Retrovirology (May 2009)

Synergistic effect of human CycT1 and CRM1 on HIV-1 propagation in rat T cells and macrophages

  • Nagai Mika,
  • Ben Fofana Ismael,
  • Zhang Xianfeng,
  • Okada Hiroyuki,
  • Suzuki Hajime,
  • Ohashi Takashi,
  • Shida Hisatoshi

DOI
https://doi.org/10.1186/1742-4690-6-43
Journal volume & issue
Vol. 6, no. 1
p. 43

Abstract

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Abstract Background In vivo studies of HIV-1 pathogenesis and testing of antiviral strategies have been hampered by the lack of an immunocompetent small animal model that is highly susceptible to HIV-1 infection. Although transgenic rats that express the HIV-1 receptor complex hCD4 and hCCR5 are susceptible to infection, HIV-1 replicates very poorly in these animals. To demonstrate the molecular basis for developing a better rat model for HIV-1 infection, we evaluated the effect of human CyclinT1 (hCycT1) and CRM1 (hCRM1) on Gag p24 production in rat T cells and macrophages using both established cell lines and primary cells prepared from hCycT1/hCRM1 transgenic rats. Results Expression of hCycT1 augmented Gag production 20–50 fold in rat T cells, but had little effect in macrophages. Expression of hCRM1 enhanced Gag production 10–15 fold in macrophages, but only marginally in T cells. Expression of both factors synergistically enhanced p24 production to levels approximately 10–40% of those detected in human cells. R5 viruses produced in rat T cells and macrophages were fully infectious. Conclusion The expression of both hCycT1 and hCRM1 appears to be fundamental to developing a rat model that supports robust propagation of HIV-1.