Novel mechanism of JNK pathway activation by adenoviral E1A

Vasily S. Romanov; Anna I. Brichkina; Helen Morrison; Tatiana V. Pospelova; Valery A. Pospelov; Peter Herrlich

doi:10.18632/oncotarget.1860

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Research Papers:

Novel mechanism of JNK pathway activation by adenoviral E1A

Vasily S. Romanov _, Anna I. Brichkina, Helen Morrison, Tatiana V. Pospelova, Valery A. Pospelov and Peter Herrlich

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Oncotarget. 2014; 5:2176-2186. https://doi.org/10.18632/oncotarget.1860

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Abstract

Vasily S. Romanov1,*, Anna I. Brichkina1,2,4,*, Helen Morrison1, Tatiana V. Pospelova2,3, Valery A. Pospelov2,3, Peter Herrlich1

1 Leibniz Institute for Age Research – Fritz Lipmann Institute (FLI), Jena, Germany

2 Institute of Cytology, Russian Academy of Sciences, St. Petersburg, Russia

3 St. Petersburg State University, St. Petersburg, Russia

4 Present address: Institute of Molecular and Cell Biology, A-STAR, Proteos, Singapore

* These authors contributed equally to this study

Correspondence:

Vasily S. Romanov, email:

Keywords: adenoviral E1A; AP-1 subunit c-Jun; JNK signaling pathway; small GTPase Rac1; ERM family proteins

Received: March 5, 2014 Accepted: March 24, 2014 Published: March 25, 2014

Abstract

The adenoviral oncoprotein E1A influences cellular regulation by interacting with a number of cellular proteins. In collaboration with complementary oncogenes, E1A fully transforms primary cells. As part of this action, E1A inhibits transcription of c-Jun:Fos target genes while promoting that of c-Jun:ATF2-dependent genes including jun. Both c-Jun and ATF2 are hyperphosphorylated in response to E1A. In the current study, E1A was fused with the ligand binding domain of the estrogen receptor (E1A-ER) to monitor the immediate effect of E1A activation. With this approach we now show that E1A activates c-Jun N-terminal kinase (JNK), the upstream kinases MKK4 and MKK7, as well as the small GTPase Rac1. Activation of the JNK pathway requires the N-terminal domain of E1A, and, importantly, is independent of transcription. In addition, it requires the presence of ERM proteins. Downregulation of signaling components upstream of JNK inhibits E1A-dependent JNK/c-Jun activation. Taking these findings together, we show that E1A activates the JNK/c-Jun signaling pathway upstream of Rac1 in a transcription-independent manner, demonstrating a novel mechanism of E1A action.

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Research Papers:

Novel mechanism of JNK pathway activation by adenoviral E1A

Abstract