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通过使用可变形弹性网络方法进行新的优化所揭示的穹窿结构和动力学的新特征。

New features of vault architecture and dynamics revealed by novel refinement using the deformable elastic network approach.

作者信息

Casañas Arnau, Querol-Audí Jordi, Guerra Pablo, Pous Joan, Tanaka Hideaki, Tsukihara Tomitake, Verdaguer Nuria, Fita Ignasi

机构信息

Institut de Biologia Molecular de Barcelona (CSIC), Parc Científic de Barcelona, Baldiri i Reixac 10, 08028 Barcelona, Spain.

出版信息

Acta Crystallogr D Biol Crystallogr. 2013 Jun;69(Pt 6):1054-61. doi: 10.1107/S0907444913004472. Epub 2013 May 14.

DOI:10.1107/S0907444913004472
PMID:23695250
Abstract

The vault particle, with a molecular weight of about 10 MDa, is the largest ribonucleoprotein that has been described. The X-ray structure of intact rat vault has been solved at a resolution of 3.5 Å [Tanaka et al. (2009), Science, 323, 384-388], showing an overall barrel-shaped architecture organized into two identical moieties, each consisting of 39 copies of the major vault protein (MVP). The model deposited in the PDB includes 39 MVP copies (half a vault) in the crystal asymmetric unit. A 2.1 Å resolution structure of the seven N-terminal repeats (R1-7) of MVP has also been determined [Querol-Audí et al. (2009), EMBO J. 28, 3450-3457], revealing important discrepancies with respect to the MVP models for repeats R1 and R2. Here, the re-refinement of the vault structure by incorporating the high-resolution information available for the R1-7 domains, using the deformable elastic network (DEN) approach and maintaining strict 39-fold noncrystallographic symmetry is reported. The new refinement indicates that at the resolution presently available the MVP shell can be described well as only one independent subunit organized with perfect D39 molecular symmetry. This refinement reveals that significant rearrangements occur in the N-terminus of MVP during the closing of the two vault halves and that the 39-fold symmetry breaks in the cap region. These results reflect the highly dynamic nature of the vault structure and represent a necessary step towards a better understanding of the biology and regulation of this particle.

摘要

穹窿体颗粒分子量约为10 MDa,是已被描述的最大核糖核蛋白。完整大鼠穹窿体的X射线结构已在3.5 Å分辨率下解析出来[田中等人(2009年),《科学》,323卷,384 - 388页],显示出整体桶状结构,由两个相同部分组成,每个部分由39个主要穹窿体蛋白(MVP)拷贝组成。存入蛋白质数据库(PDB)的模型在晶体不对称单元中包含39个MVP拷贝(半个穹窿体)。MVP七个N端重复序列(R1 - 7)的2.1 Å分辨率结构也已确定[克勒尔 - 奥迪等人(2009年),《欧洲分子生物学组织杂志》,28卷,3450 - 3457页],揭示了与R1和R2重复序列的MVP模型存在重要差异。在此,报告了通过采用可变形弹性网络(DEN)方法并保持严格的39重非晶体学对称性,结合R1 - 7结构域的高分辨率信息对穹窿体结构进行重新精修。新的精修表明,在目前可用的分辨率下,MVP外壳可以很好地描述为仅由一个具有完美D39分子对称性的独立亚基组成。这种精修揭示了在两个穹窿体半部闭合过程中,MVP的N端发生了显著重排,并且在帽区39重对称性被打破。这些结果反映了穹窿体结构的高度动态性质,是朝着更好地理解该颗粒的生物学特性和调控迈出的必要一步。

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