This work was supported by grants from Fundación para la Investig

This work was supported by grants from Fundación para la Investigación Sanitaria (FIS) del Ministerio de Sanidad y Consumo (FIS PI07/0236) and from Fundación para la Investigación y la prevención del SIDA en España (FIPSE 36644/07 and 36650/07). SR received grants from Fondo de Investigación Sanitaria (FIS) del Ministerio de Ciencia e Innovación (PI07/90201; PI08/0738), Instituto de Salud Carlos III (UIPY 1467/07) and Fundación para la Investigación y la Prevención del SIDA en España (FIPSE) (36650/07). 12 Octubre Hospital: Ivacaftor mouse M. I. González-Tomé and P. Rojo; Gregorio Marañón

Hospital: S. Resino, B. Larrú, R. Resino, J. M. Bellón, M. D. Gurbindo, M. L. Navarro, J. Saavedra and M. A. Muñoz-Fernández; La Paz Hospital: M. I. Isabel de José; Carlos III Hospital: P. Martín-Fontelos and M. J. Mellado; Niño Jesús Hospital: J. Martínez; Getafe Hospital: J. T. Ramos, S. Guillén, L. Prieto, B. Rubio and L. García San Miguel; Móstoles Hospital: M. A. Roa; Principe de Asturias Hospital: J. Beceiro; Leganés Hospital: C. Calvo. “
“After structured treatment interruption

(STI) of treatment for HIV-1, a fraction of patients maintain suppressed viral loads. Prospective identification of such patients might improve HIV-1 treatment, if selected patients are offered STI. We analysed the effect of previously identified genetic modulators of HIV-1 disease progression on patients’ ability to suppress viral replication after STI. Polymorphisms in the genes killer cell immunoglobulin-like receptor 3DLI (KIR3DL1)/KIR3DS1, human leucocyte antigen B (HLA-B) and HLA Complex P5 (HCP5), and this website a polymorphism affecting HLA-C surface expression were analysed in 130 Swiss HIV Cohort Study patients undergoing STI. Genotypes were correlated with viral load levels after STI. We observed a statistically Protein kinase N1 significant reduction in viral load

after STI in carriers of HLA-B alleles containing either the Bw480Thr or the Bw480Ile epitope (mean adjusted effect on post-STI viral load: −0.82 log HIV-1 RNA copies/ml, P < 0.001; and −1.12 log copies/ml, P < 0.001, respectively). No significant effects were detected for the other polymorphisms analysed. The likelihood of being able to control HIV-1 replication using a prespecified cut-off (viral load increase < 1000 copies/ml) increased from 39% in Bw4-negative patients to 53% in patients carrying Bw4-80Thr, and to 65% in patients carrying Bw4-80Ile (P = 0.02). These data establish a significant impact of HLA-Bw4 on the control of viral replication after STI. Antiretroviral therapy (ART) enables long-term control of HIV-1 infection through suppression of viral replication in the majority of treated individuals. This leads to substantial immune reconstitution, significantly delays morbidity and mortality, and transforms HIV infection into a chronic disease [1]. However, ART is not curative and life-long pharmacological treatment is required, which can lead to numerous adverse effects.

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