Small-Molecule Activators of Protein Phosphatase 2A for the Treatment of Castration-Resistant Prostate Cancer

McClinch, Kimberly; Avelar, Rita A.; Callejas, David; Izadmehr, Sudeh; Wiredja, Danica; Perl, Abbey; Sangodkar, Jaya; Kastrinsky, David B.; Schlatzer, Daniela; Cooper, Mark S.; Kiselar, Janna; Stachnik, Agnes; Shen, Yao; Hoon, Divya; McQuaid, Daniel; Zaware, Nilesh; Gong, Yixuan; Brautigan, David L.; Plymate, Stephen R.; Sprenger, Cynthia T.; Oh, William; Levine, Alice C.; Kirschenbaum, Alexander; Sfakianos, John P.; Sears, Rosalie C.; DiFeo, Analisa; Ioannou, Yiannis A.; Ohlmeyer, Michael; Narla, Goutham; Galsky, Matthew D.

doi:10.1158/0008-5472.can-17-0123

Cited by 62 publications

(77 citation statements)

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“…Considering the potential future development of DBK-1154 derivatives for GB therapy, DBK-1154 was evaluated in an acute rat pilot (non-GLP) toxicology study at doses up to 800 mg/kg daily. Consistently with previous SMAP in vivo studies (Sangodkar et al, 2017;McClinch et al, 2018), no significant body weight loss, deaths, or adverse behavioral or neurological effects were observed. The major morphologic finding was hepatocellular hypertrophy (panlobular) in all test article-treated groups, with increased severity as the dose level increased.…”

Section: Dbk-1154 With Higher Degree Of Brain/blood Distribution Ansupporting

confidence: 90%

“…In addition to their different in vivo brain penetrance properties, NZ-8-061 seems to have cytostatic effects at the doses tested, whereas DBK-1154 most probably induces both, decreased proliferation and cell death. On the other hand, a SMAP derivative DBK-766 defective in PP2A reactivation (Sangodkar et al, 2017;McClinch et al, 2018), failed to suppress GB cell viability. The intracellular pathways involved in the apoptosis induction by DBK-1154 in vitro were not addressed in this concise communication, but clearly remains as an important future question to be addressed.…”

Section: Dbk-1154 With Higher Degree Of Brain/blood Distribution Anmentioning

confidence: 98%

“…1A) would compromise BBB permeability, and eventually CNS availability, of the SMAPs as compared to tricyclics. We therefore started by investigating the in vitro BBB passage of NZ-8-061 (a.k.a DT-061) that has been widely used in cancers outside the CNS (Sangodkar et al, 2017;McClinch et al, 2018). Quantified by HPLC-MS/MS, NZ-8-061 was found to cross the artificial BBB (Le Joncour et al, 2019), consisting of murine brain microcapillary endothelial cells and astrocytes ( Fig.…”

Section: Development Of Blood-brain Barrier Permeable Small Molecule mentioning

confidence: 99%

“…As a pharmacologic control, U87MG, U118, or A172 cells were also treated with increasing doses of TRC-766, a structurally similar but biologically inactive derivate of SMAPs ( Supplementary Fig. 3A) (Sangodkar et al, 2017;McClinch et al, 2018).…”

Section: Nz-8-061 Potently Inhibits the Viability Of Gb Cells With Hementioning

confidence: 99%

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Monotherapy efficacy of BBB-permeable small molecule activators of PP2A in glioblastoma

Merisaari

Denisova

Doroszko

et al. 2019

Preprint

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Glioblastoma (GB) is a fatal disease in which most targeted therapies have clinically failed.However, pharmacological reactivation of tumor suppressors has not been thoroughly studied as yet as a GB therapeutic strategy. Tumor suppressor Protein Phosphatase 2A (PP2A), is inhibited by non-genetic mechanisms in GB, and thus it would be potentially amendable for therapeutic reactivation. Here we demonstrate, that small molecule activators of PP2A (SMAPs), NZ-8-061and DBK-1154, effectively cross the in vitro model of blood-brain barrier (BBB), and in vivo partition to mouse brain tissue after oral dosing. In vitro, SMAPs exhibit robust cell killing activity against five established GB cell lines, and nine patient-derived primary glioma cell lines.Collectively these cell lines have heterogenous genetic background, kinase inhibitor resistance profile, and stemness properties; and they represent different clinical GB subtypes. Oral dosing of either of the SMAPs significantly reduced growth of infiltrative intracranial GB tumors. DBK-1154, with both higher degree of brain/blood distribution, and more potent in vitro activity against all tested GB cell lines, also significantly increased survival of mice bearing orthotopic GB xenografts. In summary, this report presents a proof-of-principle data for BBB-permeable tumor suppressor reactivation therapy for glioblastoma cells of heterogenous molecular background.

