Inflammatory and Pro-resolving Lipids in Trypanosomatid Infections: A Key to Understanding Parasite Control

López‐Muñoz, Rodrigo; Molina-Berríos, Alfredo; Campos‐Estrada, Carolina; Abarca-Sanhueza, Patricio; Urrutia-Llancaqueo, Luis; Pena-Espinoza, Miguel Angel; Maya, Juan Diego

doi:10.3389/fmicb.2018.01961

Cited by 22 publications

(16 citation statements)

References 146 publications

(174 reference statements)

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“…(17) In the present study, chagasic patients (CML+CIM), who also presented with a higher density of Gal-3, showed a percentage of collagen significantly greater than the NC Group, which corroborates the literature, since it has already been demonstrated in mice that T. cruzi can be the factor direct or indirectly responsible for molecular modification in different tissues and organs, enabling the induction of cell lesions, inflammatory response, and fibrosis mediated by Gal-3. (27) Nonetheless, our study was the first to associate Gal-3 with fibrosis in Chagas disease in humans.…”

Section: ❚ Discussionmentioning

confidence: 75%

Although with intact mucosa at colonoscopy, chagasic megacolons have an overexpression of Gal-3

Garvil

Furtado

Lima

et al. 2020

Einstein (São Paulo)

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Objective: To evaluate the density of anti-galectin-3-immunostained cells, collagen percentage, mast cell density and presence of pathological processes in intestinal muscle biopsies of patients. Methods: Thirty-five patients who underwent intestinal biopsy were selected from 1997 to 2015. Patients were divided into three groups: chagasic patients with mucosal lesion (n=13), chagasic patients with intact mucosa (n=12) and non-chagasic patients with no mucosal lesion (n=10). Histological processing of the biopsied fragments and immunohistochemistry for galectin-3 were performed. Additional sections were stained with hematoxylin and eosin to evaluate the general pathological processes, picrosirius for evaluation of collagen and toluidine blue to evaluate the mast cell density. Results: Patients of mucosal lesion group had a significantly higher frequency of ganglionitis and myositis when compared to the chagasic patients with intact mucosa and non-chagasic group. The density of anti-galectin-3-immunostained cells was significantly higher in the chagasic patients with intact mucosa group when compared to the non-chagasic group. The group of chagasic patients with intact mucosa presented a higher percentage of collagen in relation to the patients with mucosal lesion and to the non-chagasic group, with a significant difference. There was no significant difference in mast cell density among the three groups. Conclusion: The higher density of anti-galectin-3-immunostained cells in patients in the chagasic patients with intact mucosa group suggested the need for greater attention in clinical evaluation of these patients, since this protein is associated with neoplastic transformation and progression.

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Section: ❚ Discussionmentioning

confidence: 75%

Although with intact mucosa at colonoscopy, chagasic megacolons have an overexpression of Gal-3

Garvil

Furtado

Lima

et al. 2020

Einstein (São Paulo)

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“…PPAR-c-d are activated by anti-inflammatory cytokines (IL-4, IL-13, IL-10), TLR receptors and a range of lipids and other stimuli, including oxidized low-density lipoprotein, PUFA (arachidonic acid, 5hydroxyeicosatetraenoic acid and 5-oxo-eicosatetraenoic acid), oxidized linoleic acid (13-HODE) and prostaglandins (D2, prostaglandin E2, prostaglandin F2, thromboxane B2), that are variously present in Leishmania granulomatous tissues. 83 Interestingly, Leishmania-derived PUFAs polarize murine macrophages toward an M2 phenotype when added exogenously. 84 As noted earlier, Leishmania amastigotes form a tight junction with the PVM, raising the possibility that parasite lipids may be directly transported to the host cell and modulate host cell signaling.…”

