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Literature DB >> 21057530

Activated MEK cooperates with Ink4a/Arf loss or Akt activation to induce gliomas in vivo.

J P Robinson¹, M W Vanbrocklin, K J Lastwika, A J McKinney, S Brandner, S L Holmen.

Abstract

The RAS/RAF mitogen-activated protein kinase pathway (MAPK) is highly active in many tumor types including the majority of high-grade gliomas and expression of activated RAS or RAF in neural progenitor cells combined with either AKT activation or Ink4a/Arf loss leads to the development of high-grade gliomas in vivo. This strongly suggests that this pathway is necessary for glioma formation and maintenance. To further define the role of this pathway in the development of high-grade gliomas, we used the established RCAS/TVA glioma mouse model to test the ability of activated MAPK/extracellular signal-regulated kinase (ERK) kinase (MEK), a RAF effector, to induce tumors in vivo in the context of activated AKT or Ink4a/Arf loss. Although expression of activated MEK alone in neural progenitor cells is not sufficient for tumorigenesis, the combination of activated MEK and AKT or MEK with Ink4a/Arf loss is transforming. The data reveal that activation of the classical RAS/MAPK pathway, which is mediated through MEK, leads to the development of high-grade gliomas in vivo and suggest that MEK may be a relevant target for glioma therapy. To test this, we treated both mouse and human glioma cells with the MEK inhibitor PD0325901. Although this treatment induced apoptosis in a significant percentage of the cells, the effect was enhanced by combined treatment with the phosphatidylinositol 3-kinase (PI3K)/mTOR inhibitor NVP-BEZ235. Our results demonstrate that combined inhibition of MEK and PI3K/mTOR is a rational strategy for the treatment of high-grade gliomas and may be an effective adjuvant therapy for this disease.

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Year: 2010 PMID： 21057530 PMCID： PMC4109988 DOI： 10.1038/onc.2010.513

Source DB: PubMed Journal: Oncogene ISSN： 0950-9232 Impact factor: 9.867

33 in total

1. Mechanism of activation of the RAF-ERK signaling pathway by oncogenic mutations of B-RAF.

Authors: Paul T C Wan; Mathew J Garnett; S Mark Roe; Sharlene Lee; Dan Niculescu-Duvaz; Valerie M Good; C Michael Jones; Christopher J Marshall; Caroline J Springer; David Barford; Richard Marais
Journal: Cell Date: 2004-03-19 Impact factor: 41.582

Review 2. Temozolomide: a review of its discovery, chemical properties, pre-clinical development and clinical trials.

Authors: E S Newlands; M F Stevens; S R Wedge; R T Wheelhouse; C Brock
Journal: Cancer Treat Rev Date: 1997-01 Impact factor: 12.111

3. Combined activation of Ras and Akt in neural progenitors induces glioblastoma formation in mice.

Authors: E C Holland; J Celestino; C Dai; L Schaefer; R E Sawaya; G N Fuller
Journal: Nat Genet Date: 2000-05 Impact factor: 38.330

4. Phase I pharmacokinetic and pharmacodynamic study of the oral MAPK/ERK kinase inhibitor PD-0325901 in patients with advanced cancers.

Authors: Patricia M LoRusso; Smitha S Krishnamurthi; John J Rinehart; Lisle M Nabell; Lisa Malburg; Paul B Chapman; Samuel E DePrimo; Steven Bentivegna; Keith D Wilner; Weiwei Tan; Alejandro D Ricart
Journal: Clin Cancer Res Date: 2010-03-09 Impact factor: 12.531

5. Tumor suppression at the mouse INK4a locus mediated by the alternative reading frame product p19ARF.

Authors: T Kamijo; F Zindy; M F Roussel; D E Quelle; J R Downing; R A Ashmun; G Grosveld; C J Sherr
Journal: Cell Date: 1997-11-28 Impact factor: 41.582

6. Human glioblastomas with no alterations of the CDKN2A (p16INK4A, MTS1) and CDK4 genes have frequent mutations of the retinoblastoma gene.

