Atomic structure of the human herpesvirus 6B capsid and capsid-associated tegument complexes

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作者
Yibo Zhang
Wei Liu
Zihang Li
Vinay Kumar
Ana L. Alvarez-Cabrera
Emily C. Leibovitch
Yanxiang Cui
Ye Mei
Guo-Qiang Bi
Steve Jacobson
Z. Hong Zhou
机构
[1] University of Science and Technology of China (USTC),Center for Integrative Imaging, Hefei National Laboratory for Physical Sciences at the Microscale, and School of Life Sciences
[2] University of California,California NanoSystems Institute
[3] Los Angeles (UCLA),Department of Microbiology
[4] Immunology and Molecular Genetics,State Key Laboratory of Precision Spectroscopy, School of Physics and Electronic Science
[5] UCLA,Viral Immunology Section, National Institute of Neurological Disorders and Stroke
[6] East China Normal University (ECNU),undefined
[7] National Institutes of Health (NIH),undefined
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Nature Communications | / 10卷
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摘要
Human herpesvirus 6B (HHV-6B) belongs to the β-herpesvirus subfamily of the Herpesviridae. To understand capsid assembly and capsid-tegument interactions, here we report atomic structures of HHV-6B capsid and capsid-associated tegument complex (CATC) obtained by cryoEM and sub-particle reconstruction. Compared to other β-herpesviruses, HHV-6B exhibits high similarity in capsid structure but organizational differences in its CATC (pU11 tetramer). 180 “VΛ”-shaped CATCs are observed in HHV-6B, distinguishing from the 255 “Λ”-shaped dimeric CATCs observed in murine cytomegalovirus and the 310 “Δ”-shaped CATCs in human cytomegalovirus. This trend in CATC quantity correlates with the increasing genomes sizes of these β-herpesviruses. Incompatible distances revealed by the atomic structures rationalize the lack of CATC’s binding to triplexes Ta, Tc, and Tf in HHV-6B. Our results offer insights into HHV-6B capsid assembly and the roles of its tegument proteins, including not only the β-herpesvirus-specific pU11 and pU14, but also those conserved across all subfamilies of Herpesviridae.
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