Abstract
Visceral leishmaniasis (VL) is characterized by expansion of myeloid cells in the liver and spleen, which leads to a severe splenomegaly associated with higher risk of mortality. This increased cellularity is thought to be a consequence of recruitment of cells to the viscera. We studied whether the local proliferation of splenic myeloid cells contributes to increased splenic cellularity. We found that a monocyte-like population of adherent splenic cells from Leishmania donovani-infected hamsters had enhanced replicative capacity ex vivo and in vivo (BrdU incorporation, p<0.0001). In vitro assays demonstrated that proliferation was more pronounced in the proinflammatory M1 environment and that intracellular infection prevented proliferation. Secondary analysis of the published splenic transcriptome in the hamster model of progressive VL revealed a gene expression signature that included division of tumoral cells (Z = 2.0), cell cycle progression (Z = 2.3), hematopoiesis (Z = 2.8), proliferation of stem cells (Z = 2.5) and overexpression of proto-oncogenes. Regulators of myeloid cell proliferation were predicted in-silico (CSF2, TLR4, IFNG, IL-6, IL-4, RTK signaling, and STAT3). The in-silico prediction was confirmed with chemical inhibitors of PI3K/AKT, MAPK and STAT3 which decreased splenic myeloid cell division ex vivo. Hamsters infected with L. donovani treated with a STAT3 inhibitor had reduced in situ splenic myeloid proliferation (p = 0.03) and parasite burden. We conclude that monocyte-like myeloid cells have increased STAT3-dependent proliferation in the spleen of hamsters with visceral leishmaniasis and that inhibition of STAT3 reduces myeloid cell proliferation and parasite burden.
Highlights
Visceral leishmaniasis is caused by infection with the intracellular protozoan parasite Leishmania. donovani or L. infantum
Inhibition of signal transducer and activator of transcription 3 (STAT3) signaling reduced in situ proliferation, accumulation of splenic myeloid cells, and splenic parasite loads
We investigated an established animal model that mimics the progressive nature of human Visceral leishmaniasis (VL) to determine whether in situ myeloid cell proliferation contributes their accumulation in the spleen after the infection
Summary
Visceral leishmaniasis is caused by infection with the intracellular protozoan parasite Leishmania. donovani or L. infantum. Diagnostic and post-mortem splenic biopsies of patients with VL demonstrate accumulation of myeloid cells and plasma cells in the white and red pulp of the spleen [1,2,3,4]. Massive splenomegaly is associated with increased risk of mortality in VL patients [4]. The mechanism(s) that drive accumulation of myeloid cells in the spleen in VL have not been clearly defined. It has been thought to be due to excessive recruitment of mature inflammatory myeloid cells from the bone marrow [5]. Mechanisms such as extramedullary hematopoiesis and local cell proliferation may contribute to this splenic myeloid cell accumulation
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