Proteomics coupled with in vitro model to study the early crosstalk occurring between newly excysted juveniles of Fasciola hepatica and host intestinal cells

Becerro-Recio, David; Serrat, Judit; López-García, Marta; Sotillo, Javier; Simón, F; González‐Miguel, Javier; Siles-Lucas, Mar

doi:10.1371/journal.pntd.0010811

Cited by 7 publications

(12 citation statements)

References 83 publications

(95 reference statements)

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“…More specifically, we identify FhCL3 and FhCB3 as potential PLG-binding proteins, and FhCL1, FhCL2 and FhCB2 to a lesser extent. This is consistent with the developmental stage-specific expression of these proteases, being FhCB1-3 and FhCL3 mostly expressed in the juvenile stages of the parasite that are found in the duodenum [ 36 , 48 , 49 ]. However, one of the limitations of our 2D-MS approach is that it is performed under denaturing conditions, which may expose internal PLG-binding epitopes in some proteins that are not employed for PLG-binding in a real physiological context.…”

Section: Discussionsupporting

confidence: 83%

Fasciola hepatica juveniles interact with the host fibrinolytic system as a potential early-stage invasion mechanism

et al. 2023

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Background The trematode Fasciola hepatica is the most widespread causative agent of fasciolosis, a parasitic disease that mainly affects humans and ruminants worldwide. During F. hepatica infection, newly excysted juveniles (FhNEJ) emerge in the duodenum of the mammalian host and migrate towards their definitive location, the intra-hepatic biliary ducts. Understanding how F. hepatica traverses the intestinal wall and migrates towards the liver is pivotal for the development of more successful strategies against fasciolosis. The central enzyme of the mammalian fibrinolytic system is plasmin, a serine protease whose functions are exploited by a number of parasite species owing to its broad spectrum of substrates, including components of tissue extracellular matrices. The aim of the present work is to understand whether FhNEJ co-opt the functions of their host fibrinolytic system as a mechanism to facilitate trans-intestinal migration. Methodology/Principal Findings A tegument-enriched antigenic extract of FhNEJ (FhNEJ-Teg) was obtained in vitro, and its capability to bind the zymogen plasminogen (PLG) and enhance its conversion to the active protease, plasmin, were analyzed by a combination of enzyme-linked immunosorbent, chromogenic and immunofluorescence assays. Additionally, PLG-binding proteins in FhNEJ-Teg were identified by bidimensional electrophoresis coupled to mass spectrometry analysis, and the interactions were validated using FhNEJ recombinant proteins. Conclusions/Significance Our results show that FhNEJ-Teg contains proteins that bind PLG and stimulate its activation to plasmin, which could facilitate the traversal of the intestinal wall by FhNEJ and contribute to the successful establishment of the parasite within its mammalian host. Altogether, our findings contribute to a better understanding of host-parasite relationships during early fasciolosis and may be exploited from a pharmacological and/or immunological perspective for the development of treatment and control strategies against this global disease.

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Section: Discussionsupporting

confidence: 83%

Fasciola hepatica juveniles interact with the host fibrinolytic system as a potential early-stage invasion mechanism

et al. 2023

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“…More specifically, we identify FhCL3 and FhCB3 as potential PLG-binding proteins, and FhCL1, FhCL2 and FhCB3 to a lesser extent. This is consistent with the developmental stage-specific expression of these proteases, being FhCB1-3 and FhCL3 mostly expressed in the juvenile stages of the parasite that are found in the duodenum (46)(47)(48). However, one of the limitations of our 2D-MS approach is that it is performed under denaturing conditions, which may expose internal PLG-binding epitopes in some proteins that are not employed for PLG-binding in a real physiological context.…”

Section: Discussionsupporting

confidence: 80%

Fasciola hepaticajuveniles interact with the host fibrinolytic system as a potential early-stage invasion mechanism

