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质型多角体病毒多角体的分子结构

The molecular organization of cypovirus polyhedra.

作者信息

Coulibaly Fasséli, Chiu Elaine, Ikeda Keiko, Gutmann Sascha, Haebel Peter W, Schulze-Briese Clemens, Mori Hajime, Metcalf Peter

机构信息

School of Biological Sciences, University of Auckland, 1010, New Zealand.

出版信息

Nature. 2007 Mar 1;446(7131):97-101. doi: 10.1038/nature05628.

DOI:10.1038/nature05628
PMID:17330045
Abstract

Cypoviruses and baculoviruses are notoriously difficult to eradicate because the virus particles are embedded in micrometre-sized protein crystals called polyhedra. The remarkable stability of polyhedra means that, like bacterial spores, these insect viruses remain infectious for years in soil. The environmental persistence of polyhedra is the cause of significant losses in silkworm cocoon harvests but has also been exploited against pests in biological alternatives to chemical insecticides. Although polyhedra have been extensively characterized since the early 1900s, their atomic organization remains elusive. Here we describe the 2 A crystal structure of both recombinant and infectious silkworm cypovirus polyhedra determined using crystals 5-12 micrometres in diameter purified from insect cells. These are the smallest crystals yet used for de novo X-ray protein structure determination. We found that polyhedra are made of trimers of the viral polyhedrin protein and contain nucleotides. Although the shape of these building blocks is reminiscent of some capsid trimers, polyhedrin has a new fold and has evolved to assemble in vivo into three-dimensional cubic crystals rather than icosahedral shells. The polyhedrin trimers are extensively cross-linked in polyhedra by non-covalent interactions and pack with an exquisite molecular complementarity similar to that of antigen-antibody complexes. The resulting ultrastable and sealed crystals shield the virus particles from environmental damage. The structure suggests that polyhedra can serve as the basis for the development of robust and versatile nanoparticles for biotechnological applications such as microarrays and biopesticides.

摘要

质型多角体病毒和杆状病毒极难根除,因为病毒粒子包埋在称为多角体的微米级蛋白质晶体中。多角体具有非凡的稳定性,这意味着这些昆虫病毒如同细菌芽孢一样,能在土壤中保持数年的传染性。多角体在环境中的持久性是家蚕茧产量大幅损失的原因,但它也被用于生物杀虫剂中对抗害虫,以替代化学杀虫剂。尽管自20世纪初以来多角体就已得到广泛研究,但其原子结构仍然未知。在此,我们描述了从昆虫细胞中纯化得到的直径为5 - 12微米的重组型和感染性家蚕质型多角体病毒多角体的2 Å晶体结构。这些是迄今用于从头测定X射线蛋白质结构的最小晶体。我们发现多角体由病毒多角体蛋白的三聚体组成,并含有核苷酸。尽管这些结构单元的形状让人联想到一些衣壳三聚体,但多角体蛋白具有一种新的折叠方式,并且已进化为在体内组装成三维立方晶体而非二十面体外壳。多角体蛋白三聚体在多角体中通过非共价相互作用广泛交联,其堆积方式具有与抗原 - 抗体复合物相似的精妙分子互补性。由此形成的超稳定且密封的晶体可保护病毒粒子免受环境破坏。该结构表明,多角体可作为开发用于生物技术应用(如微阵列和生物杀虫剂)的坚固且通用的纳米颗粒的基础。

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