<i>Trypanosoma musculi</i> Infection in Mice Critically Relies on Mannose Receptor–Mediated Arginase Induction by a <i>Tb</i>KHC1 Kinesin H Chain Homolog

Nzoumbou‐Boko, Romaric; Muylder, Géraldine De; Semballa, Silla; Lecordier, Laurence; Dauchy, Frédéric‐Antoine; Gobert, Alain P.; Holzmüller, Philippe; Lemesre, Jean-Loup; Bras-Gonçalves, Rachel; Barnabé, Christian; Courtois, Pierrette; Daulouède, Sylvie; Beschin, Alain; Pays, Étienne; Vincendeau, Philippe

doi:10.4049/jimmunol.1700179

Cited by 9 publications

(10 citation statements)

References 44 publications

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“…On the contrary, previous studies using Yersinia pseudotuberculosis showed that partial inhibition of CD209 between the interaction of hDCS and Y. pseudotuberculosis was achieved only when the triple combination of inhibitors (antireceptor antibodies, mannan oligosaccharide, and purified LPS core) was employed. In this study, even the use of a single inhibitor provided partial protection against Toxoplasma infection as was also observed in Trypanosoma musculi infection (69).…”

Section: Discussionsupporting

confidence: 75%

“…Similar results were reported in a study involving T. musculi and T. cruzi whose results showed enhanced survival in macrophages, whereas receptor blockade decreased parasite growth (69). A number of studies using different antibodies and different strains of knock-out mice have yielded a wide array of contradicting results (11,(70)(71)(72)(73)(74).…”

Section: Discussionsupporting

confidence: 72%

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CD209 C-Type Lectins Promote Host Invasion, Dissemination, and Infection of Toxoplasma gondii

Njiri

Zhang

et al. 2020

Front. Immunol.

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Toxoplasma gondii, the causative agent of toxoplasmosis and a major opportunistic parasite associated with AIDS, is able to invade host cells of animals and humans. Studies suggested that the ability of host invasion by the tachyzoite, the infectious form of T. gondii, is essential for the pathogenicity to promote its dissemination to other parts of animal hosts. However, the detailed molecular mechanisms for host invasion and dissemination of the parasites are not clear. On the other hand, viruses and bacteria are able to interact with and hijack DC-SIGN (CD209) C-type lectin on antigen presenting cells (APCs), such as dendritic cells and macrophages as the Trojan horses to promote host dissemination. In this study, we showed that invasion of T. gondii into host cells was enhanced by this parasite-CD209 interaction that were inhibited by ligand mimickingoligosaccharides and the anti-CD209 antibody. Furthermore, covering the exposures of DC-SIGN by these oligosaccharides reduced parasite burden, host spreading and mortality associated with T. gondii infection. These results suggested that interaction of T. gondii to APCs expressing DC-SIGN might promote host dissemination and infection. Can the blockage of this interaction with Mannan and/or anti-CD209 antibody be developed as a prevention or treatment method for T. gondii infection?

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Section: Discussionsupporting

confidence: 75%

Section: Discussionsupporting

confidence: 72%

CD209 C-Type Lectins Promote Host Invasion, Dissemination, and Infection of Toxoplasma gondii

Njiri

Zhang

et al. 2020

Front. Immunol.

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“…Treatment with mannose also reduced parasitemia in mice infected by T. musculi . However, whereas TbKHC1 facilitates Tbb parasitemia via the SIGN-R1 receptor, the MMR receptor was apparently the main target of T. musculi ES ( 138 ). This suggests that kinesin heavy chain-related proteins play similar roles in promoting infection in two genetically distant trypanosomes, via macrophage arginase induction, following distinct CLR targeting.…”

Section: Macrophage L -Arginine Metabolism Dysregumentioning

confidence: 99%

Trypanosomatid Infections: How Do Parasites and Their Excreted–Secreted Factors Modulate the Inducible Metabolism of l-Arginine in Macrophages?

