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Method for Producing Self-Replicating, Nucleic Acid-Loaded Virus-Like Particles
Case ID:
M22-078L
Web Published:
9/2/2022
Vaccines are an essential tool in preventing and controlling many diseases. Most approved vaccines are inactivated or live attenuated type, however, alternative platforms like mRNA and virus-like particles (VLPs) are being increasingly explored and approved because they generate potent immune responses with great safety profiles. VLPs are particularly useful because they resemble the size and shape of viruses yet are non-infectious. Further, VLPs are amenable to heterologous sequence insertions allowing the display of an antigen of interest on the surface, broadening the scope of diseases that can be targeted.
Researchers at the Biodesign Institute of Arizona State University have developed a novel self-replicating, nucleic acid-loaded VLP vaccine and drug delivery platform. This plant production-based platform can deliver products for gene therapy and vaccination for multiple different viruses or virus serotypes depending on manipulation of the VLP and DNA replicon within the system. This platform creates a combination vaccine and synergizes the potency of VLP and DNA vaccines. The self-replication mechanism is functional in both plant and mammalian cells.
This novel platform with its use of VLPs which can be nucleic acid-loaded has broad applications in vaccines, drug delivery as well as gene therapy.
Potential Applications
Vaccines
Drug delivery (nucleic acids, proteins, CRISPR/Cas9, etc.)
Can be optimized to target specific tissue and cell types
Gene therapy
Repress gene expression through RNAi
Benefits and Advantages
Easily adaptable and versatile vaccine platform
Replication in mammalian cells can be controlled through manipulation of replicons and separation of replication protein genes from VLP-DNA or RNA area of delivery
Can develop multivalent vaccines from one VLP
Vaccine can be made to offer protection from multiple serotypes of the same virus
Vaccine can be created to offer protection from multiple different viruses in a single dose
Can integrate shRNA and siRNA into the platform for RNAi gene silencing
VLP can be optimized to target specific tissue or cell types for delivery
Greater safety profile vs adenovirus associated platforms because of the inability of plant viruses to infect mammalian cells
Minimized off site target effects
Can be used to package and deliver nucleic acids, protein, antibodies, CRISPR/CAS9 and drugs
Replication mechanism is functional in both plant and mammalian cells
Has a mechanism to allow for a limited cycle of replication inside the mammalian host
For more information about the inventor(s) and their research, please see
Dr. Chen's departmental webpage
Patent Information:
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Direct Link:
https://canberra-ip.technologypublisher.com/tech?title=Method_for_Producing_S elf-Replicating%2c_Nucleic_Acid-Loaded_Virus-Like_Particles
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For Information, Contact:
Jovan Heusser
Director of Licensing and Business Development
Skysong Innovations
jovan.heusser@skysonginnovations.com