Your search keyword '"Loukas, Alex"' showing total 16 results

1. Immunomics-Guided Antigen Discovery for Praziquantel-Induced Vaccination in Urogenital Human Schistosomiasis

Author

Pearson, Mark S, Tedla, Bemnet A, Becker, Luke, Nakajima, Rie, Jasinskas, Al, Mduluza, Takafira, Mutapi, Francisca, Oeuvray, Claude, Greco, Beatrice, Sotillo, Javier, Felgner, Philip L, and Loukas, Alex

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Vaccine Related, Digestive Diseases, Orphan Drug, Infectious Diseases, Biotechnology, Prevention, Immunization, Vector-Borne Diseases, Rare Diseases, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Infection, Good Health and Well Being, Animals, Antibodies, Helminth, Antigens, Helminth, Computational Biology, Disease Models, Animal, Epitope Mapping, Helminth Proteins, Host-Pathogen Interactions, Humans, Immunoglobulin G, Mice, Parasite Load, Praziquantel, Proteomics, Protozoan Vaccines, Schistosoma haematobium, Schistosomiasis haematobia, Vaccination, cystatin, praziquantel, proteome microarray, urogenital schistosomiasis, vaccine, immunomics, Immunology, Biochemistry and cell biology, Genetics

Abstract

Despite the enormous morbidity attributed to schistosomiasis, there is still no vaccine to combat the disease for the hundreds of millions of infected people. The anthelmintic drug, praziquantel, is the mainstay treatment option, although its molecular mechanism of action remains poorly defined. Praziquantel treatment damages the outermost surface of the parasite, the tegument, liberating surface antigens from dying worms that invoke a robust immune response which in some subjects results in immunologic resistance to reinfection. Herein we term this phenomenon Drug-Induced Vaccination (DIV). To identify the antigenic targets of DIV antibodies in urogenital schistosomiasis, we constructed a recombinant proteome array consisting of approximately 1,000 proteins informed by various secretome datasets including validated proteomes and bioinformatic predictions. Arrays were screened with sera from human subjects treated with praziquantel and shown 18 months later to be either reinfected (chronically infected subjects, CI) or resistant to reinfection (DIV). IgG responses to numerous antigens were significantly elevated in DIV compared to CI subjects, and indeed IgG responses to some antigens were completely undetectable in CI subjects but robustly recognized by DIV subjects. One antigen in particular, a cystatin cysteine protease inhibitor stood out as a unique target of DIV IgG, so recombinant cystatin was produced, and its vaccine efficacy assessed in a heterologous Schistosoma mansoni mouse challenge model. While there was no significant impact of vaccination with adjuvanted cystatin on adult worm numbers, highly significant reductions in liver egg burdens (45-55%, P

Published

2021

2. The genome and developmental transcriptome of the strongylid nematode Haemonchus contortus

Author

Schwarz, Erich M, Korhonen, Pasi K, Campbell, Bronwyn E, Young, Neil D, Jex, Aaron R, Jabbar, Abdul, Hall, Ross S, Mondal, Alinda, Howe, Adina C, Pell, Jason, Hofmann, Andreas, Boag, Peter R, Zhu, Xing-Quan, Gregory, T Ryan, Loukas, Alex, Williams, Brian A, Antoshechkin, Igor, Brown, C Titus, Sternberg, Paul W, and Gasser, Robin B

Subjects

Veterinary Sciences, Agricultural, Veterinary and Food Sciences, Biological Sciences, Genetics, Biotechnology, Immunization, Orphan Drug, Human Genome, Rare Diseases, Infectious Diseases, Vaccine Related, Biodefense, Prevention, Infection, Animals, Anthelmintics, Antigens, Helminth, Drug Resistance, Female, Gene Expression Regulation, Genes, Helminth, Genome Size, Genome, Helminth, Haemonchiasis, Haemonchus, Helminth Proteins, Host-Parasite Interactions, Life Cycle Stages, Male, Peptide Hydrolases, Sheep, Sheep Diseases, Transcriptome, Environmental Sciences, Information and Computing Sciences, Bioinformatics

Abstract

BackgroundThe barber's pole worm, Haemonchus contortus, is one of the most economically important parasites of small ruminants worldwide. Although this parasite can be controlled using anthelmintic drugs, resistance against most drugs in common use has become a widespread problem. We provide a draft of the genome and the transcriptomes of all key developmental stages of H. contortus to support biological and biotechnological research areas of this and related parasites.ResultsThe draft genome of H. contortus is 320 Mb in size and encodes 23,610 protein-coding genes. On a fundamental level, we elucidate transcriptional alterations taking place throughout the life cycle, characterize the parasite's gene silencing machinery, and explore molecules involved in development, reproduction, host-parasite interactions, immunity, and disease. The secretome of H. contortus is particularly rich in peptidases linked to blood-feeding activity and interactions with host tissues, and a diverse array of molecules is involved in complex immune responses. On an applied level, we predict drug targets and identify vaccine molecules.ConclusionsThe draft genome and developmental transcriptome of H. contortus provide a major resource to the scientific community for a wide range of genomic, genetic, proteomic, metabolomic, evolutionary, biological, ecological, and epidemiological investigations, and a solid foundation for biotechnological outcomes, including new anthelmintics, vaccines and diagnostic tests. This first draft genome of any strongylid nematode paves the way for a rapid acceleration in our understanding of a wide range of socioeconomically important parasites of one of the largest nematode orders.

