The capacity of LaAg to induce IL-10 secretion in PBMCs obtained from ATL patients, together with the generation of short-lived IFN-γ-producing CD4+T cells, could result in equilibrium between inflammatory and anti-inflammatory responses, allowing parasite clearance and lesion resolution, as observed

in the immunotherapeutic protocols tested so far. Currently we are performing multiparametric flow cytometry studies with PBMCs obtained from CL, ML and disseminated CL patients infected with L. braziliensis before and after therapy, in an attempt to find better immune parameters that could correlate with the clinical manifestation and effective healing of lesions. It is to be expected that understanding the induction of Leishmania-specific multifunctional T cells in the diverse clinical manifestations of ATL will help understanding of the complex immunopathogenesis of this neglected tropical disease, and bring new and important parameters selleckchem that can find more help in the selection of antigens or adjuvants that will have better chances of working in prophylactic or therapeutic interventions against human leishmaniasis. Based on our data, we are

very tempted to suggest that the quality of the Th1 response induced by L. amazonensis antigens, involving a poor generation of multifunctional CD4+T cells and a high proportion of IFN-γ single-positive CD4+T cells, in association with its well-known capacity of inducing IL-10 production [45–47,51,53,54], can be involved in the mechanisms responsible for the susceptibility to L. amazonensis observed in ATL patients and in experimental models. In this sense we have shown,

for the first time, that multiparametric flow cytometry can bring new Protein kinase N1 important aspects to the studies of ATL immunopathogenesis, and reinforce the importance of evaluating not just the magnitude, but the quality of a pathogen-specific Th1 immune response by multiple parameters at a single-cell level, to find better and more effective biomarkers of disease and protection. We thank the following funding agencies: Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq – PAPES V), Fundação Carlos Chagas Filho de Amparo à Pesquisa do Estado do Rio de Janeiro (FAPERJ-APQ1) and Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) for fellowship. We are also grateful to Dr Joseli de Oliveira Ferreira for critical reading of the manuscript. None. “
“Citation Martínez-García EA, Sánchez-Hernández PE, Chavez-Robles B, Nuñez-Atahualpa L, Martín-Márquez BT, Arana-Argaez VE, García-Iglesias T, González-López L, Gamez-Nava JI, Petri MH, Velazquez-Rodriguez J, Salazar-Paramo M, Davalos-Rodriguez IP, Daneri-Navarro A, Vázquez-Del Mercado M. The distribution of CD56dimCD16+ and CD56brightCD16− Cells are associated with prolactin levels during pregnancy and menstrual cycle in healthy women.