Developmental origins and oncogenic pathways in malignant brain tumors

Lu, Q Richard; Qian, Lily; Zhou, Xianyao

doi:10.1002/wdev.342

Cited by 38 publications

(30 citation statements)

References 229 publications

(430 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…At present, it is not clear how this might influence tumor properties. In the future, it would be interesting to develop a similar approach to model and study prenatal and childhood tumors, such as pediatric gliomas and medulloblastomas, which should maintain a closer link to their developmental origin (Liu and Zong, 2012;Azzarelli et al, 2018;Lu et al, 2019). As medulloblastoma did not develop in organoids, even when genetic alterations typical of this tumors were introduced, it might be necessary to generate regionalized organoids (Muguruma et al, 2015;Dias and Guillemot, 2017;Renner et al, 2017;Ballabio et al, 2020) tailored to the area of origin of that specific tumor, prior to transformation.…”

Section: Advantages and Limitations: Which Model To Use?mentioning

confidence: 99%

“…The idea that tumor initiation, progression and regrowth after treatment are sustained by a subpopulation of cancer cells, the glioblastoma stem cells (GSCs), has been crucial to our current understating of glioblastoma (GBM) biology (Swartling et al, 2015;Alcantara Llaguno et al, 2016;Azzarelli et al, 2018;Hakes and Brand, 2019;Lu et al, 2019). Glioblastoma is a highly aggressive brain tumor characterized by elevated intratumor heterogeneity, which could be potentially attributed to variations in GSC behavior and stochastic consequences of their hierarchical growth pattern.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Organoid Models of Glioblastoma to Study Brain Tumor Stem Cells

Azzarelli

2020

Front. Cell Dev. Biol.

View full text Add to dashboard Cite

Glioblastoma represents an aggressive form of brain cancer characterized by poor prognosis and a 5-year survival rate of only 3-7%. Despite remarkable advances in brain tumor research in the past decades, very little has changed for patients, due in part to the recurrent nature of the disease and to the lack of suitable models to perform genotype-phenotype association studies and personalized drug screening. In vitro culture of cancer cells derived from patient biopsies has been fundamental in understanding tumor biology and for testing the effect of various drugs. These cultures emphasize the role of in vitro cancer stem cells (CSCs), which fuel tumor growth and are thought to be the cause of relapse after treatment. However, it has become clear over the years that a 2D monolayer culture of these CSCs has certain disadvantages, including the lack of heterogeneous cell-cell and cell-environment interactions, which can now be partially overcome by the introduction of 3D organoid cultures. This is a novel and expanding field of research and in this review, I describe the emerging 3D models of glioblastoma. I also discuss their potential to advance our knowledge of tumor biology and CSC heterogeneity, while debating their current limitations.

show abstract

Section: Advantages and Limitations: Which Model To Use?mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Organoid Models of Glioblastoma to Study Brain Tumor Stem Cells

Azzarelli

2020

Front. Cell Dev. Biol.

View full text Add to dashboard Cite

show abstract

“…Paediatric high-grade gliomas originate from cells along the neural stem cell lineages [31]. These cells have the capacity to generate a variety of different cell types: activated stem cells, progenitor cells and mature cells such as astrocytes, oligodendrocytes and neurons [32]. The DNA methylation pattern is strictly regulated during differentiation and development allowing each cell type to acquire its required phenotype to meet its specific functions and needs.…”

Section: Discussionmentioning

confidence: 99%

Accumulation of DNA methylation alterations in paediatric glioma stem cells following fractionated dose irradiation

