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High-Titer Self-Propagating Capsidless Chikungunya Virus Generated in Vero Cells as a Strategy for Alphavirus Vaccine Development. | LitMetric

High-Titer Self-Propagating Capsidless Chikungunya Virus Generated in Vero Cells as a Strategy for Alphavirus Vaccine Development.

J Virol

Key Laboratory of Special Pathogens and Biosafety, Wuhan Institute of Virologygrid.439104.b, Center for Biosafety Mega-Science, Chinese Academy of Sciences, Wuhan, Hubei, China.

Published: March 2022

AI Article Synopsis

  • Researchers found that a new Chikungunya virus particle (ΔC-CHIKV) was infectious and potentially useful as a live vaccine, but its low production rate limited commercial development.
  • In the current study, they successfully propagated a chimeric version (VEEV-ΔC-CHIKV) in Vero cells, enhancing yield via adaptive mutations in the viral envelope proteins.
  • The modified viral particle showed promise as a safe and effective vaccine, providing protection to mice with just one immunization, which could lead to viable vaccine options against Chikungunya virus.

Article Abstract

In our previous study, we found that a new type of Chikungunya virus particle with a complete capsid deletion (ΔC-CHIKV) is still infectious in BHK-21 cells and demonstrated its potential as a live attenuated vaccine candidate. However, the low yield as well as the disability to propagate in vaccine production cell line Vero of ΔC-CHIKV are not practical for commercial vaccine development. In this study, we not only achieved the successful propagation of the viral particle in Vero cells, but significantly improved its yield through construction of a chimeric VEEV-ΔC-CHIKV and extensive passage in Vero cells. Mechanistically, high production of VEEV-ΔC-CHIKV is due to the improvement of viral RNA packaging efficiency conferred by adaptive mutations, especially those in envelope proteins. Similar to ΔC-CHIKV, the passaged VEEV-ΔC-CHIKV is safe, immunogenic, and efficacious, which protects mice from CHIKV challenge after only one shot of immunization. Our study demonstrates that the utilization of infectious capsidless viral particle of CHIKV as a vaccine candidate is a practical strategy for the development of alphavirus vaccine. Chikungunya virus (CHIKV) is one of important emerging alphaviruses. Currently, there are no licensed vaccines against CHIKV infection. We have previously found a new type of Chikungunya virus particle with a complete capsid deletion (ΔC-CHIKV) as a live attenuated vaccine candidate that is not suitable for commercial vaccine development with the low viral titer production. In this study, we significantly improved its production through construction of a chimeric VEEV-ΔC-CHIKV. Our results proved the utilization of infectious capsidless viral particle of CHIKV as a safe and practical vaccine candidate.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8941867PMC
http://dx.doi.org/10.1128/JVI.01480-21DOI Listing

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