Your search keyword '"Stephen G. Preston"' showing total 18 results

1. Immunisation of chickens with inactivated and/or infectious H9N2 avian influenza virus leads to differential immune B-cell repertoire development

Author

Stefan Dascalu, Joshua E. Sealy, Jean-Remy Sadeyen, Patrik G. Flammer, Steven Fiddaman, Stephen G. Preston, Robert J. Dixon, Michael B. Bonsall, Adrian L. Smith, and Munir Iqbal

Subjects

avian influenza, H9N2, B cell repertoire, vaccines, IgM, IgY, Immunologic diseases. Allergy, RC581-607

Abstract

Avian influenza viruses (AIVs) are a major economic burden to the poultry industry and pose serious zoonotic risks, with human infections being reported every year. To date, the vaccination of birds remains the most important method for the prevention and control of AIV outbreaks. Most national vaccination strategies against AIV infection use whole virus-inactivated vaccines, which predominantly trigger a systemic antibody-mediated immune response. There are currently no studies that have examined the antibody repertoire of birds that were infected with and/or vaccinated against AIV. To this end, we evaluate the changes in the H9N2-specific IgM and IgY repertoires in chickens subjected to vaccination(s) and/or infectious challenge. We show that a large proportion of the IgM and IgY clones were shared across multiple individuals, and these public clonal responses are dependent on both the immunisation status of the birds and the specific tissue that was examined. Furthermore, the analysis revealed specific clonal expansions that are restricted to particular H9N2 immunisation regimes. These results indicate that both the nature and number of immunisations are important drivers of the antibody responses and repertoire profiles in chickens following H9N2 antigenic stimulation. We discuss how the repertoire biology of avian B-cell responses may affect the success of AIV vaccination in chickens, in particular the implications of public versus private clonal selection.

Published

2024

2. The influences of microbial colonisation and germ-free status on the chicken TCRβ repertoire

Author

Stefan Dascalu, Stephen G. Preston, Robert J. Dixon, Patrik G. Flammer, Steven Fiddaman, Amy Boyd, Joshua E. Sealy, Jean-Remy Sadeyen, Bernd Kaspers, Philippe Velge, Munir Iqbal, Michael B. Bonsall, and Adrian L. Smith

Subjects

T cell receptor (TCR), repertoire, chicken, microbiome, germ free, Immunologic diseases. Allergy, RC581-607

Abstract

Microbial colonisation is paramount to the normal development of the immune system, particularly at mucosal sites. However, the relationships between the microbiome and the adaptive immune repertoire have mostly been explored in rodents and humans. Here, we report a high-throughput sequencing analysis of the chicken TCRβ repertoire and the influences of microbial colonisation on tissue-resident TCRβ+ cells. The results reveal that the microbiome is an important driver of TCRβ diversity in both intestinal tissues and the bursa of Fabricius, but not in the spleen. Of note, public TCRβ sequences (shared across individuals) make a substantial contribution to the repertoire. Additionally, different tissues exhibit biases in terms of their V family and J gene usage, and these effects were influenced by the gut-associated microbiome. TCRβ clonal expansions were identified in both colonised and germ-free birds, but differences between the groups were indicative of an influence of the microbiota. Together, these findings provide an insight into the avian adaptive immune system and the influence of the microbiota on the TCRβ repertoire.

Published

2023

3. Repertoire analysis of γδ T cells in the chicken enables functional annotation of the genomic region revealing highly variable pan-tissue TCR gamma V gene usage as well as identifying public and private repertoires

Author

Robert Dixon, Stephen G. Preston, Stefan Dascalu, Patrik G. Flammer, Steven R. Fiddaman, Kirstie McLoughlin, Amy Boyd, Jiri Volf, Ivan Rychlik, Michael B. Bonsall, Bernd Kaspers, and Adrian L. Smith

Subjects

Chicken, Gamma, Repertoire, T cell, TCR, Sequencing, Biotechnology, TP248.13-248.65, Genetics, QH426-470

