Abstract
BackgroundIn a previous study, progesterone treatment of female monkeys immunized with live, attenuated SHIV89.6 abrogated the generally consistent protection from vaginal simian immunodeficiency virus (SIV) challenge. The mechanisms responsible for the loss of protection remain to be defined. The objective of the present study was to determine whether Depo-Provera® administration alters protection from intravenous SIV challenge in SHIV-immunized female macaques.Methods and FindingsTwo groups of female macaques were immunized with attenuated SHIV89.6 and then challenged intravenously with SIVmac239. Four weeks before challenge, one animal group was treated with Depo-Provera®, a commonly used injectable contraceptive progestin. As expected, SHIV-immunized monkeys had significantly lower peak and set-point plasma viral RNA levels compared to naïve controls, but in contrast to previously published findings with vaginal SIV challenge, the Depo-Provera® SHIV-immunized animals controlled SIV replication to a similar, or even slightly greater, degree than did the untreated SHIV-immunized animals. Control of viral replication from week 4 to week 20 after challenge was more consistent in the progesterone-treated, SHIV-immunized animals than in untreated, SHIV-immunized animals. Although levels of interferon-γ production were similar, the SIV-specific CD8+ T cells of progesterone-treated animals expressed more functions than the anti-viral CD8+ T cells from untreated animals.ConclusionsDepo-Provera® did not diminish the control of viral replication after intravenous SIV challenge in female macaques immunized with a live-attenuated lentivirus. This result contrasts with the previously reported effect of Depo-Provera® on protection from vaginal SIV challenge and strongly implies that the decreased protection from vaginal challenge is due to effects of progesterone on the genital tract rather than to systemic effects. Further, these results demonstrate that the effects of hormonal contraceptives on vaccine efficacy need to be considered in the context of testing and use of an AIDS vaccine.
Highlights
In the simian immunodeficiency virus (SIV) model of AIDS, only live-attenuated viruses consistently confer reliable protection against intravaginal virus inoculation [1,2]
Depo-ProveraH did not diminish the control of viral replication after intravenous SIV challenge in female macaques immunized with a live-attenuated lentivirus
These results demonstrate that the effects of hormonal contraceptives on vaccine efficacy need to be considered in the context of testing and use of an AIDS vaccine
Summary
In the simian immunodeficiency virus (SIV) model of AIDS, only live-attenuated viruses consistently confer reliable protection against intravaginal virus inoculation [1,2]. Administration of Depo-ProveraH to macaques in the commonly used dosage, 30 mg, leads to epithelial thinning [9], but genital tract epithelial thinning has not been found in women using this contraceptive at a lower dose [10,11]. It is unclear if this mechanism of enhancing susceptibility to SIV infection is relevant to women. Progesterone treatment of female monkeys immunized with live, attenuated SHIV89.6 abrogated the generally consistent protection from vaginal simian immunodeficiency virus (SIV) challenge. The objective of the present study was to determine whether Depo-ProveraH administration alters protection from intravenous SIV challenge in SHIV-immunized female macaques
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