Literature DB >> 30514821

Seneca Valley virus attachment and uncoating mediated by its receptor anthrax toxin receptor 1.

Lin Cao1,2,3,4,5, Ran Zhang5, Tingting Liu2, Zixian Sun5, Mingxu Hu5, Yuna Sun6, Lingpeng Cheng5, Yu Guo1,3, Sheng Fu4,5, Junjie Hu7, Xiangmin Li2, Chengqi Yu8, Hanyang Wang9, Huanchun Chen2, Xueming Li5, Elizabeth E Fry10, David I Stuart11, Ping Qian12, Zhiyong Lou13, Zihe Rao1,3,4,5,6.   

Abstract

Seneca Valley virus (SVV) is an oncolytic picornavirus with selective tropism for neuroendocrine cancers. SVV mediates cell entry by attachment to the receptor anthrax toxin receptor 1 (ANTXR1). Here we determine atomic structures of mature SVV particles alone and in complex with ANTXR1 in both neutral and acidic conditions, as well as empty "spent" particles in complex with ANTXR1 in acidic conditions by cryoelectron microscopy. SVV engages ANTXR1 mainly by the VP2 DF and VP1 CD loops, leading to structural changes in the VP1 GH loop and VP3 GH loop, which attenuate interprotomer interactions and destabilize the capsid assembly. Despite lying on the edge of the attachment site, VP2 D146 interacts with the metal ion in ANTXR1 and is required for cell entry. Though the individual substitution of most interacting residues abolishes receptor binding and virus propagation, a serine-to-alanine mutation at VP2 S177 significantly increases SVV proliferation. Acidification of the SVV-ANTXR1 complex results in a major reconfiguration of the pentameric capsid assemblies, which rotate ∼20° around the icosahedral fivefold axes to form a previously uncharacterized spent particle resembling a potential uncoating intermediate with remarkable perforations at both two- and threefold axes. These structures provide high-resolution snapshots of SVV entry, highlighting opportunities for anticancer therapeutic optimization.

Entities:  

Keywords:  ANTXR1; Seneca Valley virus; cryo-EM; entry; receptor recognition

Mesh:

Substances:

Year:  2018        PMID: 30514821      PMCID: PMC6304951          DOI: 10.1073/pnas.1814309115

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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