

Cited by 16 publications

References 57 publications

The Brain Microenvironment Induces DNMT1 Suppression and Indolence of Metastatic Cancer Cells

The Brain Microenvironment Induces DNMT1 Suppression and Indolence of Metastatic Cancer Cells

Prognostic value of indoleamine 2,3 dioxygenase in patients with higher‐risk myelodysplastic syndromes treated with azacytidine

Epigenetic downregulation of STAT6 increases HIF-1α expression via mTOR/S6K/S6, leading to enhanced hypoxic viability of glioma cells

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