Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 c-Jun N-terminal kinase contributes to aberrant retinoid signaling in lung cancer cells by phosphorylating and inducing proteasomal degradation of retinoic acid receptor alpha.

Literature DB >> 15657432

c-Jun N-terminal kinase contributes to aberrant retinoid signaling in lung cancer cells by phosphorylating and inducing proteasomal degradation of retinoic acid receptor alpha.

Harish Srinivas¹, Denise M Juroske, Shailaja Kalyankrishna, Dianna D Cody, Roger E Price, Xiao-Chun Xu, Ramesh Narayanan, Nancy L Weigel, Jonathan M Kurie.

Abstract

Retinoic acid (RA) is the ligand for nuclear RA receptors (RARs and RXRs) and is crucial for normal epithelial cell growth and differentiation. During malignant transformation, human bronchial epithelial cells acquire a block in retinoid signaling caused in part by a transcriptional defect in RARs. Here, we show that activation of c-Jun N-terminal kinase (JNK) contributes to RAR dysfunction by phosphorylating RARalpha and inducing degradation through the ubiquitin-proteasomal pathway. Analysis of RARalpha mutants and phosphopeptide mapping revealed that RARalpha residues Thr181, Ser445, and Ser461 are phosphorylated by JNK. Mutation of these residues to alanines prevented efficient ubiquitination of RARalpha and increased the stability of the protein. We investigated the importance of RARalpha phosphorylation by JNK as a mediator of retinoid resistance in lung cancer. Mice that develop lung cancer from activation of a latent K-ras oncogene had high intratumoral JNK activity and low RARalpha levels and were resistant to treatment with an RAR ligand. JNK inhibition in a human lung cancer cell line enhanced RARalpha levels, ligand-induced activity of RXR-RAR dimers, and growth inhibition by RA. These findings point to JNK as a key mediator of aberrant retinoid signaling in lung cancer cells.

Entities: Chemical Disease Gene Species

Mesh：

Substances：

Year: 2005 PMID： 15657432 PMCID： PMC543999 DOI： 10.1128/MCB.25.3.1054-1069.2005

Source DB: PubMed Journal: Mol Cell Biol ISSN： 0270-7306 Impact factor: 4.272

85 in total

1. Modulation of retinoic acid sensitivity in lung cancer cells through dynamic balance of orphan receptors nur77 and COUP-TF and their heterodimerization.

Authors: Q Wu; Y Li; R Liu; A Agadir; M O Lee; Y Liu; X Zhang
Journal: EMBO J Date: 1997-04-01 Impact factor: 11.598

Review 2. The ubiquitin system.

Authors: A Hershko; A Ciechanover
Journal: Annu Rev Biochem Date: 1998 Impact factor: 23.643

3. Histone acetyltransferase activity of CBP is controlled by cycle-dependent kinases and oncoprotein E1A.

Authors: S Ait-Si-Ali; S Ramirez; F X Barre; F Dkhissi; L Magnaghi-Jaulin; J A Girault; P Robin; M Knibiehler; L L Pritchard; B Ducommun; D Trouche; A Harel-Bellan
Journal: Nature Date: 1998-11-12 Impact factor: 49.962

4. Antagonism of glucocorticoid receptor transcriptional activation by the c-Jun N-terminal kinase.

Authors: I Rogatsky; S K Logan; M J Garabedian
Journal: Proc Natl Acad Sci U S A Date: 1998-03-03 Impact factor: 11.205

5. Stimulation of RAR alpha activation function AF-1 through binding to the general transcription factor TFIIH and phosphorylation by CDK7.

Authors: C Rochette-Egly; S Adam; M Rossignol; J M Egly; P Chambon
Journal: Cell Date: 1997-07-11 Impact factor: 41.582

6. All-trans-retinoic acid inhibits Jun N-terminal kinase-dependent signaling pathways.

Authors: H Y Lee; G L Walsh; M I Dawson; W K Hong; J M Kurie
Journal: J Biol Chem Date: 1998-03-20 Impact factor: 5.157

7. CBP: a signal-regulated transcriptional coactivator controlled by nuclear calcium and CaM kinase IV.

Authors: S Chawla; G E Hardingham; D R Quinn; H Bading
Journal: Science Date: 1998-09-04 Impact factor: 47.728

8. c-Jun N-terminal kinase phosphorylates peroxisome proliferator-activated receptor-gamma1 and negatively regulates its transcriptional activity.