et al. 2020

View full text Add to dashboard Cite

Background: Radiation is an important therapeutic tool. However, radiotherapy has the potential to promote coevolution of genetic and epigenetic changes that can drive tumour heterogeneity, formation of radioresistant cells and tumour relapse. There is a clinical need for a better understanding of DNA methylation alterations that may follow radiotherapy to be able to prevent the development of radiation-resistant cells. Methods:We examined radiation-induced changes in DNA methylation profiles of paediatric glioma stem cells (GSCs) in vitro. Five GSC cultures were irradiated in vitro with repeated doses of 2 or 4 Gy. Radiation was given in 3 or 15 fractions. DNA methylation profiling using Illumina DNA methylation arrays was performed at 14 days postradiation. The cellular characteristics were studied in parallel. Results: Few fractions of radiation did not result in significant accumulation of DNA methylation alterations. However, extended dose fractionations changed DNA methylation profiles and induced thousands of differentially methylated positions, specifically in enhancer regions, sites involved in alternative splicing and in repetitive regions. Radiation induced dose-dependent morphological and proliferative alterations of the cells as a consequence of the radiation exposure.Conclusions: DNA methylation alterations of sites with regulatory functions in proliferation and differentiation were identified, which may reflect cellular response to radiation stress through epigenetic reprogramming and differentiation cues.

show abstract

“…Medulloblastoma tumors are thought to originate in the cerebellum, except for the WNT subgroups that arise outside the cerebellum and are distributed within the fourth ventricle and infiltrated the dorsal surface of the brainstem (Gibson et al, 2010). Dorsal brainstem progenitor cells of cochlear, mossy fiber, and climbing fiber neurons are regarded as the potential source of these tumors (Gibson et al, 2010), following the activation of Ctnnb1 and the concurrent Trp53 deletion (Lu et al, 2019).…”

Section: Medulloblastoma Originmentioning

confidence: 99%

“…Differently, all available SHH-subtype tumors were localized away from the brainstem, within the cerebellar hemispheres. They are thought to originate from cerebellar neural stem cells (NSCs) or committed granule neuron precursor cells (GNPCs) following aberrant activation of SHH (Gibson et al, 2010;Lu et al, 2019). The group 3 MB tumors are often positioned near the fourth ventricle, pointing to cerebellar stem/progenitor cells or GNPCs as potential sources (Kawauchi et al, 2012;Pei et al, 2012;Lu et al, 2019).…”

Section: Medulloblastoma Originmentioning

confidence: 99%

The Non-coding Side of Medulloblastoma

Laneve

Caffarelli

2020

Front. Cell Dev. Biol.

View full text Add to dashboard Cite

Medulloblastoma (MB) is the most common pediatric brain tumor and a primary cause of cancer-related death in children. Until a few years ago, only clinical and histological features were exploited for MB pathological classification and outcome prognosis. In the past decade, the advancement of high-throughput molecular analyses that integrate genetic, epigenetic, and expression data, together with the availability of increasing wealth of patient samples, revealed the existence of four molecularly distinct MB subgroups. Their further classification into 12 subtypes not only reduced the wellcharacterized intertumoral heterogeneity, but also provided new opportunities for the design of targets for precision oncology. Moreover, the identification of tumorigenic and self-renewing subpopulations of cancer stem cells in MB has increased our knowledge of its biology. Despite these advancements, the origin of MB is still debated, and its molecular bases are poorly characterized. A major goal in the field is to identify the key genes that drive tumor growth and the mechanisms through which they are able to promote tumorigenesis. So far, only protein-coding genes acting as oncogenic drivers have been characterized in each MB subgroup. The contribution of the non-coding side of the genome, which produces a plethora of transcripts that control fundamental biological processes, as the cell choice between proliferation and differentiation, is still unappreciated. This review wants to fill this major gap by summarizing the recent findings on the impact of non-coding RNAs in MB initiation and progression. Furthermore, their potential role as specific MB biomarkers and novel therapeutic targets is also highlighted.

show abstract

Developmental origins and oncogenic pathways in malignant brain tumors

Cited by 38 publications

References 229 publications

Organoid Models of Glioblastoma to Study Brain Tumor Stem Cells

Organoid Models of Glioblastoma to Study Brain Tumor Stem Cells

Accumulation of DNA methylation alterations in paediatric glioma stem cells following fractionated dose irradiation

The Non-coding Side of Medulloblastoma

Contact Info

Product

Resources

About