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Human immunodeficiency virus type 1 clade B superinfection: Evidence for differential immune containment of distinct clade B strains

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  • OO Yang
  • ES Daar
  • BD Jamieson
  • A Balamurugan
  • DM Smith
  • JA Pitt
  • CJ Petropoulos
  • DD Richman
  • SJ Little
  • AJ Leigh Brown

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Original languageEnglish
Pages (from-to)860-868
Number of pages9
JournalJournal of Virology
Issue number2
Publication statusPublished - Jan 2005


Sequential infection with different strains of human immunodeficiency virus type 1 (HIV-1) is a rarely identified phenomenon with important implications for immunopathogenesis and vaccine development. Here, we identify an individual whose good initial control of viremia was lost in association with reduced containment of a superinfecting strain. Subject 2030 presented with acute symptoms of HIV-1 infection with high viremia and an incomplete seroconversion as shown by Western blotting. A low set point of viremia (similar to1,000 HTV-1 copies/ml) was initially established without drug therapy, but a new higher set point (similar to40,000 HIV-1 copies/ml) manifested about 5 months after infection. Drug susceptibility testing demonstrated a multidrug-resistant virus initially but a fully sensitive virus after 5 months, and an analysis of pol genotypes showed that these were two phylogenetically distinct strains of virus (strains A and B). Replication capacity assays suggested that the outgrowth of strain B was not due to higher fitness conferred by pol, and env sequences indicated that the two strains had the same R5 coreceptor phenotype. Delineation of CD8(+)-T-lymphocyte responses against HIV-1 showed a striking pattern of decay of the initial cellular immune responses after superinfection, followed by some adaptation of targeting to new epitopes. An examination of targeted sequences suggested that differences in the recognized epitopes contributed to the poor immune containment of strain B. In conclusion, the rapid overgrowth of a superinfecting strain of HIV-1 of the same subtype raises major concerns for effective vaccine development.

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