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一种与p65协同刺激HIV转录的核因子-κB亚基的克隆。

Cloning of an NF-kappa B subunit which stimulates HIV transcription in synergy with p65.

作者信息

Schmid R M, Perkins N D, Duckett C S, Andrews P C, Nabel G J

机构信息

Howard Hughes Medical Institute, Department of Internal Medicine, University of Michigan Medical Center, Ann Arbor 48109-0650.

出版信息

Nature. 1991 Aug 22;352(6337):733-6. doi: 10.1038/352733a0.

DOI:10.1038/352733a0
PMID:1876189
Abstract

The transcription factor NF-kappa B is a protein complex which comprises a DNA-binding subunit and an associated transactivation protein (of relative molecular masses 50,000 (50K) and 65K, respectively). Both the 50K and 65K subunits have similarity with the rel oncogene and the Drosophila maternal effect gene dorsal. The 50K DNA-binding subunit was previously thought to be a unique protein, derived from the 105K gene product (p105). We now report the isolation of a complementary DNA that encodes an alternative DNA-binding subunit of NF-kappa B. It is more similar to p105 NF-kappa B than other family members and defines a new subset of rel-related genes. It is synthesized as approximately 100K protein (p100) that is expressed in different cell types, contains cell cycle motifs and, like p105, must be processed to generate a 50K form. A 49K product (p49) can be generated independently from an alternatively spliced transcript; it has specific kappa B DNA-binding activity and can form heterodimers with other rel proteins. In contrast to the approximately 50K protein derived from p105, p49 acts in synergy with p65 to stimulate the human immunodeficiency virus (HIV) enhancer in transiently transfected Jurkat cells. p49/p100 NF-kappa B could therefore be important in the regulation of HIV and other kappa B-containing genes.

摘要

转录因子核因子-κB是一种蛋白质复合物,它由一个DNA结合亚基和一个相关的反式激活蛋白(相对分子质量分别为50,000(50K)和65K)组成。50K和65K亚基都与rel癌基因和果蝇母体效应基因背侧蛋白有相似性。50K DNA结合亚基以前被认为是一种独特的蛋白质,源自105K基因产物(p105)。我们现在报告分离出一种互补DNA,它编码核因子-κB的另一种DNA结合亚基。它比其他家族成员更类似于p105核因子-κB,并定义了rel相关基因的一个新子集。它以大约100K蛋白质(p100)的形式合成,在不同细胞类型中表达,包含细胞周期基序,并且像p105一样,必须经过加工才能产生50K形式。一种49K产物(p49)可以从一个选择性剪接的转录本独立产生;它具有特异性的κB DNA结合活性,并且可以与其他rel蛋白形成异源二聚体。与源自p105的大约50K蛋白质不同,p49与p65协同作用,在瞬时转染的Jurkat细胞中刺激人类免疫缺陷病毒(HIV)增强子。因此,p49/p100核因子-κB在HIV和其他含κB基因的调控中可能很重要。

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