Serrat

Becerro-Recio

Torres-Valle

et al. 2022

Preprint

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Background: The trematode Fasciola hepatica is the most widespread causative agent of fasciolosis, a parasitic disease that mainly affects humans and ruminants worldwide. During F. hepatica infection, newly excysted juveniles (FhNEJ) emerge in the duodenum of the mammalian host and migrate towards the definitive location of the parasite, the intra-hepatic biliary ducts. Understanding how F. hepatica traverses the intestinal wall and migrates towards the liver is pivotal for the development of more successful strategies against fasciolosis. The central enzyme of the mammalian fibrinolytic system is plasmin, a serine protease whose functions are exploited by a number of parasite species owing to its broad spectrum of substrates, including components of tissue extracellular matrices. The aim of the present work is to understand whether FhNEJ co-opt the functions of their host fibrinolytic system as a mechanism to facilitate trans-intestinal migration. Methodology/Principal Findings: An FhNEJ tegument protein extract (FhNEJ-Teg) was obtained in vitro, and its capability to bind the zymogen plasminogen (PLG) and enhance its conversion to the active protease, plasmin, were analyzed by a combination of enzyme-linked immunosorbent, chromogenic and immunofluorescence assays. Additionally, PLG-binding proteins in FhNEJ-Teg were identified by 2D electrophoresis coupled to mass-spectrometry analysis, and the interactions were validated using FhNEJ recombinant proteins. Conclusions/Significance: Our results show that FhNEJ-Teg contains proteins that bind PLG and stimulate its activation to plasmin, which could facilitate the traversal of the intestinal wall by FhNEJ and contribute to the successful establishment of the parasite within its mammalian host. Altogether, our findings contribute to a better understanding of host-parasite relationships during early fasciolosis and may be exploited from a pharmacological and/or immunological perspective for the development of treatment and control strategies against this global disease.

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“…Such analysis could however be particularly useful in revealing novel facets of the pathological mechanisms associated with human strongyloidiasis, especially when applied in comparative studies. Indeed, this strategy has already been successfully applied to the study of other helminthiases, including schistosomiasis, fasciolosis and echinococcosis, to identify proteins or biological processes altered in the pathological state compared to uninfected controls, during the disease progression or in response to treatment [66][67][68][69][70][71][72][73][74][75][76]. The most commonly investigated samples are plasma/serum and plasma/serumderived EVs (either from animal models or from patients), even though also tissue proteomics has been described [69,70].…”

Section: Proteomics To Study the Host Response To The Infectionmentioning

confidence: 99%

“…Indeed, this strategy has already been successfully applied to the study of other helminthiases, including schistosomiasis, fasciolosis and echinococcosis, to identify proteins or biological processes altered in the pathological state compared to uninfected controls, during the disease progression or in response to treatment [66][67][68][69][70][71][72][73][74][75][76]. The most commonly investigated samples are plasma/serum and plasma/serumderived EVs (either from animal models or from patients), even though also tissue proteomics has been described [69,70]. Importantly, a number of studies identified parasite proteins within the host's systemic or vesicular proteome, supporting the relevance of host proteomics also in revealing novel diagnostic markers [67,68,71,72,74,75].…”

Section: Proteomics To Study the Host Response To The Infectionmentioning

confidence: 99%

Progresses and challenges in Strongyloides spp. proteomics

Tiberti,

Manfredi,

Piubelli

et al. 2023

Phil. Trans. R. Soc. B

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The availability of high-quality data of helminth genomes provided over the past two decades has supported and accelerated large-scale ‘omics studies and, consequently, the achievement of a more in-depth molecular characterization of a number of pathogens. This has also involved Strongyloides spp. and since their genome was made available transcriptomics has been rather frequently applied to investigate gene expression regulation across their life cycle. Strongyloides proteomics characterization has instead been somehow neglected, with only a few reports performing high-throughput or targeted analyses associated with protein identification by tandem mass spectrometry. Such investigations are however necessary in order to discern important aspects associated with human strongyloidiasis, including understanding parasite biology and the mechanisms of host–parasite interaction, but also to identify novel diagnostic and therapeutic targets. In this review article, we will give an overview of the published proteomics studies investigating strongyloidiasis at different levels, spanning from the characterization of the somatic proteome and excretory/secretory products of different parasite stages to the investigation of potentially immunogenic proteins. Moreover, in the effort to try to start filling the current gap in host-proteomics, we will also present the first serum proteomics analysis in patients suffering from human strongyloidiasis. This article is part of the Theo Murphy meeting issue ‘ Strongyloides : omics to worm-free populations’.

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Proteomics coupled with in vitro model to study the early crosstalk occurring between newly excysted juveniles of Fasciola hepatica and host intestinal cells

Cited by 7 publications

References 83 publications

Fasciola hepatica juveniles interact with the host fibrinolytic system as a potential early-stage invasion mechanism

Fasciola hepatica juveniles interact with the host fibrinolytic system as a potential early-stage invasion mechanism

Fasciola hepaticajuveniles interact with the host fibrinolytic system as a potential early-stage invasion mechanism

Progresses and challenges in Strongyloides spp. proteomics

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