2020
DOI: 10.3390/microorganisms8091287
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Structural Insight into CVB3-VLP Non-Adjuvanted Vaccine

Abstract: Coxsackievirus B (CVB) enteroviruses are common pathogens that can cause acute and chronic myocarditis, dilated cardiomyopathy, aseptic meningitis, and they are hypothesized to be a causal factor in type 1 diabetes. The licensed enterovirus vaccines and those currently in clinical development are traditional inactivated or live attenuated vaccines. Even though these vaccines work well in the prevention of enterovirus diseases, new vaccine technologies, like virus-like particles (VLPs), can offer important adva… Show more

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Cited by 14 publications
(24 citation statements)
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“…Although the use of whole virus vaccines (live and inactivated) has proven their safety and efficacy against poliovirus [250], it is expensive, slow to develop, lacks flexibility to engineer new epitopes and is limited by the culturability of the target EV. To overcome such limitations, an alternative vaccine strategy has been explored for CVB1, 3 and 4, involving the use of empty VLPs as antigens [251][252][253][254]. Generated from recombinantly expressed viral structural proteins, VLPs resemble the native CVB capsid structure but lack the infectious RNA genome.…”
Section: Antiviral Vaccines and Therapeutics For T1d Preventionmentioning
confidence: 99%
See 2 more Smart Citations
“…Although the use of whole virus vaccines (live and inactivated) has proven their safety and efficacy against poliovirus [250], it is expensive, slow to develop, lacks flexibility to engineer new epitopes and is limited by the culturability of the target EV. To overcome such limitations, an alternative vaccine strategy has been explored for CVB1, 3 and 4, involving the use of empty VLPs as antigens [251][252][253][254]. Generated from recombinantly expressed viral structural proteins, VLPs resemble the native CVB capsid structure but lack the infectious RNA genome.…”
Section: Antiviral Vaccines and Therapeutics For T1d Preventionmentioning
confidence: 99%
“…Thus, VLP-based vaccines can be manufactured without culturing the virus, are modified rapidly with ease and are not subject to safety concerns associated with live virus vaccines. However, it remains to be determined whether VLP-based vaccines can offer a sufficient level of immunogenicity To overcome such limitations, an alternative vaccine strategy has been explored for CVB1, 3 and 4, involving the use of empty VLPs as antigens [251][252][253][254]. Generated from recombinantly expressed viral structural proteins, VLPs resemble the native CVB capsid structure but lack the infectious RNA genome.…”
Section: Antiviral Vaccines and Therapeutics For T1d Preventionmentioning
confidence: 99%
See 1 more Smart Citation
“…139 Stable CVB1, 3, and 4 VLP vaccines have been developed [139][140][141][142] and shown to induce a strong neutralising antibody response in C57BL/6J and BALB/c mice. [139][140][141]…”
Section: Development Of Coxsackievirus B Vaccinesmentioning
confidence: 99%
“…Although the use of whole virus vaccines (live and inactivated) have proven their safety and efficacy against poliovirus [246], it is expensive, slow to develop, lacks flexibility to engineer new epitopes and limited by the culturability of the target EV. To overcome such limitations, an alternative vaccine strategy has been explored for CVB1, 3 and 4, involving the use of empty VLPs as antigens [247][248][249][250]. Generated from recombinantly expressed viral structural proteins, VLPs resemble the native CVB capsid structure but lack the infectious RNA genome.…”
Section: Antiviral Vaccines and Therapeutics For T1d Preventionmentioning
confidence: 99%