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杜氏疏螺旋体嗜神经相关可变表面蛋白1(Vsp1)的晶体结构

Crystal structure of neurotropism-associated variable surface protein 1 (Vsp1) of Borrelia turicatae.

作者信息

Lawson Catherine L, Yung Brian H, Barbour Alan G, Zückert Wolfram R

机构信息

Department of Chemistry and Chemical Biology, 610 Taylor Road, Piscataway, NJ 08854, USA.

出版信息

J Bacteriol. 2006 Jun;188(12):4522-30. doi: 10.1128/JB.00028-06.

Abstract

Vsp surface lipoproteins are serotype-defining antigens of relapsing fever spirochetes that undergo multiphasic antigenic variation to allow bacterial persistence in spite of an immune response. Two isogenic serotypes of Borrelia turicatae strain Oz1 differ in their Vsp sequences and in disease manifestations in infected mice: Vsp1 is associated with the selection of a neurological niche, while Vsp2 is associated with blood and skin infection. We report here crystal structures of the Vsp1 dimer at 2.7 and 2.2 A. The structures confirm that relapsing fever Vsp proteins share a common helical fold with OspCs of Lyme disease-causing Borrelia. The fold features an inner stem formed by highly conserved N and C termini and an outer "dome" formed by the variable central residues. Both Vsp1 and OspC structures possess small water-filled cavities, or pockets, that are lined largely by variable residues and are thus highly variable in shape. These features appear to signify tolerance of the Vsp-OspC fold for imperfect packing of residues at its antigenic surface. Structural comparison of Vsp1 with a homology model for Vsp2 suggests that observed differences in disease manifestation may arise in part from distinct differences in electrostatic surface properties; additional predicted positively charged surface patches on Vsp2 compared to Vsp1 may be sufficient to explain the relative propensity of Vsp2 to bind to acidic glycosaminoglycans.

摘要

Vsp表面脂蛋白是回归热螺旋体的血清型定义抗原,其经历多相抗原变异以允许细菌在免疫反应存在的情况下持续存在。图里螺旋体菌株Oz1的两种同基因血清型在Vsp序列和感染小鼠的疾病表现上有所不同:Vsp1与神经龛的选择相关,而Vsp2与血液和皮肤感染相关。我们在此报告了Vsp1二聚体在2.7埃和2.2埃分辨率下的晶体结构。这些结构证实回归热Vsp蛋白与引起莱姆病的疏螺旋体的OspC蛋白具有共同的螺旋折叠。该折叠特征是由高度保守的N端和C端形成的内部茎以及由可变的中央残基形成的外部“穹顶”。Vsp1和OspC结构都具有小的充满水的腔或口袋,这些腔或口袋主要由可变残基排列,因此形状高度可变。这些特征似乎表明Vsp - OspC折叠对其抗原表面残基不完美堆积具有耐受性。Vsp1与Vsp2同源模型的结构比较表明,观察到的疾病表现差异可能部分源于静电表面性质的明显差异;与Vsp1相比,Vsp2上额外预测的带正电表面斑块可能足以解释Vsp2与酸性糖胺聚糖结合的相对倾向。

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