Promotion of glioma cell survival by acyl-CoA synthetase 5 under extracellular acidosis conditions

Mashima, Tetsuo; Sato, Shigeo; Sugimoto, Yoshikazu; Tsuruo, Takashi; Seimiya, Hiroyuki

doi:10.1038/onc.2008.355

Cited by 62 publications

(58 citation statements)

References 41 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…However, additional studies are required to determine the functional significance of DNA methylation, if any, at these genes. Our finding of differentially methylated/accessible genes previously shown to harbor mutations in GBM-COL19A1 (Sumiyoshi et al 1997), CD93 (Dieterich et al 2012), AGAP2 (Knobbe et al 2005), and ACSL5 (Mashima et al 2009)-supports the validity of this approach in identifying GBM-relevant epigenetic perturbations. Interestingly, most of the genes that were identified as differentially methylated between GBM and NSC were classified as variably methylated in NSC (Table 4, lower).…”

Section: Discussionsupporting

confidence: 77%

Multiplex mapping of chromatin accessibility and DNA methylation within targeted single molecules identifies epigenetic heterogeneity in neural stem cells and glioblastoma

et al. 2013

View full text Add to dashboard Cite

Human tumors are comprised of heterogeneous cell populations that display diverse molecular and phenotypic features. To examine the extent to which epigenetic differences contribute to intratumoral cellular heterogeneity, we have developed a high-throughput method, termed MAPit-patch. The method uses multiplexed amplification of targeted sequences from submicrogram quantities of genomic DNA followed by next generation bisulfite sequencing. This provides highly scalable and simultaneous mapping of chromatin accessibility and DNA methylation on single molecules at high resolution. Long sequencing reads from targeted regions maintain the structural integrity of epigenetic information and provide substantial depth of coverage, detecting for the first time minority subpopulations of epigenetic configurations formerly obscured by existing genome-wide and population-ensemble methodologies. Analyzing a cohort of 71 promoters of genes with exons commonly mutated in cancer, MAPit-patch uncovered several differentially accessible and methylated promoters that are associated with altered gene expression between neural stem cell (NSC) and glioblastoma (GBM) cell populations. In addition, considering each promoter individually, substantial epigenetic heterogeneity was observed across the sequenced molecules, indicating the presence of epigenetically distinct cellular subpopulations. At the divergent MLH1/EPM2AIP1 promoter, a locus with three well-defined, nucleosome-depleted regions (NDRs), a fraction of promoter copies with inaccessible chromatin was detected and enriched upon selection of temozolomide-tolerant GBM cells. These results illustrate the biological relevance of epigenetically distinct subpopulations that in part underlie the phenotypic heterogeneity of tumor cell populations. Furthermore, these findings show that alterations in chromatin accessibility without accompanying changes in DNA methylation may constitute a novel class of epigenetic biomarker.

show abstract

Section: Discussionsupporting

confidence: 77%

Multiplex mapping of chromatin accessibility and DNA methylation within targeted single molecules identifies epigenetic heterogeneity in neural stem cells and glioblastoma

et al. 2013

View full text Add to dashboard Cite

show abstract

“…Further four genes [namely, midkine (MDK), caspase 1 (CASP1), vitamin D receptor (VDR), and protein-L-isoaspartate O-methyltransferase (PCMT1)], for which the results were significantly correlated in our analyses (with MDK, CASP1 and VDR being positively correlated to TMZ resistance, and PCMT1 negatively correlated to TMZ resistance) (Fig. 2), have previously been reported to be associated with chemotherapy resistance, prognosis, tumor progression, or antiproliferation, in malignant gliomas (25)(26)(27)(28)(29).…”

Section: Resultsmentioning

confidence: 54%

“…However, again, none of these genes were identified in our microarray analysis. On the other hand, highly significant statistically positive-and negative-correlation of genes concerned with TMZ sensitivity/resistance were found as shown in Tables II and III (25)(26)(27)(28)(29), were differentially expressed in association with TMZ sensitivity/resistance in the glioma-derived cell lines. Among the genes positively correlated to TMZ resistance in our analysis, one of the most noteworthy is MGMT, as mentioned above; MGMT expression provides a resistance measure that can potentially be applied to current TMZ-based treatment strategies for malignant glioma patients.…”

Section: Discussionmentioning

confidence: 99%

Gene expression profiling predicts response to temozolomide in malignant gliomas

Yoshino

Ogino²,

Yachi³

et al. 2010

Int J Oncol

View full text Add to dashboard Cite

Abstract. Malignant gliomas are highly lethal neoplasms that cannot be cured with currently available therapies. Temozolomide (TMZ) is a recently introduced alkylating agent that has yielded significant benefits and become a key agent in the treatment of high-grade gliomas. However, its survival benefit remains unsatisfactory. Understanding the molecular basis of TMZ sensitivity/resistance is necessary for improving the treatment outcome by devising strategies that are able to circumvent primary drug resistance. We therefore combined the in vitro TMZ response with microarray gene expression data to identify genes that could potentially be used to predict the response of malignant gliomas to TMZ therapy. We first obtained the individual IC 50 values for TMZ in seven malignant glioma cell lines (A-172, AM-38, T98G, U-87MG, U-138MG, U-251MG and YH-13) and then identified the genes whose expression correlated most highly with TMZ sensitivity employing a cDNA microarray. We present here a list of the most highly up-regulated and down-regulated genes which may be involved in conferring TMZ sensitivity/resistance in malignant gliomas, although most of the genes have not been implicated as a causal factor in the TMZ response except MGMT. We also demonstrated and confirmed the MGMT methylation status, quantitative MGMT mRNA levels, and MGMT protein expression levels in TMZ resistant glioma cells in vitro. Our results are thus consistent with previous studies and suggest that a dominant mechanism conferring sensitivity/resistance to TMZ exists in malignant glioma cells. Although the present study dose have several limitations, our reported candidate genes could represent not only potential molecular markers for TMZ sensitivity/resistance but also chemotherapy targets. Furthermore, the present study could provide a foundation for alternative therapeutic strategies including novel combination treatments that incorporate additional reagents directed at overcoming resistance to TMZ.

show abstract

“…ACSL5, another ACS isoform, plays a role in the pathogenesis of cancer. It is frequently overexpressed in malignant gliomas and is involved in their growth and survival (Yamashita et al, 2000;Mashima et al, 2009). Studies with a specific inhibitor of ACS, Triacsin c, further revealed that ACS inhibition induces selective apoptosis in cancer cells through the mitochondria-mediated pathway (Mashima et al, 2005).…”

Section: Acyl-coa Synthetasementioning

confidence: 99%

De novo fatty-acid synthesis and related pathways as molecular targets for cancer therapy

2009

Self Cite

View full text Add to dashboard Cite

show abstract

Promotion of glioma cell survival by acyl-CoA synthetase 5 under extracellular acidosis conditions

Cited by 62 publications

References 41 publications

Multiplex mapping of chromatin accessibility and DNA methylation within targeted single molecules identifies epigenetic heterogeneity in neural stem cells and glioblastoma

Multiplex mapping of chromatin accessibility and DNA methylation within targeted single molecules identifies epigenetic heterogeneity in neural stem cells and glioblastoma

Gene expression profiling predicts response to temozolomide in malignant gliomas

De novo fatty-acid synthesis and related pathways as molecular targets for cancer therapy

Contact Info

Product

Resources

About