The immunomodulatory activity of ArtinM on the course of Cryptococcus gattii infection

Invasive fungal diseases are a global public health problem, that affects millions of individuals each year. Among the species that cause these diseases, Cryptococcus gattii is a major because affects immunosuppressed and immunocompetent individuals. C. gattii regulates the differentiation of helper (Th) T cells 1 (Th1) and 17 (Th17) by attenuating the proinflammatory response in the lungs. We know that the immunomodulatory capacity of ArtinM to induce the Th1 and Th17 immune response through IL-12 production by antigen presenting cells (APCs) and the CD4+ T cells activation by direct effect of ArtinM, these activities of ArtinM promoted the control of P. brasiliensis and C. albicans infection. Thus, we investigated the effects of prophylactic or therapeutic administration of ArtinM in the control of C. gattii infection. We found that C. gattii infection rapidly increase in the lungs and disseminate to the heart, liver, kidney, spleen, brain and blood after 21 days of infection. In the lung analysis, the cytokine profile showed low levels of proinflammatory cytokines and we observed an increase in the relative expression of the polarization markers for the M2 macrophages (Arginase-1 and YM-1) for all period. Given the regulatory ability of C. gattii on the host immune response, we evaluated the effect of prophylactic administration of ArtinM on the course of C. gattii infection. During 42 days of infection, the ArtinM-treated group had a reduction in the pulmonary fungal burden on days 28 and 35 post-infection, and levels of IFN-?, IL-17 and TNF-? were significantly increased in the ArtinM group. This immunomodulatory effect of prophylactic administration of ArtinM on the C. gattii infection led us to evaluate the effect of the therapeutic administration of ArtinM on the course of this infection. This new strategy for the ArtinM administration promoted a reduction in the lung fungal burden of C. gattii after 21 days of infection compared to control group. Therapeutic administration of ArtinM was able to increase the absolute number of neutrophils and lymphocytes in the peripheral blood of infected mice, but the cytokine levels did not differ between the ArtinM and control groups. In addition, the ArtinM-treated group showed decrease of the CD4+ T cell frequency in the spleen. Considering the immunomodulatory effect, the prophylactic or therapeutic administration of ArtinM promoted a partial control of C. gattii infection, and instigate us to investigate the association of ArtinM and Fluconazole. We found that the treatment with ArtinM in combination with fluconazole also promoted a reduction in the pulmonary fungal burden, which suggested that ArtinM works well inA b s t r a c t | xi association with antifungal drugs. Therefore, our data showed that the immunomodulatory activity of ArtinM, via prophylactic or therapeutic administration, was evidenced in the course of C. gattii infection and contributed the host immune response to reduce the lung fungal burden (AU)