Effect of Promoter Methylation of the p16 Gene on Phosphorylation of Retinoblastoma Gene Product and Growth of Hepatocellular Carcinoma Cells

Maeta, Yoshiko; Shiota, Goshi; Okano, Jun-ichi; Murawaki, Yoshikazu

doi:10.1159/000089288

Cited by 13 publications

(8 citation statements)

References 23 publications

(35 reference statements)

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“…136 Along similar lines, histone deacetylase inhibitors can affect the DDR by modifying the expression of proteins involved in HR. 137 Indeed, the histone deacetylase inhibitor suberoylanilide hydroxamic acid efficiently inhibits the growth of hepatocellular carcinoma cells when associated with olaparib. 138 These findings are encouraging, but need further confirmation.…”

Section: Box 2 Brcanessmentioning

confidence: 99%

Predictive biomarkers for cancer therapy with PARP inhibitors

Michels

Vitale²,

Saparbaev

et al. 2013

Oncogene

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Poly(ADP-ribose) polymerase (PARP) inhibitors have raised high expectations for the treatment of multiple malignancies. PARP inhibitors, which can be used as monotherapies or in combination with DNA-damaging agents, are particularly efficient against tumors with defects in DNA repair mechanisms, in particular the homologous recombination pathway, for instance due to BRCA mutations. Thus, deficient DNA repair provides a framework for the success of PARP inhibitors in medical oncology. Here, we review encouraging results obtained in recent clinical trials investigating the safety and efficacy of PARP inhibitors as anticancer agents. We discuss emerging mechanisms of regulation of homologous recombination and how inhibition of DNA repair might be used in cancer therapy. We surmise that the identification of patients that are likely to benefit from PARP inhibition will improve the clinical use of PARP inhibitors in a defined target population. Thus, we will place special emphasis on biomarker discovery.

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Section: Box 2 Brcanessmentioning

confidence: 99%

Predictive biomarkers for cancer therapy with PARP inhibitors

Michels

Vitale²,

Saparbaev

et al. 2013

Oncogene

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“…However, the frequency of methylation for many classically known tumor suppressors varies widely, some being as low as 15% (55–58). Using p16 as an example, analysis of the tumor samples with matched normals did not uncover tumor suppresors such as p16 and since we demonstrate the ability to detect p16 methylation in the cell line HuH7 (43) with known methylation it is likely that none of the tumors had methylation of p16 . Therefore, although improvements are always possible, we feel that our technical and analytical methods are sound.…”

Section: Discussionmentioning

confidence: 72%

“…Any ratio difference above this level was found to be methylated in one of the samples. To determine if our method could accurately identify known tumor suppressor CpG island methylation, we then analyzed the hepatocellular cancer cell line HuH7 with known methylation of the p16 promoter (43). In Figure 2F we show the detection of methylation of the region of the p16 gene CpG island commonly methylated and correlated with decreased gene transcription.…”

Section: Resultsmentioning

confidence: 99%

“…We then legitimatized the method's ability to detect methylation by bisulfite sequence validating over 15 fragments. We went on to analyze a number of samples that have been analyzed by others either by bisulfite sequencing or by other genome-wide approaches for methylation detection (43,45). In the case of Maeta et al ., we have validated specific methylation events and in the case of Sato et al .…”

Section: Discussionmentioning

confidence: 99%

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Methylation detection oligonucleotide microarray analysis: a high-resolution method for detection of CpG island methylation

Kamalakaran

Kendall

Zhao

et al. 2009

Nucleic Acids Research

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Methylation of CpG islands associated with genes can affect the expression of the proximal gene, and methylation of non-associated CpG islands correlates to genomic instability. This epigenetic modification has been shown to be important in many pathologies, from development and disease to cancer. We report the development of a novel high-resolution microarray that detects the methylation status of over 25 000 CpG islands in the human genome. Experiments were performed to demonstrate low system noise in the methodology and that the array probes have a high signal to noise ratio. Methylation measurements between different cell lines were validated demonstrating the accuracy of measurement. We then identified alterations in CpG islands, both those associated with gene promoters, as well as non-promoter-associated islands in a set of breast and ovarian tumors. We demonstrate that this methodology accurately identifies methylation profiles in cancer and in principle it can differentiate any CpG methylation alterations and can be adapted to analyze other species.

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“…Maeta et al . observed that when HCC cells were treated with demethylating agents, there was increased expression of p16 INK4a and subsequent cell growth inhibition, suggesting that modulation of the epigenetic control of these genes may be an important target in HCC therapeutics 28 . Lee et al .…”

Section: Tumour Type‐specific Methylationmentioning

confidence: 99%