The type I TGF-β receptor is covalently modified and regulated by sumoylation

被引:0
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作者
Jong Seok Kang
Elise F. Saunier
Rosemary J. Akhurst
Rik Derynck
机构
[1] Program in Cell Biology,Department of Cell and Tissue Biology
[2] University of California – San Francisco,Department of Anatomy
[3] Cancer Research Institute,undefined
[4] University of California – San Francisco,undefined
[5] University of California – San Francisco,undefined
[6] Program In Human Genetics,undefined
[7] University of California – San Francisco,undefined
来源
Nature Cell Biology | 2008年 / 10卷
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摘要
Post-translational sumoylation, the covalent attachment of a small ubiquitin-like modifier (SUMO), regulates the functions of proteins engaged in diverse processes. Often associated with nuclear and perinuclear proteins, such as transcription factors, it is not known whether SUMO can conjugate to cell-surface receptors for growth factors to regulate their functions. Here we show that the type I transforming growth factor-β (TGF-β) receptor, TβRI, is sumoylated in response to TGF-β and that its sumoylation requires the kinase activities of both TβRI and the type II TGF-β receptor, TβRII. Sumoylation of TβRI enhances receptor function by facilitating the recruitment and phosphorylation of Smad3, consequently regulating TGF-β-induced transcription and growth inhibition. TβRI sumoylation modulates the dissemination of transformed cells in a mouse model of TβRI-stimulated metastasis. TβRI sumoylation therefore controls responsiveness to TGF-β, with implications for tumour progression. Sumoylation of cell-surface receptors may regulate other growth factor responses.
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页码:654 / 664
页数:10
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