Controlled inactivation of recombinant viruses with vitamin B2

Inactivated viruses are important tools for vaccine development and gene transfer. 8-Methoxypsoralen (8-MOP) and long-wavelength ultraviolet irradiation (LWUVI) inactivates many viruses. Toxicity limits its use in animals and humans. Toxicological and photosensitizing properties of riboflavin make i...

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Bibliographic Details
Published in:Journal of virological methods 2008-03, Vol.148 (1-2), p.132-145
Main Authors: CALLAHAN, Shellie M, WONGANAN, Piyanuch, OBENAUER-KUTNER, Linda J, SUTJIPTO, Suganto, DEKKER, Joseph D, CROYLE, Maria A
Format: Article
Language:English
Subjects:
Adenoviridae - drug effects
Adenoviridae - radiation effects
Adenoviridae - ultrastructure
Animals
Antiviral Agents - pharmacology
beta-Galactosidase - biosynthesis
beta-Galactosidase - genetics
Biological and medical sciences
Dependovirus - drug effects
Dependovirus - radiation effects
Dependovirus - ultrastructure
Fundamental and applied biological sciences. Psychology
Genes, Reporter
Humans
Lentivirus - drug effects
Lentivirus - radiation effects
Lentivirus - ultrastructure
Liver - virology
Methoxsalen - pharmacology
Microbiology
Microscopy, Electron, Transmission
Photosensitizing Agents - pharmacology
Rats
Riboflavin - pharmacology
Techniques used in virology
Virology
Virus Inactivation
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Summary:Inactivated viruses are important tools for vaccine development and gene transfer. 8-Methoxypsoralen (8-MOP) and long-wavelength ultraviolet irradiation (LWUVI) inactivates many viruses. Toxicity limits its use in animals and humans. Toxicological and photosensitizing properties of riboflavin make it suitable for virus inactivation in preparations for biological use. Viruses expressing beta-galactosidase were mixed with either 8-MOP (1.5mM) or riboflavin (50 microM) and exposed to LWUVI (365 nm) for 2 h. Virus activity was determined by limiting dilution. The half-life of the adenovirus preparation treated with 8-MOP was 8.28 ns(-1) and 36.5 ns(-1) after treatment with riboflavin. Despite the difference in half-life, both preparations were completely inactivated within 45 min. In contrast, the half-lives for adeno-associated virus (AAV) preparations were similar (63 ns(-1) 8-MOP vs. 67 ns(-1) riboflavin). Each AAV preparation was fully inactivated within 90 min. The half-life of lentivirus was 193.4 ns(-1) after treatment with 8-MOP and 208 ns(-1) after exposure to riboflavin. Virus treated with riboflavin was inactivated within 20 min. Virus exposed to 8-MOP was inactivated in 90 min. DNA and RNA viruses can be inactivated by riboflavin and LWUVI and used in physiological systems sensitive to other photochemicals.
ISSN:0166-0934
1879-0984
DOI:10.1016/j.jviromet.2007.10.027