Review of Poly (ADP-ribose) Polymerase (PARP) Mechanisms of Action and Rationale for Targeting in Cancer and Other Diseases

Morales, Julio C.; Li, Long Shan; Fattah, Farjana J.; Dong, Ying; Bey, Erik A.; Patel, Malina; Gao, Jinming; Boothman, David A.

doi:10.1615/critreveukaryotgeneexpr.2013006875

Cited by 496 publications

(385 citation statements)

References 86 publications

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“…Poly ADP ribose polymerase (PARP) is an essential mediator of BER that targets single-strand breaks (SSBs) induced by DNA damage and recruits BER complex proteins (Morales et al, 2014). The peak of DNA demethylation upon 10 days of Tet2 restoration to cKit + cells correlated with increased expression of Parp and Gadd45 (Figure 7D), whose gene products function in DNA demethylation (Barreto et al, 2007; Ciccarone et al, 2012).…”

Section: Resultsmentioning

confidence: 99%

Restoration of TET2 Function Blocks Aberrant Self-Renewal and Leukemia Progression

Cimmino

Dolgalev

Wang³

et al. 2017

Cell

542

556

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SUMMARY Loss-of-function mutations in TET2 occur frequently in patients with clonal hematopoiesis, myelodysplastic syndrome (MDS), and acute myeloid leukemia (AML) and are associated with a DNA hypermethylation phenotype. To determine the role of TET2 deficiency in leukemia stem cell maintenance, we generated a reversible transgenic RNAi mouse to model restoration of endogenous Tet2 expression. Tet2 restoration reverses aberrant hematopoietic stem and progenitor cell (HSPC) self-renewal in vitro and in vivo. Treatment with vitamin C, a cofactor of Fe2+ and α-KG-dependent dioxygenases, mimics TET2 restoration by enhancing 5-hydroxymethylcytosine formation in Tet2-deficient mouse HSPCs and suppresses human leukemic colony formation and leukemia progression of primary human leukemia PDXs. Vitamin C also drives DNA hypomethylation and expression of a TET2-dependent gene signature in human leukemia cell lines. Furthermore, TET-mediated DNA oxidation induced by vitamin C treatment in leukemia cells enhances their sensitivity to PARP inhibition and could provide a safe and effective combination strategy to selectively target TET deficiency in cancer.

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Section: Resultsmentioning

confidence: 99%

Restoration of TET2 Function Blocks Aberrant Self-Renewal and Leukemia Progression

Cimmino

Dolgalev

Wang³

et al. 2017

Cell

542

556

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“…Extensive research has revealed numerous PARP1 functions spanning a diverse array of nuclear processes, including DNA damage repair (2)(3)(4)(5), chromatin remodeling (6), transcriptional regulation (6), telomere maintenance (7), and cell death (8). Owing primarily to the role of PARP1 (and the related but less abundant PARP2 and PARP3) in DNA damage repair, a number of PARP inhibitors are undergoing clinical development as anticancer agents with a focus on tumors with impaired homologous recombination (HR) capability and on combination regimens with DNA-damaging chemotherapy or radiation (9).…”

Section: Introductionmentioning

confidence: 99%

Mechanistic Dissection of PARP1 Trapping and the Impact on In Vivo Tolerability and Efficacy of PARP Inhibitors

Hopkins

Shi

Rodrı́guez

et al. 2015

Molecular Cancer Research

213

217

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Poly(ADP-ribose) polymerases (PARP1, -2, and -3) play important roles in DNA damage repair. As such, a number of PARP inhibitors are undergoing clinical development as anticancer therapies, particularly in tumors with DNA repair deficits and in combination with DNA-damaging agents. Preclinical evidence indicates that PARP inhibitors potentiate the cytotoxicity of DNA alkylating agents. It has been proposed that a major mechanism underlying this activity is the allosteric trapping of PARP1 at DNA single-strand breaks during base excision repair; however, direct evidence of allostery has not been reported. Here the data reveal that veliparib, olaparib, niraparib, and talazoparib (BMN-673) potentiate the cytotoxicity of alkylating agents. Consistent with this, all four drugs possess PARP1 trapping activity. Using biochemical and cellular approaches, we directly probe the trapping mechanism for an allosteric component. These studies indicate that trapping is due to catalytic inhibition and not allostery. The potency of PARP inhibitors with respect to trapping and catalytic inhibition is linearly correlated in biochemical systems but is nonlinear in cells. High-content imaging of gH2Ax levels suggests that this is attributable to differential potentiation of DNA damage in cells. Trapping potency is inversely correlated with tolerability when PARP inhibitors are combined with temozolomide in mouse xenograft studies. As a result, PARP inhibitors with dramatically different trapping potencies elicit comparable in vivo efficacy at maximum tolerated doses. Finally, the impact of trapping on tolerability and efficacy is likely to be context specific.Implications: Understanding the context-specific relationships of trapping and catalytic inhibition with both tolerability and efficacy will aid in determining the suitability of a PARP inhibitor for inclusion in a particular clinical regimen.

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“…Again, colony survival assays confirmed this hypothesis although it should be noted that the effect was less significant than observed at the lower oxygen level. This is perhaps not surprising given the role of PARP in the response to replication stress [79]. However, our data demonstrating that proliferating hypoxic cells are sensitive to PARP inhibition are extremely promising clinically, as these cells are more abundant and more accessible in a solid tumour.…”

Section: Targeting Tumour Hypoxia Through Parp Inhibitionmentioning

confidence: 75%

Targeting Tumour Hypoxia with PARP Inhibitors: Contextual Synthetic Lethality

Leszczynska

Temper

Bristow

et al. 2015

Cancer Drug Discovery and Development

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As previously discussed in Chap. 13 the concept of synthetic lethality is not novel and has been extensively used to dissect yeast-signalling pathways. More recently, this concept has been embraced as a more personalised approach to cancer therapy, exploiting the fact that a tumour with a defect in pathway A will show increased sensitivity to an agent-targeting pathway B. Contextual synthetic lethality refers to a situation where one of the two pathways is lost as a result of the cellular or microenvironmental context and is rendered sensitive to loss of a second pathway. The first example of contextual synthetic lethality to be described was the use of a PARP inhibitor in hypoxic tumour cells. In this chapter we will first discuss how tumour hypoxia arises and then most importantly the effect of hypoxia on the DNA repair pathways. Finally, we will review how reduced levels of homologous recombination lead to an increased sensitivity to PARP inhibitors in hypoxic tumours.

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Review of Poly (ADP-ribose) Polymerase (PARP) Mechanisms of Action and Rationale for Targeting in Cancer and Other Diseases

Cited by 496 publications

References 86 publications

Restoration of TET2 Function Blocks Aberrant Self-Renewal and Leukemia Progression

Restoration of TET2 Function Blocks Aberrant Self-Renewal and Leukemia Progression

Mechanistic Dissection of PARP1 Trapping and the Impact on In Vivo Tolerability and Efficacy of PARP Inhibitors

Targeting Tumour Hypoxia with PARP Inhibitors: Contextual Synthetic Lethality

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