A First Plasmodium vivax Natural Infection Induces Increased Activity of the Interferon Gamma-Driven Tryptophan Catabolism Pathway

Santos, Rafaella Oliveira dos; Cruz, Maria Geuziane Soares da; Lopes, Stefanie Costa Pinto; Oliveira, Lucas Barbosa; Nogueira, Paulo Afonso; Lima, Émerson Silva; Soares, Irene S.; Kano, Flora Satiko; Carvalho, Andréa Teixeira; Costa, Fábio Trindade Maranhão; Ganoza, Christian A.; Lacerda, Marcus Vinícius Guimarães; Lalwani, Pritesh

doi:10.3389/fmicb.2020.00400

Cited by 7 publications

(3 citation statements)

References 58 publications

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“…Another known inflammation biomarker, the Kyn/Trp ratio, shows surprisingly deep integration with these processes. Even though the induction of IDO in malarial infection is quite often discussed ( Sanni et al, 1998 ; Hansen et al, 2000 ; Tetsutani et al, 2007 ; Colvin and Joice Cordy, 2020 ; Santos et al, 2020 ), its biological significance for the immune response is in general poorly understood. Nonetheless, a mathematical model of the direct upregulation of IDO through IFNγ signaling quite clearly shows how the Kyn/Trp ratio changes during the infection ( Figure 5 ).…”

Section: Discussionmentioning

confidence: 99%

Dynamic Control Balancing Cell Proliferation and Inflammation is Crucial for an Effective Immune Response to Malaria

Gupta

Galinski

Voit

2022

Front. Mol. Biosci.

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Malaria has a complex pathology with varying manifestations and symptoms, effects on host tissues, and different degrees of severity and ultimate outcome, depending on the causative Plasmodium pathogen and host species. Previously, we compared the peripheral blood transcriptomes of two macaque species (Macaca mulatta and Macaca fascicularis) in response to acute primary infection by Plasmodium knowlesi. Although these two species are very closely related, the infection in M. mulatta is fatal, unless aggressively treated, whereas M. fascicularis develops a chronic, but tolerable infection in the blood. As a reason for this stark difference, our analysis suggests delayed pathogen detection in M. mulatta followed by extended inflammation that eventually overwhelms this monkey’s immune response. By contrast, the natural host M. fascicularis detects the pathogen earlier and controls the inflammation. Additionally, M. fascicularis limits cell proliferation pathways during the log phase of infection, presumably in an attempt to control inflammation. Subsequent cell proliferation suggests a cell-mediated adaptive immune response. Here, we focus on molecular mechanisms underlying the key differences in the host and parasite responses and their coordination. SICAvar Type 1 surface antigens are highly correlated with pattern recognition receptor signaling and important inflammatory genes for both hosts. Analysis of pathogen detection pathways reveals a similar signaling mechanism, but with important differences in the glutamate G-protein coupled receptor (GPCR) signaling pathway. Furthermore, differences in inflammasome assembly processes suggests an important role of S100 proteins in balancing inflammation and cell proliferation. Both differences point to the importance of Ca2+ homeostasis in inflammation. Additionally, the kynurenine-to-tryptophan ratio, a known inflammatory biomarker, emphasizes higher inflammation in M. mulatta during log phase. Transcriptomics-aided metabolic modeling provides a functional method for evaluating these changes and understanding downstream changes in NAD metabolism and aryl hydrocarbon receptor (AhR) signaling, with enhanced NAD metabolism in M. fascicularis and stronger AhR signaling in M. mulatta. AhR signaling controls important immune genes like IL6, IFNγ and IDO1. However, direct changes due to AhR signaling could not be established due to complicated regulatory feedback mechanisms associated with the AhR repressor (AhRR). A complete understanding of the exact dynamics of the immune response is difficult to achieve. Nonetheless, our comparative analysis provides clear suggestions of processes that underlie an effective immune response. Thus, our study identifies multiple points of intervention that are apparently responsible for a balanced and effective immune response and thereby paves the way toward future immune strategies for treating malaria.

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Section: Discussionmentioning

confidence: 99%

Dynamic Control Balancing Cell Proliferation and Inflammation is Crucial for an Effective Immune Response to Malaria

Gupta

Galinski

Voit

2022

Front. Mol. Biosci.

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“…Elevated kynurenine also indicates elevated indoleamine 2,3-dioxygenase (IDO) enzymatic activity and the initiation of the host’s immunotolerant responses. While tryptophan catabolites may have a neurotoxic role, the catabolism of tryptophan is likely driven by the host’s acute response to malaria, which includes both pro-inflammatory and anti-inflammatory tolerogenic programs [ 31 ].…”

Section: Introductionmentioning

confidence: 99%

Insights into malaria pathogenesis gained from host metabolomics

Colvin

Cordy

2020

PLoS Pathog

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“…IDO1 activity has been associated with many diseases including hepatitis B infection ( 233 ), malaria ( 234 ), psychiatric disorders ( 235 ), atherosclerosis ( 236 ) as well as cancer and the immune escape often observed in tumors ( 237 , 238 ). IDO1 was originally thought to be an anti-cancer molecule because of its ability to deplete the tryptophan needed for cell metabolism and growth.…”

Section: The Kynurenine Pathwaymentioning

confidence: 99%

Polyphenols: Chemoprevention and therapeutic potentials in hematological malignancies

Izuegbuna

2022

Front. Nutr.

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Polyphenols are one of the largest plant-derived natural product and they play an important role in plants’ defense as well as in human health and disease. A number of them are pleiotropic molecules and have been shown to regulate signaling pathways, immune response and cell growth and proliferation which all play a role in cancer development. Hematological malignancies on the other hand, are cancers of the blood. While current therapies are efficacious, they are usually expensive and with unwanted side effects. Thus, the search for newer less toxic agents. Polyphenols have been reported to possess antineoplastic properties which include cell cycle arrest, and apoptosis via multiple mechanisms. They also have immunomodulatory activities where they enhance T cell activation and suppress regulatory T cells. They carry out these actions through such pathways as PI3K/Akt/mTOR and the kynurenine. They can also reverse cancer resistance to chemotherapy agents. In this review, i look at some of the molecular mechanism of action of polyphenols and their potential roles as therapeutic agents in hematological malignancies. Here i discuss their anti-proliferative and anti-neoplastic activities especially their abilities modulate signaling pathways as well as immune response in hematological malignancies. I also looked at clinical studies done mainly in the last 10–15 years on various polyphenol combination and how they enhance synergism. I recommend that further preclinical and clinical studies be carried out to ensure safety and efficacy before polyphenol therapies be officially moved to the clinics.

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A First Plasmodium vivax Natural Infection Induces Increased Activity of the Interferon Gamma-Driven Tryptophan Catabolism Pathway

Cited by 7 publications

References 58 publications

Dynamic Control Balancing Cell Proliferation and Inflammation is Crucial for an Effective Immune Response to Malaria

Dynamic Control Balancing Cell Proliferation and Inflammation is Crucial for an Effective Immune Response to Malaria

Insights into malaria pathogenesis gained from host metabolomics

Polyphenols: Chemoprevention and therapeutic potentials in hematological malignancies

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