Functional interaction between Smad, CREB binding protein, and p68 RNA helicase

SMAD公司 RNA解旋酶A 细胞生物学 生物 转录因子 报告基因 分子生物学 R-SMAD CREB结合蛋白 解旋酶 基因表达 核糖核酸 奶油 信号转导 基因 生物化学 内皮糖蛋白 干细胞 川地34
作者
Dennis R. Warner,Vasker Bhattacherjee,Xiaolong Yin,Saurabh Singh,Partha Mukhopadhyay,M. Michele Pisano,Robert Greene
出处
期刊:Biochemical and Biophysical Research Communications [Elsevier]
卷期号:324 (1): 70-76 被引量:76
标识
DOI:10.1016/j.bbrc.2004.09.017
摘要

The transforming growth factors β control a diversity of biological processes including cellular proliferation, differentiation, apoptosis, and extracellular matrix production, and are critical effectors of embryonic patterning and development, including that of the orofacial region. TGFβ superfamily members signal through specific cell surface receptors that phosphorylate the cytoplasmic Smad proteins, resulting in their translocation to the nucleus and interaction with promoters of TGFβ-responsive genes. Subsequent alterations in transcription are cell type-specific and dependent on recruitment to the Smad/transcription factor complex of coactivators, such as CBP and p300, or corepressors, such as c-ski and SnoN. Since the affinity of Smads for DNA is generally low, additional accessory proteins that facilitate Smad/DNA binding are required, and are often cell- and tissue-specific. In order to identify novel Smad 3 binding proteins in developing orofacial tissue, a yeast two hybrid assay was employed in which the MH2 domain of Smad 3 was used to screen an expression library derived from mouse embryonic orofacial tissue. The RNA helicase, p68, was identified as a unique Smad binding protein, and the specificity of the interaction was confirmed through various in vitro and in vivo assays. Co-expression of Smad 3 and a CBP-Gal4 DNA binding domain fusion protein in a Gal4-luciferase reporter assay resulted in increased TGFβ-stimulated reporter gene transcription. Moreover, co-expression of p68 RNA helicase along with Smad 3 and CBP-Gal4 resulted in synergistic activation of Gal4-luciferase reporter expression. Collectively, these data indicate that the RNA helicase, p68, can directly interact with Smad 3 resulting in formation of a transcriptionally active ternary complex containing Smad 3, p68, and CBP. This offers a means of enhancing TGFβ-mediated cellular responses in developing orofacial tissue.
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