What question did this study set out to answer?

The aim is to develop a live attenuated influenza vaccine by utilizing chaperone-mediated autophagy to degrade viral proteins.

April 12, 2026

Harnessing chaperone-mediated autophagy for the development of live attenuated influenza vaccines

Key Points

The aim is to develop a live attenuated influenza vaccine by utilizing chaperone-mediated autophagy to degrade viral proteins.
Introduced a lysosome-targeting live attenuated vaccine platform (LYTAR)
Utilized chaperone-mediated autophagy for protein degradation
Conditionally degraded viral proteins to attenuate virulent influenza A viruses
The LYTAR platform effectively attenuated viral replication
Preserved the full antigenic composition of the virus
Maintained robust immunogenicity of the vaccine

Abstract

Targeted degradation of viral proteins has emerged as a powerful strategy to attenuate virulent viruses into live vaccines. In our recent study, we introduced a lysosome-targeting (LYTAR) live attenuated vaccine platform that utilizes chaperone-mediated autophagy (CMA), a lysosome-dependent degradation pathway, to conditionally degrade viral proteins and convert virulent influenza A viruses into safe and effective live attenuated vaccines. The LYTAR vaccine approach enables controlled attenuation of viral replication, while preserving the full antigenic composition of the virus and maintaining robust immunogenicity.

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Harnessing chaperone-mediated autophagy for the development of live attenuated influenza vaccines

Key Points

Abstract

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