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Syntenin-mediated regulation of Sox4 proteasomal degradation modulates transcriptional output

SOX4型 生物 基因敲除 MG132型 转录因子 异位表达 细胞生物学 蛋白酶体 癌症研究 蛋白酶体抑制剂 基因表达 细胞培养 基因 遗传学 发起人
作者
Jeffrey M. Beekman,Stephin J. Vervoort,Frederique E. G. A. Dekkers,M E van Vessem,S Vendelbosch,A Brugulat-Panès,Jorg van Loosdregt,Arie Koen Braat,Paul J. Coffer
出处
期刊:Oncogene [Springer Nature]
卷期号:31 (21): 2668-2679 被引量:42
标识
DOI:10.1038/onc.2011.445
摘要

The transcription factor Sox4 is aberrantly expressed in many human tumors and can modulate tumorigenesis and metastases of murine tumors in vivo. However, mechanisms that control Sox4 function remain poorly defined. It has recently been observed that DNA damage increases Sox4 protein expression independently of Sox4 mRNA levels, suggesting an as yet undefined post-transcriptional mechanism regulating Sox4 expression and functionality. Here, we show that Sox4 protein is rapidly degraded by the proteasome as indicated by pharmacological inhibition with Mg132 and epoxymycin. Sox4 half-life was found to be less than 1 h as evident by inhibition of protein synthesis using cycloheximide. Ectopic expression of Sox4 deletion mutants revealed that the C-terminal 33 residues of Sox4 were critical in modulating its degradation in a polyubiquitin-independent manner. Syntenin, a Sox4 binding partner, associates with this domain and was found to stabilize Sox4 expression. Syntenin-induced stabilization of Sox4 correlated with Sox4-syntenin relocalization to the nucleus, where both proteins accumulate. Syntenin overexpression or knockdown in human tumor cell lines was found to reciprocally modulate Sox4 protein expression and transcriptional activity implicating its role as a regulator of Sox4. Taken together, our data demonstrate that the Sox4 C-terminal domain regulates polyubiquitin-independent proteasomal degradation of Sox4 that can be modulated by interaction with syntenin. As aberrant Sox4 expression has been found associated with many human cancers, modulation of Sox4 proteasomal degradation may impact oncogenesis and metastatic properties of tumors.

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