Preclinical pharmacokinetics and metabolism of a novel prototype DNA-PK inhibitor NU7026

Nutley, Bernard; Smith, Norman E.; Hayes, Angela; Kèlland, Lloyd R.; Brunton, Lisa; Golding, Bernard T.; Smith, Graeme C.M.; Martin, Niall M.B.; Workman, Paul; Raynaud, Florence I.

doi:10.1038/sj.bjc.6602823

Cited by 85 publications

(69 citation statements)

References 24 publications

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“…It is plausible that PKB hyperactivity in the thymus in the absence of DNA-PK could be mediated by mTORC2, and tissue-specific disruption of the PKB/FoxO pathway could render DNA-PK-deficient thymic lymphomas susceptible to rapamycin treatment. A number of small molecule inhibitors of DNA-PK have been developed, and the inhibition of DNA-PK sensitizes cells to DNA-damaging agents (77,78). However, the use of DNA-PK inhibitors needs to be evaluated cautiously in the treatment of thymic lymphomas as loss of DNA-PK activity could lead to increased PKB signaling.…”

Section: Discussionmentioning

confidence: 99%

In Vivo Analysis of Protein Kinase B (PKB)/Akt Regulation in DNA-PKcs-null Mice Reveals a Role for PKB/Akt in DNA Damage Response and Tumorigenesis

Surucu

Bozulic

Hynx

et al. 2008

Journal of Biological Chemistry

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Section: Discussionmentioning

confidence: 99%

In Vivo Analysis of Protein Kinase B (PKB)/Akt Regulation in DNA-PKcs-null Mice Reveals a Role for PKB/Akt in DNA Damage Response and Tumorigenesis

Surucu

Bozulic

Hynx

et al. 2008

Journal of Biological Chemistry

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“…Mice were injected i.p. with the Rapamycin 37 (Sigma-Aldrich, St. Louis, MO, USA, #R0395) 7.5 mg per kg of body weight in 5% DMSO or AKT inhibitor 38 (NSC 154020, Calbiochem, Millipore) 20 mg per kg of body weight in 5% DMSO or ATM inhibitor (KU55933, Calbiochem, Millipore) 15 mg per kg of body weight in 5% DMSO or DNA-PK inhibitor 39 (NU7026, Sigma-Aldrich) 15 mg per kg of body weight in 5% DMSO or p38MAPK inhibitor 12 (SB202190, SigmaAldrich) 10 mg per kg of body weight in 5% DMSO, or GSK-3 inhibitors IX 6 (Calbiochem, Millipore) 15 mg per kg of body weight in 5% DMSO. After 6, 10, or 12 h, mice were euthanized and organs were collected for subsequent analysis.…”

Section: Methodsmentioning

confidence: 99%

Role of Gadd45a in Wip1-dependent regulation of intestinal tumorigenesis

et al. 2012

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Conversion of intestinal stem cells into tumor-initiating cells is an early step in Apc Min -induced polyposis. Wild-type p53-induced phosphatase 1 (Wip1)-dependent activation of a DNA damage response and p53 has a permanent role in suppression of stem cell conversion, and deletion of Wip1 lowers the tumor burden in Apc Min mice. Here we show that cyclin-dependent kinase inhibitor 2a, checkpoint kinase 2, and growth arrest and DNA damage gene 45a (Gadd45a) exert critical functions in the tumor-resistant phenotype of Wip1-deficient mice. We further identified Gadd45a as a haploinsufficient gene in the regulation of Wip1-dependent tumor resistance in mice. Gadd45a appears to function through its ability to activate the Jnk-dependent signaling pathway that in turn is a necessary mediator of the proapoptotic functions of p53 that respond to activation of the b-catenin signaling pathway. We propose that silencing of Gadd45a is sufficient to override p53 activation in the presence of active b-catenin under conditions of an enhanced DNA damage response. Cell Death and Differentiation (2012) 19, 1761-1768 doi:10.1038/cdd.2012; published online 4 May 2012Conversion of normal cells into tumor-initiating cells is an initial step in the course of formation of any tumor. 1 The majority of cells in an organism are terminally differentiated and thus are not capable of conversion into tumor-initiating cells, which requires cellular proliferation. In many instances, proliferative progenitors are programmed to divide only a few times before full differentiation; acquiring oncogenic mutations at this stage may also have a limited impact on tumorigenesis unless the mutation blocks differentiation. Increasing evidence in turn indicates that certain types of cancers originate from adult stem cells, the only proliferative cells that exist in the animal for a significant period of time that may be sufficient to accumulate oncogenic mutations. Several studies have demonstrated the role of adult stem cells as an origin of cancer, at least in certain tissues such as mouse intestine. 2 Stem cell-specific inactivation of Apc (adenomatous polyposis coli ), the major regulator of tumorigenesis in the intestine, results in full-blown polyposis within a few weeks. 3 In contrast, deletion of Apc in proliferative progenitors or more differentiated cell types fails to induce sustainable cancer. 3 In many instances, activation of oncogenes in normal cells sets off the defense mechanisms to protect them from potential transformation. 4 The major pathway that has had evolved to perform this function is controlled by a tumor suppressor p53. Depending on the strength of the signal, which in many cases relies on the type of oncogene, p53 activates apoptosis, transient or permanent cell cycle arrest called senescence. 5 Modulation of p53 levels and activity may therefore be critical to the regulation of cell susceptibility to oncogenic transformation. Regulation of p53 by various means to prevent oncogenic transformation may be especially important when ...