Published

2013

3. Administration of Hookworm Excretory/Secretory Proteins Improves Glucose Tolerance in a Mouse Model of Type 2 Diabetes

Author

Khudhair, Zainab, Alhallaf, Rafid, Eichenberger, Ramon M, Field, Matt, Krause, Lutz, Sotillo, Javier, Loukas, Alex, Eichenberger, Ramon M., University of Zurich, Loukas, Alex, National Health and Medical Research Council (Australia), Australian Research Council, Australian Institute of Tropical Health and Medicine, and James Cook University (Australia)

Subjects

10078 Institute of Parasitology, Ancylostomatoidea, T helper 2, 1303 Biochemistry, Interleukin-6, Diabetes, 610 Medicine & health, Biochemistry, M2 macrophage, Eosinophils, Nippostrongylus, helminth, diabetes, excretory/secretory products, eosinophils, Disease Models, Animal, Mice, Glucose, Excretory/secretory products, Diabetes Mellitus, Type 2, 600 Technology, Helminth, 1312 Molecular Biology, 570 Life sciences, biology, Animals, Insulin Resistance, Molecular Biology

Abstract

Diabetes is recognised as the world's fastest growing chronic condition globally. Helminth infections have been shown to be associated with a lower prevalence of type 2 diabetes (T2D), in part due to their ability to induce a type 2 immune response. Therefore, to understand the molecular mechanisms that underlie the development of T2D-induced insulin resistance, we treated mice fed on normal or diabetes-promoting diets with excretory/secretory products (ES) from the gastrointestinal helminth Nippostrongylus brasiliensis. We demonstrated that treatment with crude ES products from adult worms (AES) or infective third-stage larvae (L3ES) from N. brasiliensis improved glucose tolerance and attenuated body weight gain in mice fed on a high glycaemic index diet. N. brasiliensis ES administration to mice was associated with a type 2 immune response measured by increased eosinophils and IL-5 in peripheral tissues but not IL-4, and with a decrease in the level of IL-6 in adipose tissue and corresponding increase in IL-6 levels in the liver. Moreover, treatment with AES or L3ES was associated with significant changes in the community composition of the gut microbiota at the phylum and order levels. These data highlight a role for N. brasiliensis ES in modulating the immune response associated with T2D, and suggest that N. brasiliensis ES contain molecules with therapeutic potential for treating metabolic syndrome and T2D. This research was supported by a program grant from the National Health and Medical Research Council (1132975), and a strategic research initiative award from the Australian Research Council to The Australian Institute of Tropical Health and Medicine at James Cook University (SRI40200003). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Sí

Published

2022

4. Suppression of inflammatory arthritis by the parasitic worm product ES-62 is associated with epigenetic changes in synovial fibroblasts

Author

Corbet, Marlene, Pineda, Miguel A., Yang, Kun, Tarafdar, Anuradha, McGrath, Sarah, Nakagawa, Rinako, Lumb, Felicity E., Suckling, Colin J., Harnett, William, Harnett, Margaret M., and Loukas, Alex

Subjects

Male, Cell signaling, Physiology, Inflammatory arthritis, Anti-Inflammatory Agents, Arthritis, Signal transduction, ERK signaling cascade, Biochemistry, Epigenesis, Genetic, Mice, 0302 clinical medicine, Skeletal Joints, Immune Physiology, Medicine and Health Sciences, Biology (General), Musculoskeletal System, Immune Response, Cells, Cultured, 0303 health sciences, Innate Immune System, DNA methylation, Chemical Reactions, Signaling cascades, Acanthocheilonema, Helminth Proteins, Phenotype, Synoviocytes, Chromatin, 3. Good health, Cell biology, Nucleic acids, STAT signaling, Chemistry, Mice, Inbred DBA, QR180, Physical Sciences, Cytokines, Epigenetics, medicine.symptom, Anatomy, DNA modification, Chromatin modification, Research Article, Chromosome biology, musculoskeletal diseases, QH301-705.5, Immunology, Inflammation, Biology, Microbiology, Methylation, 03 medical and health sciences, Signs and Symptoms, Downregulation and upregulation, Virology, medicine, Genetics, Animals, Molecular Biology, Skeleton, 030304 developmental biology, Acanthocheilonema viteae, Biology and life sciences, DNA, RC581-607, Fibroblasts, Molecular Development, medicine.disease, biology.organism_classification, Arthritis, Experimental, Immune System, Parasitology, Gene expression, Immunologic diseases. Allergy, Clinical Medicine, 030215 immunology, Developmental Biology

