首页> 外文期刊>Journal of Molecular Biology >Three-Dimensional Structure of the HTLV-II Matrix Protein and Comparative Analysis of Matrix Proteins from the Different Classes of Pathogenic Human Retroviruses
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Three-Dimensional Structure of the HTLV-II Matrix Protein and Comparative Analysis of Matrix Proteins from the Different Classes of Pathogenic Human Retroviruses

机译:HTLV-II基质蛋白的三维结构和不同类别致病性人类逆转录病毒基质蛋白的比较分析

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The matrix protein performs similar roles in all retroviruses, initially directing membrane localization of the assembling viral particle and subsequently forming a stable structural shell associated with the inner surface of the mature viral membrane. Although conserved structural elements are likely to perform these functions in all retroviral matrix proteins, invariant motifs are not evident at the primary sequence level and three-dimensional structures have been available for only the primate lentiviral matrix proteins. We have therefore used NMR spectroscopy to determine the structure of the matrix protein from human T-cell leukemia virus type II (HTLV-II), a member of the human oncovirus subclass of retroviruses. A total of 577 distance restraints were used to build 20 refined models that superimpose with an rmsd of 0.71 A for the backbone atoms of the structured regions. The globular HTLV-II matrix structure is composed of four alpha-helices and a 3_(10) helix. Exposed basic residues near the C terminus of helix II form a putative membrane binding surface which could act in concert with the N-terminal myristoyl group to anchor the protein on the viral membrane surface. Clear structural similarities between the HTLV-II and HIV-1 matrix proteins suggest that the topology and exposed cationic membrane binding surface are likely to be conserved features of retroviral matrix proteins.
机译:基质蛋白在所有逆转录病毒中起相似的作用,首先指导组装病毒颗粒的膜定位,然后形成与成熟病毒膜内表面相关的稳定结构壳。尽管保守的结构元件可能在所有逆转录病毒基质蛋白中都具有这些功能,但不变基序在一级序列水平上并不明显,三维结构仅可用于灵长类慢病毒基质蛋白。因此,我们已使用NMR光谱法确定了来自人类T细胞白血病病毒II型(HTLV-II)(逆转录病毒的人类癌病毒亚类的成员)的基质蛋白的结构。总共使用577个距离约束来构建20个精炼模型,它们对结构化区域的主链原子的均方根值为0.71A。球形HTLV-II矩阵结构由四个alpha螺旋和一个3_(10)螺旋组成。在螺旋II的C末端附近的暴露的碱性残基形成推定的膜结合表面,其可以与N-末端肉豆蔻酰基基团协同作用以将蛋白质锚定在病毒膜表面上。 HTLV-II和HIV-1基质蛋白之间清晰的结构相似性表明,拓扑结构和暴露的阳离子膜结合表面很可能是逆转录病毒基质蛋白的保守特征。

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