The novel BMI-1 inhibitor PTC596 downregulates MCL-1 and induces p53-independent mitochondrial apoptosis in acute myeloid leukemia progenitor cells

Nishida, Yuichiro; Maeda, Aya; Kim, M J; Cao, Long; Kubota, Yasushi; Ishizawa, Jo; AlRawi, Ahmed; Kato, Yuko; Iwama, Atsushi; Fujisawa, Manabu; Matsue, Kosei; Weetall, Marla; Dumble, Melissa; Andreeff, Michael; Davis, Thomas W.; Branstrom, Arthur; Kimura, Shinya; Kojima, Kensuke

doi:10.1038/bcj.2017.8

Cited by 74 publications

(82 citation statements)

References 55 publications

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“…have been used to demonstrate that a broad panel of human AML cell lines are sensitive to small-molecule BMI1 inhibition (Mourgues et al, 2015;Nishida et al, 2015Nishida et al, , 2017 although none of these studies focused specifically on CALM-AF10-rearranged AML. In CALM-AF10, the clinical rationale for BMI1 targeting may be clearer, given that BMI1 is strongly upregulated in CALM-AF10 rearranged AML.…”

Section: Discussionmentioning

confidence: 99%

Acute Myeloid Leukemia Driven by the CALM-AF10 Fusion Gene is Dependent on BMI1

Barbosa

Ghosh

Deshpande

et al. 2019

Preprint

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A subset of acute myeloid and lymphoid leukemia cases harbor a t(10;11)(p13;q14) translocation resulting in the CALM-AF10 fusion gene. Standard chemotherapeutic strategies are often ineffective in treating patients with CALM-AF10 fusions. Hence, there is an urgent need to identify molecular pathways dysregulated in CALM-AF10-positive leukemias which may lay the foundation for novel targeted therapies. Here we demonstrate that the Polycomb Repressive Complex 1 gene BMI1 is consistently overexpressed in adult and pediatric CALM-AF10-positive leukemias. We demonstrate that genetic Bmi1 depletion abrogates CALM-AF10-mediated transformation of murine hematopoietic stem and progenitor cells (HSPCs). Furthermore, CALM-AF10-positive murine and human AML cells are profoundly sensitive to the small-molecule BMI1 inhibitor PTC209 as well as to PTC596, a compound in clinical development that has been shown to result in downstream degradation of BMI1 protein. PTC-596 significantly prolongs survival of mice injected with a human CALM-AF10 cell line in a xenograft assay. In summary, these results validate BMI1 as a bonafide candidate for therapeutic targeting in AML with CALM-AF10 rearrangements.

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Section: Discussionmentioning

confidence: 99%

Acute Myeloid Leukemia Driven by the CALM-AF10 Fusion Gene is Dependent on BMI1

Barbosa

Ghosh

Deshpande

et al. 2019

Preprint

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“…The first BMI1 inhibitor PTC-209 was reported in 2014 (12), which showed promising anti-cancer effect in pre-clinical model of several types of tumors (12-14). Unfortunately, PTC-209 has not entered clinical trials because of poor pharmacokinetic properties (15). Another BMI1 inhibitor, PTC-596, which demonstrated in vivo anti-leukemia activity and showed a favorable safety profile (15, 16), has recently entered Phase 1 clinical trials.…”

Section: Introductionmentioning

confidence: 99%

“…Unfortunately, PTC-209 has not entered clinical trials because of poor pharmacokinetic properties (15). Another BMI1 inhibitor, PTC-596, which demonstrated in vivo anti-leukemia activity and showed a favorable safety profile (15, 16), has recently entered Phase 1 clinical trials.…”

Section: Introductionmentioning

confidence: 99%

Targeting BMI1 and MCL1 for Lung Adenocarcinoma Treatment

Lin

Hsu

et al. 2018

Preprint

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Lung cancer is the leading cause of cancer-associated death worldwide. Early metastasis and the recurrence remain major challenges for lung cancer treatment in clinic. Targeting the cancer stemness could be a potential strategy to restrain tumor progression. In the current study, we found that in lung adenocarcinoma (LAC), BMI1 and MCL1 play crucial roles in invasion, chemo-resistance, and tumor initiation. JNK signaling is a link between oncogenic pathway or environment stress to cancer stemness. The activation of JNK, either by EGFR or chemotherapy agent, stabilized BMI1 and MCL1 proteins through suppressing the expression of E3-ubiquitin ligase HUWE1. In lung cancer patient samples, high level of BMI1 is correlated with poor survival, and the expression of BMI1 is positively correlated with MCL1. A novel small-molecule BI-44 was synthesized, which effectively suppressed BMI1/MCL1 expression and inhibited tumor formation and progression in preclinical models. Targeting BMI1/MCL1 provides the basis for a new therapeutic approach in the treatment of LAC.