Abstract

ES-62 is the major secreted protein of the parasitic filarial nematode, Acanthocheilonema viteae. The molecule exists as a large tetramer (MW, ~240kD), which possesses immunomodulatory properties by virtue of multiple phosphorylcholine (PC) moieties attached to N-type glycans. By suppressing inflammatory immune responses, ES-62 can prevent disease development in certain mouse models of allergic and autoimmune conditions, including joint pathology in collagen-induced arthritis (CIA), a model of rheumatoid arthritis (RA). Such protection is associated with functional suppression of “pathogenic” hyper-responsive synovial fibroblasts (SFs), which exhibit an aggressive inflammatory and bone-damaging phenotype induced by their epigenetic rewiring in response to the inflammatory microenvironment of the arthritic joint. Critically, exposure to ES-62 in vivo induces a stably-imprinted CIA-SF phenotype that exhibits functional responses more typical of healthy, Naïve-SFs. Consistent with this, ES-62 “rewiring” of SFs away from the hyper-responsive phenotype is associated with suppression of ERK activation, STAT3 activation and miR-155 upregulation, signals widely associated with SF pathogenesis. Surprisingly however, DNA methylome analysis of Naïve-, CIA- and ES-62-CIA-SF cohorts reveals that rather than simply preventing pathogenic rewiring of SFs, ES-62 induces further changes in DNA methylation under the inflammatory conditions pertaining in the inflamed joint, including targeting genes associated with ciliogenesis, to programme a novel “resolving” CIA-SF phenotype. In addition to introducing a previously unsuspected aspect of ES-62’s mechanism of action, such unique behaviour signposts the potential for developing DNA methylation signatures predictive of pathogenesis and its resolution and hence, candidate mechanisms by which novel therapeutic interventions could prevent SFs from perpetuating joint inflammation and destruction in RA. Pertinent to these translational aspects of ES-62-behavior, small molecule analogues (SMAs) based on ES-62’s active PC-moieties mimic the rewiring of SFs as well as the protection against joint disease in CIA afforded by the parasitic worm product., Author summary The Hygiene Hypothesis proposes that the recent eradication of parasitic worms and other pathogens has resulted in chronically unbalanced, hyperactive immune systems that likely contribute to the corresponding dramatically increased incidence of allergic, autoimmune and metabolic conditions worldwide. Collectively, epidemiological and experimental animal model data supporting this hypothesis have focused interest in developing “helminth therapies”, based on infections with worms or their immunomodulatory products. Reflecting this, ES-62, an anti-inflammatory protein we discovered in the secretions of the filarial nematode Acanthocheilonema viteae, can prevent disease initiation and progression in mouse models of asthma, dermatitis, RA, SLE and the comorbidities arising from obesity-accelerated ageing. We now show that its protection against arthritis is associated with an ability to stably reprogram stromal cells in the joint away from a pathogenic bone-damaging population to a novel “safe” phenotype. Signposting of such pathogenic and “safe” molecular signatures may now provide starting points for developing novel therapies to prevent joint disease in RA. In the broader context, our discovery that a defined parasitic worm product can reprogram host cell responses furthers both our understanding of the host-pathogen interaction and identifies new directions for developing anthelmintics and therapies to resolve inflammation and induce tissue repair in humans.

Published

2021

5. The parasite’s new clothes

Author

Pearson, Mark S and Loukas, Alex

Subjects

0301 basic medicine, QH301-705.5, Science, Population, Short Report, parasitic diseases, Bioinformatics, General Biochemistry, Genetics and Molecular Biology, Host-Parasite Interactions, 03 medical and health sciences, stem cells, Parasite hosting, Animals, Humans, Parasites, S. mansoni, Biology (General), education, Flatworm, education.field_of_study, Microbiology and Infectious Disease, General Immunology and Microbiology, biology, General Neuroscience, General Medicine, Schistosoma mansoni, 030108 mycology & parasitology, biology.organism_classification, Virology, Schistosomiasis mansoni, Adult Stem Cells, 030104 developmental biology, Developmental Biology and Stem Cells, Infectious disease (medical specialty), Medicine, Other, Stem cell, Insight, Developmental biology

