Nuclear export of Smad2 and Smad3 by RanBP3 facilitates termination of TGF-beta signaling.

Dai F; Lin X; Chang C; Feng XH

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Nuclear export of Smad2 and Smad3 by RanBP3 facilitates termination of TGF-beta signaling.

机译：RanBP3的Smad2和Smad3核输出促进了TGF-beta信号的终止。

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Smad2 and Smad3 (Smad2/3) are key intracellular signal transducers for TGF-beta signaling, and their transcriptional activities are controlled through reversible phosphorylation and nucleocytoplasmic shuttling. However, the precise mechanism underlying nuclear export of Smad2/3 remains elusive. Here we report the essential function of RanBP3 in selective nuclear export of Smad2/3 in the TGF-beta pathway. RanBP3 directly recognizes dephosphorylated Smad2/3, which results from the activity of nuclear Smad phosphatases, and mediates nuclear export of Smad2/3 in a Ran-dependent manner. As a result, increased expression of RanBP3 inhibits TGF-beta signaling in mammalian cells and Xenopus embryos. Conversely, depletion of RanBP3 expression or dominant-negative inhibition of RanBP3 enhances TGFbeta-induced antiproliferative and transcriptional responses. In conclusion, our study supports a definitive role for RanBP3 in mediating Smad2/3 nuclear export and terminating TGF-beta signaling.

机译：Smad2和Smad3（Smad2 / 3）是TGF-β信号转导的关键细胞内信号转导子，其转录活性通过可逆的磷酸化和核质穿梭控制。但是，Smad2 / 3核出口的确切机制仍然难以捉摸。在这里，我们报告在TGF-β途径的Smad2 / 3选择性核出口中RanBP3的基本功能。 RanBP3直接识别由核Smad磷酸酶的活性引起的去磷酸化Smad2 / 3，并以Ran依赖的方式介导Smad2 / 3的核输出。结果，RanBP3的表达增加抑制了哺乳动物细胞和爪蟾胚胎中的TGF-β信号传导。相反，RanBP3表达的耗尽或RanBP3的显性负抑制作用会增强TGFbeta诱导的抗增殖和转录反应。总之，我们的研究支持RanBP3在介导Smad2 / 3核输出和终止TGF-beta信号传导中的明确作用。

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《Developmental cell 》 |2009年第3期| 共13页
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Dai F; Lin X; Chang C; Feng XH;
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中图分类细胞生物学 ;
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1. Nuclear export of Smad2 and Smad3 by RanBP3 facilitates termination of TGF-beta signaling. [J] . Dai F, Lin X, Chang C, Developmental cell . 2009 ,第3期

机译：RanBP3的Smad2和Smad3核输出促进了TGF-beta信号的终止。
2. PPM1A dephosphorylates RanBP3 to enable efficient nuclear export of Smad2 and Smad3 [J] . Dai F., Shen T., Li Z., EMBO reports . 2011 ,第11期

机译：PPM1A使RanBP3脱磷酸化，以实现Smad2和Smad3的有效核出口
3. Sumoylation of Smad3 stimulates its nuclear export during PIASy-mediated suppression of TGF-beta signaling. [J] . Imoto S, Ohbayashi N, Ikeda O, Biochemical and Biophysical Research Communications . 2008 ,第2期

机译：Smad3的Sumoylation刺激其PIASy介导的TGF-beta信号转导抑制过程中的核出口。
4. Regulatory issues in spent nuclear fuel management after the safe termination ofnuclear activities [C] . Paliukhovich V.M. Lessons Learned From the Decommissioning of Nuclear Facilities and the Safe Termination of Nuclear Activities . 2007

机译：安全终止核活动后乏核燃料管理中的监管问题
5. Cex1p is a novel component of the Saccharomyces cerevisiae nuclear tRNA export machinery that facilitates dissociation of the tRNA-export receptor complex at the cytoplasmic face of the nuclear pore complex. [D] . McGuire, Andrew T. 2011

机译：Cex1p是啤酒酵母核tRNA出口机制的新型组件，可促进tRNA出口受体复合物在核孔复合体的胞质面上解离。
6. Nuclear export of Smad2 and Smad3 by RanBP3 facilitates termination of TGF-β signaling [O] . Fangyan Dai, Xia Lin, Chenbei Chang, -1

机译：RanBP3核输出Smad2和Smad3促进TGF-β信号传导的终止
7. Nuclear Export of Smad2 and Smad3 by RanBP3 Facilitates Termination of TGF-β Signaling [O] . Dai Fangyan, Lin Xia, Chang Chenbei, 2009

机译：RanBP3核输出Smad2和Smad3有助于终止TGF-β信号传导。
8. Studying the Roles of GRK2-Mediated Smad2/3 Phosphorylation as a Negative Feedback Mechanism of TGF-Beta Signaling and a Target of Breast Cancer Therapeutics. [R] . J. Guo 2014

机译：研究GRK2介导的smad2 / 3磷酸化作为TGF-β信号的负反馈机制和乳腺癌治疗靶点的作用。

Nuclear export of Smad2 and Smad3 by RanBP3 facilitates termination of TGF-beta signaling.

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