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Section: Dbk-1154 With Higher Degree Of Brain/blood Distribution Ansupporting

confidence: 90%

Section: Dbk-1154 With Higher Degree Of Brain/blood Distribution Anmentioning

confidence: 98%

Section: Development Of Blood-brain Barrier Permeable Small Molecule mentioning

confidence: 99%

Section: Nz-8-061 Potently Inhibits the Viability Of Gb Cells With Hementioning

confidence: 99%

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Monotherapy efficacy of BBB-permeable small molecule activators of PP2A in glioblastoma

Merisaari

Denisova

Doroszko

et al. 2019

Preprint

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“…In accordance with the major theme of this review, a recent study demonstrated that combination of SET targeting and tyrosine kinase inhibitor provides an effective therapeutic approach in human T‐cell acute lymphoblastic leukemia . Apart of small‐molecules targeting the PIPs, the novel series of orally bioavailable and nontoxic PP2A reactivator molecules with profound in vivo therapeutic activities in KRAS mutant lung cancers and castration‐resistant prostate cancer , provide a very encouraging example that PP2A indeed is druggable . In the context of this review, these small‐molecule PP2A activators were recently shown to transform the cytostatic MEK inhibitor responses to cytotoxic, and to greatly promote in vivo therapeutic effects of MEK inhibitor AZD6244 in two KRAS mutant lung cancer xenograft models .…”

Section: Therapeutic Targeting Of Pp2amentioning

confidence: 60%

Targeted therapies don't work for a reason; the neglected tumor suppressor phosphatase PP2A strikes back

Westermarck

2018

The FEBS Journal

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Therapies targeting tyrosine and serine/threonine kinases have raised enormous interest as potential cure for cancer patients in many common cancer types. However, except for the success story with BCR/ABL tyrosine kinase inhibitors in chronic myeloid leukemia (CML), critical review of results of a large number of clinical trials indicates that the clinical success with kinase inhibitors has been overall disappointing. These alarming results call for critical assessment of whether there is some fundamental flaw in the design of strategies to target phosphorylation-dependent oncogenic signaling for cancer therapy. This viewpoint debates on one potential, but thus far largely neglected, molecular explanation why inhibition of protein kinases is not sufficient for cancer cure. We note that the phosphorylation status, and thus the oncogenic potential of any given protein, is not regulated only by kinases, but rather by an intimate balance between kinases and their antagonist phosphatases. We further review the supporting functional evidence that for oncogenic transformation of human cells it is not enough to activate kinase signaling by activated kinases, if a group of counteracting tumor suppressor phosphatases is not inactivated. Based on these considerations, and a very recently emerged role of oncogenic function of a group of phosphatase inhibitor proteins as human oncoproteins, we propose that in order to efficiently inhibit phosphorylation-dependent signaling in cancer cells, and thus provide better therapeutic index, the kinase inhibitors should be combined with strategies to reactivate tumor suppressor phosphatases such as Protein Phosphatase 2A (PP2A).

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Biology of the adenovirus E4orf4 protein: from virus infection to cancer cell death

Kleinberger

2019

FEBS Letters

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The adenovirus (Ad) early region 4 open reading frame 4 (E4orf4) protein is a small 14‐kDa polypeptide endowed with important viral regulatory functions. Although deletion of E4orf4 does not have a major effect on Ad replication due to redundancy among many Ad proteins, E4orf4 provides several functions that improve viral replication. E4orf4 contributes to temporal regulation of virus infection by downregulating early viral gene expression and by altering splicing patterns of Ad mRNAs. It also optimizes the cellular environment for Ad replication by activating the mammalian target of rapamycin pathway to increase viral protein production and by impacting the cell cycle. In addition, E4orf4 participates in the inhibition of the host DNA damage response, promoting the ability of Ad to counteract this antiviral defense mechanism. To fulfill these functions, E4orf4 interacts with numerous cellular proteins, including the major E4orf4 partner, protein phosphatase 2A (PP2A). When expressed alone, outside the context of virus infection, E4orf4 induces an evolutionarily conserved, caspase‐independent, cancer‐selective cell death with many interesting characteristics. This review critically describes E4orf4’s contribution to Ad infection and cancer‐cell death.

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Small-Molecule Activators of Protein Phosphatase 2A for the Treatment of Castration-Resistant Prostate Cancer

Cited by 62 publications

References 50 publications

Monotherapy efficacy of BBB-permeable small molecule activators of PP2A in glioblastoma

Monotherapy efficacy of BBB-permeable small molecule activators of PP2A in glioblastoma

Targeted therapies don't work for a reason; the neglected tumor suppressor phosphatase PP2A strikes back

Biology of the adenovirus E4orf4 protein: from virus infection to cancer cell death

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