Mitoxantrone in combination with an inhibitor of DNA‐dependent protein kinase: a potential therapy for high risk B‐cell chronic lymphocytic leukaemia

Elliott, Sarah; Crawford, Clark; Mulligan, Evan A.; Summerfield, Geoffrey; Newton, Paula; Wallis, Jonathan P.; Mainou‐Fowler, Tryfonia; Evans, Paul; Bedwell, Clare; Durkacz, Barbara W.; Willmore, Elaine

doi:10.1111/j.1365-2141.2010.08425.x

Cited by 35 publications

(26 citation statements)

References 28 publications

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“…The potential for on-target interactions between DDR inhibition and coadministered conventional DNAdamaging cytotoxic modalities requires investigation. Antagonism of the DDR may sensitize it to sequentially scheduled chemotherapy 48 or radiotherapy. 39,40 Additionally, p53-independent BMF induction by BEZ235 could be beneficial in combination with corticosteroids (which also induce BMF 29 ), potentially abrogating glucocorticoid resistance.…”

Section: Discussionmentioning

confidence: 99%

“…To further define the relative importance of these kinases in apoptotic responses, we used a panel of inhibitors that selectively inhibited different BEZ235 targets ( Figure 1; Table 1). Specifically, BEZ235 was compared with BKM120 (PI3K-selective inhibitor 46 ), KU63794 (ATP-competitive mTORC1/2 inhibitor 47 ), KU55933 (ATM inhibitor), and KU57788 (DNA-PK inhibitor 48 ). Although these inhibitors have an affinity for their respective targets in the nanomolar concentration range (Table 1), none recapitulated the apoptotic response observed with BEZ235 ( Figure 5A).…”

Section: Selective Inhibition Of Individual Pi3k-related Kinases Is Lmentioning

confidence: 99%

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Combined inhibition of PI3K-related DNA damage response kinases and mTORC1 induces apoptosis in MYC-driven B-cell lymphomas

Shortt

Martin

Newbold

et al. 2013

Blood

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Key Points• MYC-driven lymphomas demonstrate activation of mTORC1 and an endogenous DNA damage response.• BEZ235 inhibits PI3K-related DNA damage response kinases and mTORC1, inducing p53-independent upregulation of proapoptotic BMF.Pharmacological strategies capable of directly targeting MYC are elusive. Previous studies have shown that MYC-driven lymphomagenesis is associated with mammalian target of rapamycin (mTOR) activation and a MYC-evoked DNA damage response (DDR) transduced by phosphatidylinositol-3-kinase (PI3K)-related kinases (DNA-PK, ATM, and ATR). Here we report that BEZ235, a multitargeted pan-PI3K/dual-mTOR inhibitor, potently killed primary Myc-driven B-cell lymphomas and human cell lines bearing IGcMYC translocations. Using pharmacologic and genetic dissection of PI3K/mTOR signaling, dual DDR/mTORC1 inhibition was identified as a key mediator of apoptosis. Moreover, apoptosis was initiated at drug concentrations insufficient to antagonize PI3K/mTORC2-regulated AKT phosphorylation. p53-independent induction of the proapoptotic BH3-only protein BMF was identified as a mechanism by which dual DDR/mTORC1 inhibition caused lymphoma cell death. BEZ235 treatment induced apoptotic tumor regressions in vivo that correlated with suppression of mTORC1-regulated substrates and reduced H2AX phosphorylation and also with feedback phosphorylation of AKT. These mechanistic studies hold important implications for the use of multitargeted PI3K inhibitors in the treatment of hematologic malignancies. In particular, the newly elucidated role of PI3K-related DDR kinases in response to PI3K inhibitors offers a novel therapeutic opportunity for the treatment of hematologic malignancies with an MYC-driven DDR. (Blood. 2013;121(15):2964-2974