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“…Additionally, the p53 transcription factor can induce cell cycle arrest, DNA damage, cellular senescence, and apoptosis in different cancer cell types [22,23]. p53 independent apoptosis cascade formation also now considerable issue [24,25]. NF-κB (p65), a pro-inflammatory transcription factor that is activated by numerous inflammatory agents, tumor promoters, carcinogens, and the tumor microenvironment could also promote tumorigenesis.…”

Section: Introductionmentioning

confidence: 99%

Resveratrol Sensitizes Lung Cancer Cell to TRAIL by p53 Independent and Suppression of Akt/NF-κB Signaling

Rasheduzzaman

Jeong

Park

2018

Preprint

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Aims: TRAIL is a promising anticancer agent that has the potential to sensitize a wide variety of cancer or transformed cells by inducing apoptosis. However, resistance to TRAIL is a growing concern. Current manuscript aimed to employ combination treatment to investigate resveratrol induced TRAIL sensitization in NSCLC. Method: A549 and HCC-15 cells were used in an experimental design. Cell viability was determined by morphological image, crystal violet staining and MTT assay. Apoptosis was evaluated by LDH assay, Annexin V and DAPI staining. Autophagy and apoptosis indicator protein were examined by western blotting. TEM and puncta assay was carried out to evaluate the autophagy. MTP and ROS activity was evaluated by JC-1 and H 2 DCFDA staining. Findings: Resveratrol is a polyphenolic compound capable of activation of tumor suppressor p53 and its proapoptotic modulator PUMA. Herein, we showed the p53-independent apoptosis by decrease the expression of phosphorylated Akt-mediated suppression of NF-κB that is also substantiated with the downregulation of antiapoptotic factors Bcl-2 and Bcl-xl in NSCLC, resulting in an attenuation of TRAIL resistance in combined treatment. Furthermore, apoptosis was induced in TRAIL-resistant lung cancer cells with a co-treatment of resveratrol and TRAIL assessed by the loss of MMP, ROS generations which resulting the translocation of cytochrome c from the mitochondria into the cytosol due to mitochondrial dysfunction. Moreover, autophagy flux was not affected by resveratrol-induced TRAIL-mediated apoptosis in NSCLC. Significance: Overall, targeting the NF-κB (p65) pathway via resveratrol attenuates TRAIL resistance and induces TRAIL-mediated apoptosis which could be the effective TRAIL-based cancer therapy regimen.

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The novel BMI-1 inhibitor PTC596 downregulates MCL-1 and induces p53-independent mitochondrial apoptosis in acute myeloid leukemia progenitor cells

Cited by 74 publications

References 55 publications

Acute Myeloid Leukemia Driven by the CALM-AF10 Fusion Gene is Dependent on BMI1

Acute Myeloid Leukemia Driven by the CALM-AF10 Fusion Gene is Dependent on BMI1

Targeting BMI1 and MCL1 for Lung Adenocarcinoma Treatment

Resveratrol Sensitizes Lung Cancer Cell to TRAIL by p53 Independent and Suppression of Akt/NF-κB Signaling

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The novel BMI-1 inhibitor PTC596 downregulates MCL-1 and induces p53-independent mitochondrial apoptosis in acute myeloid leukemia progenitor cells

Cited by 74 publications

References 55 publications

Acute Myeloid Leukemia Driven by the CALM-AF10 Fusion Gene is Dependent on BMI1

Acute Myeloid Leukemia Driven by the CALM-AF10 Fusion Gene is Dependent on BMI1

Targeting BMI1 and MCL1 for Lung Adenocarcinoma Treatment

Resveratrol Sensitizes Lung Cancer Cell to TRAIL by p53 Independent and Suppression of Akt/NF-&kappa;B Signaling

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Resveratrol Sensitizes Lung Cancer Cell to TRAIL by p53 Independent and Suppression of Akt/NF-κB Signaling