PLoS ONE (Jan 2014)

A regulatory polymorphism in HAVCR2 modulates susceptibility to HIV-1 infection.

  • Manuela Sironi,
  • Mara Biasin,
  • Federica Gnudi,
  • Rachele Cagliani,
  • Irma Saulle,
  • Diego Forni,
  • Veronica Rainone,
  • Daria Trabattoni,
  • Micaela Garziano,
  • Francesco Mazzotta,
  • Luis Miguel Real,
  • Antonio Rivero-Juarez,
  • Antonio Caruz,
  • Sergio Lo Caputo,
  • Mario Clerici

DOI
https://doi.org/10.1371/journal.pone.0106442
Journal volume & issue
Vol. 9, no. 9
p. e106442

Abstract

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The HAVCR2 gene encodes TIM-3, an immunoglobulin superfamily member expressed by exhausted CD8+ T cells during chronic viral infection. We investigated whether genetic variation at HAVCR2 modulates the susceptibility to HIV-1 acquisition; specifically we focused on a 3' UTR variant (rs4704846, A/G) that represents a natural selection target. We genotyped rs4704846 in three independent cohorts of HIV-1 exposed seronegative (HESN) individuals with different geographic origin (Italy and Spain) and distinct route of exposure to HIV-1 (sexual and injection drug use). Matched HIV-1 positive subjects and healthy controls were also analyzed. In all case-control cohorts the minor G allele at rs4704846 was more common in HIV-1 infected individuals than in HESN, with healthy controls showing intermediate frequency. Results from the three association analyses were combined through a random effect meta-analysis, which revealed no heterogeneity among samples (Cochrane's Q, p value = 0.89, I2 = 0) and yielded a p value of 6.8 ×10(-4). The minor G allele at rs4704846 was found to increase HAVCR2 expression after in vitro HIV-1 infection. Thus, a positively selected polymorphism in the 3' UTR, which modulates HAVCR2 expression, is associated with the susceptibility to HIV-1 infection. These data warrant further investigation into the role of TIM-3 in the prevention and treatment of HIV-1/AIDS.