首页> 外文期刊>Molecular and Cellular Biology >Functional interference between the ubiquitous and constitutive octamer transcription factor 1 (OTF-1) and the glucocorticoid receptor by direct protein-protein interaction involving the homeo subdomain of OTF-1.
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Functional interference between the ubiquitous and constitutive octamer transcription factor 1 (OTF-1) and the glucocorticoid receptor by direct protein-protein interaction involving the homeo subdomain of OTF-1.

机译:遍在和组成型八聚体转录因子1(OTF-1)和糖皮质激素受体之间的功能干扰是通过涉及OTF-1同源域的直接蛋白质-蛋白质相互作用而实现的。

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The ubiquitous and constitutive octamer transcription factor OTF-1 (Oct 1) is the target of positive regulation by the potent herpes simplex virus trans-activator VP16, which forms a complex with the homeodomain of OTF-1. Here we present evidence that the glucocorticoid receptor can negatively regulate OTF-1 function by a mechanism that is independent of DNA binding. In vivo-expressed glucocorticoid receptor inhibited in a hormone-dependent manner activation of a minimal promoter construct carrying a functional octamer site. Moreover, expression of the receptor in vivo resulted in hormone-dependent repression of OTF-1-dependent DNA-binding activity in nuclear extract. In vitro, the DNA-binding activity of partially purified OTF-1 was repressed following incubation with purified glucocorticoid receptor. Cross-linking and immunoprecipitation experiments indicated that the functional interference may be due to a strong association between these two proteins in solution. Finally, preliminary evidence indicates that the homeo subdomain of OTF-1 that directs formation of a complex with VP16 may also be critical for interaction with the glucocorticoid receptor. Thus, OTF-1 is a target for both positive and negative regulation by protein-protein interaction. Moreover, the functional interference between OTF-1 and the glucocorticoid receptor represents a novel regulatory mechanism in the cross-coupling of signal transduction pathways of nuclear receptors and constitutive transcription factors.
机译:普遍存在的组成型八聚体转录因子OTF-1(10月1日)是有效的单纯疱疹病毒反式激活因子VP16(与OTF-1的同源域形成复合体)正调控的目标。在这里,我们提供证据表明糖皮质激素受体可以通过独立于DNA结合的机制来负调节OTF-1功能。体内表达的糖皮质激素受体以激素依赖性方式抑制带有功能性八聚体位点的最小启动子构建体的活化。此外,该受体在体内的表达导致核提取物中激素依赖性的OTF-1依赖性DNA结合活性的抑制。在体外,与纯化的糖皮质激素受体孵育后,部分纯化的OTF-1的DNA结合活性受到抑制。交联和免疫沉淀实验表明,功能干扰可能是由于溶液中这两种蛋白质之间的强缔合所致。最后,初步证据表明,引导与VP16形成复合物的OTF-1的homeo子域对于与糖皮质激素受体的相互作用也可能至关重要。因此,OTF-1是通过蛋白质-蛋白质相互作用进行正调控和负调控的靶标。此外,OTF-1和糖皮质激素受体之间的功能干扰代表核受体和组成型转录因子的信号转导途径的交叉偶联中的新型调节机制。

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