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孤儿受体Rev-ErbAα通过一种新型反应元件激活转录。

The orphan receptor Rev-ErbA alpha activates transcription via a novel response element.

作者信息

Harding H P, Lazar M A

机构信息

Department of Medicine, University of Pennsylvania School of Medicine, Philadelphia 19104.

出版信息

Mol Cell Biol. 1993 May;13(5):3113-21. doi: 10.1128/mcb.13.5.3113-3121.1993.

Abstract

Rev-ErbA alpha (Rev-Erb) is a nuclear hormone receptor-related protein encoded on the opposite strand of the alpha-thyroid hormone receptor (TR) gene. This unusual genomic arrangement may have a regulatory role, but the conservation of human and rodent Rev-Erb amino acid sequences suggests that the protein itself has an important function, potentially as a sequence-specific transcriptional regulator. However, despite its relationship to the TR, Rev-Erb bound poorly to TR binding sites. To determine its DNA-binding specificity in an unbiased manner, Rev-Erb was synthesized in Escherichia coli, purified, and used to select specific binding-sites from libraries of random double-stranded DNA sequences. We found that Rev-Erb binds to a unique site consisting of a specific 5-bp A/T-rich sequence adjacent to a TR half-site. Rev-Erb contacts this entire asymmetric 11-bp sequence, which is the longest nonrepetitive element specifically recognized by a member of the thyroid/steroid hormone receptor superfamily, and mutations in either the A/T-rich or TR half-site regions abolished specific binding. The binding specificity of wild-type Rev-Erb was nearly identical to that of C- and N-terminally truncated forms. This binding was not enhanced by retinoid X receptor, TR, or other nuclear proteins, none of which formed heterodimers with Rev-Erb. Rev-Erb also appeared to bind to the selected site as a monomer. Furthermore, Rev-Erb activates transcription through this binding site even in the absence of exogenous ligand. Thus, Rev-Erb is a transcriptional activator whose properties differ dramatically from those of classical nuclear hormone receptors, including the TR encoded on the opposite strand of the same genomic locus.

摘要

Rev-ErbAα(Rev-Erb)是一种与核激素受体相关的蛋白质,由α-甲状腺激素受体(TR)基因的反义链编码。这种不同寻常的基因组排列可能具有调节作用,但人类和啮齿动物Rev-Erb氨基酸序列的保守性表明,该蛋白质本身具有重要功能,可能作为一种序列特异性转录调节因子。然而,尽管Rev-Erb与TR有关系,但它与TR结合位点的结合能力较差。为了以无偏见的方式确定其DNA结合特异性,在大肠杆菌中合成、纯化Rev-Erb,并用于从随机双链DNA序列文库中选择特异性结合位点。我们发现Rev-Erb与一个独特的位点结合,该位点由与TR半位点相邻的特定5个碱基的富含A/T序列组成。Rev-Erb与这个完整的不对称11个碱基序列接触,这是甲状腺/类固醇激素受体超家族成员特异性识别的最长非重复元件,富含A/T或TR半位点区域的突变会消除特异性结合。野生型Rev-Erb的结合特异性与C端和N端截短形式的几乎相同。类视黄醇X受体、TR或其他核蛋白均未增强这种结合,它们均未与Rev-Erb形成异二聚体。Rev-Erb似乎也以单体形式与所选位点结合。此外,即使在没有外源配体的情况下,Rev-Erb也通过该结合位点激活转录。因此,Rev-Erb是一种转录激活因子,其特性与经典核激素受体有很大不同,包括同一基因组位点反义链上编码的TR。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/98db/359704/70ffe00e64ed/molcellb00017-0489-a.jpg

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