The establishment of an effective and regulated immune response d

The establishment of an effective and regulated immune response directed against Leishmania is critical for resolution of infection PI3K Inhibitor Library in vivo and limitation of pathology. Leishmaniasis is considered as an emergent and re-emergent

disease and encompasses visceral and tegumentary forms, including cutaneous and mucocutaneous forms [1–3]. Infection with the protozoa parasite Leishmania braziliensis can cause several clinical forms of disease, and in Brazil it is responsible for at least two major clinical forms: cutaneous (CL) and mucosal (ML) leishmaniasis [1,2]. Human tegumentary leishmaniasis is usually limited to the skin and lymphatic system, but it may recur in the mucous membranes of the mouth, nose or pharynx in ML [4,5]. In experimental CL, development of protective immunity is dependent upon the generation Opaganib cost of specific cytokine-producing T cells with a regulated T helper type 1 (Th1)-like profile [6,7]. In the majority of CL patients, effective cell-mediated immunity, as evidenced by a positive delayed-type hypersensitivity (DTH) reaction [8,9], as well as production of interferon (IFN)-γ and tumour necrosis factor (TNF)-α by peripheral T cells and cutaneous lesion

cells found in inflammatory infiltrates, show the same profile seen in experimental models [10–13]. IFN-γ is an important cytokine that activates infected macrophages to check eliminate parasites and improve antigen processing and presentation, as well as aiding in creating an effective microenvironment for generation of Th1 T cells. At the same time, the lack of proper regulation of this response may lead to the formation of exacerbated lesions, as seen in mucosal disease [12–14]. Recently, we demonstrated that Leishmania-specific T cells from CL patients displayed a regulated inflammatory T cell response

as measured by correlation between the frequency of proinflammatory (IFN-γ and TNF-α) and anti-inflammatory (IL-10) cytokine-producing cells [10,13]. Interestingly, our group also observed positive correlations between immunological and clinical measurements in CL patients. This work demonstrated a positive correlation between the Montenegro skin test (MST) size and the frequency of recent activated CD4+ T cells analysed ex vivo. Moreover, the larger the lesions, the higher the frequencies of inflammatory cytokine (IFN-γ or TNF-α)-producing Leishmania-specific lymphocytes [15]. Given that specific T cell responses against Leishmania antigens play a critical role in the formation of protective and pathogenic immune responses in human leishmaniasis, it is clear that the elucidation of which T cell subpopulations are involved in the response will aid in the identification of possible dominant antigens used by the human immune response.

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