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“…Nutley et al determined that NU7026 potentiated the effects of IR, although predominantly after prolonged exposure i.e. 6 or 24 h. Hence, the most intensive effects of NU7026 will be hardly achievable in vivo because the level of NU7026 was undetectable 4 h after application 56 . NU7441, another inhibitor from chromenone library, is the most potent and selective inhibitor of DNA-PK so far, with IC 50 : 14 nM, it is 100-fold more selective inhibitor of DNA-PK in comparison to other PI3-K kinases 52,60 .…”

Section: Dna-pk Inhibitorsmentioning

confidence: 99%

“…Unlike wortmannin or LY294002, NU7026 had no effect on PI3-K (ref. 56 ). Cells treated with etoposide and NU7026 showed G 2 /M cell cycle arrest 59 .…”

Section: Dna-pk Inhibitorsmentioning

confidence: 99%

“…NU7026, an inhibitor from chromenone library, is a cell permeable, ATP-competitive inhibitor of DNA-PK and ATM, but predominantly affects DNA-PK with IC 50 : 0,23 μM, IC 50 for ATM is more than 100 μM (ref. 56,57 ). Tichy et al observed the complete growth inhibition of leukemic cells after combination of 10 μM NU7026 and the dose of 1 Gy.…”

Section: Dna-pk Inhibitorsmentioning

confidence: 99%

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Chemical inhibition of DNA repair kinases as a promising tool in oncology

Ďurišová¹,

Šalovská²,

Pejchal³

et al. 2016

BIOMED PAP

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Background. DNA repair pathways play a major role in tumour resistance towards chemo-and radiotherapy. Therefore, inhibitors of specific DNA repair pathways might be advantageous when used in combination with DNA-damaging agents, such as ionizing radiation. This review put particular emphasis on the key DNA repair enzymes: DNA-dependent protein kinase (DNA-PK), ataxia-telangiectasia mutated kinase (ATM) and ATM-Rad3-related kinase (ATR) and their specific inhibitors in the context of radio-sensitization. Results. We reviewed recent studies on novel and potent inhibitors and found evidence that inhibitors of DNA repair pathways such as small molecule inhibitors could be efficient and selective in tumour cells. Interpretation of recent literature results accompanied with implications for practice and further research are presented. Conclusions. The prospects of targeting DNA repair enzymes to treat cancer are optimistic, but future work will show if this approach has a significant in vivo efficacy, since we are still waiting for the inhibitor which would pass all phases in clinical trials. In spite of the fact that a number of drugs possess interesting synergy of radiotherapy in vitro, the future use will depend on developing compounds with improved solubility and the serum half-life. Normal tissue toxicity leading to a significant increase of radiotherapy efficiency remains a key question that might be answered only by clinical trials.

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Preclinical pharmacokinetics and metabolism of a novel prototype DNA-PK inhibitor NU7026

Cited by 85 publications

References 24 publications

In Vivo Analysis of Protein Kinase B (PKB)/Akt Regulation in DNA-PKcs-null Mice Reveals a Role for PKB/Akt in DNA Damage Response and Tumorigenesis

In Vivo Analysis of Protein Kinase B (PKB)/Akt Regulation in DNA-PKcs-null Mice Reveals a Role for PKB/Akt in DNA Damage Response and Tumorigenesis

Role of Gadd45a in Wip1-dependent regulation of intestinal tumorigenesis

Chemical inhibition of DNA repair kinases as a promising tool in oncology

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