AI Article Synopsis

  • Hydrophobic aryl azides can inactivate enveloped viruses through a process of UVA irradiation, which leads to viral protein aggregation due to reactive oxygen species (ROS) formation.
  • Prolonged irradiation allows the surface antigenic epitopes to remain intact, making the aggregates resistant to detergents, which could help develop new methods for virus inactivation in vaccine preparation.
  • Studies show that ROS-modified HIV virus preparations treated with Triton X-100 result in higher concentrations of key viral proteins in sediment after centrifugation, with some aggregates displaying characteristics of covalent bonding and recognizable virus fragments seen via electron microscopy.

Article Abstract

Previously we reported that hydrophobic aryl azides partition into hydrophobic regions of the viral membrane of enveloped viruses and inactivate the virus upon UVA irradiation for 2 min. Prolonged irradiation (15 min) resulted in viral protein aggregation as visualized via Western blot analysis, due to reactive oxygen species (ROS) formation, with preservation of the surface antigenic epitopes. Herein, we demonstrate that these aggregates show detergent resistance and that this property may be useful towards the creation of a novel orthogonal virus inactivation strategy for use in preparing experimental vaccines. When ROS-modified HIV virus preparations were treated with 1% Triton X-100, there was an increase in the percent of viral proteins (gp41, p24) in the viral pellet after ultracentrifugation through sucrose. Transmission electron microscopy (TEM) of these detergent-resistant pellets shows some recognizable virus fragments, and immunoprecipitation studies of the gp41 aggregates suggest the aggregation is covalent in nature, involving short-range interactions.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3152596PMC
http://dx.doi.org/10.1016/j.virol.2011.06.007DOI Listing

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