Abstract

Schistosomes infect more than 200 million of the world's poorest people. These parasites live in the vasculature, producing eggs that spur a variety of chronic, potentially life-threatening, pathologies exacerbated by the long lifespan of schistosomes, that can thrive in the host for decades. How schistosomes maintain their longevity in this immunologically hostile environment is unknown. Here, we demonstrate that somatic stem cells in Schistosoma mansoni are biased towards generating a population of cells expressing factors associated exclusively with the schistosome host-parasite interface, a structure called the tegument. We show cells expressing these tegumental factors are short-lived and rapidly turned over. We suggest that stem cell-driven renewal of this tegumental lineage represents an important strategy for parasite survival in the context of the host vasculature. DOI: http://dx.doi.org/10.7554/eLife.12473.001, eLife digest Schistosomes are parasitic worms that infect and cause chronic disease in hundreds of millions of people in the developing world. A major reason these parasites are so damaging is that they are capable of living and reproducing in the human bloodstream for decades. Previous research had shown that schistosomes have a population of stem cells that are proposed to promote the parasite’s survival inside the host’s bloodstream. However, it was not clear what role these cells play in the worms. Collins et al. have now found that, in a parasitic worm called Schistosoma mansoni, a large number of these stem cells are destined to become cells that generate the parasite’s skin. This unique tissue is known as the tegument, and had long been thought to have evolved in parasitic flatworms to help them survive in their host and evade its immune defenses. Therefore, Collins et al.’s findings suggest a new mechanism by which stem cells can promote the survival of a parasite inside its host. In the long-term, these findings could lead to new treatments for parasitic infections and may shed light on the evolution of parasitic flatworms. An important future challenge will be to determine if disrupting these parasites’ stem cells, and their ability to generate new tegumental cells, has any effect on the parasite inside its host. DOI: http://dx.doi.org/10.7554/eLife.12473.002

Published

2016

6. Experimental hookworm infection and escalating gluten challenges are associated with increased microbial richness in celiac subjects

Author

Giacomin, Paul, Zakrzewski, Martha, Croese, John, Su, Xiaopei, Sotillo, Javier, McCann, Leisa, Navarro, Severine, Mitreva, Makedonka, Krause, Lutz, Loukas, Alex, Cantacessi, Cinzia, Cantacessi, Cinzia [0000-0001-6863-2950], and Apollo - University of Cambridge Repository

Subjects

Ancylostomatoidea, Glutens, High-Throughput Nucleotide Sequencing, Biodiversity, digestive system, Article, Gastrointestinal Microbiome, Immunomodulation, Celiac Disease, Feces, Hookworm Infections, fluids and secretions, Case-Control Studies, parasitic diseases, Animals, Humans, Metagenome, Metagenomics

Abstract

The intestinal microbiota plays a critical role in the development of the immune system. Recent investigations have highlighted the potential of helminth therapy for treating a range of inflammatory disorders, including celiac disease (CeD); however, the mechanisms by which helminths modulate the immune response of the human host and ameliorate CeD pathology are unknown. In this study, we investigated the potential role of alterations in the human gut microbiota in helminth-mediated suppression of an inflammatory disease. We assessed the qualitative and quantitative changes in the microbiota of human volunteers with CeD prior to and following infection with human hookworms, and following challenge with escalating doses of dietary gluten. Experimental hookworm infection of the trial subjects resulted in maintenance of the composition of the intestinal flora, even after a moderate gluten challenge. Notably, we observed a significant increase in microbial species richness over the course of the trial, which could represent a potential mechanism by which hookworms can regulate gluten-induced inflammation and maintain intestinal immune homeostasis.

Published

2015

7. Vaccination of hamsters with Opisthorchis viverrini extracellular vesicles and vesicle-derived recombinant tetraspanins induces antibodies that block vesicle uptake by cholangiocytes and reduce parasite burden after challenge infection.

Author

Chaiyadet, Sujittra, Sotillo, Javier, Krueajampa, Watchara, Thongsen, Sophita, Brindley, Paul J., Sripa, Banchob, Loukas, Alex, and Laha, Thewarach

Subjects

OPISTHORCHIS viverrini, TREMATODA, CLONORCHIS sinensis, HAMSTERS, RECOMBINANT proteins, LIVER flukes, VACCINATION

Abstract

Background: The liver fluke Opisthorchis viverrini infects several million people in Southeast Asia. Adult flukes live in the bile ducts of humans, where they cause hepatobiliary pathology, including cholangiocarcinoma. Here, we investigated the potential of extracellular vesicles (EVs) secreted by the fluke and defined recombinant proteins derived from EVs to generate protective immunity in a hamster vaccination-challenge model. Methodology/Principal findings: EVs isolated from the excretory-secretory products of O. viverrini and two recombinant EV surface proteins encoding the large extracellular loops (LEL) of Ov-TSP-2 (rOv-TSP-2) and Ov-TSP-3 (rOv-TSP-3) were adjuvanted and used to vaccinate hamsters intraperitoneally followed by challenge infection with O. viverrini metacercariae. The number of adult flukes recovered from hamsters immunized with EVs, rOv-TSP-2, rOv-TSP-3 and rOv-TSP-2+rOv-TSP-3 were significantly reduced compared to control animals vaccinated with adjuvant alone. The number of eggs per gram feces was also significantly reduced in hamsters vaccinated with rOv-TSP-2 compared to controls, but no significant differences were found in the other groups. The average length of worms recovered from hamsters vaccinated with EVs, rOv-TSP-2 and rOv-TSP-3 was significantly shorter than that of worms recovered from the control group. Anti-EV IgG levels in serum and bile were significantly higher in hamsters vaccinated with EVs compared to control hamsters both pre- and post-challenge. In addition, levels of anti-rOv-TSP antibodies in the serum and bile were significantly higher than control hamsters both pre- and post-challenge. Finally, antibodies against rOv-TSP-2 and rOv-TSP-3 blocked uptake of EVs by human primary cholangiocyte in vitro, providing a plausible mechanism by which these vaccines exert partial efficacy and reduce the intensity of O. viverrini infection. Conclusion/Significance: Liver fluke EVs and recombinant tetraspanins derived from the EV surface when administered to hamsters induce antibody responses that block EV uptake by target bile duct cells and exert partial efficacy and against O. viverrini challenge. [ABSTRACT FROM AUTHOR]

