Tumour Necrosis Factor-alpha (TNF-α) and its soluble receptor type1 (sTNFR I) in human active and healed leishmaniases.

Abstract

The role of tumour necrosis factor-alpha (TNF-α) is not fully understood in human leishmaniasis. We analysed the alterations in the levels of TNF-α, soluble TNF receptor type 1 (sTNFR I), IL-17 and IL-22 productions in active and healed leishmaniases. Blood samples were collected from volunteers with active cutaneous leishmaniasis (ACL), the same subjects after lesion healing (healed CL=HCL), volunteers with active visceral leishmaniasis (AVL), healed VL (HVL) and healthy controls. Levels of cytokines were titrated on Leishmania Ag-stimulated PBMC culture. The mean level of TNF-α production from stimulated cells was significantly higher in ACL than controls (P<0·001) and significantly reduced after treatment in HCL volunteers (P<0·05). The mean level of sTNFR I production was significantly higher in ACL than controls (P<0·001) and significantly reduced after treatment in HCL volunteers (P<0·05). The mean level of IL-22 production in AVL was significantly higher than controls (P<0·05) and was significantly lower in HVL compared with AVL (P<0·001) and controls (P<0·05). The levels of TNF-α (P=0·0025) and sTNFR I (P<0·01) productions from PBMCs showed significant decreasing trend after treatment in each CL volunteer. Reduction in TNF-α is associated with clinical response to treatment and healing of CL lesions due to L.major.