首页> 美国卫生研究院文献>Acta Crystallographica Section F: Structural Biology and Crystallization Communications >The structure at 2.5 Å resolution of human basophilic leukemia-expressed protein BLES03
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The structure at 2.5 Å resolution of human basophilic leukemia-expressed protein BLES03

机译:人嗜碱性粒细胞白血病蛋白BLES03的分辨率为2.5Å的结构

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摘要

The crystal structure of the human basophilic leukemia-expressed protein (BLES03, p5326, Hs.433573) was determined by single-wavelength anomalous diffraction and refined to an R factor of 18.8% (R free = 24.5%) at 2.5 Å resolution. BLES03 shows no detectable sequence similarity to any functionally characterized proteins using state-of-the-art sequence-comparison tools. The structure of BLES03 adopts a fold similar to that of eukaryotic transcription initiation factor 4E (eIF4E), a protein involved in the recognition of the cap structure of eukaryotic mRNA. In addition to fold similarity, the electrostatic surface potentials of BLES03 and eIF4E show a clear conservation of basic and acidic patches. In the crystal lattice, the acidic amino-terminal helices of BLES03 monomers are bound within the basic cavity of symmetry-related monomers in a manner analogous to the binding of mRNA by eIF4E. Interestingly, the gene locus encoding BLES03 is located between genes encoding the proteins DRAP1 and FOSL1, both of which are involved in transcription initiation. It is hypothesized that BLES03 itself may be involved in a biochemical process that requires recognition of nucleic acids.
机译:通过单波长反常衍射测定人类嗜碱性粒细胞白血病表达蛋白(BLES03,p5326,Hs.433573)的晶体结构,并以2.5Å的分辨率将其精制到R因子为18.8%(R free = 24.5%)。使用最新的序列比较工具,BLES03与任何功能表征的蛋白质均无可检测的序列相似性。 BLES03的结构具有与真核转录起始因子4E(eIF4E)类似的折叠,真核转录起始因子4E(eIF4E)是参与识别真核mRNA帽结构的蛋白质。除了折叠相似性之外,BLES03和eIF4E的静电表面电势还显示出碱性和酸性补丁的明显保守性。在晶格中,BLES03单体的酸性氨基末端螺旋以类似于eIF4E与mRNA结合的方式结合在对称相关单体的基本腔内。有趣的是,编码BLES03的基因座位于编码蛋白质DRAP1和FOSL1的基因之间,二者均参与转录起始。假设BLES03本身可能参与需要识别核酸的生化过程。

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