Section: Downstream Pathways: Ppar Signaling and Lipid Metabolismmentioning

confidence: 99%

Immunometabolism of Leishmania granulomas

Saunders

McConville

2020

Immunol Cell Biol

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Leishmania are parasitic protists that cause a spectrum of diseases in humans characterized by the formation of granulomatous lesions in the skin or other tissues, such as liver and spleen. The extent to which Leishmania granulomas constrain or promote parasite growth is critically dependent on the host Thelper type 1/T-helper type 2 immune response and the localized functional polarization of infected and noninfected macrophages toward a classically (M1) or alternatively (M2) activated phenotype. Recent studies have shown that metabolic reprograming of M1 and M2 macrophages underpins the capacity of these cells to act as permissive or nonpermissive host reservoirs, respectively. In this review, we highlight the metabolic requirements of Leishmania amastigotes and the evidence that these parasites induce and/or exploit metabolic reprogramming of macrophage metabolism. We also focus on recent studies highlighting the role of key macrophage metabolic signaling pathways, such as mechanistic target of rapamycin, adenosine monophosphate-activated protein kinase and peroxisome proliferator receptor gamma in regulating the pathological progression of Leishmania granulomas. These studies highlight the intimate connectivity between Leishmania and host cell metabolism, the need to investigate these interactions in vivo and the potential to exploit host cell metabolic signaling pathways in developing new host-directed therapies.

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“…However, the in vivo cellular source of IL-10 and the window within which these cells exert their function during the course of African trypanosomiasis, as well as the associated molecular mechanism(s) implicated in its production, remain poorly understood. Hence, knowledge about the inflammation resolution process is necessary to understand the host-parasite interplay and might pave the way to improve or develop more efficient therapies that reduce the devastating effect of chronic protozoan infections [21].…”

Section: Introductionmentioning

confidence: 99%

Hepatocyte-derived IL-10 plays a crucial role in attenuating pathogenicity during the chronic phase of T. congolense infection

et al. 2020

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Bovine African Trypanosomosis is an infectious parasitic disease affecting livestock productivity and thereby impairing the economic development of Sub-Saharan Africa. The most important trypanosome species implicated is T. congolense, causing anemia as most important pathological feature. Using murine models, it was shown that due to the parasite's efficient immune evasion mechanisms, including (i) antigenic variation of the variable surface glycoprotein (VSG) coat, (ii) induction of polyclonal B cell activation, (iii) loss of B cell memory and (iv) T cell mediated immunosuppression, disease prevention through vaccination has so far been impossible. In trypanotolerant models a strong, early pro-inflammatory immune response involving IFN-γ, TNF and NO, combined with a strong humoral anti-VSG response, ensures early parasitemia control. This potent protective inflammatory response is counterbalanced by the production of the anti-inflammatory cytokine IL-10, which in turn prevents early death of the host from uncontrolled hyper-inflammation-mediated immunopathologies. Though at this stage different hematopoietic cells, such as NK cells, T cells and B cells as well as myeloid cells (i.e. alternatively activated myeloid cells (M2) or Ly6cmonocytes), were found to produce IL-10, the contribution of non-hematopoietic cells as potential IL-10 source during experimental T. congolense infection has not been addressed. Here, we report for the first time that during the chronic stage of T. congolense infection nonhematopoietic cells constitute an important source of IL-10. Our data shows that hepatocyte-derived IL-10 is mandatory for host survival and is crucial for the control of trypanosomosis-induced inflammation and associated immunopathologies such as anemia, hepatosplenomegaly and excessive tissue injury.

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Inflammatory and Pro-resolving Lipids in Trypanosomatid Infections: A Key to Understanding Parasite Control

Cited by 22 publications

References 146 publications

Although with intact mucosa at colonoscopy, chagasic megacolons have an overexpression of Gal-3

Although with intact mucosa at colonoscopy, chagasic megacolons have an overexpression of Gal-3

Immunometabolism of Leishmania granulomas

Hepatocyte-derived IL-10 plays a crucial role in attenuating pathogenicity during the chronic phase of T. congolense infection

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