Osteopontin in the host response to Leishmania amazonensis

Emilie Giraud,Evie Melanitou,Jean-Hervé Colle,Laurence Fiette,Despoina Smirlis,Eline Rouault

doi:10.1186/s12866-019-1404-z

Emilie Giraud, Evie Melanitou + Show 4 more

Open Access

https://doi.org/10.1186/s12866-019-1404-z

Copy DOI

Abstract

BackgroundLeishmania (L.) spp are intracellular eukaryotic parasites responsible for cutaneous or visceral leishmaniasis, replicating predominantly in macrophages (MF). In C57BL/6 mice virulence with L. amazonensis has been associated with inhibition of Th1 immune responses and an uncontrolled lesion development, whereas DBA/2 mice control any lesion. Parasitic clearance by the MFs requires the activation of proper immune responses. One of the immune related genes expressed in immune cells including MF, codes for osteopontin (OPN). OPN is a secreted glycoprotein, acting as an immune regulator. Its implication in promoting Th1 immunity in response to infectious microorganisms and its known protective effect against viral and bacterial infections via activation of the immune response, render OPN a molecule of interest in the study of the host response to L. amazonensis.ResultsWe examined the host response to L. amazonensis of opn mutant and wild type C57BL/6 mice. Bone marrow derived MFs were infected with the parasites in vitro, and opn mutant and wild type mice were inoculated in vivo by intradermal injection in the ears. The DBA/2 strain known to control L. amazonensis infection was also used for comparison. Our data indicate that the parasites increased opn gene expression and OPN protein while parasitic proliferation was contained in the presence of OPN. In the presence of parasites the expression of inflammation-related transcripts was inhibited. Interleukin-1-beta (IL-1β), and transcripts of the NLR–family (NLRC4, NLRP3) were down regulated after L. amazonensis infection. In the absence of OPN, the inhibition by the parasites of IL-1β transcripts was less efficient and a pyroptosis-like cell phenotype was detected in vitro, suggesting a central role of OPN in the host-response to L. amazonensis. Similarly, in vivo, in the absence of OPN, while the clinical inflammatory phenotype is more severe, an increase of these transcripts was observed.ConclusionsL. amazonensis infection induces opn gene expression and protein, which in turn participates in shaping the host response to the parasites, seemingly by decreasing the activation of inflammation. OPN, further evaluated as a target for Leishmaniasis control represents an additional interest in improving vaccination strategies against the parasites.

Highlights

Leishmania (L.) spp are intracellular eukaryotic parasites responsible for cutaneous or visceral leishmaniasis, replicating predominantly in macrophages (MF)
OPN restricts parasitic proliferation in vitro To gain a first insight into a potential role of OPN during L. amazonensis infection, we evaluated the replication of the parasites in Bone marrow-derived Macrophage (BMF) from mice lacking the opn gene
Evaluation of parasite intensity confirmed increased parasite numbers in the opn mutant cells (Fig. 1c), in particular, mean intensity and parasite crowding differences between the opn WT and KO macrophages were more pronounced at 48 h p.i. (P = 0.0075, CI 95% and P < 0.05, CI 95% respectively), (Fig. 1c) and Additional file 2: Table S1A)

Summary

Introduction

Leishmania (L.) spp are intracellular eukaryotic parasites responsible for cutaneous or visceral leishmaniasis, replicating predominantly in macrophages (MF). Leishmania parasites affect a variety of organs and tissues depending on the Giraud et al BMC Microbiology (2019) 19:32 midgut [3, 4] This is the replicative form of the parasite in the insect host. This stage is marked by the arrest of replication and subsequent migration of the parasites to the insect proboscides whereas the metacyclogenesis takes place resulting to the differentiated infective form: the metacyclic promastigotes [5, 6] The latter, once delivered into the mammal dermis during the blood feeding bite of the female insect, differentiate as amastigotes and are mainly found within the resident dermal macrophages (MF) [7] and in dendritic cells (DC) [8]. The host’s immune response may lead to resistance or susceptibility to the infection, while in mouse strains the response to Leishmania spp is dependent upon the genetic background

Methods

Results

Discussion

Conclusion