Interaction of antiproliferative protein Tob with the CCR4-NOT deadenylase complex

Takashi Miyasaka; Masahiro Morita; Kentaro Ito; Toru Suzuki; Hiroyuki Fukuda; Shizu Takeda; Jun Ichiro Inoue; Kentaro Semba; Tadashi Yamamoto

doi:10.1111/j.1349-7006.2008.00746.x

Interaction of antiproliferative protein Tob with the CCR4-NOT deadenylase complex

Takashi Miyasaka, Masahiro Morita, Kentaro Ito, Toru Suzuki, Hiroyuki Fukuda, Shizu Takeda, Jun Ichiro Inoue, Kentaro Semba, Tadashi Yamamoto

Producción científica: Article › revisión exhaustiva

33 Citas (Scopus)

Resumen

Tob protein, when overexpressed, suppresses growth of NIH3T3 cells, presumably by regulating expression of various growth-related genes. However, the molecular mechanisms underlying Tob-mediated regulation of gene expression have been obscure. To address this issue we established stable Tob-expressing cell lines and used a proteomics approach to identify Tob-interacting proteins. We found that Tob associates with the CCR4-NOT complex. The carboxyl-terminal half of Tob interacted with Cnot1, a core protein of the CCR4-NOT complex. We further showed that the deadenylase activity associated with the complex was suppressed in vitro by Tob. These results suggest that the antiproliferative activity of Tob is shown post-transcriptionally by controlling the stability of the target mRNAs in addition to its involvement in transcriptional regulation, reported previously.

Idioma original	English (US)
Páginas (desde-hasta)	755-761
Número de páginas	7
Publicación	Cancer Science
Volumen	99
N.º	4
DOI	https://doi.org/10.1111/j.1349-7006.2008.00746.x
Estado	Published - abr 2008
Publicado de forma externa	Sí

ASJC Scopus subject areas

Oncology
Cancer Research

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title = "Interaction of antiproliferative protein Tob with the CCR4-NOT deadenylase complex",

abstract = "Tob protein, when overexpressed, suppresses growth of NIH3T3 cells, presumably by regulating expression of various growth-related genes. However, the molecular mechanisms underlying Tob-mediated regulation of gene expression have been obscure. To address this issue we established stable Tob-expressing cell lines and used a proteomics approach to identify Tob-interacting proteins. We found that Tob associates with the CCR4-NOT complex. The carboxyl-terminal half of Tob interacted with Cnot1, a core protein of the CCR4-NOT complex. We further showed that the deadenylase activity associated with the complex was suppressed in vitro by Tob. These results suggest that the antiproliferative activity of Tob is shown post-transcriptionally by controlling the stability of the target mRNAs in addition to its involvement in transcriptional regulation, reported previously.",

author = "Takashi Miyasaka and Masahiro Morita and Kentaro Ito and Toru Suzuki and Hiroyuki Fukuda and Shizu Takeda and Inoue, {Jun Ichiro} and Kentaro Semba and Tadashi Yamamoto",

note = "Funding Information: Funding: B. Tampe was supported by the Research program, University Medical Center, University of G{\"o}ttingen, Germany (1403720). The funding sources had no involvement in the design, collection, analysis, interpretation, writing or decision to submit the article. Competing interests: none declared.",

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doi = "10.1111/j.1349-7006.2008.00746.x",

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AU - Miyasaka, Takashi

AU - Morita, Masahiro

AU - Ito, Kentaro

AU - Suzuki, Toru

AU - Fukuda, Hiroyuki

AU - Takeda, Shizu

AU - Inoue, Jun Ichiro

AU - Semba, Kentaro

AU - Yamamoto, Tadashi

N1 - Funding Information: Funding: B. Tampe was supported by the Research program, University Medical Center, University of Göttingen, Germany (1403720). The funding sources had no involvement in the design, collection, analysis, interpretation, writing or decision to submit the article. Competing interests: none declared.

PY - 2008/4

Y1 - 2008/4

N2 - Tob protein, when overexpressed, suppresses growth of NIH3T3 cells, presumably by regulating expression of various growth-related genes. However, the molecular mechanisms underlying Tob-mediated regulation of gene expression have been obscure. To address this issue we established stable Tob-expressing cell lines and used a proteomics approach to identify Tob-interacting proteins. We found that Tob associates with the CCR4-NOT complex. The carboxyl-terminal half of Tob interacted with Cnot1, a core protein of the CCR4-NOT complex. We further showed that the deadenylase activity associated with the complex was suppressed in vitro by Tob. These results suggest that the antiproliferative activity of Tob is shown post-transcriptionally by controlling the stability of the target mRNAs in addition to its involvement in transcriptional regulation, reported previously.

AB - Tob protein, when overexpressed, suppresses growth of NIH3T3 cells, presumably by regulating expression of various growth-related genes. However, the molecular mechanisms underlying Tob-mediated regulation of gene expression have been obscure. To address this issue we established stable Tob-expressing cell lines and used a proteomics approach to identify Tob-interacting proteins. We found that Tob associates with the CCR4-NOT complex. The carboxyl-terminal half of Tob interacted with Cnot1, a core protein of the CCR4-NOT complex. We further showed that the deadenylase activity associated with the complex was suppressed in vitro by Tob. These results suggest that the antiproliferative activity of Tob is shown post-transcriptionally by controlling the stability of the target mRNAs in addition to its involvement in transcriptional regulation, reported previously.

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Interaction of antiproliferative protein Tob with the CCR4-NOT deadenylase complex

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ASJC Scopus subject areas

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