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Oct-1的POU特异性结构域可通过稳定基础转录复合物SNAPc来刺激小核RNA基因转录。

The Oct-1 POU-specific domain can stimulate small nuclear RNA gene transcription by stabilizing the basal transcription complex SNAPc.

作者信息

Mittal V, Cleary M A, Herr W, Hernandez N

机构信息

Howard Hughes Medical Institute, State University of New York at Stony Brook, New York 11794, USA.

出版信息

Mol Cell Biol. 1996 May;16(5):1955-65. doi: 10.1128/MCB.16.5.1955.

Abstract

The RNA polymerase II and III human small nuclear RNA promoters have a common basal element, the proximal sequence element, which binds the TATA box-binding protein-containing complex SNAPc. They also contain an enhancer characterized by a highly conserved octamer sequence, which constitutes a binding site for the broadly expressed POU domain transcription factor Oct-1. The POU domain is a bipartite DNA-binding domain consisting of a POU-homeo (POUH) domain and a POU-specific (POUs) domain joined by a flexible linker. Here, we show that the Oct-1 POU domain but not the related Pit-1 POU domain can facilitate the binding of SNAPc to the proximal sequence element, and activate transcription. The effect is probably mediated by protein-protein contacts, and 1 of 30 amino acid differences between the Oct-1 and Pit-1 POUs domains is the key determinant for the differential interaction with SNAPc and the ability to activate transcription. These results show that a function that is the hallmark of activation domains, namely, recruitment of a basal transcription complex resulting in activation of transcription, can be performed by a DNA-binding domain. In this case, subtle changes between activator DNA-binding domains, as subtle as a single amino acid difference, can profoundly affect interaction with the basal transcription machinery.

摘要

RNA聚合酶II和III的人类小核RNA启动子有一个共同的基础元件,即近端序列元件,它能结合含TATA盒结合蛋白的复合物SNAPc。它们还含有一个以高度保守的八聚体序列为特征的增强子,该序列构成了广泛表达的POU结构域转录因子Oct-1的结合位点。POU结构域是一个二分DNA结合结构域,由一个POU同源(POUH)结构域和一个POU特异性(POUs)结构域通过一个柔性接头连接而成。在这里,我们表明Oct-1的POU结构域而非相关的Pit-1的POU结构域能够促进SNAPc与近端序列元件的结合,并激活转录。这种效应可能是由蛋白质-蛋白质相互作用介导的,Oct-1和Pit-1的POU结构域之间30个氨基酸差异中的1个是与SNAPc差异相互作用以及激活转录能力的关键决定因素。这些结果表明,激活结构域的一个标志性功能,即募集基础转录复合物从而激活转录,可以由一个DNA结合结构域来执行。在这种情况下,激活剂DNA结合结构域之间的细微变化,细微到单个氨基酸差异,都能深刻影响与基础转录机制的相互作用。

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