Development of a skin- and neuro-attenuated live vaccine for varicella

Varicella caused by the primary infection of varicella-zoster virus (VZV) exerts a considerable disease burden globally. Current varicella vaccines consisting of the live-attenuated vOka strain of VZV are generally safe and effective. However, vOka retains full neurovirulence and can establish laten...

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Published inNature communications Vol. 13; no. 1; p. 824
Main Authors Wang, Wei, Pan, Dequan, Fu, Wenkun, Ye, Xiangzhong, Han, Jinle, Yang, Lianwei, Jia, Jizong, Liu, Jian, Zhu, Rui, Zhang, Yali, Liu, Che, Ye, Jianghui, Selariu, Anca, Que, Yuqiong, Zhao, Qinjian, Wu, Ting, Li, Yimin, Zhang, Jun, Cheng, Tong, Zhu, Hua, Xia, Ningshao
Format Journal Article
LanguageEnglish
Published England Nature Publishing Group 11.02.2022
Nature Publishing Group UK
Nature Portfolio
Subjects
Animal models
Animal species
Animals
Attenuation
Cell Line
Chicken pox
Chickenpox - immunology
Chickenpox - prevention & control
Chickenpox Vaccine - immunology
Complications
Female
Fibroblasts
Guinea Pigs
Herpes zoster
Herpes Zoster - virology
Herpesvirus 3, Human
Humans
Immunogenicity
Immunogenicity, Vaccine
Infections
Latency
Lung
Male
Mice
Neurons - pathology
Neurovirulence
Primates
Rabbits
Rats
Risk management
Skin
Skin - immunology
Skin - pathology
Vaccination
Vaccines
Vaccines, Attenuated - immunology
Varicella
Viral Vaccines
Viruses
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Summary:Varicella caused by the primary infection of varicella-zoster virus (VZV) exerts a considerable disease burden globally. Current varicella vaccines consisting of the live-attenuated vOka strain of VZV are generally safe and effective. However, vOka retains full neurovirulence and can establish latency and reactivate to cause herpes zoster in vaccine recipients, raising safety concerns. Here, we rationally design a live-attenuated varicella vaccine candidate, v7D. This virus replicates like wild-type virus in MRC-5 fibroblasts and human PBMCs, the carrier for VZV dissemination, but is severely impaired for infection of human skin and neuronal cells. Meanwhile, v7D shows immunogenicity comparable to vOka both in vitro and in multiple small animal species. Finally, v7D is proven well-tolerated and immunogenic in nonhuman primates. Our preclinical data suggest that v7D is a promising candidate as a safer live varicella vaccine with reduced risk of vaccine-related complications, and could inform the design of other herpes virus vaccines.
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ISSN:2041-1723
2041-1723
DOI:10.1038/s41467-022-28329-1