PLoS Pathogens (Oct 2009)

Autocrine production of beta-chemokines protects CMV-Specific CD4 T cells from HIV infection.

  • Joseph P Casazza,
  • Jason M Brenchley,
  • Brenna J Hill,
  • Ribka Ayana,
  • David Ambrozak,
  • Mario Roederer,
  • Daniel C Douek,
  • Michael R Betts,
  • Richard A Koup

DOI
https://doi.org/10.1371/journal.ppat.1000646
Journal volume & issue
Vol. 5, no. 10
p. e1000646

Abstract

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Induction of a functional subset of HIV-specific CD4+ T cells that is resistant to HIV infection could enhance immune protection and decrease the rate of HIV disease progression. CMV-specific CD4+ T cells, which are less frequently infected than HIV-specific CD4+ T cells, are a model for such an effect. To determine the mechanism of this protection, we compared the functional response of HIV gag-specific and CMV pp65-specific CD4+ T cells in individuals co-infected with CMV and HIV. We found that CMV-specific CD4+ T cells rapidly up-regulated production of MIP-1alpha and MIP-1beta mRNA, resulting in a rapid increase in production of MIP-1alpha and MIP-1beta after cognate antigen stimulation. Production of beta-chemokines was associated with maturational phenotype and was rarely seen in HIV-specific CD4+ T cells. To test whether production of beta-chemokines by CD4+ T cells lowers their susceptibility to HIV infection, we measured cell-associated Gag DNA to assess the in vivo infection history of CMV-specific CD4+ T cells. We found that CMV-specific CD4+ T cells which produced MIP-1beta contained 10 times less Gag DNA than did those which failed to produce MIP-1beta. These data suggest that CD4+ T cells which produce MIP-1alpha and MIP-1beta bind these chemokines in an autocrine fashion which decreases the risk of in vivo HIV infection.