Literature DB >> 28848257

Solute carrier protein family 11 member 1 (Slc11a1) activation efficiently inhibits Leishmania donovani survival in host macrophages.

Nisha Singh1,2, Mallikarjuna Rao Gedda1, Neeraj Tiwari1, Suya P Singh1, Surabhi Bajpai1,3, Rakesh K Singh1.   

Abstract

Visceral leishmaniasis (kala-azar), a life threatening disease caused by L. donovani, is a latent threat to more than 147 million people living in disease endemic South East Asia region of the Indian subcontinent. The therapeutic option to control leishmanial infections are very limited, and at present comprise only two drugs, an antifungal amphotericin B and an antitumor miltefosine, which are also highly vulnerable for parasitic resistance. Therefore, identification and development of alternate control measures is an exigent requirement to control leishmanial infections. In this study, we report that functionally induced expression of solute carrier protein family 11 member 1 (Slc11a1), a transmembrane divalent cationic transporter recruited on the surface of phagolysosomes after phagocytosis of parasites, effectively inhibits Leishmania donovani growth in host macrophages. Further, the increased Slc11a1 functionality also resulted in increased production of NOx, TNF-α and IL-12 by activated macrophages. The findings of this study signify the importance of interplay between Slc11a1 expression and macrophages activation that can be effectively used to control of Leishmania growth and survival.

Entities:  

Keywords:  Leishmania; Macrophage; Slc11a1; Survival

Year:  2016        PMID: 28848257      PMCID: PMC5555910          DOI: 10.1007/s12639-016-0864-4

Source DB:  PubMed          Journal:  J Parasit Dis        ISSN: 0971-7196


  37 in total

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