Peroxisome Proliferator-Activated Receptor γ-Retinoid X Receptor Agonists Increase CD36-Dependent Phagocytosis of<i>Plasmodium falciparum</i>-Parasitized Erythrocytes and Decrease Malaria-Induced TNF-α Secretion by Monocytes/Macrophages

Serghides, Lena; Kain, Kevin C.

doi:10.4049/jimmunol.166.11.6742

Cited by 101 publications

(119 citation statements)

References 69 publications

(57 reference statements)

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“…Interestingly, it was also observed in this clinical trial that the administration of Rosiglitazone led to lower parasite clearance time 145. This observation might be explained from another study, which showed that Rosiglitazone preferentially increases the expression of CD36 on macrophages146 with minimal effect on endothelial cells148 and this would potentially lead to increased phagocytosis by these cells 149. Taken together, this study shows that targeting inflammatory responses at higher exposures might indeed be protective, but these processes need to be adequately investigated.…”

Section: Taking Advantage Of Immune Regulationsupporting

confidence: 61%

“…The molecular mechanism(s) that explain(s) how this compound down‐modulates the release of proinflammatory mediators is yet to be deciphered; however, it is known that Rosiglitazone regulates Toll‐like receptor (TLR) signalling in immune cells,146 and controls (increases) the expression of CD36 in innate immune cells146 via cross‐regulation147; therefore, this might provide insights to how Rosiglitazone modulates the proinflammatory responses in immune cells. Interestingly, it was also observed in this clinical trial that the administration of Rosiglitazone led to lower parasite clearance time 145.…”

Section: Taking Advantage Of Immune Regulationmentioning

confidence: 99%

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Evaluating antidisease immunity to malaria and implications for vaccine design

Ademolue

Awandare

2017

Immunology

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SummaryImmunity to malaria could be categorized broadly as antiparasite or antidisease immunity. While most vaccine research efforts have focused on antiparasite immunity, the evidence from endemic populations suggest that antidisease immunity is an important component of natural immunity to malaria. The processes that mediate antidisease immunity have, however, attracted little to no attention, and most interests have been directed towards the antibody responses. This review evaluates the evidence for antidisease immunity in endemic areas and discusses the possible mechanisms responsible for it. Given the key role that inflammation plays in the pathogenesis of malaria, regulation of the inflammatory response appears to be a major mechanism for antidisease immunity in naturally exposed individuals.

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Section: Taking Advantage Of Immune Regulationsupporting

confidence: 61%

Section: Taking Advantage Of Immune Regulationmentioning

confidence: 99%

Evaluating antidisease immunity to malaria and implications for vaccine design

Ademolue

Awandare

2017

Immunology

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“…Support for this hypothesis came from the fact that previous studies have demonstrated that the phagocytosis of P. falciparum-parasitized erythrocytes is enhanced by PPARc ligands without TNF-a production [11]. In addition, it has previously been shown that Th2 cytokines like IL-4 activate PPARc in Mu [18] while this cytokine down-regulates TLR2 expression [42], suggesting that TLR2 and PPARc are opposite signaling pathways.…”

Section: Discussionmentioning

confidence: 99%

“…Thus, all these results suggest that CD36 could be considered as functioning in an analogous way to CD14, which concentrates the LPS signal for transduction through TLR4 [40]. On the contrary, CD36 also has an established role in the phagocytosis of endogenous ligands (such as apoptotic cells) [41] or with P. falciparum, without enhancing proinflammatory signaling [10,11]. These data suggest that, depending on the ligands and the environment, CD36 could enhance different mechanisms to favor immune response activation or to eliminate endogenous ligands without inflammation.…”

Section: Discussionmentioning

confidence: 99%

“…Recently, McGilvray and colleagues [10] described a CD36-dependent nonopsonic phagocytosis of erythrocytes containing P. falciparum, by monocytes and culture-derived Mu, and a decrease in the parasiteinduced TNF secretion by monocytes/Mu. These processes were accentuated by CD36 up-regulation by peroxisome proliferator-activated receptor (PPAR) activators [11]. PPARc is a member of a family of ligandactivated nuclear transcription factors that form heterodimers with the retinoic X receptors, and binds to PPARresponsive elements (PPRE) in the promoter regions of target genes.…”

