O<sup>6</sup>‐methylguanine DNA methyltransferase and p53 status predict temozolomide sensitivity in human malignant glioma cells

Hermisson, Mirjam; Klumpp, Andrea; Wick, Wolfgang; Wischhusen, Jörg; Nagel, Georg; Roos, Wynand P.; Kaina, Bernd; Weller, Michael

doi:10.1111/j.1471-4159.2005.03583.x

Cited by 294 publications

(291 citation statements)

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“…Similarly, p53 was shown to function as a survival factor in the gastrointestinal tract under conditions of severe irradiation, which was attributed to increased sensitivity of vascular endothelial cells (Komarova et al, 2004;Burdelya et al, 2006). Furthermore, other reports have identified conditions in which absence of p53 led to elevated apoptosis, but a direct causal role for p53 in providing survival signals has not been described (Lassus et al, 1996;Lackinger and Kaina, 2000;Hermisson et al, 2006;Batista et al, 2007;Roepke et al, 2007;Roos et al, 2007). Notwithstanding these occasional reports, the major observations that p53 activation often leads to apoptosis or DNA repair have been overwhelming, and hence, have overshadowed the exploration of the survival-promoting properties of p53.…”

Section: Discussionmentioning

confidence: 99%

“…For example, absence of p53 has been shown to promote taxol-mediated death owing to failure of cell arrest in the G 1 phase of the cell cycle, and hence, allowing cells to accumulate in the G 2 /M phase where they undergo mitotic cell death (Vikhanskaya et al, 1998). In addition, cells with wild-type p53 have been shown to be more resistant to cytotoxic drug treatment in some cases (Hermisson et al, 2006;Batista et al, 2007;Roos et al, 2007). Other reports have also shown that absence of p53 leads to sensitization to UV irradiation and alkalyting agents in mouse embryonic fibroblasts (MEFs), and to thymoquinone-induced apoptosis in human cells (Lackinger and Kaina, 2000;Roepke et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

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p53 promotes cellular survival in a context-dependent manner by directly inducing the expression of haeme-oxygenase-1

Nam

Sabapathy

2011

Oncogene

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

p53 promotes cellular survival in a context-dependent manner by directly inducing the expression of haeme-oxygenase-1

Nam

Sabapathy

2011

Oncogene

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“…Neither dexamethsone nor irradiation induced MGMT gene transcription in glioma cells in vitro. 68 In tissue culture and animal studies, however, temozolomide strongly induced MGMT protein expression in temozolomide-resistant glioma cells lacking MGMT promoter methylation. 69 Loss of MGMT promoter methylation might represent a key mechanism by which patients with initially methylated tumors eventually acquire resistance to temozolomide, leading to progression or relapse.…”

Section: A Role For Routine Mgmt Testing?mentioning

confidence: 99%

MGMT promoter methylation in malignant gliomas: ready for personalized medicine?

et al. 2009

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The DNA repair enzyme O 6 -methylguanine-DNA methyltransferase (MGMT) antagonizes the genotoxic effects of alkylating agents. MGMT promoter methylation is the key mechanism of MGMT gene silencing and predicts a favorable outcome in patients with glioblastoma who are exposed to alkylating agent chemotherapy. This biomarker is on the verge of entering clinical decision-making and is currently used to stratify or even select glioblastoma patients for clinical trials. In other subtypes of glioma, such as anaplastic gliomas, the relevance of MGMT promoter methylation might extend beyond the prediction of chemosensitivity, and could reflect a distinct molecular profile.Here, we review the most commonly used assays for evaluation of MGMT status, outline the prerequisites for standardized tests, and evaluate reasons for difficulties in reproducibility. We critically discuss the prognostic and predictive value of MGMT silencing, reviewing trials in which patients with different types of glioma were treated with various chemotherapy schedules, either upfront or at recurrence. Standardization of MGMT testing requires comparison of different technologies across laboratories, and prospectively validated cut-off values for prognostic or predictive effects. Moreover, future clinical trials will need to determine, for each subtype of glioma, the degree to which MGMT promoter methylation is predictive or prognostic, and whether testing should become routine clinical practice.

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“…For assessment of TMZ concentrations and doses of radiation the protocol of Hermisson et al (2006) was adapted. Cytotoxicity assays were done afterwards to optimize the doses for Hs683 cells (data not shown).…”

Section: Irradiation and Tmz Treatmentmentioning

confidence: 99%

Downregulation of PRDX1 by promoter hypermethylation is frequent in 1p/19q-deleted oligodendroglial tumours and increases radio- and chemosensitivity of Hs683 glioma cells in vitro

et al. 2011

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Deletions of chromosomal arms 1p and 19q are frequent in oligodendroglial tumours and linked to radio-and chemotherapy response as well as longer survival. The molecular mechanisms underlying this clinically important association are as yet unknown. Here, we studied the peroxiredoxin 1 (PRDX1) gene at 1p34.1 for promoter methylation and expression in primary gliomas and investigated its role in radio-and chemosensitivity of glioma cells in vitro. In total, we screened primary glioma tissues from 93 patients for methylation of the 5 0 -CpG island of PRDX1 by sodium bisulfite sequencing. PRDX1 mRNA and protein expression levels were determined in subsets of the tumours by quantitative PCR and western blot analysis, respectively. PRDX1 hypermethylation and reduced expression were frequently detected in oligodendroglial tumours and secondary glioblastomas, but not in primary glioblastomas. In oligodendroglial tumours, both PRDX1 hypermethylation and reduced mRNA expression were significantly associated with 1p/19q-deletion. Stable knockdown of PRDX1 by lentiviral transduction of shorthairpin (sh)RNA constructs significantly increased apoptosis and reduced cell viability of Hs683 glioma cells exposed to ionizing irradiation or temozolomide in vitro. Taken together, our findings indicate that epigenetic silencing of PRDX1 is frequent in 1p/19q-deleted oligodendroglial tumours and likely contributes to radioand chemosensitivity of these tumours.

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O⁶‐methylguanine DNA methyltransferase and p53 status predict temozolomide sensitivity in human malignant glioma cells

Cited by 294 publications

References 50 publications

p53 promotes cellular survival in a context-dependent manner by directly inducing the expression of haeme-oxygenase-1

p53 promotes cellular survival in a context-dependent manner by directly inducing the expression of haeme-oxygenase-1

MGMT promoter methylation in malignant gliomas: ready for personalized medicine?

Downregulation of PRDX1 by promoter hypermethylation is frequent in 1p/19q-deleted oligodendroglial tumours and increases radio- and chemosensitivity of Hs683 glioma cells in vitro

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O6‐methylguanine DNA methyltransferase and p53 status predict temozolomide sensitivity in human malignant glioma cells

Cited by 294 publications

References 50 publications

p53 promotes cellular survival in a context-dependent manner by directly inducing the expression of haeme-oxygenase-1

p53 promotes cellular survival in a context-dependent manner by directly inducing the expression of haeme-oxygenase-1

MGMT promoter methylation in malignant gliomas: ready for personalized medicine?

Downregulation of PRDX1 by promoter hypermethylation is frequent in 1p/19q-deleted oligodendroglial tumours and increases radio- and chemosensitivity of Hs683 glioma cells in vitro

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O⁶‐methylguanine DNA methyltransferase and p53 status predict temozolomide sensitivity in human malignant glioma cells