Enhanced expression of poly(ADP‐ribose) synthetase gene in malignant lymphoma

Tomoda, Takashi; Kurashige, Takanobu; Moriki, Toshiaki; Yamamoto, Hiroshi; Fujimoto, Shigeyoshi; Taniguchi, Tadatsugu

doi:10.1002/ajh.2830370402

Cited by 67 publications

(39 citation statements)

References 19 publications

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“…Consistent with these findings are the data from a number of PARP inhibitors based on nicotinamide analogues, ranging from those with low micromolar activity, such as 3-aminobenzamide (Durkacz et al, 1980) to the more potent and specific PARP inhibitors that have been generated more recently (Southan and Szabo, 2003;Curtin, 2005;Farmer et al, 2005;Ratnam and Low, 2007). Enhanced PARP-1 expression or activity has been observed in a number of different tumour cell lines (Tomoda et al, 1991;Shiobara et al, 2001) and could provide a greater level of resistance to both endogenous genotoxic stress, as well as to DNA damage-inducing therapeutic agents. Evidence that PARP inhibitors can sensitize tumour cells to cytotoxic therapies such as temozolomide, topoisomerase I inhibitors, platinums and radiation (for example Calabrese et al, 2004;Miknyoczki et al, 2003;Chalmers et al, 2004) has consequently provided sufficient interest for a number of these compounds to be developed as clinical candidates (see Table 2 and Plummer, 2005;Fong et al, 2006).…”

Section: Inhibitors Of Parpsupporting

confidence: 72%

Targeted cancer therapies based on the inhibition of DNA strand break repair

2007

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Both DNA double-and single-strand break repair are highly coordinated processes utilizing signal transduction cascades and post-translational modifications such as phosphorylation, acetylation and ADP ribosylation. 'Drugable' targets within these networks have been identified that could potentially lead to novel therapeutic approaches within the oncology arena. Key regulators within these signalling cascades, such as DNA-dependent protein kinase, ataxia-telangiectasia mutated, checkpoint kinase 1 (CHK1), checkpoint kinase 2 (CHK2) and poly(ADPribose) polymerase, use either ATP or nicotinamide adenine dinucleotide for their enzymatic functions and are therefore readily accessible to small molecule inhibition at their catalytic sites. A range of highly potent and selective inhibitors of these DNA damage response pathways has now been identified through drug discovery efforts, with candidate molecules either approaching or already in clinical trials. This review will describe the small molecule inhibitors and drug discovery activities that focus on DNA break repair, along with the therapeutic rationale behind chemosensitization and the concept of synthetic lethality. We will also describe the emerging clinical data coming from this exciting new approach to targeted cancer therapy.

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Section: Inhibitors Of Parpsupporting

confidence: 72%

Targeted cancer therapies based on the inhibition of DNA strand break repair

2007

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“…A higher level of PARP-1 mRNA was observed in malignant lymphoma cells compared with normal lymph nodes (Tomoda et al, 1991) and in colorectal adenocarcinoma biopsies compared with adjacent non-tumour tissues and hyperplastic polyps (Nosho et al, 2006). Evaluation of PARP-1 protein expression in hepatocellular carcinoma (HCC) by western blotting revealed that it was significantly increased in HCC, especially moderately differentiated, compared with the non-tumour samples (Shimizu et al, 2004).…”

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confidence: 94%

Poly(ADP-ribose) polymerase-1 polymorphisms, expression and activity in selected human tumour cell lines

et al. 2009

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BACKGROUND: Poly(ADP-ribose) polymerase-1 (PARP-1) is a DNA-binding enzyme activated by DNA breaks and involved in DNA repair and other cellular processes. Poly(ADP-ribose) polymerase activity can be higher in cancer than in adjacent normal tissue, but cancer predisposition is reported to be greater in individuals with a single-nucleotide polymorphism (SNP) V762A (T2444C) in the catalytic domain that reduces PARP-1 activity. METHODS: To resolve these divergent observations, we determined PARP-1 polymorphisms, PARP-1 protein expression and activity in a panel of 19 solid and haematological, adult and paediatric human cancer cell lines. RESULTS: There was a wide variation in PARP activity in the cell line panel (coefficient of variation, CV ¼ 103%), with the lowest and the highest activity being 2460 pmol PAR/10 6 (HS-5 cells) and 85 750 pmol PAR/10 6 (NGP cells). Lower variation (CV ¼ 32%) was observed in PARP-1 protein expression with the lowest expression being 2.0 ng mg À1 (HS-5 cells) and the highest being 7.1 ng mg À1 (ML-1 cells). The mean activity in the cancer cells was 45-fold higher than the mean activity in normal human lymphocytes and the PARP-1 protein levels were 23-fold higher. CONCLUSIONS: Surprisingly, there was no significant correlation between PARP activity and PARP-1 protein level or the investigated polymorphisms, T2444C and CA.

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“…For example, PARP mRNA levels were found to be enhanced in malignant lymphomas but not in normal lymph nodes or reactive proliferative lymph nodes (17). Elevated PARP activity was identified in peripheral lymphocytes from patients with low-grade malignant non -Hodgkin's lymphoma (18), hepatocellular carcinomas (19,20), small-cell lung cancer lines (21), cervical cancer cells from patients (22), and the prostate cancer cell line LnCaP (23).…”

Section: Introductionmentioning

confidence: 99%

Potentiation of Temozolomide Cytotoxicity by Poly(ADP)Ribose Polymerase Inhibitor ABT-888 Requires a Conversion of Single-Stranded DNA Damages to Double-Stranded DNA Breaks

Liu¹,

Shi²,

Guan³

et al. 2008

Molecular Cancer Research

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Poly(ADP-ribose) polymerase (PARP) senses DNA breaks and facilitates DNA repair via the polyADP-ribosylation of various DNA binding and repair proteins. We explored the mechanism of potentiation of temozolomide cytotoxicity by the PARP inhibitor ABT-888. We showed that cells treated with temozolomide need to be exposed to ABT-888 for at least 17 to 24 hours to achieve maximal cytotoxicity. The extent of cytotoxicity correlates with the level of double-stranded DNA breaks as indicated by ;H2AX levels. In synchronized cells, damaging DNA with temozolomide in the presence of ABT-888 during the S phase generated high levels of double-stranded breaks, presumably because the single-stranded DNA breaks resulting from the cleavage of the methylated nucleotides were converted into double-stranded breaks through DNA replication. As a result, treatment of temozolomide and ABT-888 during the S phase leads to higher levels of cytotoxicity. ABT-888 inhibits poly(ADP-ribose) formation in vivo and enhances tumor growth inhibition by temozolomide in multiple models. ABT-888 is well tolerated in animal models. ABT-888 is currently in clinical trials in combination with temozolomide. (Mol Cancer Res 2008;6(10):1621 -9)

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Enhanced expression of poly(ADP‐ribose) synthetase gene in malignant lymphoma

Cited by 67 publications

References 19 publications

Targeted cancer therapies based on the inhibition of DNA strand break repair

Targeted cancer therapies based on the inhibition of DNA strand break repair

Poly(ADP-ribose) polymerase-1 polymorphisms, expression and activity in selected human tumour cell lines

Potentiation of Temozolomide Cytotoxicity by Poly(ADP)Ribose Polymerase Inhibitor ABT-888 Requires a Conversion of Single-Stranded DNA Damages to Double-Stranded DNA Breaks

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