Extracellular vesicles induce protective immunity against <i>Trichuris muris</i>

Shears, Rebecca K.; Bancroft, Allison J.; Hughes, Gareth W.; Grencis, Richard K.; Thornton, David J.

doi:10.1111/pim.12536

Cited by 76 publications

(84 citation statements)

References 52 publications

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“…They are produced by extraovarian tissues, secreted into the circulatory system and then taken up by the developing oocytes through receptor mediated endocytosis to provide the growing embryo with amino acids [36]. On the other hand, the detection of PCHTP-2 as the second most frequently detected protein is in accordance to Shears and collaborators [37] who found it to be the most abundant protein in the T. muris adult secretome; even though a speci c function has not been assigned yet. Likewise, Bancroft and collaborators [38] identi ed PCHTP-2 as the most abundant protein in cecal mucus from chronically infected mice with T. muris and con rmed its expression in all developmental stages.…”

Section: Discussionsupporting

confidence: 53%

“…Shears and collaborators [37] identi ed VgNVD in extracellular vesicles (EVs) of T. muris as a potential immunogenic candidate. Antigenic homologs have been identi ed in both free-living nematodes such as C. elegans, and adult parasites secretomes of Ascaris suum, Nippostrongylus brasiliensis, Heligmosomoides polygyrus and Litomosoides sigmodontis [56][57][58][59] and also in H. polygyrus eggs [60].…”

Section: Antigenic Pro Le Of T Trichiura Ee and Fe Extracts And Idenmentioning

confidence: 99%

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Proteomic Analysis Of Trichuris Trichiura Egg Extract Reveals Potential Immunomodulators And Diagnostic Targets

cruz¹,

Marcilla²,

Kelly³

et al. 2020

Preprint

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Background: Trichuris trichiura embryonated eggs are the infectious developmental stage and the first signal to the immune system of the definitive host. Each infective T. trichiura egg carries the antigens needed to challenge the immune system with a wide variety of proteins present in the shell, larvae’s surface, and the accompanying fluid that contains their excretions/secretions. The parasite eggs constitute the first antigenic stimuli to evoke the host response to this intestinal parasite with direct life cycle and enteric development.Methods: The soluble egg extract of T. trichiura obtained from naturally infected African green monkeys (Chlorocebus sabaeus) was investigated using a proteomic approach by mass spectrometry. The antigenic profile of the egg soluble proteins against sera IgG from C. sabaeus with trichuriasis was also investigated by Western blot and LC-MS/MS from the corresponding SDS-PAGE gel.Results: A total of 231 proteins were accurately identified, 168 with known molecular functions. The proteome of the egg lysate revealed common protein families including energy and metabolism; cytoskeleton, motility and muscle; proteolysis; signaling; stress and detoxification; transcription and translation and; lipid binding and transport. Vitellogenin N and VWD and DUF1943 domain containing protein, Poly-cysteine and histidine tailed protein isoform 2, Heat shock protein 70, Glyceraldehyde-3-phosphate dehydrogenase, Actin and Enolase, were among the potential immunoactive proteins. Conclusions: To our knowledge, this study represents the first attempt to identify the proteome of the T. trichiura egg extract as a novel source of immunomodulators and targets for immunodiagnosis able to contribute to the treatment of human autoimmune diseases and to the control of this neglected disease.

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Section: Discussionsupporting

confidence: 53%

Section: Antigenic Pro Le Of T Trichiura Ee and Fe Extracts And Idenmentioning

confidence: 99%

Proteomic Analysis Of Trichuris Trichiura Egg Extract Reveals Potential Immunomodulators And Diagnostic Targets

cruz¹,

Marcilla²,

Kelly³

et al. 2020

Preprint

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“…Helminths produce EVs which are involved in parasite‐parasite and in parasite‐host communication . They can be released by the tegument and are found in ES products .…”

Section: Introductionmentioning

confidence: 99%

“…5 Helminths produce EVs which are involved in parasite-parasite and in parasite-host communication. [6][7][8][9][10] They can be released by the tegument and are found in ES products. 7 Although not associated with the term EVs at the time, vesicles were first detected on the tegument surfaces of Fasciola hepatica and Echinostoma caproni.…”

mentioning

confidence: 99%

Trichinella spiralis muscle larvae release extracellular vesicles with immunomodulatory properties

Kosanović

Cvetković

Gruden-Movsesijan

et al. 2019

Parasite Immunology

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Aims Extracellular vesicles (EVs) represent a newly discovered but universal communication tool between cells or organisms. However, few data exist on nematode EVs and none for Trichinella spiralis. Here, we aimed to investigate whether T spiralis muscle larvae produce EVs, whether they carry immunomodulatory proteins and whether they have a role in immunomodulation as a component of excretory‐secretory muscle larvae products (ES L1). Methods and results EVs were enriched from conditioned medium of T spiralis muscle larvae. Transmission electron microscopy images showed T spiralis EVs to be 30‐80 nm in size, and Western blot confirmed the presence of two out of three glycoproteins with the immunodominant epitope characteristic for muscle larvae of the genus Trichinella. Using a peripheral blood mononuclear cell (PBMC) stimulation assay, it was shown that these EVs elevated production of IL10 and IL6. Conclusion T spiralis muscle larvae produce EVs. Those EVs carry immunomodulatory proteins and have the capacity independently to induce regulatory responses in the same way as the T spiralis excretory‐secretory muscle larvae products from which they were isolated.

