AI Article Synopsis

  • Researchers introduced a new method using ring-opening metathesis polymerization (ROMP) to control VLP disassembly without relying on specific environmental factors like pH and temperature.
  • The study demonstrated that this ROMP strategy was effective for the P22 bacteriophage-derived VLP, allowing the release of a GFP reporter and showing potential for adapting this method for other VLPs in drug delivery applications.

Article Abstract

Virus-like particles (VLPs) show considerable promise for the delivery of therapeutic compounds such as bioactive venom peptides. While loading and targeting protocols have been developed for numerous VLP prototypes, induced disassembly under physiological conditions of neutral pH, moderate temperature, and aqueous medium remain a challenge. Here, we implement and evaluate a general mechanism, based on ring-opening metathesis polymerization (ROMP), for controllable VLP disassembly. This mechanism is independent of cell-specific factors or the manipulation of environmental conditions such as pH and temperature that cannot be readily controlled The ROMP substrate norbornene is covalently conjugated to surface-exposed lysine residues of a P22 bacteriophage-derived VLP, and ROMP is induced by treatment with the water-soluble ruthenium catalyst AquaMet. Disruption of the P22 shell and release of a GFP reporter is confirmed via native agarose electrophoresis, TEM, and dynamic light scattering (DLS) analyses. Our ROMP disassembly strategy does not depend on the particular structure or morphology of the P22 nanocontainer and is adaptable to other VLP prototypes for the potential delivery of venom peptides for pharmacological applications.

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Source
http://dx.doi.org/10.1021/acs.bioconjchem.0c00494DOI Listing

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