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	Provedor de dados Nature Precedings (2) Autor Peter ten Dijke (2) Aya Tanaka (1) Chris Lu (1) Craig Mickanin (1) Eliza Wiercinska (1) Ewa Snaar-Jagalska (1) Fangfang Zhou (1) Hiroshi Shibuya (1) Huizhe Huang (1) Kelly-Ann Sheppard (1) Kiyotoshi Satoh (1) Liang Shi (1) Long Zhang (1) Masako Inamitsu (1) Mitsuyasu Kato (1) Naoko Nakano (1) Susumu Itoh (1) Yukihide Watanabe (1) Yvette Drabsch (1) Mais... Palavra-chave Cancer (2) Molecular Cell Biology (2) Biotechnology (1) Developmental Biology (1) Genetics & Genomics (1) Pharmacology (1) Mais... Tipo do documento Manuscript (2) Ano 2012 (1) 2007 (1) País United Kingdom (2)		Ordenar por:  Relevância Autor Título Ano Registros recuperados: 2 Primeira ... 1 ... Última USP4 is regulated by Akt phosphorylation and deubiquitylates TGF-beta type I receptor Nature Precedings Long Zhang; Fangfang Zhou; Yvette Drabsch; Ewa Snaar-Jagalska; Craig Mickanin; Huizhe Huang; Kelly-Ann Sheppard; Chris Lu; Peter ten Dijke. Stability and membrane localization of Transforming growth factor-β (TGF-β) type I receptor (TβRI) is essential for controlling TGF-β signaling. TβRI is targeted for ubiquitination-mediated degradation by Smad7/Smurf2 complex. However, it is unclear whether polyubiquitin modified TβRI can be reversed. Here we performed a genome-wide gain of function screen and identified ubiquitin-specific protease (USP) 4 as a strong inducer of TGF-β signaling. Putative oncogenic USP4 was found to interact with TβRI as deubiquitinating enzyme thus maintains TβR1 levels at the plasma membrane. Depletion of USP4 mitigates TGF-β-induced breast cancer cell migration, epithelial... Tipo: Manuscript Palavras-chave: Biotechnology; Cancer; Developmental Biology; Genetics & Genomics; Molecular Cell Biology; Pharmacology. Ano: 2012 URL: http://precedings.nature.com/documents/6804/version/1 TMEPAI, a transmembrane TGF-β-inducible protein, sequesters Smad proteins in TGF-β signaling Nature Precedings Susumu Itoh; Yukihide Watanabe; Kiyotoshi Satoh; Masako Inamitsu; Liang Shi; Naoko Nakano; Aya Tanaka; Eliza Wiercinska; Hiroshi Shibuya; Peter ten Dijke; Mitsuyasu Kato. Transforming growth factor-[beta] (TGF-[beta]) is a multifunctional cytokine of key importance for controlling embryogenesis and tissue homeostasis. How TGF-[beta] signals are attenuated and terminated is not well understood. Here, we show that TMEPAI, a direct target gene of TGF-[beta] signaling, antagonizes TGF-[beta] signaling by interfering with TGF-[beta] type I receptor (T[beta]RI)-induced R-Smad phosphorylation. TMEPAI can directly interact with R-Smads via a Smad interaction motif (SIM). TMEPAI competes with Smad anchor for receptor activation (SARA) for R-Smad binding, thereby sequestering R-Smads from T[beta]RI kinase activation. In mammalian cells, ectopic expression of TMEPAI inhibited TGF-[beta]-induced PAI-1 production, whereas specific... Tipo: Manuscript Palavras-chave: Cancer; Molecular Cell Biology. Ano: 2007 URL: http://precedings.nature.com/documents/1403/version/1 Registros recuperados: 2 Primeira ... 1 ... Última

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