Published

2019

8. In-depth proteomic characterization of Schistosoma haematobium: Towards the development of new tools for elimination.

Author

Sotillo, Javier, Pearson, Mark S., Becker, Luke, Mekonnen, Gebeyaw G., Amoah, Abena S., van Dam, Govert, Corstjens, Paul L. A. M., Murray, Janice, Mduluza, Takafira, Mutapi, Francisca, and Loukas, Alex

Subjects

SCHISTOSOMA haematobium, PROTEIN fractionation, TREMATODA, HOOKWORM disease, SQUAMOUS cell carcinoma, ANTIBODY formation, MASS spectrometry

Abstract

Background: Schistosomiasis is a neglected disease affecting hundreds of millions worldwide. Of the three main species affecting humans, Schistosoma haematobium is the most common, and is the leading cause of urogenital schistosomiasis. S. haematobium infection can cause different urogential clinical complications, particularly in the bladder, and furthermore, this parasite has been strongly linked with squamous cell carcinoma. A comprehensive analysis of the molecular composition of its different proteomes will contribute to developing new tools against this devastating disease. Methods and findings: By combining a comprehensive protein fractionation approach consisting of OFFGEL electrophoresis with high-throughput mass spectrometry, we have performed the first in-depth characterisation of the different discrete proteomes of S. haematobium that are predicted to interact with human host tissues, including the secreted and tegumental proteomes of adult flukes and secreted and soluble egg proteomes. A total of 662, 239, 210 and 138 proteins were found in the adult tegument, adult secreted, soluble egg and secreted egg proteomes, respectively. In addition, we probed these distinct proteomes with urine to assess urinary antibody responses from naturally infected human subjects with different infection intensities, and identified adult fluke secreted and tegument extracts as being the best predictors of infection. Conclusion: We provide a comprehensive dataset of proteins from the adult and egg stages of S. haematobium and highlight their utility as diagnostic markers of infection intensity. Protein composition was markedly different between the different extracts, highlighting the distinct subsets of proteins that different development stages present in their different niches. Furthermore, we have identified adult fluke ES and tegument extracts as best predictors of infection using urine antibodies of naturally infected people. This study provides the first steps towards the development of novel tools to control this important neglected tropical disease. [ABSTRACT FROM AUTHOR]

Published

2019

9. A novel blood-feeding detoxification pathway in Nippostrongylus brasiliensis L3 reveals a potential checkpoint for arresting hookworm development.

Author

Bouchery, Tiffany, Filbey, Kara, Shepherd, Amy, Chandler, Jodie, Patel, Deepa, Schmidt, Alfonso, Camberis, Mali, Peignier, Adeline, Smith, Adam A. T., Johnston, Karen, Painter, Gavin, Pearson, Mark, Giacomin, Paul, Loukas, Alex, Bottazzi, Maria-Elena, Hotez, Peter, and LeGros, Graham

Subjects

NIPPOSTRONGYLUS brasiliensis, NECATOR americanus, HOOKWORMS, HEMOGLOBINS, HEME

Abstract

As part of on-going efforts to control hookworm infection, the “human hookworm vaccine initiative” has recognised blood feeding as a feasible therapeutic target for inducing immunity against hookworm infection. To this end, molecular approaches have been used to identify candidate targets, such as Necator americanus (Na) haemoglobinase aspartic protease-1 (APR-1), with immunogenicity profiled in canine and hamster models. We sought to accelerate the immune analysis of these identified therapeutic targets by developing an appropriate mouse model. Here we demonstrate that Nippostrongylus brasiliensis (Nb), a phylogenetically distant strongylid nematode of rodents, begins blood feeding early in its development and that immunisation with Na-APR-1 can block its growth and completion of its life cycle. Furthermore, we identify a new haem detoxification pathway in Nb required for blood feeding that can be blocked by drugs of the quinolone family, reducing both infection burden and the associated anaemia in rodents. Collectively, our findings show that haem metabolism has potential as a checkpoint for interrupting hookworm development in early stages of the hookworm life cycle and that the Nippostrongylus brasiliensis rodent model is relevant for identifying novel therapeutic targets against human hookworm. [ABSTRACT FROM AUTHOR]

Published

2018

10. Polypyridylruthenium(II) complexes exert anti-schistosome activity and inhibit parasite acetylcholinesterases.

Author

Sundaraneedi, Madhu K., Tedla, Bemnet, Eichenberger, Ramon M., Becker, Luke, Pickering, Darren, Smout, Michael J., Rajan, Siji, Wangchuk, Phurpa, Keene, F. Richard, Loukas, Alex, Collins, J. Grant, and Pearson, Mark S.