Authors: H S Camp; S R Tafuri; T Leff
Journal: Endocrinology Date: 1999-01 Impact factor: 4.736

9. JNKK1 organizes a MAP kinase module through specific and sequential interactions with upstream and downstream components mediated by its amino-terminal extension.

Authors: Y Xia; Z Wu; B Su; B Murray; M Karin
Journal: Genes Dev Date: 1998-11-01 Impact factor: 11.361

10. Activity of anti-erbB-2 recombinant toxin OLX-209 on lung cancer cell lines in the absence of erbB-2 gene amplification.

Authors: P G Kasprzyk; T L Sullivan; J D Hunt; C T Gubish; C A Scoppa; M Oelkuct; R Bird; P H Fischer; J M Siegfried; C R King
Journal: Clin Cancer Res Date: 1996-01 Impact factor: 12.531

19 in total

10. Redundant roles for cJun-N-terminal kinase 1 and 2 in interleukin-1beta-mediated reduction and modification of murine hepatic nuclear retinoid X receptor alpha.

Authors: Astrid Kosters; Damara D White; Hongdan Sun; Sundararajah Thevananther; Saul J Karpen
Journal: J Hepatol Date: 2009-08-20 Impact factor: 25.083

c-Jun N-terminal kinase contributes to aberrant retinoid signaling in lung cancer cells by phosphorylating and inducing proteasomal degradation of retinoic acid receptor alpha.

1. Modulation of retinoic acid sensitivity in lung cancer cells through dynamic balance of orphan receptors nur77 and COUP-TF and their heterodimerization.

Review 2. The ubiquitin system.

3. Histone acetyltransferase activity of CBP is controlled by cycle-dependent kinases and oncoprotein E1A.

4. Antagonism of glucocorticoid receptor transcriptional activation by the c-Jun N-terminal kinase.

5. Stimulation of RAR alpha activation function AF-1 through binding to the general transcription factor TFIIH and phosphorylation by CDK7.

6. All-trans-retinoic acid inhibits Jun N-terminal kinase-dependent signaling pathways.

7. CBP: a signal-regulated transcriptional coactivator controlled by nuclear calcium and CaM kinase IV.

8. c-Jun N-terminal kinase phosphorylates peroxisome proliferator-activated receptor-gamma1 and negatively regulates its transcriptional activity.

9. JNKK1 organizes a MAP kinase module through specific and sequential interactions with upstream and downstream components mediated by its amino-terminal extension.

10. Activity of anti-erbB-2 recombinant toxin OLX-209 on lung cancer cell lines in the absence of erbB-2 gene amplification.

Review 1. Uses for JNK: the many and varied substrates of the c-Jun N-terminal kinases.

2. Akt phosphorylates and suppresses the transactivation of retinoic acid receptor alpha.

3. High glucose-induced repression of RAR/RXR in cardiomyocytes is mediated through oxidative stress/JNK signaling.

4. An ATRActive future for differentiation therapy in AML.

5. Cocaine induces nuclear export and degradation of neuronal retinoid X receptor-γ via a TNF-α/JNK- mediated mechanism.

Review 6. JNK Signaling: Regulation and Functions Based on Complex Protein-Protein Partnerships.

7. BMAL1 shuttling controls transactivation and degradation of the CLOCK/BMAL1 heterodimer.

8. Quantitative Proteomic Atlas of Ubiquitination and Acetylation in the DNA Damage Response.

Review 9. Vitamin A and retinoid signaling: genomic and nongenomic effects.

10. Redundant roles for cJun-N-terminal kinase 1 and 2 in interleukin-1beta-mediated reduction and modification of murine hepatic nuclear retinoid X receptor alpha.