Abstract

Abstract Background Despite increasing interest in γδ T cells and their non-classical behaviour, most studies focus on animals with low numbers of circulating γδ T cells, such as mice and humans. Arguably, γδ T cell functions might be more prominent in chickens where these cells form a higher proportion of the circulatory T cell compartment. The TCR repertoire defines different subsets of γδ T cells, and such analysis is facilitated by well-annotated TCR loci. γδ T cells are considered at the cusp of innate and adaptive immunity but most functions have been identified in γδ low species. A deeper understanding of TCR repertoire biology in γδ high and γδ low animals is critical for defining the evolution of the function of γδ T cells. Repertoire dynamics will reveal populations that can be classified as innate-like or adaptive-like as well as those that straddle this definition. Results Here, a recent discrepancy in the structure of the chicken TCR gamma locus is resolved, demonstrating that tandem duplication events have shaped the evolution of this locus. Importantly, repertoire sequencing revealed large differences in the usage of individual TRGV genes, a pattern conserved across multiple tissues, including thymus, spleen and the gut. A single TRGV gene, TRGV3.3, with a highly diverse private CDR3 repertoire dominated every tissue in all birds. TRGV usage patterns were partly explained by the TRGV-associated recombination signal sequences. Public CDR3 clonotypes represented varying proportions of the repertoire of TCRs utilising different TRGVs, with one TRGV dominated by super-public clones present in all birds. Conclusions The application of repertoire analysis enabled functional annotation of the TCRG locus in a species with a high circulating γδ phenotype. This revealed variable usage of TCRGV genes across multiple tissues, a pattern quite different to that found in γδ low species (human and mouse). Defining the repertoire biology of avian γδ T cells will be key to understanding the evolution and functional diversity of these enigmatic lymphocytes in an animal that is numerically more reliant on them. Practically, this will reveal novel ways in which these cells can be exploited to improve health in medical and veterinary contexts.

Published

2021

4. High resolution parallel sequencing reveals multistrain Campylobacter in broiler chicken flocks testing ‘negative’ by conventional culture methods: implications for control of Campylobacter infection

Author

Frances M. Colles, Daniela Karasova, Magdalena Crhanova, Stephen G. Preston, Adrian L. Smith, Marian S. Dawkins, Ivan Rychlik, and Sabine G. Gebhardt-Henrich

Subjects

broiler, campylobacter, parallel sequencing, multistrain, Animal culture, SF1-1100

Abstract

ABSTRACT: Contaminated chicken meat is a major source of human Campylobacteriosis and rates of infection remain high, despite efforts to limit the colonisation of broiler (meat) chicken flocks on farms. Using conventional testing methods of culture or qPCR, Campylobacter is typically detected amongst broiler flocks from 3 wk of age, leading to the assumption that infection is introduced horizontally into chicken rearing houses at this time. In this study, we use parallel sequencing of a fragment of the Campylobacter outer membrane protein, encoded by the porA gene, to test for presence of Campylobacter DNA amongst fresh fecal samples collected from broiler flocks aged 23 to 28 d. Campylobacter DNA was detected in all of the 290 samples tested using the porA target, and in 48% of samples using 16S bacterial profiling, irrespective of whether or not Campylobacter could be detected using conventional qPCR thresholds. A single porAf2 variant was predominant among flocks that would be determined to be Campylobacter ‘positive’ by conventional means, but a diverse pattern was seen among flocks that were Campylobacter ‘negative’. The ability to routinely detect low levels of Campylobacter amongst broiler flocks at a much earlier age than would conventionally be identified requires a re-examination of how and when biosecurity measures are best applied for live birds. In addition, it may be useful to investigate why single Campylobacter variants proliferate in some broiler flocks and not others.

Published

2022

5. Correction to: Repertoire analysis of γδ T cells in the chicken enables functional annotation of the genomic region revealing highly variable pan-tissue TCR gamma V gene usage as well as identifying public and private repertoires

Author

Robert Dixon, Stephen G. Preston, Stefan Dascalu, Patrik G. Flammer, Steven R. Fiddaman, Kirstie McLoughlin, Amy Boyd, Jiri Volf, Ivan Rychlik, Michael B. Bonsall, Bernd Kaspers, and Adrian L. Smith

Subjects

Biotechnology, TP248.13-248.65, Genetics, QH426-470

Published

2021

6. Parallel Sequencing Reveals Campylobacter spp. in Commercial Meat Chickens Less than 8 Days Old

Author

Stephen G. Preston, K. K. Barfod, Frances M. Colles, Robert Dixon, Pauline Creach, Martin C. J. Maiden, Sabine G. Gebhardt-Henrich, Adrian Smith, Sophie J Hedges, P. Thornhill, and Marian Stamp Dawkins

Subjects

DNA, Bacterial, Veterinary medicine, Microbiological culture, Biosecurity, Biology, medicine.disease_cause, Applied Microbiology and Biotechnology, RNA, Ribosomal, 16S, Campylobacter Infections, medicine, Animals, Feces, Massive parallel sequencing, Ecology, Zoonotic Infection, Public and Environmental Health Microbiology, Campylobacter, biology.organism_classification, United Kingdom, France, Flock, Chickens, Switzerland, Bacteria, Food Science, Biotechnology

