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RFX1的二聚化/抑制结构域与其酵母同源物Crt1和Sak1的一个保守区域相关:一种古老基序的新功能。

The dimerization/repression domain of RFX1 is related to a conserved region of its yeast homologues Crt1 and Sak1: a new function for an ancient motif.

作者信息

Katan-Khaykovich Y, Spiegel I, Shaul Y

机构信息

Department of Molecular Genetics, The Weizmann Institute of Science, Rehovot, 76100, Israel.

出版信息

J Mol Biol. 1999 Nov 19;294(1):121-37. doi: 10.1006/jmbi.1999.3245.

Abstract

The RFX protein family includes members from yeast to humans, which function in various biological systems, and share a DNA-binding domain and a conserved C-terminal region. In the human transcription regulator RFX1, the conserved C terminus is an independent functional domain, which mediates dimerization and transcriptional repression. This dimerization domain has a unique ability to mediate the formation of two alternative homodimeric DNA-protein complexes, the upper of which has been linked to repression. Here, we localize the complex formation capacity to several different RFX1 C-terminal subregions, each of which can function independently to generate the upper complex and repress transcription, thus correlating complex formation with repression. To gain an evolutionary perspective, we have examined whether the different properties of the RFX1 C terminus exist in the two yeast RFX proteins, which are involved in signaling pathways. Replacement of the RFX1 C terminus with those of Sak1 and Crt1, its orthologues from Schizosaccharomyces pombe and Saccharomyces cerevisiae, respectively, and analysis of fusions with the Gal4 DNA-binding domain, revealed that the ability to generate the two alternative complexes is conserved in the RFX family, from S. cerevisiae to man. While sharing this unique biochemical property, the three C termini differed from each other in their ability to mediate dimerization and transcriptional repression. In both functions, RFX1, Sak1, and Crt1 showed high capacity, moderate capacity, and no capacity, respectively. This comparative analysis of the RFX proteins, representing different evolutionary stages, suggests a gradual development of the conserved C terminus, from the appearance of the ancestral motif (Crt1), to the later acquisition of the dimerization/repression functions (Sak1), and finally to the enhancement of these functions to generate a domain mediating highly stable protein-protein interactions and potent transcriptional repression (RFX1).

摘要

RFX蛋白家族包括从酵母到人类的成员,它们在各种生物系统中发挥作用,并共享一个DNA结合结构域和一个保守的C末端区域。在人类转录调节因子RFX1中,保守的C末端是一个独立的功能结构域,它介导二聚化和转录抑制。这个二聚化结构域具有独特的能力,可介导形成两种不同的同型二聚体DNA-蛋白质复合物,其中上层复合物与抑制作用相关。在这里,我们将复合物形成能力定位到几个不同的RFX1 C末端亚区域,每个亚区域都可以独立发挥作用以产生上层复合物并抑制转录,从而将复合物形成与抑制作用联系起来。为了获得进化视角,我们研究了参与信号通路的两种酵母RFX蛋白中是否存在RFX1 C末端的不同特性。分别用粟酒裂殖酵母和酿酒酵母的直系同源物Sak1和Crt1的C末端替换RFX1的C末端,并分析与Gal4 DNA结合结构域的融合情况,结果表明,从酿酒酵母到人类,RFX家族中产生两种不同复合物的能力是保守的。虽然共享这种独特的生化特性,但这三个C末端在介导二聚化和转录抑制的能力上彼此不同。在这两种功能中,RFX1、Sak1和Crt1分别表现出高能力、中等能力和无能力。对代表不同进化阶段的RFX蛋白的这种比较分析表明,保守的C末端是逐渐发展的,从祖先基序(Crt1)的出现,到后来获得二聚化/抑制功能(Sak1),最后到这些功能的增强,以产生一个介导高度稳定的蛋白质-蛋白质相互作用和有效转录抑制的结构域(RFX1)。

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