Alterations in the Noxa/Mcl-1 axis determine sensitivity of small cell lung cancer to the BH3 mimetic ABT-737

Hauck, Paula M.; Chao, Bo H.; Litz, Julie; Krystal, Geoffrey W.

doi:10.1158/1535-7163.mct-08-1118

Cited by 62 publications

(61 citation statements)

References 39 publications

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“…In many cell types, Noxa has also been shown to mediate proteasome degradation of Mcl-1 (9,10). However, in SCLC, we have shown that Noxa-mediated degradation of Mcl-1 was lost in all four cell lines examined, either because Mcl-1 levels were insensitive to changes in Noxa expression or because endogenous Noxa expression was absent (5). This observation suggests that maintenance of Mcl-1 expression in the face of stimuli that induce Noxa may be involved in the pathogenesis or progression of SCLC.…”

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confidence: 72%

“…One important factor in the development of chemotherapy resistance is the overexpression of prosurvival members of the Bcl-2 family (2). In SCLC, overexpression of Bcl-2 has been shown (3), and Bcl-X L and Mcl-1 are also expressed at varying levels as well (4,5). BH3-mimetic drugs represent an exciting new development in cancer therapeutics designed to counteract the effects of prosurvival Bcl-2 family proteins by blocking their ability to bind and inactivate the BH3 domain-containing proapoptotic Bcl-2 family members, thus allowing the proapoptotic proteins to directly or indirectly induce permeablization of the outer mitochondrial membrane and activation of the intrinsic apoptotic caspase cascade (6).…”

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confidence: 99%

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Actinomycin D Decreases Mcl-1 Expression and Acts Synergistically with ABT-737 against Small Cell Lung Cancer Cell Lines

Krystal

2010

Clinical Cancer Research

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Purpose: ABT-737, which blocks the function of Bcl-2 and Bcl-X L but not Mcl-1, has shown singleagent activity in preclinical models of small cell lung cancer (SCLC). Elevated expression of Mcl-1 induces resistance to ABT-737 in SCLC. Based on the short half-life of Mcl-1 mRNA and protein, we hypothesized that the actinomycin D could reverse Mcl-1-induced resistance to ABT-737.Experimental Design: The dose-response of multiple SCLC cell lines to actinomycin D in the absence and presence of ABT-737 was followed by the assessment of Bcl-2 family expression and poly ADP ribose polymerase cleavage by Western blot, viability by tetrazolium dye reduction and clonogenic assay, and cell cycle kinetics by flow cytometry.Results: Actinomycin D decreased Mcl-1 expression and resulted in a cell line-dependent increase in Noxa expression. Clinically relevant concentrations of actinomycin D from 0.4 to 4 ng/mL showed singleagent activity across a panel of SCLC cell lines. When combined with low micromolar doses of ABT-737, near complete loss of viability was seen with synergistic combination indices of 0.5 to 0.7. Exposure to 4 ng/mL actinomycin was only required for the first 24 hours of the combined incubation, mimicking a clinically achievable area under the curve, but the presence of ABT-737 was required for an additional 48 hours to obtain maximal effect.Conclusions: Clinically relevant concentrations of actinomycin D act synergistically with ABT-737 to induce SCLC apoptosis, which can be at least partially attributed to the actinomycin D-induced decrease in Mcl-1 and increase in Noxa expression. Taken together, these data suggest the feasibility of combining actinomycin D with BH3-mimetic drugs in the clinical setting. Clin Cancer Res; 16(17); 4392-400. ©2010 AACR.

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confidence: 72%

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confidence: 99%

Actinomycin D Decreases Mcl-1 Expression and Acts Synergistically with ABT-737 against Small Cell Lung Cancer Cell Lines

Krystal

2010

Clinical Cancer Research

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“…Importantly, abolishing sunitinib-mediated induction of MCL-1 by the combination with a subtoxic dose of sorafenib was associated with a dramatic sensitization to treatment with lower dose of sunitinib, while neither of these treatments evoked apparent cell death ( Figure 3C and Supplemental Figure 5, A and B). The sunintinib/ABT737 combination did not show such synergism, but if anything, sunitinib seemed to desensitize cells to ABT737 treatment, possibly through MCL-1 stabilization, which is known to mediate resistance to ABT737 (40,41). Replating equal numbers of surviving HCT116 cells from all the previous conditions in fresh medium without drugs showed that the antiproliferative effect of the sunitinib/sorafenib combination was irreversible, as cells pretreated with this combination could not recover and died within the ensuing 48 hours, while cells from other treatments proliferated normally ( Figure 3D).…”

Section: Sunitinib Exerts Dual Effects On Mcl-1 and Mtor In Tolerant Andmentioning

confidence: 95%

Dual modulation of MCL-1 and mTOR determines the response to sunitinib

Elgendy

Abdel-Aziz

Renne

et al. 2016

Journal of Clinical Investigation

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“…High-affinity binding of BH3 peptides to both BCL-2 and BCL-X L is mediated primarily by interactions in two hydrophobic pockets, termed P2 and P4, and navitoclax specifically binds to these P2 and P4 pockets 39 . The efficacy of ABT-263 and its related compound, ABT-737, has been demonstrated in lung cancer 8,[41][42][43][44][45][46] . Because of the key role of MCL1 in protecting malignant cells against anticancer treatments, combinatorial therapy with BH3-binding molecules such as navitoclax may enhance the therapeutic effects of radiotherapy and other treatments.…”

Section: The Role Of Mcl1 and Its Targeted Therapy In Lung Cancermentioning

confidence: 99%

The anti-apoptotic protein MCL1, a novel target of lung cancer therapy

Tanaka¹

2017

J Cancer Treat & Diagnosis

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Evasion of apoptosis is one of the typical hallmarks of cancer and a major mechanism for cancer development, tumor growth, and acquisition of resistance to chemotherapy. The anti-apoptotic Bcl-2 protein family, particularly MCL1 and BCL-XL, play an important role in acquisition of apoptosis evasion. MCL1 is a highly unstable protein that is constantly degraded by the ubiquitinproteasome system. An increase in MCL1 protein has been reported in many cancers, including lung cancer, through high mRNA expression or impairment of its degradation systems. To date, much evidence has shown that MCL1 is important for cancer cell survival and drug resistance in lung cancers. In this review, we discuss the role and mechanism of high MCL1 expression in lung cancer.

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Alterations in the Noxa/Mcl-1 axis determine sensitivity of small cell lung cancer to the BH3 mimetic ABT-737

Cited by 62 publications

References 39 publications

Actinomycin D Decreases Mcl-1 Expression and Acts Synergistically with ABT-737 against Small Cell Lung Cancer Cell Lines

Actinomycin D Decreases Mcl-1 Expression and Acts Synergistically with ABT-737 against Small Cell Lung Cancer Cell Lines

Dual modulation of MCL-1 and mTOR determines the response to sunitinib

The anti-apoptotic protein MCL1, a novel target of lung cancer therapy

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