Abstract

Campylobacter from contaminated poultry meat is a major source of human gastroenteritis worldwide. To date, attempts to control this zoonotic infection with on-farm biosecurity measures have been inconsistent in outcome. A cornerstone of these efforts has been the detection of chicken infection with microbiological culture, where Campylobacter is generally not detectable until birds are at least 21 days old. Using parallel sequence-based bacterial 16S profiling analysis and targeted sequencing of the porA gene, Campylobacter was identified at very low levels in all commercial flocks at less than 8 days old that were tested from the United Kingdom, Switzerland, and France. These young chicks exhibited a much greater diversity of porA types than older birds testing positive for Campylobacter by culture or quantitative PCR (qPCR). This suggests that as the bacteria multiply sufficiently to be detected by culture methods, one or two variants, as indicated by porA type, dominate the infection. The findings that (i) most young chicks carry some Campylobacter and (ii) not all flocks become Campylobacter positive by culture suggest that efforts to control infection, and therefore avoid contamination of poultry meat, should concentrate on how to limit Campylobacter to low levels by the prevention of the overgrowth of single strains. IMPORTANCE Our results demonstrate the presence of Campylobacter DNA among fecal samples from a range of commercially reared meat chicks that are less than 8 days of age, consistent across 3 European countries. The recently developed, sensitive detection method indicates that infection occurs on commercial farms much earlier and more widely than previously thought, which opens up new opportunities to control Campylobacter contamination at the start of the food chain and reduce the unacceptably high levels of human disease.

Published

2021

7. Alpha globin variation in the long-tailed macaque suggests malaria selection

Author

Bridget S. Penman, Sunetra Gupta, F. Rangkuti, B. Bia, Andrew P. Dobson, Patrik G. Flammer, Amy Boyd, Stephen G. Preston, N. J. Rose, Frédéric B. Piel, Christina L. Faust, and Adrian Smith

Subjects

Genetics, biology, Genetic linkage, biology.animal, medicine, Missense mutation, Copy-number variation, Adaptation, Alpha globulin, medicine.disease, Gene, Macaque, Malaria

Abstract

Human haemoglobin variants, such as sickle, confer protection against death from malaria; consequently, frequencies of such variants are often greatly elevated in humans from malaria endemic regions. Among non-human primates, the long-tailed macaque,Macaca fascicularis, also displays substantial haemoglobin variation. Almost allM. fascicularishaemoglobin variation is in the alpha globin chain, encoded by two linked genes:HBA1andHBA2. We demonstrate that alpha globin variation inM. fasciculariscorrelates with the strength of malaria selection. We identify a range of missense mutations inM. fascicularisalpha globin and demonstrate that some of these exhibit a strikingHBA1orHBA2specificity, a pattern consistent with computational simulations of selection on genes exhibiting copy number variation. We propose thatM. fascicularisaccumulated amino acid substitutions in its alpha globin genes under malaria selection, in a process that closely mirrors, but does not entirely converge with, human malaria adaptation.

Published

2020

8. A review of a decade of lessons from one of the world’s largest MPAs: conservation gains and key challenges

Author

Charles Sheppard, Margaux Steyaert, Heather J. Koldewey, Mark G. Meekan, David Tickler, David M. P. Jacoby, Robert B. Dunbar, Julian Engel, Mark Spalding, Robin Freeman, Stephen G. Preston, Clara Diaz, Aaron B. Carlisle, Stephen C. Votier, Ines D. Lange, Nicole Esteban, Guy Stevens, David J. Curnick, Jamie M. McDevitt-Irwin, Ana Nuno, Jeanne A. Mortimer, Matthew Gollock, Emma Levy, Catherine E. I. Head, Anne Sheppard, Nigel E. Hussey, Adrian Smith, Joanna L. Harris, Nicholas A. J. Graham, Emma V. Sheehan, Malcolm A. C. Nicoll, Phil Hosegood, John R. Turner, Francesco Ferretti, Sivajyodee Sannassy Pilly, Taylor K. Chapple, Melissa Schiele, Robert J. Schallert, Kerry L. Howell, Cassandra E. Benkwitt, Daniel T. I. Bayley, Brett M. Taylor, Alice M. Trevail, Sarah Stiffel, Hannah Wood, Samantha Andrzejaczek, Nicola L. Foster, Shanta C. Barley, Dannielle S. Eager, Fiorenza Micheli, Graeme C. Hays, Ronan C. Roche, Rachel Jones, Barbara A. Block, Tom B. Letessier, Mathilde Lindhart, Edward Robinson, Alex Rattray, Nicholas Dunn, Jessica J. Meeuwig, Andrew O. M. Mogg, Peter W. Carr, Gareth J. Williams, Michael J. Williamson, Bry Wilson, Pablo Trueba, Martin J. Attrill, Clare B. Embling, Chris T. Perry, Benjamin Williamson, Claire Collins, David A. Mucciarone, and Bradley Soule