Subjects

SCHISTOSOMIASIS treatment, ACETYLCHOLINESTERASE, PRAZIQUANTEL, RUTHENIUM compounds, SCHISTOSOMA mansoni, TREATMENT effectiveness

Abstract

Background: Schistosomiasis affects over 200 million people and there are concerns whether the current chemotherapeutic control strategy (periodic mass drug administration with praziquantel (PZQ)—the only licenced anti-schistosome compound) is sustainable, necessitating the development of new drugs. Methodology/Principal findings: We investigated the anti-schistosome efficacy of polypyridylruthenium(II) complexes and showed they were active against all intra-mammalian stages of S. mansoni. Two compounds, Rubb12-tri and Rubb7-tnl, which were among the most potent in their ability to kill schistosomula and adult worms and inhibit egg hatching in vitro, were assessed for their efficacy in a mouse model of schistosomiasis using 5 consecutive daily i.v. doses of 2 mg/kg (Rubb12-tri) and 10 mg/kg (Rubb7-tnl). Mice treated with Rubb12-tri showed an average 42% reduction (P = 0.009), over two independent trials, in adult worm burden. Liver egg burdens were not significantly decreased in either drug-treated group but ova from both of these groups showed significant decreases in hatching ability (Rubb12-tri—68%, Rubb7-tnl—56%) and were significantly morphologically altered (Rubb12-tri—62% abnormal, Rubb7-tnl—35% abnormal). We hypothesize that the drugs exerted their activity, at least partially, through inhibition of both neuronal and tegumental acetylcholinesterases (AChEs), as worms treated in vitro showed significant decreases in activity of these enzymes. Further, treated parasites exhibited a significantly decreased ability to uptake glucose, significantly depleted glycogen stores and withered tubercules (a site of glycogen storage), implying drug-mediated interference in this nutrient acquisition pathway. Conclusions/Significance: Our data provide compelling evidence that ruthenium complexes are effective against all intra-mammalian stages of schistosomes, including schistosomula (refractory to PZQ) and eggs (agents of disease transmissibility). Further, the results of this study suggest that schistosome AChE is a target of ruthenium drugs, a finding that can inform modification of current compounds to identify analogues which are even more effective and selective against schistosomes. [ABSTRACT FROM AUTHOR]

Published

2017

11. Helminth infection–induced malignancy.

Author

Brindley, Paul J. and Loukas, Alex

Subjects

*HELMINTHIASIS, *CHOLANGIOCARCINOMA, *SQUAMOUS cell carcinoma, *FRESHWATER fishes, *METACERCARIA, *CELL proliferation

Abstract

The article discusses a research on Helminth pathogens infection-induced malignancy. It mentions how infection with helminths leads to cholangiocarcinoma and squamous cell carcinoma of the urinary bladder. It also mentions impact of ingestion of undercooked freshwater fish infected with the metacercaria stage of species of liver flukes. It mentions Cancer occur in the DNA of the genome of the target cell, while the mutations lead to uncontrolled cellular proliferation and metastasis.

Published

2017

12. Differential Protein Expression in the Hemolymph of Bithynia siamensis goniomphalos Infected with Opisthorchis viverrini.

Author

Suwannatrai, Kulwadee, Suwannatrai, Apiporn, Tabsripair, Pairat, Welbat, Jariya Umka, Tangkawattana, Sirikachorn, Cantacessi, Cinzia, Mulvenna, Jason, Tesana, Smarn, Loukas, Alex, and Sotillo, Javier

Subjects

BITHYNIA (Mollusks), HEMOLYMPH, PROTEIN expression, OPISTHORCHIS viverrini, IMMUNE system

Abstract

Bithynia siamensis goniomphalos is a freshwater snail that serves as the first intermediate host of the human liver fluke Opisthorchis viverrini. This parasite is a major public health problem in different countries throughout the Greater Mekong sub-region (Thailand, southern Vietnam, Lao PDR and Cambodia). Chronic O. viverrini infection also results in a gradual increase of fibrotic tissues in the biliary tract that are associated with hepatobiliary diseases and contribute to cholangiocarcinoma (a fatal type of bile duct cancer). Infectivity of the parasite in the snail host is strongly correlated with destruction of helminths by the snail’s innate immune system, composed of cellular (hemocyte) and humoral (plasma) defense factors. To better understand this important host-parasite interface we applied sequential window acquisition of all theoretical spectra mass spectrometry (SWATH-MS) to identify and quantify the proteins from the hemolymph of B. siamensis goniomphalos experimentally infected with O. viverrini and compare them to non-infected snails (control group). A total of 362 and 242 proteins were identified in the hemocytes and plasma, respectively. Of these, 145 and 117 proteins exhibited significant differences in expression upon fluke infection in hemocytes and plasma, respectively. Among the proteins with significantly different expression patterns, we found proteins related to immune response (up-regulated in both hemocyte and plasma of infected snails) and proteins belonging to the structural and motor group (mostly down-regulated in hemocytes but up-regulated in plasma of infected snails). The proteins identified and quantified in this work will provide important information for the understanding of the factors involved in snail defense against O. viverrini and might facilitate the development of new strategies to control O. viverrini infection in endemic areas. [ABSTRACT FROM AUTHOR]

Published

2016

13. Compounds Derived from the Bhutanese Daisy, Ajania nubigena, Demonstrate Dual Anthelmintic Activity against Schistosoma mansoni and Trichuris muris.

