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鉴定变形表皮自调节因子-1(DEAF-1)中的核输出信号和蛋白质相互作用结构域。

Identification of a nuclear export signal and protein interaction domains in deformed epidermal autoregulatory factor-1 (DEAF-1).

作者信息

Jensik Philip J, Huggenvik Jodi I, Collard Michael W

机构信息

Department of Physiology, Southern Illinois University School of Medicine, Carbondale, Illinois 62901, USA.

出版信息

J Biol Chem. 2004 Jul 30;279(31):32692-9. doi: 10.1074/jbc.M400946200. Epub 2004 May 25.

DOI:10.1074/jbc.M400946200
PMID:15161925
Abstract

Deformed epidermal autoregulatory factor-1 (DEAF-1) is a DNA-binding protein required for embryonic development and linked to clinical depression and suicidal behavior in humans. Although primarily nuclear, cytoplasmic localization of DEAF-1 has been observed, and this suggests the presence of a nuclear export signal (NES). Using a series of fluorescent fusion proteins, an NES with a novel spacing of leucines (LXLX(6)LLX(5)LX(2)L) was identified near the COOH-terminal MYND domain at amino acids 454-476. The NES was leptomycin B-sensitive and mutation of the leucine residues decreased or eliminated nuclear export activity. In vitro pull downs and an in vivo fluorescent protein interaction assay identified a DEAF-1/DEAF-1 protein interaction domain within the NES region. DNA binding had been previously mapped to a positively charged surface patch in the novel DNA binding fold called the "SAND" domain. A second protein-protein interaction domain was identified at amino acids 243-306 that contains the DNA-binding SAND domain and also an adjacent zinc binding motif and a monopartite nuclear localization signal (NLS). Deletion of these adjacent sequences or mutation of the conserved cysteines or histidine in the zinc binding motif not only inhibits protein interaction but also eliminates DNA binding, demonstrating that DEAF-1 protein-protein interaction is required for DNA recognition. The identification of an NES and NLS provides a basis for the control of DEAF-1 subcellular localization and function, whereas the requirement of protein-protein interaction by the SAND domain appears to be unique among this class of transcription factors.

摘要

畸形表皮自调节因子1(DEAF-1)是一种胚胎发育所必需的DNA结合蛋白,与人类临床抑郁症和自杀行为有关。尽管DEAF-1主要定位于细胞核,但也观察到其存在于细胞质中,这表明存在核输出信号(NES)。通过一系列荧光融合蛋白,在氨基酸454 - 476的COOH末端MYND结构域附近鉴定出一个具有新型亮氨酸间隔(LXLX(6)LLX(5)LX(2)L)的NES。该NES对雷帕霉素B敏感,亮氨酸残基的突变会降低或消除核输出活性。体外下拉实验和体内荧光蛋白相互作用分析在NES区域内鉴定出一个DEAF-1/DEAF-1蛋白相互作用结构域。DNA结合先前已定位到名为“SAND”结构域的新型DNA结合折叠中的一个带正电荷的表面区域。在氨基酸243 - 306处鉴定出第二个蛋白 - 蛋白相互作用结构域,其包含DNA结合SAND结构域以及相邻的锌结合基序和一个单部分核定位信号(NLS)。这些相邻序列的缺失或锌结合基序中保守的半胱氨酸或组氨酸的突变不仅会抑制蛋白相互作用,还会消除DNA结合,表明DEAF-1蛋白 - 蛋白相互作用是DNA识别所必需的。NES和NLS的鉴定为控制DEAF-1亚细胞定位和功能提供了基础,而SAND结构域对蛋白 - 蛋白相互作用的需求在这类转录因子中似乎是独特的。

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