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当腺病毒纤维轴序列在N端与噬菌体T4纤维连接蛋白折叠三聚化基序融合时,会折叠成天然的三重β-螺旋折叠。

Adenovirus fibre shaft sequences fold into the native triple beta-spiral fold when N-terminally fused to the bacteriophage T4 fibritin foldon trimerisation motif.

作者信息

Papanikolopoulou Katerina, Teixeira Susana, Belrhali Hassan, Forsyth V Trevor, Mitraki Anna, van Raaij Mark J

机构信息

Institut de Biologie Structurale Jean-Pierre Ebel, 41 rue Jules Horowitz, F-38042 Grenoble, France.

出版信息

J Mol Biol. 2004 Sep 3;342(1):219-27. doi: 10.1016/j.jmb.2004.07.008.

DOI:10.1016/j.jmb.2004.07.008
PMID:15313619
Abstract

Adenovirus fibres are trimeric proteins that consist of a globular C-terminal domain, a central fibrous shaft and an N-terminal part that attaches to the viral capsid. In the presence of the globular C-terminal domain, which is necessary for correct trimerisation, the shaft segment adopts a triple beta-spiral conformation. We have replaced the head of the fibre by the trimerisation domain of the bacteriophage T4 fibritin, the foldon. Two different fusion constructs were made and crystallised, one with an eight amino acid residue linker and one with a linker of only two residues. X-ray crystallographic studies of both fusion proteins shows that residues 319-391 of the adenovirus type 2 fibre shaft fold into a triple beta-spiral fold indistinguishable from the native structure, although this is now resolved at a higher resolution of 1.9 A. The foldon residues 458-483 also adopt their natural structure. The intervening linkers are not well ordered in the crystal structures. This work shows that the shaft sequences retain their capacity to fold into their native beta-spiral fibrous fold when fused to a foreign C-terminal trimerisation motif. It provides a structural basis to artificially trimerise longer adenovirus shaft segments and segments from other trimeric beta-structured fibre proteins. Such artificial fibrous constructs, amenable to crystallisation and solution studies, can offer tractable model systems for the study of beta-fibrous structure. They can also prove useful for gene therapy and fibre engineering applications.

摘要

腺病毒纤维是三聚体蛋白,由球状C末端结构域、中央纤维状杆部和连接病毒衣壳的N末端部分组成。在球状C末端结构域存在的情况下(这对于正确的三聚化是必需的),杆部片段呈现出三股β-螺旋构象。我们用噬菌体T4纤维蛋白的三聚化结构域——折叠子,替换了纤维的头部。制备并结晶了两种不同的融合构建体,一种带有八个氨基酸残基的连接子,另一种带有仅两个残基的连接子。对这两种融合蛋白的X射线晶体学研究表明,2型腺病毒纤维杆部的319 - 391位残基折叠成与天然结构无法区分的三股β-螺旋折叠,尽管现在其分辨率提高到了1.9埃。折叠子的458 - 483位残基也呈现出它们的天然结构。中间的连接子在晶体结构中无序排列。这项工作表明,当与外源C末端三聚化基序融合时,杆部序列保留了折叠成其天然β-螺旋纤维折叠的能力。它为人工三聚化更长的腺病毒杆部片段以及其他三聚体β结构纤维蛋白的片段提供了结构基础。这种易于结晶和进行溶液研究的人工纤维构建体,可以为β-纤维结构的研究提供易于处理的模型系统。它们对于基因治疗和纤维工程应用也可能很有用。

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