In fact, recent studies have described that neutrophils recruited to the site of Leishmania infections internalize the parasite [26, 27], and saliva enhances neutrophil migration to the site of infection [28]. Previous studies have also observed that parasite internalization
delays the apoptosis of neutrophils and induces MIP-1β release, which recruits macrophages to the site of infection. The migrated macrophages ingest the infected apoptotic neutrophils, which stimulates the release of TGF-β and PGE2 and downregulates https://www.selleckchem.com/products/i-bet-762.html macrophage activation consequently contributing to Leishmania infection establishment [26, 27]. Together, these findings suggest that the parasites use granulocytes as “Trojan horses” to attack the macrophages [26]. In this context, the inhibition of both neutrophils and macrophages by saliva pre-exposure as described in the present investigation may represent an additional mechanism to explain the ability of Phlebotomine saliva pre-inoculation to protect mice against Leishmania infection. Stressing the relevance of our finding, we demonstrated for the first time that Phlebotomine
saliva increases regulatory T cell (Treg) recruitment to the lesion AMN-107 site. We demonstrated that inoculation of saliva once (SGE-1X) in the absence of parasites induces the recruitment of high numbers of CD4+CD25+ cells that, although being commonly accepted phenotype of Tregs also could be related to activated cells. Accordingly, parasites co-inoculated with saliva (SGE-1X) caused an increase in the recruitment of CD4+Foxp3+ cells to the infection site, suggesting that saliva of L. longipalpis increases Tregs during the infection. Despite the fact that the parasite alone is able to induce Treg migration, saliva strengthens this migration, which maintains the persistence of the parasite in the chronic phase of infection, and suggests that the recruitment of Tregs by the saliva may contribute to the C646 mw infectivity of Leishmania. In fact, increased
numbers of parasites at later time points were observed in the ears of mice co-inoculated with saliva and parasite, which corresponds to the point at which the disease becomes resolved and the parasitic burden decreases in oxyclozanide the ears of mice infected with parasite only. Previous studies have also demonstrated that during infection with L. major, the persistence of the pathogen within the skin of L. major-resistant mice is controlled by an endogenous population of Treg cells that act to suppress the immune response against L. major. Treg cells are involved in maintaining the latency status of Leishmania infections and facilitate the survival of the parasite [29]. Our group reported that CD4+CD25+ T cells present in skin lesions of patients with cutaneous leishmaniasis display phenotypic and functional characteristics of natural Treg cells [30]. Thus, Treg cells induced by saliva play an important role in modulating the immune response during Leishmania infections.