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Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity

Monkeypox was declared a global health emergency by the World Health Organization, and as of March 2023, 86,000 confirmed cases and 111 deaths across 110 countries have been reported. Its causal agent, monkeypox virus (MPV) belongs to a large family of double-stranded DNA viruses, Orthopoxviridae, t...

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Autores principales: Zhang, Niubing, Cheng, Xiang, Zhu, Yilong, Mo, Ouyang, Yu, Huiqing, Zhu, Liqi, Zhang, Juan, Kuang, Linlin, Gao, Ying, Cao, Ruiyuan, Liang, Xiaozhen, Wang, Haikun, Li, Honglin, Li, Song, Zhong, Wu, Li, Xuan, Li, Xiao, Hao, Pei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Science China Press 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10257374/
https://www.ncbi.nlm.nih.gov/pubmed/37300753
http://dx.doi.org/10.1007/s11427-023-2378-x
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author Zhang, Niubing
Cheng, Xiang
Zhu, Yilong
Mo, Ouyang
Yu, Huiqing
Zhu, Liqi
Zhang, Juan
Kuang, Linlin
Gao, Ying
Cao, Ruiyuan
Liang, Xiaozhen
Wang, Haikun
Li, Honglin
Li, Song
Zhong, Wu
Li, Xuan
Li, Xiao
Hao, Pei
author_facet Zhang, Niubing
Cheng, Xiang
Zhu, Yilong
Mo, Ouyang
Yu, Huiqing
Zhu, Liqi
Zhang, Juan
Kuang, Linlin
Gao, Ying
Cao, Ruiyuan
Liang, Xiaozhen
Wang, Haikun
Li, Honglin
Li, Song
Zhong, Wu
Li, Xuan
Li, Xiao
Hao, Pei
author_sort Zhang, Niubing
collection PubMed
description Monkeypox was declared a global health emergency by the World Health Organization, and as of March 2023, 86,000 confirmed cases and 111 deaths across 110 countries have been reported. Its causal agent, monkeypox virus (MPV) belongs to a large family of double-stranded DNA viruses, Orthopoxviridae, that also includes vaccinia virus (VACV) and others. MPV produces two distinct forms of viral particles during its replication cycles: the enveloped viron (EV) that is released via exocytosis, and the mature viron (MV) that is discharged through lysis of host cells. This study was designed to develop multi-valent mRNA vaccines against monkeypox EV and MV surface proteins, and examine their efficacy and mechanism of action. Four mRNA vaccines were produced with different combinations of surface proteins from EV (A35R and B6R), MV (A29L, E8L, H3L and M1R), or EV and MV, and were administered in Balb/c mice to assess their immunogenicity potentials. A dynamic immune response was observed as soon as seven days after initial immunization, while a strong IgG response to all immunogens was detected with ELISA after two vaccinations. The higher number of immunogens contributed to a more robust total IgG response and correlating neutralizing activity against VACV, indicating the additive potential of each immunogen in generating immune response and nullifying VACV infection. Further, the mRNA vaccines elicited an antigen-specific CD4(+) T cell response that is biased towards Th1. The mRNA vaccines with different combinations of EV and MV surface antigens protected a mouse model from a lethal dose VACV challenge, with the EV and MV antigens-combined vaccine offering the strongest protection. These findings provide insight into the protective mechanism of multi-valent mRNA vaccines against MPV, and also the foundation for further development of effective and safe mRNA vaccines for enhanced protection against monkeypox virus outbreak. SUPPORTING INFORMATION: The supporting information is available online at 10.1007/s11427-023-2378-x. The supporting materials are published as submitted, without typesetting or editing. The responsibility for scientific accuracy and content remains entirely with the authors.
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spelling pubmed-102573742023-06-12 Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity Zhang, Niubing Cheng, Xiang Zhu, Yilong Mo, Ouyang Yu, Huiqing Zhu, Liqi Zhang, Juan Kuang, Linlin Gao, Ying Cao, Ruiyuan Liang, Xiaozhen Wang, Haikun Li, Honglin Li, Song Zhong, Wu Li, Xuan Li, Xiao Hao, Pei Sci China Life Sci Research Paper Monkeypox was declared a global health emergency by the World Health Organization, and as of March 2023, 86,000 confirmed cases and 111 deaths across 110 countries have been reported. Its causal agent, monkeypox virus (MPV) belongs to a large family of double-stranded DNA viruses, Orthopoxviridae, that also includes vaccinia virus (VACV) and others. MPV produces two distinct forms of viral particles during its replication cycles: the enveloped viron (EV) that is released via exocytosis, and the mature viron (MV) that is discharged through lysis of host cells. This study was designed to develop multi-valent mRNA vaccines against monkeypox EV and MV surface proteins, and examine their efficacy and mechanism of action. Four mRNA vaccines were produced with different combinations of surface proteins from EV (A35R and B6R), MV (A29L, E8L, H3L and M1R), or EV and MV, and were administered in Balb/c mice to assess their immunogenicity potentials. A dynamic immune response was observed as soon as seven days after initial immunization, while a strong IgG response to all immunogens was detected with ELISA after two vaccinations. The higher number of immunogens contributed to a more robust total IgG response and correlating neutralizing activity against VACV, indicating the additive potential of each immunogen in generating immune response and nullifying VACV infection. Further, the mRNA vaccines elicited an antigen-specific CD4(+) T cell response that is biased towards Th1. The mRNA vaccines with different combinations of EV and MV surface antigens protected a mouse model from a lethal dose VACV challenge, with the EV and MV antigens-combined vaccine offering the strongest protection. These findings provide insight into the protective mechanism of multi-valent mRNA vaccines against MPV, and also the foundation for further development of effective and safe mRNA vaccines for enhanced protection against monkeypox virus outbreak. SUPPORTING INFORMATION: The supporting information is available online at 10.1007/s11427-023-2378-x. The supporting materials are published as submitted, without typesetting or editing. The responsibility for scientific accuracy and content remains entirely with the authors. Science China Press 2023-06-01 /pmc/articles/PMC10257374/ /pubmed/37300753 http://dx.doi.org/10.1007/s11427-023-2378-x Text en © Science China Press 2023 This article is made available via the PMC Open Access Subset for unrestricted research re-use and secondary analysis in any form or by any means with acknowledgement of the original source. These permissions are granted for the duration of the World Health Organization (WHO) declaration of COVID-19 as a global pandemic.
spellingShingle Research Paper
Zhang, Niubing
Cheng, Xiang
Zhu, Yilong
Mo, Ouyang
Yu, Huiqing
Zhu, Liqi
Zhang, Juan
Kuang, Linlin
Gao, Ying
Cao, Ruiyuan
Liang, Xiaozhen
Wang, Haikun
Li, Honglin
Li, Song
Zhong, Wu
Li, Xuan
Li, Xiao
Hao, Pei
Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity
title Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity
title_full Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity
title_fullStr Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity
title_full_unstemmed Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity
title_short Multi-valent mRNA vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity
title_sort multi-valent mrna vaccines against monkeypox enveloped or mature viron surface antigens demonstrate robust immune response and neutralizing activity
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10257374/
https://www.ncbi.nlm.nih.gov/pubmed/37300753
http://dx.doi.org/10.1007/s11427-023-2378-x
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