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果蝇中与Fos相关的AP-1蛋白是一种受发育调控的转录因子。

The Drosophila Fos-related AP-1 protein is a developmentally regulated transcription factor.

作者信息

Perkins K K, Admon A, Patel N, Tjian R

机构信息

Howard Hughes Medical Institute, Department of Molecular and Cell Biology, University of California, Berkeley 94720.

出版信息

Genes Dev. 1990 May;4(5):822-34. doi: 10.1101/gad.4.5.822.

Abstract

Drosophila AP-1 consists of two proteins (dFRA and dJRA) that have functional and structural properties in common with mammalian Fos and Jun proto-oncogene products. Here, we report the isolation and characterization of cDNAs encoding the full-length dFRA and dJRA proteins. The predicted amino acid sequences reveal that both proteins contain a bipartite DNA-binding domain consisting of a leucine repeat and an adjacent basic region, which are characteristic of members of the AP-1 family. By using protein translated in vitro or expressed in Escherichia coli, we demonstrate that dFRA, in contrast to the mammalian cFos proteins, recognizes the AP-1 site on its own and activates transcription in vitro in the absence of dJRA or Jun. Heteromeric complexes formed between dFRA and dJRA bind the AP-1 site better than either protein alone, and the two proteins activate transcription synergistically in vitro. In the developing embryo, dFRA mRNA is first expressed in a limited set of cells in the head and is later restricted to a subset of peripheral neurons, several epidermal cells near the muscle attachment sites, and a portion of the gut. In contrast, dJRA appears to be uniformly expressed at a low level in all cell types. These results indicate that dFRA is a developmentally regulated transcription factor and suggest that its potential interplay with dJRA plays an important role in cell-type-specific transcription during Drosophila embryonic development.

摘要

果蝇AP-1由两种蛋白质(dFRA和dJRA)组成,它们在功能和结构特性上与哺乳动物的Fos和Jun原癌基因产物有共同之处。在此,我们报告了编码全长dFRA和dJRA蛋白的cDNA的分离和特性分析。预测的氨基酸序列显示,这两种蛋白质都含有一个由亮氨酸重复序列和相邻碱性区域组成的双分型DNA结合结构域,这是AP-1家族成员的特征。通过使用体外翻译或在大肠杆菌中表达的蛋白质,我们证明,与哺乳动物的cFos蛋白不同,dFRA自身就能识别AP-1位点,并在没有dJRA或Jun的情况下在体外激活转录。dFRA和dJRA之间形成的异源复合物比单独的任何一种蛋白质都能更好地结合AP-1位点,并且这两种蛋白质在体外协同激活转录。在发育中的胚胎中,dFRA mRNA首先在头部的一组有限的细胞中表达,随后局限于外周神经元的一个子集、肌肉附着部位附近的几个表皮细胞以及肠道的一部分。相比之下,dJRA似乎在所有细胞类型中都以低水平均匀表达。这些结果表明,dFRA是一种受发育调控的转录因子,并表明其与dJRA的潜在相互作用在果蝇胚胎发育过程中的细胞类型特异性转录中起重要作用。

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