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“…EVs from helminths also contain vaccine candidate antigens. For example, EVs from S. mansoni contain molecules that have known vaccine efficacy in animal models of schistosomiasis [27], and vaccination of mice with helminth EVs stimulates the production of protective immune responses that significantly reduce faecal egg counts, worm burdens and symptom severity and mortality induced by infection after parasite challenge [25,41-44]. Moreover, antibodies produced against recombinant forms of Opisthorchis viverrini EV surface proteins hinders the uptake of EVs by cholangiocytes and suppresses the immune response that fuels pathogenesis [29,42].…”

Section: Introductionmentioning

confidence: 99%

Schistosoma haematobiumextracellular vesicle proteins confer protection in a heterologous model of schistosomiasis

Mekonnen

Tedla

Pickering

et al. 2020

Preprint

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29Helminth parasites release extracellular vesicles which interact with the surrounding host 30 tissues, mediating host-parasite communication and other fundamental processes of 31 parasitism. As such, vesicle proteins present attractive targets for the development of 32 novel intervention strategies to control these parasites and the diseases they cause. Herein, 33 we describe the first proteomic analysis by LC-MS/MS of two types of extracellular 34 vesicles (exosome-like, 120k pellet vesicles and microvesicle-like, 15k pellet vesicles) 35 from adult Schistosoma haematobium worms. A total of 57 and 330 proteins were 36 identified in the 120k pellet vesicles and larger 15k pellet vesicles, respectively, and some 37 of the most abundant molecules included homologues of known helminth vaccine and 38 diagnostic candidates such as Sm-TSP2, Sm23, glutathione S-tranferase, saposins and 39 aminopeptidases. Tetraspanins were highly represented in the analysis and found in both 40 vesicle types. Vaccination of mice with recombinant versions of three of these 41 tetraspanins induced protection in a heterologous challenge (S. mansoni) model of 42 infection, resulting in significant reductions (averaged across two independent trials) in 43 liver (47%, 38% and 41%) and intestinal (47%, 45% and 41%) egg burdens. These 44 findings offer insight into the mechanisms by which anti-tetraspanin antibodies confer 45 protection and highlight the potential that extracellular vesicle surface proteins offer as 46 anti-helminth vaccines.47 48 Introduction 52Schistosomiasis is the second most important parasitic disease, only after malaria, 53 in terms of social, economic and public health impact [1]. Schistosoma haematobium, the 54 causative agent of urogenital schistosomiasis, is highly prevalent in 53 Middle East and 55 African countries [1] and it is also sporadically seen in India [2] and France [3]. Urogenital 56 schistosomiasis affects more than 90 million people, mostly in sub-Saharan Africa where 57 180 million inhabitants are at risk, and is responsible for 150,000 deaths per year [4]. 58Furthermore, the most common complications associated with this disease include 59 schistosomal haematuria, bladder wall pathology, hydronephrosis, and dysuria [4]. 60The current control programs against schistosomiasis are aimed at reducing the 61 morbidity caused by the parasite by regularly treating infected populations with 62 praziquantel [5]. Despite the efforts made to control this devastating disease, 63 schistosomiasis is still spreading to new geographical areas [3,6]. Furthermore, 64 praziquantel has shown reduced efficacy in field studies [7] and is not effective against 65 the immature stages of the parasite [8,9]. Hence, a vaccine that reduces disease severity 66 and/or reduces transmission is needed to control and eliminate schistosomiasis [10,11]. 67Despite efforts over decades, there is no licensed vaccine [1,12]. Even though various 68 vaccine candidates have advanced into clinical trials targeting Schistosoma mansoni, ...

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Extracellular vesicles induce protective immunity against Trichuris muris

Cited by 76 publications

References 52 publications

Proteomic Analysis Of Trichuris Trichiura Egg Extract Reveals Potential Immunomodulators And Diagnostic Targets

Proteomic Analysis Of Trichuris Trichiura Egg Extract Reveals Potential Immunomodulators And Diagnostic Targets

Trichinella spiralis muscle larvae release extracellular vesicles with immunomodulatory properties

Schistosoma haematobiumextracellular vesicle proteins confer protection in a heterologous model of schistosomiasis

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