Authors: K Ichimura; E E Schmidt; H M Goike; V P Collins
Journal: Oncogene Date: 1996-09-05 Impact factor: 9.867

7. ARF promotes MDM2 degradation and stabilizes p53: ARF-INK4a locus deletion impairs both the Rb and p53 tumor suppression pathways.

Authors: Y Zhang; Y Xiong; W G Yarbrough
Journal: Cell Date: 1998-03-20 Impact factor: 41.582

8. Interdependent domains controlling the enzymatic activity of mitogen-activated protein kinase kinase 1.

Authors: S J Mansour; J M Candia; J E Matsuura; M C Manning; N G Ahn
Journal: Biochemistry Date: 1996-12-03 Impact factor: 3.162

9. Alternative reading frames of the INK4a tumor suppressor gene encode two unrelated proteins capable of inducing cell cycle arrest.

Authors: D E Quelle; F Zindy; R A Ashmun; C J Sherr
Journal: Cell Date: 1995-12-15 Impact factor: 41.582

10. A new regulatory motif in cell-cycle control causing specific inhibition of cyclin D/CDK4.

Authors: M Serrano; G J Hannon; D Beach
Journal: Nature Date: 1993-12-16 Impact factor: 49.962

22 in total

1. Urothelial tumor initiation requires deregulation of multiple signaling pathways: implications in target-based therapies.

Authors: Haiping Zhou; Hong-ying Huang; Ellen Shapiro; Herbert Lepor; William C Huang; Moosa Mohammadi; Ian Mohr; Moon-shong Tang; Chuanshu Huang; Xue-ru Wu
Journal: Carcinogenesis Date: 2012-01-27 Impact factor: 4.944

Activated MEK cooperates with Ink4a/Arf loss or Akt activation to induce gliomas in vivo.

1. Mechanism of activation of the RAF-ERK signaling pathway by oncogenic mutations of B-RAF.

Review 2. Temozolomide: a review of its discovery, chemical properties, pre-clinical development and clinical trials.

3. Combined activation of Ras and Akt in neural progenitors induces glioblastoma formation in mice.

4. Phase I pharmacokinetic and pharmacodynamic study of the oral MAPK/ERK kinase inhibitor PD-0325901 in patients with advanced cancers.

5. Tumor suppression at the mouse INK4a locus mediated by the alternative reading frame product p19ARF.

6. Human glioblastomas with no alterations of the CDKN2A (p16INK4A, MTS1) and CDK4 genes have frequent mutations of the retinoblastoma gene.

7. ARF promotes MDM2 degradation and stabilizes p53: ARF-INK4a locus deletion impairs both the Rb and p53 tumor suppression pathways.

8. Interdependent domains controlling the enzymatic activity of mitogen-activated protein kinase kinase 1.

9. Alternative reading frames of the INK4a tumor suppressor gene encode two unrelated proteins capable of inducing cell cycle arrest.

10. A new regulatory motif in cell-cycle control causing specific inhibition of cyclin D/CDK4.

1. Urothelial tumor initiation requires deregulation of multiple signaling pathways: implications in target-based therapies.

2. Qualitative network modeling of the Myc-p53 control system of cell proliferation and differentiation.

Review 3. Will kinase inhibitors make it as glioblastoma drugs?

4. p53 is positively regulated by miR-542-3p.

5. MNK1 pathway activity maintains protein synthesis in rapalog-treated gliomas.

Review 6. PI3K and Akt as molecular targets for cancer therapy: current clinical outcomes.

7. Gα13 mediates human cytomegalovirus-encoded chemokine receptor US28-induced cell death in melanoma.

Review 8. Review: insights gained from modelling high-grade glioma in the mouse.

9. Akt signaling accelerates tumor recurrence following ras inhibition in the context of ink4a/arf loss.

10. Akt signaling is required for glioblastoma maintenance in vivo.