et al. 2018

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Mononuclear phagocytes (monocytes, dendritic cells, and macrophages) are among the first host cells to face intra- and extracellular protozoan parasites such as trypanosomatids, and significant expansion of macrophages has been observed in infected hosts. They play essential roles in the outcome of infections caused by trypanosomatids, as they can not only exert a powerful antimicrobial activity but also promote parasite proliferation. These varied functions, linked to their phenotypic and metabolic plasticity, are exerted via distinct activation states, in which l-arginine metabolism plays a pivotal role. Depending on the environmental factors and immune response elements, l-arginine metabolites contribute to parasite elimination, mainly through nitric oxide (NO) synthesis, or to parasite proliferation, through l-ornithine and polyamine production. To survive and adapt to their hosts, parasites such as trypanosomatids developed mechanisms of interaction to modulate macrophage activation in their favor, by manipulating several cellular metabolic pathways. Recent reports emphasize that some excreted–secreted (ES) molecules from parasites and sugar-binding host receptors play a major role in this dialog, particularly in the modulation of the macrophage’s inducible l-arginine metabolism. Preventing l-arginine dysregulation by drugs or by immunization against trypanosomatid ES molecules or by blocking partner host molecules may control early infection and is a promising way to tackle neglected diseases including Chagas disease, leishmaniases, and African trypanosomiases. The present review summarizes recent knowledge on trypanosomatids and their ES factors with regard to their influence on macrophage activation pathways, mainly the NO synthase/arginase balance. The review ends with prospects for the use of biological knowledge to develop new strategies of interference in the infectious processes used by trypanosomatids, in particular for the development of vaccines or immunotherapeutic approaches.

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Section: Introductionmentioning

confidence: 99%

“…The secretome, (excreted/secreted factors), of trypanosomes is a complex mixture of proteins, carbohydrates and lipids excreted from the surface of the parasite or secreted via exocytotic vesicles by a parasite-specific organelle called the flagellar pocket. [12][13][14] Some of these components are implicated in T brucei evasion of host innate response 15,16 and others in the virulence process. [17][18][19][20][21] Because of the fundamental role of DCs during trypanosomiasis but limited human data, we investigated the effects of T gambiense and its secretome on human monocytes-derived DCs.…”

mentioning

confidence: 99%

Trypanosoma brucei gambiense excreted/secreted factors impair lipopolysaccharide‐induced maturation and activation of human monocyte‐derived dendritic cells

Dauchy

Contin‐Bordes

Nzoumbou‐Boko

et al. 2019

Parasite Immunology

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Trypanosoma brucei gambiense, an extracellular eukaryotic flagellate parasite, is the main etiological agent of human African trypanosomiasis (HAT) or sleeping sickness. Dendritic cells (DCs) play a pivotal role at the interface between innate and adaptive immune response and are implicated during HAT. In this study, we investigated the effects of T gambiense and its excreted/secreted factors (ESF) on the phenotype of human monocyte‐derived DCs (Mo‐DCs). Mo‐DCs were cultured with trypanosomes, lipopolysaccharide (LPS), ESF derived from T gambiense bloodstream strain Biyamina (MHOM/SD/82), or both ESF and LPS. Importantly, ESF reduced the expression of the maturation markers HLA‐DR and CD83, as well as the secretion of IL‐12, TNF‐alpha and IL‐10, in LPS‐stimulated Mo‐DCs. During mixed‐leucocyte reactions, LPS‐ plus ESF‐exposed DCs induced a non‐significant decrease in the IFN‐gamma/IL‐10 ratio of CD4 + T‐cell cytokines. Based on the results presented here, we raise the hypothesis that T gambiense has developed an immune escape strategy through the secretion of paracrine mediators in order to limit maturation and activation of human DCs. The identification of the factor(s) in the T gambiense ESF and of the DCs signalling pathway(s) involved may be important in the development of new therapeutic targets.

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Trypanosoma musculi Infection in Mice Critically Relies on Mannose Receptor–Mediated Arginase Induction by a TbKHC1 Kinesin H Chain Homolog

Cited by 9 publications

References 44 publications

CD209 C-Type Lectins Promote Host Invasion, Dissemination, and Infection of Toxoplasma gondii

CD209 C-Type Lectins Promote Host Invasion, Dissemination, and Infection of Toxoplasma gondii

Trypanosomatid Infections: How Do Parasites and Their Excreted–Secreted Factors Modulate the Inducible Metabolism of l-Arginine in Macrophages?

Trypanosoma brucei gambiense excreted/secreted factors impair lipopolysaccharide‐induced maturation and activation of human monocyte‐derived dendritic cells

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