AI Article Synopsis

  • HCV quasispecies variability is crucial for mutation selection and drug resistance, with amino acid changes in NS3 linked to reduced susceptibility to protease inhibitors.
  • Massively parallel sequencing revealed significant genetic heterogeneity in treatment-naïve patients with HCV genotype 1, showing amino acid substitutions related to drug resistance in 85.7% of cases.
  • The study found that HIV-coinfected patients had lower NS3 heterogeneity and highlighted the need for further research to understand this difference, while suggesting that advanced sequencing techniques may aid in studying viral dynamics.

Article Abstract

HCV quasispecies variability represents the background for the selection of mutations and for the development of drug resistance. Natural aminoacid changes in NS3, associated with reduced protease inhibitor susceptibility, have been observed in treatment-naïve patients. Massively parallel sequencing has been used to analyze NS3 quasispecies in patients infected with HCV genotype 1, naive to anti-HCV treatment, with/without HIV-coinfection, to establish the genetic heterogeneity and the presence of amino acid substitutions at positions responsible for drug resistance. Genomes carrying substitutions represented either predominant or minority components of viral quasispecies, and were observed in 85.7% of patients. Multiple substitutions, frequently associated on the same haplotype, were observed in 46.4% of patients. High resistance combinations were not detected, neither on the same genome, nor in the whole quasispecies. Heterogeneity of HCV NS3 was lower in HIV-coinfected as compared to HCV-monoinfected patients, but factors underlying this difference remain to be established. Although the relevance of naturally occurring mutations with respect of resistance development and probability of success of direct acting antivirals is questioned, UDPS may be beneficial to help understanding viral dynamics, providing high resolution view of viral diversity.

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Source
http://dx.doi.org/10.1016/j.virusres.2013.08.001DOI Listing

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