Reciprocal Potentiation of the Antitumoral Activities of FK866, an Inhibitor of Nicotinamide Phosphoribosyltransferase, and Etoposide or Cisplatin in Neuroblastoma Cells

Travelli, Cristina; Drago, Valentina; Maldi, Elena; Kaludercic, Nina; Galli, Ubaldina; Boldorini, Renzo; Lisa, Fabio Di; Tron, Gian Cesare; Canonico, Pier Luigi; Genazzani, Armando A.

doi:10.1124/jpet.111.184630

Cited by 37 publications

(32 citation statements)

References 38 publications

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“…Because a previous study linked cell death induced by FK866 combined with cisplatin/etoposide to apoptosis in neuroblastoma cells, 12 we next examined whether FK866 added to bortezomib also triggered apoptosis in MM cells. Indeed, we observed that combining low doses of these drugs markedly increased proteolytic cleavage of caspase-3, caspase-8, caspase-9, and PARP in both bortezomib-sensitive and -resistant MM cell lines ( Figure 3A).…”

Section: Targeting Nampt and Proteasome Activity Triggers Synergisticmentioning

confidence: 99%

“…Remarkably, the combination of FK866 plus bortezomib dramatically reduced intracellular NAD 1 to undetectable levels in all MM cells analyzed, enhancing the metabolic consequences of FK866 treatment alone ( Figure 6A). Because intracellular NAD 1 and adenosine triphosphate (ATP) levels, whose depletion follows NAD 1 shortage, 12,27 share the capacity to affect proteasome enzymatic activity, we next turned our attention to a possible synergism at this level.…”

Section: Combined Fk866 and Bortezomib Inhibits The Ups And Nf-kb Patmentioning

confidence: 99%

“…In vivo studies in murine xenograft models of human MM showed that FK866 is well tolerated, prolongs survival, and reduces tumor growth. Numerous studies in other cancers have also revealed promising results by combining NAD 1 -depleting agents with TRAIL, 9 DNA damaging agents (daunorubicin, cisplatin, Ara-C, and melphalan), [10][11][12] and ionizing radiation. 13 Proteasome inhibitor bortezomib has transformed therapy of relapsed MM, as well as prolonged event-free and overall survival when used as initial therapy for newly diagnosis disease.…”

Section: Introductionmentioning

confidence: 99%

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Intracellular NAD+ depletion enhances bortezomib-induced anti-myeloma activity

Cagnetta

Cea

Calimeri

et al. 2013

Blood

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Key Points• FK866 combined with bortezomib induces synergistic anti-MM cell death.• Addition of low doses of NAD1-depleting agent FK866 overcomes bortezomib resistance in MM cells.We recently demonstrated that Nicotinamide phosphoribosyltransferase (Nampt) inhibition depletes intracellular NAD 1 content leading, to autophagic multiple myeloma (MM) cell death. Bortezomib has remarkably improved MM patient outcome, but doselimiting toxicities and development of resistance limit its long-term utility. Here we observed higher Nampt messenger RNA levels in bortezomib-resistant patient MM cells, which correlated with decreased overall survival. We demonstrated that combining the NAD 1 depleting agent FK866 with bortezomib induces synergistic anti-MM cell death and overcomes bortezomib resistance. This effect is associated with (1) activation of caspase-8, caspase-9, caspase-3, poly (ADP-ribose) polymerase, and downregulation of Mcl-1; (2) enhanced intracellular NAD 1 depletion; (3) inhibition of chymotrypsin-like, caspase-like, and trypsin-like proteasome activities; (4) inhibition of nuclear factor kB signaling; and (5) inhibition of angiogenesis. Furthermore, Nampt knockdown significantly enhances the anti-MM effect of bortezomib, which can be rescued by ectopically overexpressing Nampt. In a murine xenograft MM model, lowdose combination FK866 and Bortezomib is well tolerated, significantly inhibits tumor growth, and prolongs host survival. Taken together, these findings indicate that intracellular NAD 1 level represents a major determinant in the ability of bortezomib to induce apoptosis in MM cells and provide proof of concept for the combination with FK866 as a new strategy to enhance sensitivity or overcome resistance to bortezomib. (Blood. 2013;122(7):1243-1255

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Section: Targeting Nampt and Proteasome Activity Triggers Synergisticmentioning

confidence: 99%

Section: Combined Fk866 and Bortezomib Inhibits The Ups And Nf-kb Patmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Intracellular NAD+ depletion enhances bortezomib-induced anti-myeloma activity

Cagnetta

Cea

Calimeri

et al. 2013

Blood

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“…FK866 reduces intracellular NAD content, resulting in selective cancer cell death in solid tumors (22,(25)(26)(27), and emerging evidence suggests that it is also active in blood cancers (28)(29)(30)(31)(32)(33). FK866 has been demonstrated to be effective in blood cancer cell lines, where it leads to ATP reduction and delayed induction of cell death.…”

