Krystyna Cwiklinski1, Mark W Robinson2, Sheila Donnelly3,4, John P Dalton3. 1. Zoology Department, School of Natural Sciences, Centre for One Health, Ryan Institute, National University of Ireland Galway, Galway, Ireland. krystyna.cwiklinski@nuigalway.ie. 2. School of Biological Sciences, Queen's University Belfast, Belfast, Northern Ireland, UK. 3. Zoology Department, School of Natural Sciences, Centre for One Health, Ryan Institute, National University of Ireland Galway, Galway, Ireland. 4. The School of Life Sciences, University of Technology, Sydney, Australia.
Abstract
BACKGROUND: The major pathogenesis associated with Fasciola hepatica infection results from the extensive tissue damage caused by the tunnelling and feeding activity of immature flukes during their migration, growth and development in the liver. This is compounded by the pathology caused by host innate and adaptive immune responses that struggle to simultaneously counter infection and repair tissue damage. RESULTS: Complementary transcriptomic and proteomic approaches defined the F. hepatica factors associated with their migration in the liver, and the resulting immune-pathogenesis. Immature liver-stage flukes express ~ 8000 transcripts that are enriched for transcription and translation processes reflective of intensive protein production and signal transduction pathways. Key pathways that regulate neoblast/pluripotent cells, including the PI3K-Akt signalling pathway, are particularly dominant and emphasise the importance of neoblast-like cells for the parasite's rapid development. The liver-stage parasites display different secretome profiles, reflecting their distinct niche within the host, and supports the view that cathepsin peptidases, cathepsin peptidase inhibitors, saposins and leucine aminopeptidases play a central role in the parasite's destructive migration, and digestion of host tissue and blood. Immature flukes are also primed for countering immune attack by secreting immunomodulating fatty acid binding proteins (FABP) and helminth defence molecules (FhHDM). Combined with published host microarray data, our results suggest that considerable immune cell infiltration and subsequent fibrosis of the liver tissue exacerbates oxidative stress within parenchyma that compels the expression of a range of antioxidant molecules within both host and parasite. CONCLUSIONS: The migration of immature F. hepatica parasites within the liver is associated with an increase in protein production, expression of signalling pathways and neoblast proliferation that drive their rapid growth and development. The secretion of a defined set of molecules, particularly cathepsin L peptidases, peptidase-inhibitors, saponins, immune-regulators and antioxidants allow the parasite to negotiate the liver micro-environment, immune attack and increasing levels of oxidative stress. This data contributes to the growing F. hepatica -omics information that can be exploited to understand parasite development more fully and for the design of novel control strategies to prevent host liver tissue destruction and pathology.
BACKGROUND: The major pathogenesis associated with Fasciola hepatica infection results from the extensive tissue damage caused by the tunnelling and feeding activity of immature flukes during their migration, growth and development in the liver. This is compounded by the pathology caused by host innate and adaptive immune responses that struggle to simultaneously counter infection and repair tissue damage. RESULTS: Complementary transcriptomic and proteomic approaches defined the F. hepatica factors associated with their migration in the liver, and the resulting immune-pathogenesis. Immature liver-stage flukes express ~ 8000 transcripts that are enriched for transcription and translation processes reflective of intensive protein production and signal transduction pathways. Key pathways that regulate neoblast/pluripotent cells, including the PI3K-Akt signalling pathway, are particularly dominant and emphasise the importance of neoblast-like cells for the parasite's rapid development. The liver-stage parasites display different secretome profiles, reflecting their distinct niche within the host, and supports the view that cathepsin peptidases, cathepsin peptidase inhibitors, saposins and leucine aminopeptidases play a central role in the parasite's destructive migration, and digestion of host tissue and blood. Immature flukes are also primed for countering immune attack by secreting immunomodulating fatty acid binding proteins (FABP) and helminth defence molecules (FhHDM). Combined with published host microarray data, our results suggest that considerable immune cell infiltration and subsequent fibrosis of the liver tissue exacerbates oxidative stress within parenchyma that compels the expression of a range of antioxidant molecules within both host and parasite. CONCLUSIONS: The migration of immature F. hepatica parasites within the liver is associated with an increase in protein production, expression of signalling pathways and neoblast proliferation that drive their rapid growth and development. The secretion of a defined set of molecules, particularly cathepsin L peptidases, peptidase-inhibitors, saponins, immune-regulators and antioxidants allow the parasite to negotiate the liver micro-environment, immune attack and increasing levels of oxidative stress. This data contributes to the growing F. hepatica -omics information that can be exploited to understand parasite development more fully and for the design of novel control strategies to prevent host liver tissue destruction and pathology.
Authors: Wafaa M Rehim; Iman A Sharaf; Mohamed Hishmat; Mervat A el-Toukhy; Nayer Abo Rawash; Howayda N Fouad Journal: Arzneimittelforschung Date: 2003
Authors: David Smith; Irina G Tikhonova; Heather L Jewhurst; Orla C Drysdale; Jan Dvořák; Mark W Robinson; Krystyna Cwiklinski; John P Dalton Journal: J Biol Chem Date: 2016-07-15 Impact factor: 5.157
Authors: Richard Lalor; Krystyna Cwiklinski; Nichola Eliza Davies Calvani; Amber Dorey; Siobhán Hamon; Jesús López Corrales; John Pius Dalton; Carolina De Marco Verissimo Journal: Virulence Date: 2021-12 Impact factor: 5.882
Authors: Krystyna Cwiklinski; Orla Drysdale; Jesús López Corrales; Yolanda Corripio-Miyar; Carolina De Marco Verissimo; Heather Jewhurst; David Smith; Richard Lalor; Tom N McNeilly; John P Dalton Journal: Vaccines (Basel) Date: 2022-01-20
Authors: Caoimhe M Herron; Anna O'Connor; Emily Robb; Erin McCammick; Claire Hill; Nikki J Marks; Mark W Robinson; Aaron G Maule; Paul McVeigh Journal: Front Cell Infect Microbiol Date: 2022-02-10 Impact factor: 5.293
Authors: David Becerro-Recio; Judit Serrat; Marta López-García; Verónica Molina-Hernández; José Pérez-Arévalo; Álvaro Martínez-Moreno; Javier Sotillo; Fernando Simón; Javier González-Miguel; Mar Siles-Lucas Journal: PLoS Negl Trop Dis Date: 2022-09-16
Authors: Raúl Pérez-Caballero; F Javier Martínez-Moreno; Yolanda Corripio-Miyar; Tom N McNeilly; Krystyna Cwiklinski; John P Dalton; Rafael Zafra; José Pérez; Álvaro Martínez-Moreno; Leandro Buffoni Journal: Vet Res Date: 2021-07-02 Impact factor: 3.683