Evaluation of monovalent and bivalent vaccines against lethal<i>Enterovirus</i>71 and<i>Coxsackievirus</i>A16 infection in newborn mice

Sun, Shiqi; Jiang, Liping; Liang, Zhenglun; Mao, Qunying; Su, Weiheng; Zhang, Huafei; Li, Xiaojun; Jin, Jun; Xu, Lin; Zhao, Dandan; Fan, Peihu; An, Dong; Yang, Ping; Lu, Jin‐Jian; Lv, Xiuping; Sun, Bo; Xu, Fengyuan; Kong, Wei; Jiang, Chunlai

doi:10.4161/hv.29823

Cited by 42 publications

(30 citation statements)

References 53 publications

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“…Passive transfer of immune sera conferred protection in newborn mice against lethal challenge with both viruses although bivalent VLPs vaccines were more potent than individual VLPs formulations. 174 Multivalent HFMD vaccines: the ultimate need, the ultimate goal…”

Section: Development Of a Bivalent Ev-a71/cv-a16 Vaccinementioning

confidence: 99%

“…In this regard, the introduction of a protective bivalent EV-A71/CV-A16 vaccine on the market should markedly reduce the number of HFMD cases. [170][171][172][173][174] CV-A16 strains of the B genotype that have elicited both homologous and heterologous protection against genotypes A and B in pre-clinical studies are potential candidates for a multivalent HFMD vaccine. [166][167][168] The selection of CV-A6, CV-A10, CV-B3, CV-B5 and E-30 vaccine strains will have to be based on comprehensive epidemiological information to identify the most prevalent circulating genotype(s) for each enterovirus serotype.…”

Section: Cross-protective Ability Of a Multivalent Vaccine And Selectmentioning

confidence: 99%

“…Although inactivated poliovirus and EV-A71 vaccines have been successfully developed and inactivated CV-A16 candidate vaccines are very promising, there is some indication that VLP-based bivalent vaccines are more immunogenic than a combination of inactivated EV-A71/CV-A16 vaccines. 174 It is not clear at the present time whether the production yields for EV-A71 and other HFMDassociated viruses will be sufficient to meet global needs. The selection process for an ideal vaccine strains needs to be addressed in the light of comprehensive epidemiological surveys, the optimal technology to efficiently produce potent and safe immunogens must be defined for each serotype, and clinical trials will have to be conducted for each individual vaccine before combining them.…”

Section: Vaccine Manufacturingmentioning

confidence: 99%

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Is a multivalent hand, foot, and mouth disease vaccine feasible?

Klein¹,

Chong

2015

Human Vaccines & Immunotherapeutics

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Keywords: bivalent and multivalent vaccines, coxsackievirus A16, coxsackieviruses B3 and B5, echovirus 30, epidemiology, enterovirus A (EV-A), enterovirus A71, hand, foot and mouth diseases, inactivated whole virion vaccines, monovalent, EV-A71 vaccine Enterovirus A infections are the primary cause of hand, foot and mouth disease (HFMD) in infants and young children. Although enterovirus 71 (EV-A71) and coxsackievirus A16 (CV-A16) are the predominant causes of HFMD epidemics worldwide, EV-A71 has emerged as a major neurovirulent virus responsible for severe neurological complications and fatal outcomes. HFMD is a serious health threat and economic burden across the Asia-Pacific region. Inactivated EV-A71 vaccines have elicited protection against EV-A71 but not against CV-A16 infections in large efficacy trials. The current development of a bivalent inactivated EV-A71/CV-A16 vaccine is the next step toward that of multivalent HFMD vaccines. These vaccines should ultimately include other prevalent pathogenic coxsackieviruses A (CV-A6 and CV-A10), coxsackieviruses B (B3 and B5) and echovirus 30 that often co-circulate during HFMD epidemics and can cause severe HFMD, aseptic meningitis and acute viral myocarditis. The prospect and challenges for the development of such multivalent vaccines are discussed.

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Section: Development Of a Bivalent Ev-a71/cv-a16 Vaccinementioning

confidence: 99%

Section: Cross-protective Ability Of a Multivalent Vaccine And Selectmentioning

confidence: 99%

Section: Vaccine Manufacturingmentioning

confidence: 99%

See 1 more Smart Citation

Is a multivalent hand, foot, and mouth disease vaccine feasible?

Klein¹,

Chong

2015

Human Vaccines & Immunotherapeutics

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“…After purification by ultracentrifugation, the EV71 VLP or formalin-inactivated vaccine was used to immunize mice at a dose of 10 mg (VP1), which induced similar neutralization antibody titer and prevented EV71 infection in newborn mice. 18 Three inactivated EV71 vaccine candidates have been studied in detail on their immunogenicity and protective efficacy including ED 50 in newborn mice before entering the clinical trials. 19,20 ED 50 is a measure method to evaluate the potency of a preparation.…”

Section: Introductionmentioning

confidence: 99%

Immunogenicity and protective efficacy of an EV71 virus-like particle vaccine against lethal challenge in newborn mice

Sun

Gao

Mao

et al. 2015

Human Vaccines & Immunotherapeutics

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“…Although studies of EV-A71 have already resulted in two CFDA-approved HFMD vaccines, multivalent HFMD vaccines to control different EV-A71 genotypes and also co-circulating CV-A16 are the next goal. The proof-of-concept studies for such vaccines are promising [148,178], but further work is needed to identify the optimal combination of antigens for balanced, broadly protective immunity. Targeting multiple viruses with a single vaccine also requires delivery systems for the effective presentation of multiple epitopes.…”

Section: Conclusion and Future Perspectivesmentioning

confidence: 99%

Human picornaviruses associated with neurological diseases and their neutralization by antibodies

Anastasina

Domanska

Palm

et al. 2017

Journal of General Virology

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Picornaviruses are the most commonly encountered infectious agents in mankind. They typically cause mild infections of the gastrointestinal or respiratory tract, but sometimes also invade the central nervous system. There, they can cause severe diseases with long-term sequelae and even be lethal. The most infamous picornavirus is poliovirus, for which significant epidemics of poliomyelitis were reported from the end of the nineteenth century. A successful vaccination campaign has brought poliovirus close to eradication, but neurological diseases caused by other picornaviruses have increasingly been reported since the late 1990s. In this review we focus on enterovirus 71, coxsackievirus A16, enterovirus 68 and human parechovirus 3, which have recently drawn attention because of their links to severe neurological diseases. We discuss the clinical relevance of these viruses and the primary role of humoral immunity in controlling them, and summarize current knowledge on the neutralization of such viruses by antibodies.

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Evaluation of monovalent and bivalent vaccines against lethalEnterovirus71 andCoxsackievirusA16 infection in newborn mice

Cited by 42 publications

References 53 publications

Is a multivalent hand, foot, and mouth disease vaccine feasible?

Is a multivalent hand, foot, and mouth disease vaccine feasible?

Immunogenicity and protective efficacy of an EV71 virus-like particle vaccine against lethal challenge in newborn mice

Human picornaviruses associated with neurological diseases and their neutralization by antibodies

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