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首页> 外文期刊>Journal of Molecular Biology >REFINED CRYSTAL STRUCTURE OF RECOMBINANT MURINE INTERFERON-BETA AT 2.15 ANGSTROM RESOLUTION
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REFINED CRYSTAL STRUCTURE OF RECOMBINANT MURINE INTERFERON-BETA AT 2.15 ANGSTROM RESOLUTION

机译:在2.15埃分辨率下重组鼠干扰素-BET的精细晶体结构

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The crystal structure of recombinant murine interferon-beta (reMuIFN-beta) has been refined at 2.15 Angstrom resolution using newly collected synchrotron data. Based on 11,228 reflections (8.0 to 2.15 Angstrom), a final R-factor of 19.1% (with a free R-factor of 25.8%) was obtained with a model obeying standard geometry within 0.013 Angstrom in bond lengths and 1.4 degrees in bond angles. Compared with the previously reported model, several amino acid residues in helix A are frame-shifted, the conformations are changed for parts of loops AB and BC, helix C is extended and a new short helix exists in loop CD. Evolutionary considerations taken together, the type I interferons appear to share common structural features with respect to the chain-folding topology and the hydrogen-bond networks between various polypeptide segments. Specifically, the disposition of the C-terminal segment of loop AB (after Arg33), known to be an important receptor-binding site, seems to be strictly maintained among the type I interferons. The exposed amino acid residues on helices A and C, which have recently been implicated as the binding site for another receptor molecule, are less well conserved. This may be responsible for varied cellular effects among the subtypes of type I interferons. (C) 1995 Academic Press Limited [References: 70]
机译:重组鼠干扰素-β(reMuIFN-β)的晶体结构已使用新收集的同步加速器数据以2.15埃的分辨率精制。基于11,228个反射(8.0至2.15埃),最终模型的模型遵循标准几何尺寸,键长为0.013埃,键角为1.4度,最终R因子为19.1%(自由R因子为25.8%)。 。与先前报道的模型相比,螺旋A中的几个氨基酸残基发生了移码,环AB和BC部分的构象发生了变化,螺旋C扩展了,在环CD中存在一个新的短螺旋。综合考虑进化因素,I型干扰素似乎在各种多肽片段之间的链折叠拓扑和氢键网络方面具有共同的结构特征。具体地,在I型干扰素中似乎严格维持已知为重要受体结合位点的环AB的C末端区段(在Arg33之后)的布置。螺旋A和C上暴露的氨基酸残基保守性较差,最近被暗示为另一个受体分子的结合位点。这可能是导致I型干扰素亚型中各种细胞效应的原因。 (C)1995 Academic Press Limited [参考号:70]

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