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IL-10 production from dendritic cells is associated with DC SIGN in human leprosy

Publication Type : Journal Article

Publisher : Elsevier BV

Source : Immunobiology

Url : https://doi.org/10.1016/j.imbio.2013.05.004

Keywords : DC SIGN, Leprosy, ManLAM, Mycobacterium leprae , NF-κB, p300

Campus : Faridabad

School : School of Medicine

Department : Dermatology

Year : 2013

Abstract : The defective antigen presenting ability of antigen presenting cells (APCs) modulates host cytokines and co-stimulatory signals that may lead to severity of leprosy. In the present study, we sought to evaluate the phenotypic features of APCs along with whether DC SIGN (DC-specific intercellular adhesion molecule-grabbing nonintegrin) influences IL-10 production while moving from tuberculoid (BT/TT) to lepromatous (BL/LL) pole in leprosy pathogenesis. The study revealed an increased expression of DC SIGN on CD11c+ cells from BL/LL patients and an impaired form of CD83 (∼50kDa). However, the cells after treatment with GM-CSF+IL-4+ManLAM showed an increased expression of similar form of CD83 on DCs. Upon treatment with ManLAM, DCs were found to show increased nuclear presence of NF-κB, thus leading to higher IL-10 production. High IL-10 production from ManLAM treated PBMCs further suggested the role of DC SIGN in subverting the DCs function towards BL/LL pole of leprosy. Anti-DC SIGN treatment resulting in restricted nuclear ingression of NF-κB as well as its acetylation along with enhanced T cell proliferation validated our findings. In conclusion, Mycobacterium leprae component triggers DC SIGN on DCs to induce production of IL-10 by modulating intracellular signalling pathway at the level of transcription factor NF-κB towards BL/LL pole of disease.

Cite this Research Publication : Sudhir Kumar, Raza Ali Naqvi, Ajaz A. Bhat, Richa Rani, Riyasat Ali, Abhishek Agnihotri, Neena Khanna, D.N. Rao, IL-10 production from dendritic cells is associated with DC SIGN in human leprosy, Immunobiology, Elsevier BV, 2013, https://doi.org/10.1016/j.imbio.2013.05.004

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