Author

Wangchuk, Phurpa, Pearson, Mark S., Giacomin, Paul R., Becker, Luke, Sotillo, Javier, Pickering, Darren, Smout, Michael J., and Loukas, Alex

Subjects

ANTHELMINTICS, SCHISTOSOMA mansoni, WHIPWORMS, DRUG therapy, TRADITIONAL medicine

Abstract

Background: Whipworms and blood flukes combined infect almost one billion people in developing countries. Only a handful of anthelmintic drugs are currently available to treat these infections effectively; there is therefore an urgent need for new generations of anthelmintic compounds. Medicinal plants have presented as a viable source of new parasiticides. Ajania nubigena, the Bhutanese daisy, has been used in Bhutanese traditional medicine for treating various diseases and our previous studies revealed that small molecules from this plant have antimalarial properties. Encouraged by these findings, we screened four major compounds isolated from A. nubigena for their anthelmintic properties. Methodology/Principal Findings: Here we studied four major compounds derived from A. nubigena for their anthelmintic properties against the nematode whipworm Trichuris muris and the platyhelminth blood fluke Schistosoma mansoni using the xWORM assay technique. Of four compounds tested, two compounds—luteolin (3) and (3R,6R)-linalool oxide acetate (1)—showed dual anthelmintic activity against S. mansoni (IC50 range = 5.8–36.9 μg/mL) and T. muris (IC50 range = 9.7–20.4 μg/mL). Using scanning electron microscopy, we determined luteolin as the most efficacious compound against both parasites and additionally was found effective against the schistosomula, the infective stage of S. mansoni (IC50 = 13.3 μg/mL). Luteolin induced tegumental damage to S. mansoni and affected the cuticle, bacillary bands and bacillary glands of T. muris. Our in vivo assessment of luteolin (3) against T. muris infection at a single oral dosing of 100 mg/kg, despite being significantly (27.6%) better than the untreated control group, was markedly weaker than mebendazole (93.1%) in reducing the worm burden in mice. Conclusions/Significance: Among the four compounds tested, luteolin demonstrated the best broad-spectrum activity against two different helminths—T. muris and S. mansoni—and was effective against juvenile schistosomes, the stage that is refractory to the current gold standard drug, praziquantel. Medicinal chemistry optimisation including cytotoxicity analysis, analogue development and structure-activity relationship studies are warranted and could lead to the identification of more potent chemical entities for the control of parasitic helminths of humans and animals. [ABSTRACT FROM AUTHOR]

Published

2016

14. Novel antiinflammatory biologics shaped by parasite–host coevolution

Author

Stephanie M. Ryan, Roland Ruscher, Wayne A. Johnston, Darren A. Pickering, Malcolm W. Kennedy, Brian O. Smith, Linda Jones, Geraldine Buitrago, Matt A. Field, Adrian J. Esterman, Connor P. McHugh, Daniel J. Browne, Martha M. Cooper, Rachael Y. M. Ryan, Denise L. Doolan, Christian R. Engwerda, Kim Miles, Makedonka Mitreva, John Croese, Tony Rahman, Kirill Alexandrov, Paul R. Giacomin, Alex Loukas, Ryan, Stephanie M, Ruscher, Roland, Johnston, Wayne A, Pickering, Darren A, Esterman, Adrian J, and Loukas, Alex

Subjects

Biological Products, Multidisciplinary, IBD, Anti-Inflammatory Agents, Helminth Proteins, Colitis, Inflammatory Bowel Diseases, Mice, therapeutic, Helminths, Animals, Humans, hookworm, protein, helminth

Abstract

Refereed/Peer-reviewed Parasitic helminth infections, while a major cause of neglected tropical disease burden, negatively correlate with the incidence of immune-mediated inflammatory diseases such as inflammatory bowel diseases (IBD). To evade expulsion, helminths have developed sophisticated mechanisms to regulate their host’s immune responses. Controlled experimental human helminth infections have been assessed clinically for treating inflammatory conditions; however, such a radical therapeutic modality has challenges. An alternative approach is to harness the immunomodulatory properties within the worm’s excretory–secretory (ES) complement, its secretome. Here, we report a biologics discovery and validation pipeline to generate and screen in vivo a recombinant cell-free secretome library of helminth-derived immunomodulatory proteins. We successfully expressed 78 recombinant ES proteins from gastrointestinal hookworms and screened the crude in vitro translation reactions for anti-IBD properties in a mouse model of acute colitis. After statistical filtering and ranking, 20 proteins conferred significant protection against various parameters of colitis. Lead candidates from distinct protein families, including annexins, transthyretins, nematode-specific retinol-binding proteins, and SCP/TAPS were identified. Representative proteins were produced in mammalian cells and further validated, including ex vivo suppression of inflammatory cytokine secretion by T cells from IBD patient colon biopsies. Proteins identified herein offer promise as novel, safe, and mechanistically differentiated biologics for treating the globally increasing burden of inflammatory diseases.

