RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation

Inflammation is a complex biological host reaction to tissue damage, infection and trauma. Extensive study of the inflammatory response has led to the identification of several protein kinases that are essential for signaling and could be potential therapeutic targets. The RSK family of kinases has...

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Autores principales: Yao, Ke, Lee, Sung-Young, Peng, Cong, Lim, Do Young, Yamamoto, Hiroyuki, Ryu, Joohyun, Lim, Tae-Gyu, Chen, Hanyong, Jin, Guoguo, Zhao, Zhenjiang, Han, Yaping, Ma, Wei-Ya, Bode, Ann M., Dong, Zigang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2018
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6023753/
https://www.ncbi.nlm.nih.gov/pubmed/29563609
http://dx.doi.org/10.1038/s41388-018-0167-6
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author Yao, Ke
Lee, Sung-Young
Peng, Cong
Lim, Do Young
Yamamoto, Hiroyuki
Ryu, Joohyun
Lim, Tae-Gyu
Chen, Hanyong
Jin, Guoguo
Zhao, Zhenjiang
Han, Yaping
Ma, Wei-Ya
Bode, Ann M.
Dong, Zigang
author_facet Yao, Ke
Lee, Sung-Young
Peng, Cong
Lim, Do Young
Yamamoto, Hiroyuki
Ryu, Joohyun
Lim, Tae-Gyu
Chen, Hanyong
Jin, Guoguo
Zhao, Zhenjiang
Han, Yaping
Ma, Wei-Ya
Bode, Ann M.
Dong, Zigang
author_sort Yao, Ke
collection PubMed
description Inflammation is a complex biological host reaction to tissue damage, infection and trauma. Extensive study of the inflammatory response has led to the identification of several protein kinases that are essential for signaling and could be potential therapeutic targets. The RSK family of kinases has multiple cellular functions. In our study, we found that RSK2 is a mediator for inflammation signaling and interacts with TRAF6. In vitro kinase assay results indicated that RSK2 strongly phosphorylates TRAF6 at serines 46, 47 and 48. Ectopic over-expression of TRAF6 or knocking down RSK2 expression confirmed that RSK2 is a positive regulator of TRAF6 K63 ubiquitination. TRAF6 is also required for RSK2 ubiquitination. TRAF6 bridges the TNF receptor superfamily and intracellular signaling for the induction of pro-inflammatory cytokines. We developed a colon inflammation model using RSK2 wild type (WT) and knockout (KO) mice. As expected, F4/80 and CD3 infiltration were significantly upregulated in WT mice compared to RSK2 KO mice. Furthermore, inflammation signaling, including Ikkα/β, p38 and JNKs, was dramatically up-regulated in WT mice. Colon tissue immunoprecipitation results further confirmed that TRAF6 K63 ubiquitination was lower in RSK2 KO mice. Overall, these results indicate that phosphorylation of TRAF6 (S46, 47, 48) by RSK2 is required for TRAF6 K63 ubiquitination and inflammation signaling.
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spelling pubmed-60237532018-09-22 RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation Yao, Ke Lee, Sung-Young Peng, Cong Lim, Do Young Yamamoto, Hiroyuki Ryu, Joohyun Lim, Tae-Gyu Chen, Hanyong Jin, Guoguo Zhao, Zhenjiang Han, Yaping Ma, Wei-Ya Bode, Ann M. Dong, Zigang Oncogene Article Inflammation is a complex biological host reaction to tissue damage, infection and trauma. Extensive study of the inflammatory response has led to the identification of several protein kinases that are essential for signaling and could be potential therapeutic targets. The RSK family of kinases has multiple cellular functions. In our study, we found that RSK2 is a mediator for inflammation signaling and interacts with TRAF6. In vitro kinase assay results indicated that RSK2 strongly phosphorylates TRAF6 at serines 46, 47 and 48. Ectopic over-expression of TRAF6 or knocking down RSK2 expression confirmed that RSK2 is a positive regulator of TRAF6 K63 ubiquitination. TRAF6 is also required for RSK2 ubiquitination. TRAF6 bridges the TNF receptor superfamily and intracellular signaling for the induction of pro-inflammatory cytokines. We developed a colon inflammation model using RSK2 wild type (WT) and knockout (KO) mice. As expected, F4/80 and CD3 infiltration were significantly upregulated in WT mice compared to RSK2 KO mice. Furthermore, inflammation signaling, including Ikkα/β, p38 and JNKs, was dramatically up-regulated in WT mice. Colon tissue immunoprecipitation results further confirmed that TRAF6 K63 ubiquitination was lower in RSK2 KO mice. Overall, these results indicate that phosphorylation of TRAF6 (S46, 47, 48) by RSK2 is required for TRAF6 K63 ubiquitination and inflammation signaling. 2018-03-22 2018-06 /pmc/articles/PMC6023753/ /pubmed/29563609 http://dx.doi.org/10.1038/s41388-018-0167-6 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Yao, Ke
Lee, Sung-Young
Peng, Cong
Lim, Do Young
Yamamoto, Hiroyuki
Ryu, Joohyun
Lim, Tae-Gyu
Chen, Hanyong
Jin, Guoguo
Zhao, Zhenjiang
Han, Yaping
Ma, Wei-Ya
Bode, Ann M.
Dong, Zigang
RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation
title RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation
title_full RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation
title_fullStr RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation
title_full_unstemmed RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation
title_short RSK2 is required for TRAF6 phosphorylation-mediated colon inflammation
title_sort rsk2 is required for traf6 phosphorylation-mediated colon inflammation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6023753/
https://www.ncbi.nlm.nih.gov/pubmed/29563609
http://dx.doi.org/10.1038/s41388-018-0167-6
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