A novel cystatin derived from Trichinella spiralis suppresses macrophage-mediated inflammatory responses

Kobpornchai, Porntida; Flynn, Robin J.; Reamtong, Onrapak; Rittisoonthorn, Nonglucksanawan; Kosoltanapiwat, Nathamon; Boonnak, Kobporn; Boonyuen, Usa; Ampawong, Sumate; Jiratanh, Montakan; Tattiyapong, Muncharee; Adisakwattana, Poom

doi:10.1371/journal.pntd.0008192

Cited by 34 publications

(33 citation statements)

References 57 publications

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“…Breg cells participate in the suppression of experimental autoimmune encephalomyelitis (Wolf et al ., 1996). ES molecules that are secreted from T. spiralis induce Breg cells (Kobpornchai et al ., 2020); however, the molecules that are involved in this induction remain unclear.…”

Section: Contribution Of Immunology To Clearing Host Inflammation In mentioning

confidence: 99%

“…As new identified molecular from T. spiralis , T. spiralis calreticulin (Ts-CRT) can bind to host complement C1q, which not only reduces C1q-mediated activation of classical complement pathway but also inhibits the C1q-induced non-complement activation of macrophages (Zhao et al ., 2017). Trichinella spiralis novel cystatin (TsCstN) elicits an anti-inflammatory property by suppressing proinflammatory cytokines and interfering with the antigen presentation process through depletion of MHC class II expression (Kobpornchai et al ., 2020). As an immune-modulator, T. spiralis glutathione-S-transferase (TsGST) participates in regulating maturation and function of DCs and induces the Th2-type immune response of its host (Jin et al ., 2019; Yang et al ., 2020a).…”

Section: Molecules Released By T Spiralismentioning

confidence: 99%

“…Trichinella spiralis ES products that enable cross-talk between the parasite and the host have attracted a lot of attention (Wang et al ., 2017). Obtained results indicated that this protein complex mixture from ES products and its particular components (either in native or recombinant form) could largely reproduce the effects of infection on the host immune system (by shifting the immune response from pro- to anti-inflammatory type) (Aranzamendi et al ., 2013a; Yang et al ., 2014; Kobpornchai et al ., 2020). Therefore, almost any research performed in the field seeks to explore the molecular mechanisms and to identify molecules important for creation of the anti-inflammatory milieu achieved by this parasite.…”

Section: Introductionmentioning

confidence: 99%

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Trichinella spiralis:inflammation modulator

et al. 2020

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The hygiene hypothesis posits that the decreased incidence of parasitic infection in developed countries may underlie an increased prevalence of allergic and autoimmune diseases in these countries. As unique inflammation modulator of intracellular parasitism, Trichinella spiralis, or its excretory–secretory (ES) product, shows improved responses to allergies, autoimmune diseases, inflammatory bowel disease, type 1 diabetes, rheumatic arthritis and autoimmune encephalomyelitis by exerting immunomodulatory effects on both innate and adaptive immune cells in animal models. Research has shown that T. spiralis differs from other helminths in manipulation of the host immune response not only by well-known characteristics of its life cycle, but also by its inflammation modulation pathway. How the parasite achieves inflammation modulation has not been fully elucidated yet. This review will generalize the mechanism and focuses on ES immunomodulatory molecules of T. spiralis that may be important for developing new therapeutics for inflammatory disorders.

