PLoS ONE (Oct 2009)

Characterization of the molecular determinants of primary HIV-1 Vpr proteins: impact of the Q65R and R77Q substitutions on Vpr functions.

  • Guillaume Jacquot,
  • Erwann Le Rouzic,
  • Priscilla Maidou-Peindara,
  • Marion Maizy,
  • Jean-Jacques Lefrère,
  • Vincent Daneluzzi,
  • Carlos M R Monteiro-Filho,
  • Duanping Hong,
  • Vicente Planelles,
  • Laurence Morand-Joubert,
  • Serge Benichou

DOI
https://doi.org/10.1371/journal.pone.0007514
Journal volume & issue
Vol. 4, no. 10
p. e7514

Abstract

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Although HIV-1 Vpr displays several functions in vitro, limited information exists concerning their relevance during infection. Here, we characterized Vpr variants isolated from a rapid and a long-term non-progressor (LTNP). Interestingly, vpr alleles isolated from longitudinal samples of the LTNP revealed a dominant sequence that subsequently led to diversity similar to that observed in the progressor patient. Most of primary Vpr proteins accumulated at the nuclear envelope and interacted with host-cell partners of Vpr. They displayed cytostatic and proapoptotic activities, although a LTNP allele, harboring the Q65R substitution, failed to bind the DCAF1 subunit of the Cul4a/DDB1 E3 ligase and was inactive. This Q65R substitution correlated with impairment of Vpr docking at the nuclear envelope, raising the possibility of a functional link between this property and the Vpr cytostatic activity. In contradiction with published results, the R77Q substitution, found in LTNP alleles, did not influence Vpr proapoptotic activity.