Dual regulation of Notch1 signaling pathway by adaptor protein Fe65

KimM.-Y.; MoJ.-S.; AnnE.-J.YoonJ.-H.ParkH.-S.

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Dual regulation of Notch1 signaling pathway by adaptor protein Fe65

机译：衔接蛋白Fe65对Notch1信号通路的双重调控

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Notch1 receptor functions as a critical controller of cell fate decisions and also as a key regulator of cell growth, differentiation, and proliferation in invertebrates and vertebrates. In this study, we have demonstrated that the adaptor protein Fe65 attenuates Notch1 signaling via the accelerated degradation of the membrane-tethered Notch1 in the cytoplasm. Fe65 also suppresses Notch1 transcriptional activity via the dissociation of the Notch1-IC-recombining binding protein suppressor of hairless (RBP)-Jk complex within the nucleus. Fe65 is capable of forming a trimeric complex with Itch and membrane-tethered Notch1, and Fe65 enhances the protein degradation of membrane- tethered Notch1 via an Itch-dependent proteasomal pathway. Collectively, our results demonstrate that Fe65 carries out different functions depending on its location in the regulation of Notch1 signaling.

机译：Notch1 受体是细胞命运决定的关键控制者，也是无脊椎动物和脊椎动物细胞生长、分化和增殖的关键调节因子。在这项研究中，我们已经证明接头蛋白 Fe65 通过加速细胞质中膜系系 Notch1 的降解来减弱 Notch1 信号传导。Fe65 还通过解离细胞核内无毛（RBP）-Jk 复合物的 Notch1-IC 重组结合蛋白抑制因子来抑制 Notch1 转录活性。Fe65 能够与 Itch 和膜系留的 Notch1 形成三聚体复合物，并且 Fe65 通过 Itch 依赖性蛋白酶体途径增强膜系系 Notch1 的蛋白质降解。总的来说，我们的结果表明，Fe65 根据其在 Notch1 信号调节中的位置执行不同的功能。

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《The Journal of biological chemistry》 |2012年第7期|4690-4701|共12页
作者
KimM.-Y.; MoJ.-S.; AnnE.-J.YoonJ.-H.ParkH.-S.;
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Hormone Research Center, School of Biological Sciences and Technology, Chonnam National University;

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正文语种英语
中图分类生物化学;
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Dual regulation of Notch1 signaling pathway by adaptor protein Fe65

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