MAP Kinase-Interacting Kinases—Emerging Targets against Cancer

Diab, Sarah; Kumarasiri, Malika; Yu, Mingfeng; Teo, Theodosia; Proud, Christopher G.; Milne, Robert W.; Wang, Shudong

doi:10.1016/j.chembiol.2014.01.011

Cited by 83 publications

(85 citation statements)

References 64 publications

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“…MNK1a has low basal activity, and is activated and tightly regulated by ERK and p38 kinases in response to mitogens and stress [25,48]. MNK2 displays high basal activity and is predominantly regulated by ERK1/2, although MNK2a is regulated by mTORC1 through at least one site in its C-terminal region [49,50].…”

Section: Mapk-interacting Kinasesmentioning

confidence: 99%

Dual Abrogation of Mnk and Mtor: A Novel Therapeutic Approach for the Treatment of Aggressive Cancers

2017

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Targeting the translational machinery has emerged as a promising therapeutic option for cancer treatment. Cancer cells require elevated protein synthesis and exhibit augmented activity to meet the increased metabolic demand. Eukaryotic translation initiation factor 4E is necessary for mRNA translation, its availability and phosphorylation are regulated by the PI3K/AKT/mTOR and MNK1/2 pathways. The phosphorylated form of eIF4E drives the expression of oncogenic proteins including those involved in metastasis. In this article, we will review the role of eIF4E in cancer, its regulation and discuss the benefit of dual inhibition of upstream pathways. The discernible interplay between the MNK and mTOR signaling pathways provides a novel therapeutic opportunity to target aggressive migratory cancers through the development of hybrid molecules.

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Section: Mapk-interacting Kinasesmentioning

confidence: 99%

Dual Abrogation of Mnk and Mtor: A Novel Therapeutic Approach for the Treatment of Aggressive Cancers

2017

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“…The oncogenic role of eIF4E has been reported in the cell cycle progression (Diab et al, 2014a). D-type cyclins, as G 1 progression factors, play a vital role in enhancing the G 1 to S transition through binding to CDK4/6 (Sherr, 1995).…”

Section: Mapk-interacting Kinase Inhibition In Amlmentioning

confidence: 99%

“…D-type cyclins, as G 1 progression factors, play a vital role in enhancing the G 1 to S transition through binding to CDK4/6 (Sherr, 1995). Elevated eIF4E levels have been shown to enhance the translational levels of a wide array of malignancy-related mRNAs involved in the regulation of cell senescence, proliferation, and apoptosis, including cyclin D1 and Mcl-1 (Zimmer et al, 2000), whereas the oncogenic functions of eIF4E are closely linked to its phosphorylation by Mnks Diab et al, 2014a). Consistent with previous studies (Zhang et al, 2008;Diab et al, 2014b;Teo et al, 2015), Mnk inhibitors in the current study triggered a cell cycle arrest in both MOLM-13 and MV4-11 cells by disrupting the transition of the G 1 phase to the S phase.…”

Section: Mapk-interacting Kinase Inhibition In Amlmentioning

confidence: 99%

Pharmacologic Inhibition of MNKs in Acute Myeloid Leukemia

Teo

Lam

et al. 2015

Mol Pharmacol

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The Ras/Raf/MAPK and PI3K/Akt/mTOR pathways are key signaling cascades involved in the regulation of cell proliferation and survival, and have been implicated in the pathogenesis of several types of cancers, including acute myeloid leukemia (AML). The oncogenic activity of eIF4E driven by the Mnk kinases is a convergent determinant of the two cascades, suggesting that targeting the Mnk/eIF4E axis may provide therapeutic opportunity for the treatment of cancer. Herein, a potent and selective Mnk2 inhibitor (MNKI-85) and a dual-specific Mnk1 and Mnk2 inhibitor (MNKI-19), both derived from a thienopyrimidinyl chemotype, were selected to explore their antileukemic properties. MNKI-19 and MNKI-85 are effective in inhibiting the growth of AML cells that possess an M5 subtype with FLT3-internal tandem duplication mutation. Further mechanistic studies show that the downstream effects with respect to the selective Mnk1/2 kinase inhibition in AML cells causes G 1 cell cycle arrest followed by induction of apoptosis. MNKI-19 and MNKI-85 demonstrate similar Mnk2 kinase activity and cellular antiproliferative activity but exhibit different time-dependent effects on cell cycle progression and apoptosis. Collectively, this study shows that pharmacologic inhibition of both Mnk1 and Mnk2 can result in a more pronounced cellular response than targeting Mnk2 alone. However, MNKI-85, a first-in-class inhibitor of Mnk2, can be used as a powerful pharmacologic tool in studying the Mnk2/eIF4E-mediated tumorigenic mechanism. In conclusion, this study provides a better understanding of the mechanism underlying the inhibition of AML cell growth by Mnk inhibitors and suggests their potential utility as a therapeutic agent for AML.

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“…eIF4E is a key component of the cap-binding complex required for mRNA translation of mitogenic proteins, including cyclins, c-Myc, and Bcl-xl, and its activity has been linked to leukemogenesis and malignant cell proliferation. [7][8][9] The phosphorylation and activation of eIF4E by Mnk1/2 on serine 209 (Ser209) is critical for its oncogenic activity. 10,11 As Mnk1/2 double knockout mice have a normal phenotype, 12 Mnk1/2 are attractive targets for cancer therapy as their inhibition could conceivably target selectively malignant cells.…”

Section: Introductionmentioning

confidence: 99%