Objective: It is unclear whether the ability to respond to vaccines is restored by antiretroviral therapy. We evaluated the influenza-specific immune responses elicited by a virosomal vaccine in HIV-infected children on long-term successful highly active antiretroviral therapy (HAART). Methods: This was an observational, prospective, open-label study enrolling 24 HIV-infected, HAART-treated (85 months’ mean exposure), vaccine-naive children (median age = 11.9 years) and 14 age- and gender-matched healthy controls. Mean CD4 T-cell counts (.900 cells/mL) and percentages (.37%) were comparable. The HIV RNA level was ,50 copies/mL in all patients. Children received a single dose of trivalent virosome-adjuvanted influenza vaccine. A/H3N2-, A/H1N1-, and B-antigen–specific antibody (Ab) titers and subclasses and vaccine-specific interferon-g (IFNg)– and interleukin (IL)-2–producing T lymphocytes were analyzed at baseline and 1 and 6 months after immunization. Results: Seroconversion ($4-fold Ab titer raise in .40% of patients) and seroprotection (Ab titer $1:40 in .70% of patients) was achieved at 1 month in both groups; however, fewer HIV-infected children fulfilled these criteria. The A/H3N2- and A/H1N1-specific Ab geometric mean titers were lower in HIV-infected children compared with healthy controls at 1 and 6 months; interestingly, a boost in vaccine-specific IgG3 T helper 1 type Ab was seen in healthy controls alone. Finally, vaccine specific-IFNg– and IL-2–producing T lymphocytes were reduced at both time points in HIV-infected children compared with healthy controls. Conclusions: One injection of virosomal-adjuvanted influenza vaccine stimulates good immune responses, although the humoral and cellular immune responses are reduced in HIV-infected children compared to healthy children. This indicates that immunologic function impairments may persist upon HIV infection even if HIV-positive viremia is suppressed and immune recovery seems to be achieved.
Humoral and cellular response to influenza vaccine in HIV-infected children with full viroimmunologic response to antiretroviral therapy / A. Viganò, G.V. Zuccotti, M. Pacei, P. Erba, E. Castelletti, V. Giacomet, A. Amendola, E. Pariani, E. Tanzi, M. Clerici. - In: JOURNAL OF ACQUIRED IMMUNE DEFICIENCY SYNDROMES. - ISSN 1525-4135. - 48:3(2008), pp. 289-296.
Humoral and cellular response to influenza vaccine in HIV-infected children with full viroimmunologic response to antiretroviral therapy
G.V. Zuccotti;M. Pacei;P. Erba;E. Castelletti;V. Giacomet;A. Amendola;E. Pariani;E. Tanzi;M. Clerici
2008
Abstract
Objective: It is unclear whether the ability to respond to vaccines is restored by antiretroviral therapy. We evaluated the influenza-specific immune responses elicited by a virosomal vaccine in HIV-infected children on long-term successful highly active antiretroviral therapy (HAART). Methods: This was an observational, prospective, open-label study enrolling 24 HIV-infected, HAART-treated (85 months’ mean exposure), vaccine-naive children (median age = 11.9 years) and 14 age- and gender-matched healthy controls. Mean CD4 T-cell counts (.900 cells/mL) and percentages (.37%) were comparable. The HIV RNA level was ,50 copies/mL in all patients. Children received a single dose of trivalent virosome-adjuvanted influenza vaccine. A/H3N2-, A/H1N1-, and B-antigen–specific antibody (Ab) titers and subclasses and vaccine-specific interferon-g (IFNg)– and interleukin (IL)-2–producing T lymphocytes were analyzed at baseline and 1 and 6 months after immunization. Results: Seroconversion ($4-fold Ab titer raise in .40% of patients) and seroprotection (Ab titer $1:40 in .70% of patients) was achieved at 1 month in both groups; however, fewer HIV-infected children fulfilled these criteria. The A/H3N2- and A/H1N1-specific Ab geometric mean titers were lower in HIV-infected children compared with healthy controls at 1 and 6 months; interestingly, a boost in vaccine-specific IgG3 T helper 1 type Ab was seen in healthy controls alone. Finally, vaccine specific-IFNg– and IL-2–producing T lymphocytes were reduced at both time points in HIV-infected children compared with healthy controls. Conclusions: One injection of virosomal-adjuvanted influenza vaccine stimulates good immune responses, although the humoral and cellular immune responses are reduced in HIV-infected children compared to healthy children. This indicates that immunologic function impairments may persist upon HIV infection even if HIV-positive viremia is suppressed and immune recovery seems to be achieved.
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