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一个复合基因内沉默子结构域对骨特异性骨钙素基因表现出负向和正向转录调控:启动子和细胞类型需求。

A composite intragenic silencer domain exhibits negative and positive transcriptional control of the bone-specific osteocalcin gene: promoter and cell type requirements.

作者信息

Frenkel B, Montecino M, Stein J L, Lian J B, Stein G S

机构信息

Department of Cell Biology, University of Massachusetts Medical Center, Worcester 01655.

出版信息

Proc Natl Acad Sci U S A. 1994 Nov 8;91(23):10923-7. doi: 10.1073/pnas.91.23.10923.

Abstract

The osteocalcin (OC) silencer is a unique example of exonic sequences contributing to negative transcriptional control of mammalian gene expression. In this paper we demonstrate, using a reporter transfection assay, that multiple elements reside within the OC +24/+151 domain. Thirty-fold repression is mediated by the +49/+104 fragment, experimentally relocated 3' of the poly(A) signal. Deletion of either the +49/+54 protein-coding sequence or the +98/+104 intronic part of this fragment results in loss of repression activity, suggesting a bipartite organization of the +49/+104 silencer. Of particular interest, we have mapped an antisilencer activity to the ACCCTCTCT motif (+40/+48), found in silencers associated with several other genes. Extension of the +49/+104 silencer to include the +24/+48 and/or the +105/+151 sequences results in increased silencer activity up to 170-fold, suggesting the presence of additional silencer elements within these sequences. The activity of the silencer contained within the +24/+151 OC sequence is directed to the basal promoter and is not dependent on 5' distal enhancer elements, including those that mediate responsiveness of OC transcription to vitamin D. The OC silencer represses the heterologous thymidine kinase promoter and is operative in osseous (normal diploid osteoblasts, ROS 17/2.8 osteosarcoma) as well as HeLa cells. Our results, which suggest the presence of at least five regulatory elements downstream of the OC transcription start site, indicate the complexity of sequences that mediate repression of OC promoter activity.

摘要

骨钙素(OC)沉默子是外显子序列对哺乳动物基因表达负转录调控起作用的一个独特例子。在本文中,我们通过报告基因转染实验证明,多个元件存在于OC +24/+151结构域内。由+49/+104片段介导30倍的抑制作用,该片段经实验重新定位到多聚腺苷酸信号的3'端。删除该片段的+49/+54蛋白质编码序列或+98/+104内含子部分会导致抑制活性丧失,这表明+49/+104沉默子具有二分结构。特别值得关注的是,我们已将一种抗沉默子活性定位到ACCCTCTCT基序(+40/+48),该基序存在于与其他几个基因相关的沉默子中。将+49/+104沉默子扩展到包括+24/+48和/或+105/+151序列会使沉默子活性增加至170倍,这表明这些序列中存在额外的沉默子元件。+24/+151 OC序列内所含沉默子的活性作用于基础启动子,且不依赖于5'端远端增强子元件,包括那些介导OC转录对维生素D反应性的元件。OC沉默子可抑制异源胸苷激酶启动子,并且在骨细胞(正常二倍体成骨细胞、ROS 17/2.8骨肉瘤)以及HeLa细胞中均有作用。我们的结果表明在OC转录起始位点下游至少存在五个调控元件,这表明介导OC启动子活性抑制的序列具有复杂性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/54b8/45138/c022dcedbf99/pnas01145-0176-a.jpg

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