Pregnancy enhances the innate immune response in experimental cutaneous leishmaniasis through hormone‐modulated nitric oxide production

The maintenance of host defense during pregnancy may depend on heightened innate immunity. We evaluated the immune response of pregnant hamsters during early infection with Leishmania (Viannia) panamensis , a cause of American cutaneous leishmaniasis. At 7 days post‐infection, pregnant animals showed a lower parasite burden compared with nonpregnant controls at the cutaneous infection site ( P =0.0098) and draining lymph node ( P =0.02). Resident peritoneal macrophages and neutrophils from pregnant animals had enhanced Leishmania killing capacity compared with nonpregnant controls ( P =0.018 each). This enhanced resistance during pregnancy was associated with increased expression of inducible NO synthase (iNOS) mRNA in lymph node cells ( P =0.02) and higher NO production by neutrophils ( P =0.0001). Macrophages from nonpregnant hamsters infected with L. panamensis released high amounts of NO upon estrogen exposure ( P =0.05), and addition of the iNOS inhibitor L‐N6‐(1‐iminoethyl) lysine blocked the induction of NO production ( P =0.02). Infected, nonpregnant females treated with estrogen showed a higher percentage of cells producing NO at the infection site than controls ( P =0.001), which correlated with lower parasite burdens ( P =0.036). Cultured macrophages or neutrophils from estrogen‐treated hamsters showed significantly increased NO production and Leishmania killing compared with untreated controls. iNOS was identified as the likely source of estrogen‐induced NO in primed and naïve macrophages, as increased transcription was evident by real‐time PCR. Thus, the innate defense against Leishmania infection is heightened during pregnancy, at least in part as a result of estrogen‐mediated up‐regulation of iNOS expression and NO production.