Section: Introductionmentioning

confidence: 99%

On-Target Effect of FK866, a Nicotinamide Phosphoribosyl Transferase Inhibitor, by Apoptosis-Mediated Death in Chronic Lymphocytic Leukemia Cells

Gehrke

Bouchard

Beiggi

et al. 2014

Clinical Cancer Research

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Purpose: Chronic lymphocytic leukemia (CLL) remains incurable despite advances in therapy. In this study, we characterize the effect of nicotinamide phosphoribosyltransferase (NAMPT) inhibition by FK866 in primary CLL cells from patients with various clinical prognostic markers.Experimental Design: CLL cells were treated with FK866 to assess viability by Annexin V/PI staining. Functional analysis of FK866 included time-and concentration-dependent evaluation of cellular NAD, ATP, mitochondrial membrane potential (MMP), reactive oxygen species (ROS), and apoptotic signaling. Chemosensitization potential by FK866 to fludarabine was also assessed. Prognostic markers were correlated with drug response.Results: FK866 induced CLL cell death by depleting cellular NAD content by day 1, followed by a drop in ATP on day 2. We observed loss of MMP, ROS increase, and induction of apoptotic signaling at day 3. Ontarget activity of FK866 was confirmed by NAD-mediated rescue of NAD and ATP loss, apoptotic signaling, and viability. The response to FK866 was independent of most prognostic markers. Higher doses were required with short lymphocyte doubling time and positive CD38 status, whereas CLL cells resistant to fludarabine in vitro and from patients with del17p13.1 were equally sensitive to FK866. FK866 did not upregulate the p53-target p21, nor did the p53 activator Nutlin improve FK866-mediated cell death. Furthermore, fludarabine and FK866 were synergistic at clinically relevant concentrations.Conclusions: NAMPT inhibition by FK866 may be a potential treatment for CLL, including patients with del17p13

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“…GMX1777 is a soluble prodrug of GMX used for in vivo studies (5,6). NAMPT inhibitors, including GMX1778 (GMX) and FK866, have shown preclinical activity alone and in combination with several therapeutic DNA-damaging agents, but the mechanism of synergy has not been clearly elucidated (7)(8)(9)(10).…”

Section: Introductionmentioning

confidence: 99%

Synergy between the NAMPT Inhibitor GMX1777(8) and Pemetrexed in Non–Small Cell Lung Cancer Cells Is Mediated by PARP Activation and Enhanced NAD Consumption

et al. 2014

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GMX1778 and its prodrug GMX1777 represent a new class of cancer drugs that targets nicotinamide phosphoribosyltransferase (NAMPT) as a new strategy to interfere with biosynthesis of the key enzymatic cofactor NAD, which is critical for a number of cell functions, including DNA repair. Using a genome-wide synthetic lethal siRNA screen, we identified the folate pathway-related genes, deoxyuridine triphosphatase and dihydrofolate reductase, the silencing of which sensitized non-small cell lung carcinoma (NSCLC) cells to the cytotoxic effects of GMX. Pemetrexed is an inhibitor of dihydrofolate reductase currently used to treat patients with nonsquamous NSCLC. We found that combining pemetrexed with GMX1777 produced a synergistic therapeutic benefit in A549 and H1299 NSCLC cells in vitro and in a mouse A549 xenograft model of lung cancer. Pemetrexed is known to activate PARPs, thereby accelerating NAD consumption. Genetic or pharmacologic blockade of PARP activity inhibited this effect, impairing cell death by pemetrexed either alone or in combination with GMX1777. Conversely, inhibiting the base excision repair pathway accentuated NAD decline in response to GMX and the cytotoxicity of both agents either alone or in combination. These findings provide a mechanistic rationale for combining GMX1777 with pemetrexed as an effective new therapeutic strategy to treat nonsquamous NSCLC. Cancer Res; 74(21); 5948-54. Ó2014 AACR.

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Reciprocal Potentiation of the Antitumoral Activities of FK866, an Inhibitor of Nicotinamide Phosphoribosyltransferase, and Etoposide or Cisplatin in Neuroblastoma Cells

Cited by 37 publications

References 38 publications

Intracellular NAD+ depletion enhances bortezomib-induced anti-myeloma activity

Intracellular NAD+ depletion enhances bortezomib-induced anti-myeloma activity

On-Target Effect of FK866, a Nicotinamide Phosphoribosyl Transferase Inhibitor, by Apoptosis-Mediated Death in Chronic Lymphocytic Leukemia Cells

Synergy between the NAMPT Inhibitor GMX1777(8) and Pemetrexed in Non–Small Cell Lung Cancer Cells Is Mediated by PARP Activation and Enhanced NAD Consumption

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