Subjects

0106 biological sciences, Marine conservation, geography, geography.geographical_feature_category, Ecology, Coral bleaching, 010604 marine biology & hydrobiology, Atoll, Pelagic zone, Marine life, Coral reef, Aquatic Science, Biology, 010603 evolutionary biology, 01 natural sciences, Fishery, Archipelago, Marine protected area, Ecology, Evolution, Behavior and Systematics

Abstract

Given the recent trend towards establishing very large marine protected areas (MPAs) and the high potential of these to contribute to global conservation targets, we review outcomes of the last decade of marine conservation research in the British Indian Ocean Territory (BIOT), one of the largest MPAs in the world. The BIOT MPA consists of the atolls of the Chagos Archipelago, interspersed with and surrounded by deep oceanic waters. Islands around the atoll rims serve as nesting grounds for sea birds. Extensive and diverse shallow and mesophotic reef habitats provide essential habitat and feeding grounds for all marine life, and the absence of local human impacts may improve recovery after coral bleaching events. Census data have shown recent increases in the abundance of sea turtles, high numbers of nesting seabirds and high fish abundance, at least some of which is linked to the lack of recent harvesting. For example, across the archipelago the annual number of green turtle clutches (Chelonia mydas) is ~ 20,500 and increasing and the number of seabirds is ~ 1 million. Animal tracking studies have shown that some taxa breed and/or forage consistently within the MPA (e.g. some reef fishes, elasmobranchs and seabirds), suggesting the MPA has the potential to provide long-term protection. In contrast, post-nesting green turtles travel up to 4000 km to distant foraging sites, so the protected beaches in the Chagos Archipelago provide a nesting sanctuary for individuals that forage across an ocean basin and several geopolitical borders. Surveys using divers and underwater video systems show high habitat diversity and abundant marine life on all trophic levels. For example, coral cover can be as high as 40–50%. Ecological studies are shedding light on how remote ecosystems function, connect to each other and respond to climate-driven stressors compared to other locations that are more locally impacted. However, important threats to this MPA have been identified, particularly global heating events, and Illegal, Unreported and Unregulated (IUU) fishing activity, which considerably impact both reef and pelagic fishes.

Published

2020

9. Epidemiological insights from a large-scale investigation of intestinal helminths in Medieval Europe

Author

Rainer Weiss, Tony Waldron, Valerie Palmowski, Rebecca L. Nicholson, Ernst Rümmele, Katarina Fellgiebel, Louise Loe, Jiří Macháček, Adrian Smith, Greger Larson, Dirk Rieger, Isabelle Jasch-Boley, Madita-Sophie Kairies, Renáta Přichystalová, Patrik G. Flammer, Beate Schmid, Stephen G. Preston, Sonja Boschert, Ben Reeves, Sylvia Warren, Mark Pollard, Christopher Guy, Hannah Ryan, and Joachim Wahl

Subjects

0301 basic medicine, Male, Diphyllobothrium latum, Trichuris, Nematoda, Physiology, Eggs, RC955-962, Prevalence, Helminthiasis, Geographical Locations, Soil, 0302 clinical medicine, Medical Conditions, Reproductive Physiology, Arctic medicine. Tropical medicine, Medicine and Health Sciences, Toilet Facilities, Child, Nematode Infections, Aged, 80 and over, Anthelmintics, Ascariasis, biology, Ascaris, Neglected Diseases, Eukaryota, Middle Aged, 3. Good health, Europe, Intestines, Infectious Diseases, Geography, Helminth Infections, Child, Preschool, Female, Public aspects of medicine, RA1-1270, Research Article, Adult, Adolescent, 030231 tropical medicine, 03 medical and health sciences, Young Adult, Environmental health, Helminths, parasitic diseases, medicine, Parasitic Diseases, Animals, Humans, Trichuriasis, Aged, Public Health, Environmental and Occupational Health, Infant, Newborn, Organisms, Genetic Variation, Infant, Biology and Life Sciences, biology.organism_classification, medicine.disease, Invertebrates, 030104 developmental biology, Nematode infection, People and Places, Trichuris trichiura, Taenia, Zoology

