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一种爬行动物腺病毒的结构揭示了一种稳定脊椎动物病毒衣壳的噬菌体尾刺折叠结构。

Structure of a Reptilian Adenovirus Reveals a Phage Tailspike Fold Stabilizing a Vertebrate Virus Capsid.

作者信息

Menéndez-Conejero Rosa, Nguyen Thanh H, Singh Abhimanyu K, Condezo Gabriela N, Marschang Rachel E, van Raaij Mark J, San Martín Carmen

机构信息

Departamento de Estructura de Macromoléculas, Centro Nacional de Biotecnología (CNB-CSIC), Darwin 3, 28049 Madrid, Spain.

Departamento de Estructura de Macromoléculas, Centro Nacional de Biotecnología (CNB-CSIC), Darwin 3, 28049 Madrid, Spain; Genetic Engineering Laboratory, Institute of Biotechnology (IBT-VAST), 18 Hoang Quoc Viet, Cau Giay, Hanoi, Vietnam.

出版信息

Structure. 2017 Oct 3;25(10):1562-1573.e5. doi: 10.1016/j.str.2017.08.007. Epub 2017 Sep 21.

Abstract

Although non-human adenoviruses (AdVs) might offer solutions to problems posed by human AdVs as therapeutic vectors, little is known about their basic biology. In particular, there are no structural studies on the complete virion of any AdV with a non-mammalian host. We combine mass spectrometry, cryo-electron microscopy, and protein crystallography to characterize the composition and structure of a snake AdV (SnAdV-1, Atadenovirus genus). SnAdV-1 particles contain the genus-specific proteins LH3, p32k, and LH2, a previously unrecognized structural component. Remarkably, the cementing protein LH3 has a trimeric β helix fold typical of bacteriophage host attachment proteins. The organization of minor coat proteins differs from that in human AdVs, correlating with higher thermostability in SnAdV-1. These findings add a new piece to the intriguing puzzle of virus evolution, hint at the use of cell entry pathways different from those in human AdVs, and will help development of new, thermostable SnAdV-1-based vectors.

摘要

尽管非人类腺病毒(AdVs)可能为人类腺病毒作为治疗载体所带来的问题提供解决方案,但其基本生物学特性却鲜为人知。特别是,对于任何一种感染非哺乳动物宿主的腺病毒的完整病毒体,都没有结构研究。我们结合质谱分析、冷冻电子显微镜和蛋白质晶体学来表征一种蛇腺病毒(SnAdV-1,腺病毒属)的组成和结构。SnAdV-1病毒颗粒包含属特异性蛋白LH3、p32k和LH2,其中LH2是一种此前未被识别的结构成分。值得注意的是,黏合蛋白LH3具有典型的噬菌体宿主附着蛋白的三聚体β螺旋结构。次要衣壳蛋白的组织方式与人类腺病毒不同,这与SnAdV-1更高的热稳定性相关。这些发现为病毒进化这一有趣谜题增添了新的内容,暗示了其可能采用与人类腺病毒不同的细胞进入途径,并将有助于开发基于SnAdV-1的新型热稳定载体。

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