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NRC-Interacting Factor 1 Is a Novel Cotransducer That Interacts with and Regulates the Activity of the Nuclear Hormone Receptor Coactivator NRC

机译:NRC相互作用因子1是一种新型的共转导物可与核激素受体共激活物NRC相互作用并调节其活性。

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摘要

We previously reported the cloning and characterization of a novel nuclear hormone receptor transcriptional coactivator, which we refer to as NRC. NRC is a 2,063-amino-acid nuclear protein which contains a potent N-terminal activation domain and several C-terminal modules which interact with CBP and ligand-bound nuclear hormone receptors as well as c-Fos and c-Jun. In this study we sought to clone and identify novel factors that interact with NRC to modulate its transcriptional activity. Here we describe the cloning and characterization of a novel protein we refer to as NIF-1 (NRC-interacting factor 1). NIF-1 was cloned from rat pituitary and human cell lines and was found to interact in vivo and in vitro with NRC. NIF-1 is a 1,342-amino-acid nuclear protein containing a number of conserved domains, including six Cys-2/His-2 zinc fingers, an N-terminal stretch of acidic amino acids, and a C-terminal leucine zipper-like motif. Zinc fingers 1 to 3 are potential DNA-binding BED finger domains recently proposed to play a role in altering local chromatin architecture. We mapped the interaction domains of NRC and NIF-1. Although NIF-1 does not directly interact with nuclear receptors, it markedly enhances ligand-dependent transcriptional activation by nuclear hormone receptors in vivo as well as activation by c-Fos and c-Jun. These results, and the finding that NIF-1 interacts with NRC in vivo, suggest that NIF-1 functions to regulate transcriptional activation through NRC. We suggest that NIF-1, and factors which associate with coactivators but not receptors, be referred to as cotransducers, which act in vivo either as part of a coactivator complex or downstream of a coactivator complex to modulate transcriptional activity. Our findings suggest that NIF-1 may be a functional component of an NRC complex and acts as a regulator or cotransducer of NRC function.
机译:我们以前报道了一种新型核激素受体转录共激活剂的克隆和表征,我们将其称为NRC。 NRC是一个2063个氨基酸的核蛋白,包含一个有效的N端激活结构域和几个C端模块,这些模块与CBP和配体结合的核激素受体以及c-Fos和c-Jun相互作用。在这项研究中,我们试图克隆和鉴定与NRC相互作用以调节其转录活性的新因子。在这里,我们描述了一种称为NIF-1(NRC相互作用因子1)的新型蛋白质的克隆和表征。 NIF-1是从大鼠垂体和人类细胞系克隆而来的,发现它在体内和体外均与NRC相互作用。 NIF-1是一个1,342个氨基酸的核蛋白,包含多个保守域,包括六个Cys-2 / His-2锌指,一个酸性氨基酸的N端延伸序列和一个C末端的亮氨酸拉链样主题。锌指1至3是最近被提议在改变局部染色质结构中起作用的潜在的DNA结合BED指结构域。我们绘制了NRC和NIF-1的相互作用域。尽管NIF-1不直接与核受体相互作用,但它显着增强了体内核激素受体的配体依赖性转录激活以及c-Fos和c-Jun的激活。这些结果以及NIF-1在体内与NRC相互作用的发现表明,NIF-1的功能是通过NRC调节转录激活。我们建议将NIF-1和与共激活因子而不是受体相关的因子称为共转导子,它们在体内作为共激活因子复合物的一部分或在共激活复合物的下游调节转录活性。我们的发现表明,NIF-1可能是NRC复合体的功能组件,并充当NRC功能的调节剂或共转导剂。

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