miRNA-mediated loss of m6A increases nascent translation in glioblastoma

Zepecki, John P.; Karambizi, David; Fajardo, J. Eduardo; Snyder, Kristin M.; Guetta-Terrier, Charlotte; Tang, Oliver Y.; Chen, Jia-Shu; Sarkar, Atom; Fiser, András; Toms, Steven; Tapinos, Nikos

doi:10.1371/journal.pgen.1009086

Cited by 26 publications

(18 citation statements)

References 70 publications

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“…S4B and C). To determine the in vivo efficacy of anti-Chi3l1 antibody as localized treatment for glioblastoma, we generated orthotopic xenograft glioblastoma in immunocompromised mice using patient derived GSCs as shown before (16,17). 28 days following the stereotactic implantation of GSCs, mice were implanted with an intracranial catheter connected to an osmotic pump (Alzet) for continuous infusion of anti-Chi3l1 antibody.…”

Section: Localized Treatment With Anti-chi3l1 Antibody Results In Significant Reduction Of Human Glioblastoma Growthmentioning

confidence: 99%

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Chi3l1 is a modulator of glioma stem cell states and a therapeutic vulnerability for glioblastoma

Guetta-Terrier

Karambizi

Akosman

et al. 2021

Preprint

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Chi3l1 (Chitinase 3-like 1) is a secreted protein highly expressed in glioblastoma. Here, we show that exposure of glioma stem cells (GSCs) to Chi3l1 reduces the CD133+/SOX2+ cells and increases the CD44+/Chi3l1+ cells. Chi3l1 binds to CD44 and induces phosphorylation and nuclear translocation of beta-catenin, Akt and STAT3. Single cell RNA-seq and RNA velocity following incubation of GSCs with Chi3l1 show significant changes in GSC state dynamics driving GSCs towards a mesenchymal expression profile and reducing transition probabilities towards terminal cellular states. ATAC-seq reveals that Chi3l1 increases accessibility of promoters containing MAZ transcription factor footprint. Inhibition of MAZ directly regulates genes with highest expression in cellular clusters exhibiting significant cell state transitions. Finally, targeting Chi3l1 in vivo with a blocking antibody, resets the transcriptomic profile of glioblastoma and inhibits tumor growth. Our work implicates Chi3l1 as modulator of GSC cellular states and demonstrates pre-clinical efficacy of anti-Chi3l1 antibody treatment.

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Section: Localized Treatment With Anti-chi3l1 Antibody Results In Significant Reduction Of Human Glioblastoma Growthmentioning

confidence: 99%

“…GSCs from patients with IDH wild type primary glioblastoma have been characterized by RNA-seq and shown to recapitulate the patient's tumor in orthotopic xenografts (16,17). GSC1 and GSC2 both exhibit chromosome 10 deletion and amplification of chromosome 7.…”

Section: Chi3l1 Induces Expression Of Mesenchymal Markers In Proneural Gscsmentioning

confidence: 99%

Chi3l1 is a modulator of glioma stem cell states and a therapeutic vulnerability for glioblastoma

Guetta-Terrier

Karambizi

Akosman

et al. 2021

Preprint

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“…Primary GSCs were cultured from human glioma samples as previously described 57–59 . GSCs were used between passages 12 and 18 for all experiments and cultured as neurospheres in the following conditions: Neurobasal A (Gibco), 2% B27 (Gibco), 2 mM GlutaMAX (Gibco), 2 μg/ml heparin solution (Stem Cell Technologies), 2% Antibiotic‐Antimycotic (Gibco), 20 ng/ml Epidermal Growth Factor (EGF) and 20 ng/ml basic Fibroblast Growth Factor (bFGF) (both from Peprotech).…”

