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Sp-1结合由RB蛋白调控的启动子元件,并且RB共表达可刺激Sp-1介导的转录。

Sp-1 binds promoter elements regulated by the RB protein and Sp-1-mediated transcription is stimulated by RB coexpression.

作者信息

Udvadia A J, Rogers K T, Higgins P D, Murata Y, Martin K H, Humphrey P A, Horowitz J M

机构信息

Section of Cell Growth, Regulation and Oncogenesis, Duke University Medical Center, Durham, NC 27710.

出版信息

Proc Natl Acad Sci U S A. 1993 Apr 15;90(8):3265-9. doi: 10.1073/pnas.90.8.3265.

Abstract

The retinoblastoma (RB) protein is implicated in transcriptional regulation of at least five cellular genes, including c-fos, c-myc, and transforming growth factor beta 1. Cotransfection of RB and truncated promoter constructs has defined a discrete element (retinoblastoma control element; RCE) within the promoters of each of these genes as being necessary for RB-mediated transcription control. Previously, we have shown that RCEs form protein-DNA complexes in vitro with three heretofore unidentified nuclear proteins and mutation of their DNA-binding site within the c-fos RCE results in an abrogation of RCE-dependent transcription in vivo. Here, we demonstrate that one of the nuclear proteins that binds the c-fos, c-myc, and transforming growth factor beta 1 RCEs in vitro is Sp-1 and that Sp-1 stimulates RCE-dependent transcription in vivo. Moreover, we show that Sp-1-mediated transcription is stimulated by the transient coexpression of RB protein. We conclude from these observations that RB may regulate transcription in part by virtue of its ability to functionally interact with Sp-1.

摘要

视网膜母细胞瘤(RB)蛋白与至少五个细胞基因的转录调控有关,包括c-fos、c-myc和转化生长因子β1。RB与截短的启动子构建体的共转染已确定这些基因各自启动子内的一个离散元件(视网膜母细胞瘤控制元件;RCE)对于RB介导的转录控制是必需的。此前,我们已表明RCEs在体外与三种迄今未鉴定的核蛋白形成蛋白质-DNA复合物,并且其在c-fos RCE内的DNA结合位点发生突变会导致体内RCE依赖性转录的废除。在此,我们证明在体外与c-fos、c-myc和转化生长因子β1 RCEs结合的一种核蛋白是Sp-1,并且Sp-1在体内刺激RCE依赖性转录。此外,我们表明RB蛋白的瞬时共表达会刺激Sp-1介导的转录。我们从这些观察结果得出结论,RB可能部分凭借其与Sp-1功能相互作用的能力来调节转录。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/60e5/46280/4c8de8b8c453/pnas01467-0159-a.jpg

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