Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
3370006 | Journal of Clinical Virology | 2008 | 7 Pages |
BackgroundInfluenza A has the ability to rapidly mutate and become resistant to the commonly prescribed influenza therapeutics, thereby complicating treatment decisions.ObjectiveTo design a cost-effective low-density microarray for use in detection of influenza resistance to the adamantanes.Study designWe have taken advantage of functional genomics and microarray technology to design a DNA microarray that can detect the two most common mutations in the M2 protein associated with adamantane resistance, V27A and S31N.ResultsIn a blind study of 22 influenza isolates, the antiviral resistance-chip (AVR-Chip) had a success rate of 95% for detecting these mutations. Microarray data from a larger set of samples were further analyzed using an artificial neural network and resulted in a correct identification rate of 94% for influenza virus samples that had V27A and S31N mutations.ConclusionsThe AVR-Chip provided a method for rapidly screening influenza viruses for adamantane sensitivity, and the general approach could be easily extended to detect resistance to other chemotherapeutics.