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Section: Discussionmentioning

confidence: 99%

Section: Selective Inhibition Of Individual Pi3k-related Kinases Is Lmentioning

confidence: 99%

Combined inhibition of PI3K-related DNA damage response kinases and mTORC1 induces apoptosis in MYC-driven B-cell lymphomas

Shortt

Martin

Newbold

et al. 2013

Blood

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“…In consequence, use of wortmanin, an inhibitor of PI3-Kinases along with DNA-PKcs (which is PI3-K like kinase), was able to potentialize cytotoxic effect of chlorambucil in CLL cells (Christodoulopoulos et al, 1998). Also, a DNA-PKcs specific inhibitor Nu7441 combined with drugs inducing DNA DSBs has been pointed as a potential therapy for high risk CLL (Elliott et al, 2011). After genotoxic stress and first cell division, structural chromosomal aberrations (dicentric, acentric or ring chromosomes) occurred more frequently in resistant than in sensitive CLL cells (Blaise et al, 2001), suggesting an accelerated but certainly unfaithful DNA repair.…”

Section: Dna Repair Defect?mentioning

confidence: 99%

DNA Damage Response/Signaling and Genome (In)Stability as the New Reliable Biological Parameters Defining Clinical Feature of CLL

Delić¹,

Marteau²,

Maloum³

et al. 2012

Chronic Lymphocytic Leukemia

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“…Les criblages sont réalisés in vitro sur la base de l'activité de phosphorylation du complexe car le manque de résolution des structures ne permet pas une approche in silico. Les molécules sélectionnées montrent une efficacité sur des cellules leucé-miques (LLC) traitées par le chlorambucile (Veuger et al 2003 ;Willmore et al 2008) ou la mithoxantrone (Elliott et al 2011). De plus, ces inhibiteurs conduisent à une action synergique avec l'irinotécan, un inhibiteur de la topoisomérase I dans le traitement in vitro de cellules tumorales coliques (Davidson et al 2011).…”

Section: Activité Kinase De La Dna-pkunclassified

Inhibition de la réparation des cassures double-brin de l'ADN: quel intérêt en radiothérapie et pharmacologie antitumorale?

Salles¹

2012

bavf

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(Communication présentée le 21 juin 2012)Parmi les thérapeutiques antitumorales, il est largement fait appel à la radiothérapie et /ou de la chimiothérapie non ciblée. Ces traitements induisent pour la grande majorité d'entre eux des lésions de l'ADN qui seront réparées en fonction de la dose utilisée. Les mécanismes de réparation des lésions de l'ADN représentent une cible pharmacologique d'intérêt car leur inhibition conduit à une sensibilisation cellulaire pouvant être mise à profit pour un traitement adjuvant. Parmi ces traitements, les rayonnements ionisants et des agents chimiothérapeutiques majeurs induisent directement ou indirectement des cassures double-brin (CDB). La réparation des CDB repose majoritairement sur le méca-nisme de la recombinaison non homologue ou NHEJ (Non Homologous End-Joining). La compréhension du mécanisme NHEJ et des facteurs protéiques impliqués a permis de sélectionner des molécules inhibitrices de cette voie dans le but de sensibiliser les cellules tumorales à un traitement clastogène. Cette approche est présentée et discutée dans une perspective d'amélioration de l'efficacité thérapeutique en cancérologie. Mots

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Mitoxantrone in combination with an inhibitor of DNA‐dependent protein kinase: a potential therapy for high risk B‐cell chronic lymphocytic leukaemia

Cited by 35 publications

References 28 publications

Combined inhibition of PI3K-related DNA damage response kinases and mTORC1 induces apoptosis in MYC-driven B-cell lymphomas

Combined inhibition of PI3K-related DNA damage response kinases and mTORC1 induces apoptosis in MYC-driven B-cell lymphomas

DNA Damage Response/Signaling and Genome (In)Stability as the New Reliable Biological Parameters Defining Clinical Feature of CLL

Inhibition de la réparation des cassures double-brin de l'ADN: quel intérêt en radiothérapie et pharmacologie antitumorale?

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