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Section: Contribution Of Immunology To Clearing Host Inflammation In mentioning

confidence: 99%

Section: Molecules Released By T Spiralismentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Trichinella spiralis:inflammation modulator

et al. 2020

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“…Specifically, Bm cystatin led to increased Tregs in the colon and alternative activation of peritoneal macrophages. Recently, cystatin from the ES products of the zoonotic nematode T. spiralis , rTsCstN, was discovered as structurally homologous to human cystatin ( Kobpornchai et al, 2020 ). Functionally, rTsCstN suppressed inflammatory cytokine production by LPS-treated mouse bone marrow derived macrophages.…”

Section: Immunomodulatory Moleculesmentioning

confidence: 99%

The Two Faces of Nematode Infection: Virulence and Immunomodulatory Molecules From Nematode Parasites of Mammals, Insects and Plants

2020

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Helminths stage a powerful infection that allows the parasite to damage host tissue through migration and feeding while simultaneously evading the host immune system. This feat is accomplished in part through the release of a diverse set of molecules that contribute to pathogenicity and immune suppression. Many of these molecules have been characterized in terms of their ability to influence the infectious capabilities of helminths across the tree of life. These include nematodes that infect insects, known as entomopathogenic nematodes (EPN) and plants with applications in agriculture and medicine. In this review we will first discuss the nematode virulence factors, which aid parasite colonization or tissue invasion, and cause many of the negative symptoms associated with infection. These include enzymes involved in detoxification, factors essential for parasite development and growth, and highly immunogenic ES proteins. We also explore how these parasites use several classes of molecules (proteins, carbohydrates, and nucleic acids) to evade the host’s immune defenses. For example, helminths release immunomodulatory molecules in extracellular vesicles that may be protective in allergy and inflammatory disease. Collectively, these nematode-derived molecules allow parasites to persist for months or even years in a host, avoiding being killed or expelled by the immune system. Here, we evaluate these molecules, for their individual and combined potential as vaccine candidates, targets for anthelminthic drugs, and therapeutics for allergy and inflammatory disease. Last, we evaluate shared virulence and immunomodulatory mechanisms between mammalian and non-mammalian plant parasitic nematodes and EPNs, and discuss the utility of EPNs as a cost-effective model for studying nematode-derived molecules. Better knowledge of the virulence and immunomodulatory molecules from both entomopathogenic nematodes and soil-based helminths will allow for their use as beneficial agents in fighting disease and pests, divorced from their pathogenic consequences.

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“…Downmodulation of HLA-DR and CD86 expression by the parasite cystatins suggest an alternative receptor-mediated effect of cystatin on APC. Recombinant tick cystatin and Trichinella spiralis cystatin also show similar modulatory effects on APC hampering antigen presentation and downregulation of surface expression of CD80 and CD86 [ 65 , 66 , 67 ].…”

Section: Parasite Cystatins As Immunomodulatorsmentioning

confidence: 99%

Parasite Cystatin: Immunomodulatory Molecule with Therapeutic Activity against Immune Mediated Disorders

2020

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The use of parasites or their products for treating chronic inflammation associated diseases (CIADs) has generated significant attention recently. Findings from basic and clinical research have provided valuable information on strengthening the notion that parasites’ molecules can be developed as biotherapeutic agents. Completion of the genome, secreotome, and proteome of the parasites has provided an excellent platform for screening and identifying several host immunomodulatory molecules from the parasites and evaluate their therapeutic potential for CIADs. One of the widely studied host immunomodulatory molecules of the parasites is the cysteine protease inhibitor (cystatin), which is primarily secreted by the parasites to evade host immune responses. In this review, we have attempted to summarize the findings to date on the use of helminth parasite-derived cystatin as a therapeutic agent against CIADs. Although several studies suggest a role for alternatively activated macrophages, other regulatory cells, and immunosuppressive molecules, in this immunoregulatory activity of the parasite-derived cystatin, there is still no clear demonstration as to how cystatin induces its anti-inflammatory effect in suppressing CIADs.

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A novel cystatin derived from Trichinella spiralis suppresses macrophage-mediated inflammatory responses

Cited by 34 publications

References 57 publications

Trichinella spiralis:inflammation modulator

Trichinella spiralis:inflammation modulator

The Two Faces of Nematode Infection: Virulence and Immunomodulatory Molecules From Nematode Parasites of Mammals, Insects and Plants

Parasite Cystatin: Immunomodulatory Molecule with Therapeutic Activity against Immune Mediated Disorders

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