DNA Methylation and Somatic Mutations Converge on the Cell Cycle and Define Similar Evolutionary Histories in Brain Tumors

Mazor, Tali; Pankov, Aleksandr; Johnson, Brett; Hong, Chibo; Hamilton, Emily G.; Bell, Robert J.A.; Смирнов, Иван; Reis, Gerald F.; Phillips, Joanna J.; Barnes, Michael J.; Idbaïh, Ahmed; Alentorn, Agustí; Kloezeman, Jenneke J.; Lamfers, Martine L.M.; Bollen, Andrew W.; Taylor, Barry S.; Molinaro, Annette M.; Olshen, Adam B.; Chang, Susan M.; Song, Jun S.; Costello, J

doi:10.1016/j.ccell.2015.07.012

Cited by 236 publications

(243 citation statements)

References 56 publications

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“…Analysis of ITH in gliomas (Mazor et al, 2015) as well as prostate cancers (Aryee et al, 2013) and esophageal squamous cell carcinomas (Hao et al, 2016) has suggested that the extent of ITH calculated from DNA methylation mirrors ITH measures captured at the genomic level.…”

Section: How Much Heterogeneity Is There?mentioning

confidence: 99%

Clonal Heterogeneity and Tumor Evolution: Past, Present, and the Future

McGranahan

Swanton

2017

Cell

2,102

1,694

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Intratumor heterogeneity, which fosters tumor evolution, is a key challenge in cancer medicine. Here we review data and technologies that have revealed intra-tumor heterogeneity across cancer types, and the dynamics, constraints and contingencies inherent to tumor evolution. We emphasize the importance of macro-evolutionary leaps, often involving large-scale chromosomal alterations, in driving tumor evolution and metastasis, and consider the role of the tumor microenvironment in engendering heterogeneity and drug-resistance. We suggest that bold approaches to drug development, harnessing the adaptive properties of the immunemicroenvironment whilst limiting those of the tumor, combined with advances in clinical trial-design, will improve patient outcome.

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Section: How Much Heterogeneity Is There?mentioning

confidence: 99%

Clonal Heterogeneity and Tumor Evolution: Past, Present, and the Future

McGranahan

Swanton

2017

Cell

2,102

1,694

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“…Segregating clones based on the presence of independent or shared mutations has revealed part of the tumor development process (27)(28)(29)(35)(36)(37). The clonal evolution model posits that tumor formation is initiated in a cell of origin and is followed by the accumulation of single or multiple somatic genetic alterations, leading to advantages in survival or growth (38).…”

Section: Complexity Of Tumor Heterogeneity In Gbmmentioning

confidence: 99%

“…The fittest cell populations likely establish precancerous clones, although we have little direct evidence to support this process in human GBM because of limitations in detecting the early steps in brain cell transformation (42,43). Divergent genetic alterations in early transformed cells can subsequently give rise to a variety of clones under the selective pressure of the evolutionary ecosystem in the tumor (27)(28)(29)(35)(36)(37). A cell's spatial location in the tumor is related to its divergent genomic profile, and clones with similar types of genetic alterations are more proximal to each other than those with dissimilar profiles (Figure 1B and refs.…”

Section: Complexity Of Tumor Heterogeneity In Gbmmentioning

confidence: 99%

“…Surgical debulking reduces intratumoral heterogeneity by removing many subclones from the tumor. This conclusion is based on two observations: first, there is regional diversity in primary tumor clones, suggesting limited cell mixing (27-29, 36, 37, 44), and second, comparison of primary/ recurrent tumors of patients having only received surgery shows that the recurrences diverge early from the primary tumor and lack the end mutations found in the primary tumor (27,36). Postoperative chemo-and radiotherapies can likely also reduce clonal diversity when only biopsy or partial surgical resection is possible, (106), and ID1 (107).…”

Section: What Type Of Clone Can Initiate Tumor Recurrence?mentioning

confidence: 99%

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Overcoming therapeutic resistance in glioblastoma: the way forward

Osuka¹,

Meir²

2017

Journal of Clinical Investigation

388

311

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“…20,21 For instance, patients with IDH mutation showed hypermethylation of the CpG island and increased histone demethylation. [22][23][24] IDH converts isocitrate to a-ketoglutarate (a-KG) during normal TCA cycle, whereas mutant IDH converts a-KG to D-2-hydroxyglutarate (D-2HG) in an NADPH-dependent manner that has been associated with secondary GBM. [22][23][24][25][26] Nonetheless, 4 independent cases of MRI-classified SVZassociated GBM used in this study do not contain IDH mutation (Fig.…”

Section: Mri-classified Svz-associated Gbm Has Alteration Of Epigenetmentioning

confidence: 99%

Comparative analyses identify molecular signature of MRI-classified SVZ-associated glioblastoma

et al. 2017

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Glioblastoma (GBM) is a highly aggressive brain cancer with limited therapeutic options. While efforts to identify genes responsible for GBM have revealed mutations and aberrant gene expression associated with distinct types of GBM, patients with GBM are often diagnosed and classified based on MRI features. Therefore, we seek to identify molecular representatives in parallel with MRI classification for group I and group II primary GBM associated with the subventricular zone (SVZ). As group I and II GBM contain stemlike signature, we compared gene expression profiles between these 2 groups of primary GBM and endogenous neural stem progenitor cells to reveal dysregulation of cell cycle, chromatin status, cellular morphogenesis, and signaling pathways in these 2 types of MRI-classified GBM. In the absence of IDH mutation, several genes associated with metabolism are differentially expressed in these subtypes of primary GBM, implicating metabolic reprogramming occurs in tumor microenvironment. Furthermore, histone lysine methyltransferase EZH2 was upregulated while histone lysine demethylases KDM2 and KDM4 were downregulated in both group I and II primary GBM. Lastly, we identified 9 common genes across large data sets of gene expression profiles among MRI-classified group I/II GBM, a large cohort of GBM subtypes from TCGA, and glioma stem cells by unsupervised clustering comparison. These commonly upregulated genes have known functions in cell cycle, centromere assembly, chromosome segregation, and mitotic progression. Our findings highlight altered expression of genes important in chromosome integrity across all GBM, suggesting a common mechanism of disrupted fidelity of chromosome structure in GBM.

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DNA Methylation and Somatic Mutations Converge on the Cell Cycle and Define Similar Evolutionary Histories in Brain Tumors

Cited by 236 publications

References 56 publications

Clonal Heterogeneity and Tumor Evolution: Past, Present, and the Future

Clonal Heterogeneity and Tumor Evolution: Past, Present, and the Future

Overcoming therapeutic resistance in glioblastoma: the way forward

Comparative analyses identify molecular signature of MRI-classified SVZ-associated glioblastoma

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