Section: Methodsmentioning

confidence: 99%

FOXO3 regulates a common genomic program in aging and glioblastoma stem cells

et al. 2021

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Background Glioblastoma (GBM) is an aggressive, age‐associated malignant glioma that contains populations of cancer stem cells. These glioma stem cells (GSCs) evade therapeutic interventions and repopulate tumors due to their existence in a slowly cycling quiescent state. Although aging is well known to increase cancer initiation, the extent to which the mechanisms supporting GSC tumorigenicity are related to physiological aging remains unknown. Aims Here, we investigate the transcriptional mechanisms by which Forkhead Box O3 (FOXO3), a transcriptional regulator that promotes healthy aging, affects GSC function and the extent to which FOXO3 transcriptional networks are dysregulated in aging and GBM. Methods and results We performed transcriptome analysis of clinical GBM tumors and observed that high FOXO3 activity is associated with gene expression signatures of stem cell quiescence, reduced oxidative metabolism, and improved patient outcomes. Consistent with these findings, we show that elevated FOXO3 activity significantly reduces the proliferation of GBM‐derived GSCs. Using RNA‐seq, we find that functional ablation of FOXO3 in GSCs rewires the transcriptional circuitry associated with metabolism, epigenetic stability, quiescence, and differentiation. Since FOXO3 has been implicated in healthy aging, we then investigated the extent to which it regulates common transcriptional programs in aging neural stem cells (NSCs) and GSCs. We uncover a shared transcriptional program and, most strikingly, find that FOXO3‐regulated pathways are associated with altered mitochondrial functions in both aging and GBM. Conclusions This work identifies a FOXO‐associated transcriptional program that correlates between GSCs and aging NSCs and is enriched for metabolic and stemness pathways connected with GBM and aging.

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“…The Dynamic m 6 A Epitranscriptome in Glioma Stem Cell Plasticity and Function DOI: http://dx.doi.org/10.5772/intechopen.96792 performed an integrated whole genome meRIP-seq, RNA-seq and ribo-seq analysis in three patient-derived GSCs and differentiated progenies [52]. This allowed for the interrogation of transcriptional, epitranscriptional and translational kinetics during cell state transition [52]. In the study, we deliberately avoid m6A machinery perturbation and simply attempt to unravel what happens in one of the most basic process of GSCs plasticity (differentiation) in the context of m6A dynamics.…”

Section: Role Of M6a In Cellular Plasticity In Glioblastomamentioning

confidence: 99%

The Dynamic m⁶A Epitranscriptome in Glioma Stem Cell Plasticity and Function

Karambizi¹,

Tapinos²

2022

Central Nervous System Tumors

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Glioblastoma multiforme is one of the most aggressive tumors of the central nervous system. The current standard-of-care includes maximal resection followed by chemotherapy, radiation and more recently, tumor treating fields (TTFs). Despite this multimodal approach, glioblastoma remains refractory to therapy. Glioblastoma resistance, recurrence and malignancy are believed to be driven by a subpopulation of glioma stem cells (GSCs) within the tumor bulk which are characterized by the retention of self-renewal potential as well as the capacity to recapitulate tumor heterogeneity. Within the dynamic intratumoral niche, GSCs demonstrate a high degree of cellular plasticity, reversibly interconverting between stem-like states and more differentiated states as a result of environmental cues/signaling fluctuations. Such plastic adaptive properties are mostly driven by multiple dynamic, reversible epigenetic modifications. We posit that reversible post-transcriptional methylation of RNA transcripts at the m6A position may be one such regulatory mechanism employed by GSCs to efficiently maintain plasticity and adaptive phenotypic transitions. In this section, we discuss the concept of cellular plasticity, introduce dynamic m6a epitranscriptomic mechanisms as potential key regulators of GSC plasticity and finally propose epigenetic based therapeutics as a mean of attenuating glioblastoma plasticity to improve patient outcome.

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miRNA-mediated loss of m6A increases nascent translation in glioblastoma

Cited by 26 publications

References 70 publications

Chi3l1 is a modulator of glioma stem cell states and a therapeutic vulnerability for glioblastoma

Chi3l1 is a modulator of glioma stem cell states and a therapeutic vulnerability for glioblastoma

FOXO3 regulates a common genomic program in aging and glioblastoma stem cells

The Dynamic m⁶A Epitranscriptome in Glioma Stem Cell Plasticity and Function

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miRNA-mediated loss of m6A increases nascent translation in glioblastoma

Cited by 26 publications

References 70 publications

Chi3l1 is a modulator of glioma stem cell states and a therapeutic vulnerability for glioblastoma

Chi3l1 is a modulator of glioma stem cell states and a therapeutic vulnerability for glioblastoma

FOXO3 regulates a common genomic program in aging and glioblastoma stem cells

The Dynamic m6A Epitranscriptome in Glioma Stem Cell Plasticity and Function

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The Dynamic m⁶A Epitranscriptome in Glioma Stem Cell Plasticity and Function