Published

2022

15. Helminth coinfection and COVID-19: an alternate hypothesis

Author

Robyn McDermott, Paul R. Giacomin, Doris Pierce, Alex Loukas, Peter Bourke, Russell Hays, Hays, Russell, Pierce, Doris, Giacomin, Paul, Loukas, Alex, Bourke, Peter, and McDermott, Robyn

Subjects

0301 basic medicine, Viral Diseases, Physiology, Epidemiology, RC955-962, Helminthiasis, Medical Conditions, Endocrinology, 0302 clinical medicine, fluids and secretions, Immune Physiology, Arctic medicine. Tropical medicine, Medicine and Health Sciences, Medicine, Immune Response, Innate Immune System, Coinfection, Eukaryota, Type 2 Diabetes, Viewpoints, Infectious Diseases, Helminth Infections, helminth infection, Cytokines, Public aspects of medicine, RA1-1270, Coronavirus Infections, Infection, Pneumonia (non-human), Parasitic infection, 2019-20 coronavirus outbreak, Helminth infections, Coronavirus disease 2019 (COVID-19), Endocrine Disorders, Pneumonia, Viral, Immunology, 030231 tropical medicine, Betacoronavirus, 03 medical and health sciences, Immune system, Helminths, parasitic diseases, Parasitic Diseases, Diabetes Mellitus, Humans, Animals, Pandemics, SARS-CoV-2, business.industry, Comment, Organisms, Public Health, Environmental and Occupational Health, Biology and Life Sciences, COVID-19, Covid 19, Molecular Development, medicine.disease, Invertebrates, 030104 developmental biology, Viral infection, Immune System, Metabolic Disorders, business, Zoology, Developmental Biology

Abstract

As COVID-19 spreads through the world, most cases to date are in middle- and high-income nations. The impact on resource-poor nations remains unknown. Amongst many factors likely to affect the impact of COVID-19 in these areas, co-infections need to be considered. Here, we discuss whether the immunomodulatory effects of helminth infections may affect COVID-19 severity., Helminth co-infections can skew systemic immunity towards type 2 responses. Here, Bradbury and colleagues consider how this may impact the severity of COVID-19 in helminth-endemic regions.

Published

2020

16. Does Strongyloides stercoralis infection protect against type 2 diabetes in humans? Evidence from Australian Aboriginal adults

Author

Robyn McDermott, Russell Hays, Adrian Esterman, Alex Loukas, Paul R. Giacomin, Hays, Russell, Esterman, Adrian, Giacomin, Paul, Loukas, Alex, and McDermott, Robyn

Subjects

Adult, Male, medicine.medical_specialty, Native Hawaiian or Other Pacific Islander, endocrine system diseases, Endocrinology, Diabetes and Metabolism, Type 2 diabetes, Strongyloides stercoralis, Leukocyte Count, Endocrinology, Diabetes mellitus, Internal medicine, Internal Medicine, medicine, Prevalence, Animals, Humans, Practical implications, biology, business.industry, Australia, Type 2 Diabetes Mellitus, nutritional and metabolic diseases, General Medicine, Middle Aged, medicine.disease, biology.organism_classification, chronic infection, Blood pressure, Cross-Sectional Studies, Diabetes Mellitus, Type 2, Northern australia, improved metabolic profile, Immunology, Propensity score matching, Strongyloidiasis, Female, business

Abstract

Objective To explore the relationship between infection with Strongyloides stercoralis and the likelihood of having type 2 diabetes mellitus (T2DM). Methods Cross-sectional survey of 259 Aboriginal adults living in a remote community in northern Australia during 2013. Prior infection with S. stercoralis was determined by ELISA testing on serum. Main outcomes were eosinophil count, T2DM diagnosis, HbA1c, BMI, fasting lipids, Hb, blood pressure. Findings Ninety two participants (36%) had prior infection with S. stercoralis and 131 (51%) had T2DM. Those with previous S. stercoralis infection (ELISA titre ≥0.3) were 61% less likely to have a diagnosis of T2DM than those uninfected, adjusted for age, triglycerides, blood pressure and BMI using propensity score (adjusted OR = 0.39, 0.23–0.67, P = 0.001). Interpretation: In this remote community where prevalence of both S. stercoralis and T2DM is very high, infection with S. stercoralis appears to be associated with a significantly reduced risk of T2DM in adults. A plausible immunological mechanism has been identified in animal models. If confirmed, this result may have practical implications for the prevention of T2DM and associated metabolic disorders in humans. This finding should be explored further with larger longitudinal studies in transitional populations where the risk of both conditions is high. Funding No external funding was required for this study.

Published

2014