同源结构域蛋白CDP和SATB1相互作用:组织特异性调控的潜力。
Homeoproteins CDP and SATB1 interact: potential for tissue-specific regulation.
作者信息
Liu J, Barnett A, Neufeld E J, Dudley J P
机构信息
Department of Microbiology and Institute for Cellular and Molecular Biology, The University of Texas at Austin, Austin, Texas 78712, USA.
出版信息
Mol Cell Biol. 1999 Jul;19(7):4918-26. doi: 10.1128/MCB.19.7.4918.
Homeoproteins are known to participate in development and cell type specification. The homeoproteins CCAAT displacement protein (CDP) and special AT-rich sequence binding protein 1 (SATB1) have been shown to bind to nuclear matrix-associated regions and to act as repressors of many cellular genes. Moreover, binding of SATB1 to the mouse mammary tumor virus (MMTV) promoter region dramatically affects the tissue-specific transcription of this retrovirus. Because protein-protein interactions are a common means of regulating homeoprotein function, we tested whether SATB1 and CDP interact in vivo and in vitro. SATB1 interacted with CDP through its DNA-binding domain, as demonstrated by glutathione S-transferase (GST) pull-down assays. GST pull-down assays also showed that CDP associated with SATB1 through three of its four DNA-binding domains (CR1, CR2, and the homeodomain). SATB1-specific antisera, but not preimmune sera, precipitated CDP from nuclear extracts, and CDP-specific antisera precipitated SATB1 from the same extracts. Far-Western blotting detected interaction of SATB1 and CDP in several different tissue extracts. Association of purified SATB1 and CDP in vitro resulted in the inability of each protein to bind to DNA in gel retardation assays. CDP overexpression in cultured T cells led to a loss of detectable SATB1 binding to the MMTV promoter region, as measured by gel shift experiments. CDP overexpression also elevated MMTV long terminal repeat reporter gene activity in transient-transfection assays, a result consistent with neutralization of the SATB1 repressor function in T cells. SATB1 is very abundant in certain tissues, particularly thymus, whereas CDP is relatively ubiquitous, except in certain terminally differentiated cell types. Because of the tissue and cell type distribution of SATB1 and CDP, we propose that the SATB1-to-CDP ratio in different tissues is a novel mechanism for homeoproteins to control gene expression and differentiation in mammals.
已知同源结构域蛋白参与发育和细胞类型的特异性分化。同源结构域蛋白CCAAT置换蛋白(CDP)和富含AT序列的特殊结合蛋白1(SATB1)已被证明可与核基质相关区域结合,并作为许多细胞基因的阻遏物发挥作用。此外,SATB1与小鼠乳腺肿瘤病毒(MMTV)启动子区域的结合会显著影响该逆转录病毒的组织特异性转录。由于蛋白质-蛋白质相互作用是调节同源结构域蛋白功能的常见方式,我们测试了SATB1和CDP在体内和体外是否相互作用。谷胱甘肽S-转移酶(GST)下拉实验表明,SATB1通过其DNA结合结构域与CDP相互作用。GST下拉实验还表明,CDP通过其四个DNA结合结构域中的三个(CR1、CR2和同源结构域)与SATB1相关联。SATB1特异性抗血清而非免疫前血清能从核提取物中沉淀出CDP,而CDP特异性抗血清能从相同提取物中沉淀出SATB1。Far-Western印迹法检测到SATB1和CDP在几种不同组织提取物中的相互作用。体外纯化的SATB1和CDP的结合导致每种蛋白质在凝胶阻滞实验中无法与DNA结合。通过凝胶迁移实验测量,培养的T细胞中CDP的过表达导致可检测到的SATB1与MMTV启动子区域的结合丧失。在瞬时转染实验中,CDP的过表达也提高了MMTV长末端重复报告基因的活性,这一结果与T细胞中SATB1阻遏功能的中和一致。SATB1在某些组织中非常丰富,尤其是胸腺,而CDP相对普遍存在,但在某些终末分化细胞类型中除外。由于SATB1和CDP的组织和细胞类型分布,我们提出不同组织中SATB1与CDP的比例是同源结构域蛋白控制哺乳动物基因表达和分化的一种新机制。
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