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confidence: 99%

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IL‐13 induces expression of CD36 in human monocytes through PPARγ activation

et al. 2007

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The class B scavenger receptor CD36 is a component of the pattern recognition receptors on monocytes that recognizes a variety of molecules. CD36 expression in monocytes depends on exposure to soluble mediators. We demonstrate here that CD36 expression is induced in human monocytes following exposure to IL-13, a Th2 cytokine, via the peroxisome proliferator-activated receptor (PPAR)c pathway. Induction of CD36 protein was paralleled by an increase in CD36 mRNA. The PPARc pathway was demonstrated using transfection of a PPARc expression plasmid into the murine macrophage cell line RAW264.7, expressing very low levels of PPARc, and in peritoneal macrophages from PPARc-conditional null mice. We also show that CD36 induction by IL-13 via PPARc is dependent on phospholipase A2 activation and that IL-13 induces the production of endogenous 15-deoxy-D 12,14 -prostaglandin J 2 , an endogenous PPARc ligand, and its nuclear localization in human monocytes. Finally, we demonstrate that CD36 and PPARc are involved in IL-13-mediated phagocytosis of Plasmodium falciparum-parasitized erythrocytes. These results reveal a novel role for PPARc in the alternative activation of monocytes by IL-13, suggesting that endogenous PPARc ligands, produced by phospholipase A2 activation, could contribute to the biochemical and cellular functions of CD36.Leukocyte signaling * These 2 authors contributed equally to this work. IntroductionThe innate immune system protects the host in the early phase of infection. Circulating monocytes and tissue macrophages (Mu) mediate much of this innate immune response [1]. The strategy of recognition in the innate response is mediated by the coordinated action of pathogen-associated molecular patterns and pattern recognition receptors. Scavenger receptors and mannose receptor are important pattern recognition receptors in monocytes/Mu [2,3]. The modulation of the expression of these receptors may be critical in the role of these cells in antigen processing, scavenging, and host defence against pathogens. Several members of the scavenger receptor family, including Mu class A scavenger receptors and CD36, have been identified as receptors for modified lipoproteins on Mu, and their relevance to lipid uptake has been demonstrated in vitro and in vivo [4]. The scavenger receptor CD36, an 88-kDa integral membrane protein, is a class B scavenger receptor expressed on a wide variety of cells, in particular on monocytes and monocytederived Mu [5,6]. CD36 is known as a receptor for the uptake of oxidatively modified low-density lipoprotein (LDL) [7] and is also able to bind anionic phospholipid phosphatidylserine [8]. This scavenger receptor is implicated in the clearance of apoptotic cells [9]. Recently, McGilvray and colleagues [10] described a CD36-dependent nonopsonic phagocytosis of erythrocytes containing P. falciparum, by monocytes and culture-derived Mu, and a decrease in the parasiteinduced TNF secretion by monocytes/Mu. These processes were accentuated by CD36 up-regulation by peroxisome proliferator-acti...

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Core Principles in Nutrition: Nutrient Needs, Metabolism, and Potential Influences on Infectious Diseases

Barffour

Humphries

2020

Nutrition and Infectious Diseases

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Peroxisome Proliferator-Activated Receptor γ-Retinoid X Receptor Agonists Increase CD36-Dependent Phagocytosis ofPlasmodium falciparum-Parasitized Erythrocytes and Decrease Malaria-Induced TNF-α Secretion by Monocytes/Macrophages

Cited by 101 publications

References 69 publications

Evaluating antidisease immunity to malaria and implications for vaccine design

Evaluating antidisease immunity to malaria and implications for vaccine design

IL‐13 induces expression of CD36 in human monocytes through PPARγ activation

Core Principles in Nutrition: Nutrient Needs, Metabolism, and Potential Influences on Infectious Diseases

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