1. The role of sentrin-specific protease 2 substrate recognition in TGF-β-induced tumorigenesis
- Author
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Chia Ju Lin, Tsai Ling Ho, Yen Sung Huang, Ruei Ting Chang, Hsiu-Ming Shih, Jen Chong Jeng, Ying Mei Lin, Shin Mei Liu, Chun Chen Ho, Chun A. Changou, and Che Chang Chang
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0301 basic medicine ,Cellular pathology ,Carcinogenesis ,SUMO protein ,lcsh:Medicine ,Matrix metalloproteinase ,medicine.disease_cause ,Article ,Substrate Specificity ,03 medical and health sciences ,Cell Movement ,Transforming Growth Factor beta ,Spheroids, Cellular ,medicine ,Humans ,Author Correction ,lcsh:Science ,Psychological repression ,Smad4 Protein ,Multidisciplinary ,biology ,Chemistry ,lcsh:R ,Sumoylation ,Cell migration ,Transforming growth factor beta ,Cell biology ,Cysteine Endopeptidases ,030104 developmental biology ,biology.protein ,lcsh:Q ,Transforming growth factor ,Protein Binding ,Signal Transduction - Abstract
Smad4, a common-mediator of Smads, plays a central role in forming complexes with receptor-phosphorylated Smads, and then transduces transforming growth factor (TGF)-β signals into the nuclei. Although many cellular factors are involved in TGF-β induced epithelial-to-mesenchymal transition (EMT) and cell migration, very little is known with the mechanism of Smad4 regulation on pro-oncogenes response by TGF-β. Herein, we demonstrate the interaction of Sentrin-specific protease 2 (SENP2) with Smad4 through SENP2 residue 363~400. The same segment is also important for desumoylation of Smad4, and able to relieve sumoylation-mediated TGF-β repression. The SENP2363~400 segment is critical for TGF-β-induced cell migration, which is correlated with SENP2363~400 deletion mutant failed to increase matrix metalloproteinase (MMP)-9 and EMT marker gene expression. Moreover, our results suggest that the interaction and desumoylation between SENP2 and Smad4 promote cell migration in triple-negative breast cancer cells. Altogether, our data show how SENP2 regulates its substrate for desumoylation, and also the role of SENP2 in TGF-β induced cancer cell migration.
- Published
- 2018
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