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结构转录因子LEF-1使DNA弯曲的结构基础。

Structural basis for DNA bending by the architectural transcription factor LEF-1.

作者信息

Love J J, Li X, Case D A, Giese K, Grosschedl R, Wright P E

机构信息

Department of Molecular Biology, Scripps Research Institute, La Jolla, California 92037, USA.

出版信息

Nature. 1995 Aug 31;376(6543):791-5. doi: 10.1038/376791a0.

Abstract

Lymphoid enhancer-binding factor (LEF-1) and the closely related T-cell factor 1 (TCF-1) are sequence-specific and cell-type-specific DNA-binding proteins that play important regulatory roles in organogenesis and thymocyte differentiation. LEF-1 participates in regulation of the enhancer associated with the T cell receptor (TCR)-alpha gene by inducing a sharp bend in the DNA and facilitating interactions between Ets-1, PEBP2-alpha, and ATF/CREB, transcription factors bound at sites flanking the LEF-1 site. It seems that LEF-1 plays an architectural role in the assembly and function of this regulatory nucleoprotein complex. LEF-1 recognizes a specific nucleotide sequence through a high-mobility-group (HMG) domain. Proteins containing HMG domains bind DNA in the minor groove, bend the double helix, and recognize four-way junctions and other irregular DNA structures. Here we report the solution structure of a complex of the LEF-1 HMG domain and adjacent basic region with its cognate DNA. The structure reveals the HMG domain bound in the widened minor groove of a markedly distorted and bent double helix. The basic region binds across the narrowed major groove and contributes to DNA recognition.

摘要

淋巴样增强子结合因子(LEF-1)和密切相关的T细胞因子1(TCF-1)是序列特异性和细胞类型特异性的DNA结合蛋白,在器官发生和胸腺细胞分化中发挥重要的调节作用。LEF-1通过诱导DNA产生急剧弯曲并促进Ets-1、PEBP2-α和ATF/CREB(这些转录因子结合在LEF-1位点两侧的位点上)之间的相互作用,参与对与T细胞受体(TCR)-α基因相关的增强子的调控。看来LEF-1在这种调节性核蛋白复合物的组装和功能中起构建作用。LEF-1通过一个高迁移率族(HMG)结构域识别特定的核苷酸序列。含有HMG结构域的蛋白质在小沟中结合DNA,使双螺旋弯曲,并识别四向接头和其他不规则的DNA结构。在此我们报道了LEF-1的HMG结构域和相邻碱性区域与其同源DNA形成的复合物的溶液结构。该结构显示HMG结构域结合在明显扭曲和弯曲的双螺旋的变宽小沟中。碱性区域跨狭窄的大沟结合并有助于DNA识别。

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