Abstract

Helminth infections are among the World Health Organization’s top neglected diseases with significant impact in many Less Economically Developed Countries. Despite no longer being endemic in Europe, the widespread presence of helminth eggs in archaeological deposits indicates that helminths represented a considerable burden in past European populations. Prevalence of infection is a key epidemiological feature that would influence the elimination of endemic intestinal helminths, for example, low prevalence rates may have made it easier to eliminate these infections in Europe without the use of modern anthelminthic drugs. To determine historical prevalence rates we analysed 589 grave samples from 7 European sites dated between 680 and 1700 CE, identifying two soil transmitted nematodes (Ascaris spp. and Trichuris trichiura) at all locations, and two food derived cestodes (Diphyllobothrium latum and Taenia spp.) at 4 sites. The rates of nematode infection in the medieval populations (1.5 to 25.6% for T. trichiura; 9.3–42.9% for Ascaris spp.) were comparable to those reported within modern endemically infected populations. There was some evidence of higher levels of nematode infection in younger individuals but not at all sites. The genetic diversity of T. trichiura ITS-1 in single graves was variable but much lower than with communal medieval latrine deposits. The prevalence of food derived cestodes was much lower (1.0–9.9%) than the prevalence of nematodes. Interestingly, sites that contained Taenia spp. eggs also contained D. latum which may reflect local culinary practices. These data demonstrate the importance of helminth infections in Medieval Europe and provide a baseline for studies on the epidemiology of infection in historical and modern contexts. Since the prevalence of medieval STH infections mirror those in modern endemic countries the factors affecting STH decline in Europe may also inform modern intervention campaigns., Author summary Parasitic helminths (worms) are important infections of humans in many less well developed countries, particularly those in tropical and sub-tropical regions. These infections are not a major problem in modern Europe but parasite eggs are readily detected in archaeological contexts. To estimate a key epidemiological parameter, the prevalence of infection, we examined large numbers of single graves from Medieval Europe and found that the rates of infection with two soil transmitted nematodes (Ascaris spp. and Trichuris trichiura) were as prevalent as in many modern endemic areas. We also identified two cestodes that humans acquire from eating undercooked red meat (Taenia spp.) or freshwater fish (Diphyllobothrium latum). Using prevalence and ancient DNA data we explored helminth epidemiology in Medieval European populations and factors that may influence infection including age, sex, sanitation, hygiene and culinary practices. The Medieval prevalence rates provide a historical baseline for Europe and an interesting comparator for modern epidemiological studies in other parts of the world. It is noteworthy that helminths were endemic in historical Europe but were eradicated prior to the development of modern drugs. In this sense studying changes in helminth prevalence in historical Europe may provide insights into control efforts in modern endemic regions.

Published

2020

10. Deep sequencing reveals Campylobacter in commercial meat chickens less than 8 days old

Author

Sophie J Hedges, Phoebe Thornhill, Kenneth K Barfod, Marian Stamp Dawkins, Adrian Smith, Stephen G. Preston, Pauline Creach, Frances M. Colles, Martin C. J. Maiden, Sabine G. Gebhardt-Henrich, and Robert Dixon

Subjects

Veterinary medicine, Microbiological culture, Zoonotic Infection, Campylobacter, Biosecurity, medicine, Microbiome, Flock, Biology, medicine.disease_cause, biology.organism_classification, Deep sequencing, Bacteria

Abstract

Campylobacter from contaminated poultry meat is a major source of human gastroenteritis worldwide. To date, attempts to control this zoonotic infection with on-farm biosecurity measures have been inconsistent. A cornerstone of these efforts has been the detection of chicken infection with microbiological culture, which typically does not occur until birds are at least 21 days old. Using molecular methods for detecting Campylobacter presence, 16S microbiome analysis and deep sequencing of the Campylobacter porA gene, Campylobacter can be identified at very low levels in most or all flocks fewer than 8 days old. These young chicks exhibit a much greater diversity of porA types than older birds testing positive for Campylobacter by culture or qPCR. This suggests that, as the bacteria multiply sufficiently to be detected by culture methods, one or two strains, as indicated by porA type, dominate the infection. The findings that (i) most young chicks carry some Campylobacter and (ii) not all flocks become Campylobacter positive by culture, suggests that efforts to control infection should concentrate on how to maintain Campylobacter at low levels by the prevention of the overgrowth of single strains, which ultimately leads to the contamination of food.

Published

2020

11. Parallel sequencing of porA reveals a complex pattern of Campylobacter genotypes that differs between broiler and broiler breeder chickens

Author

Frances M, Colles, Stephen G, Preston, Kenneth Klingenberg, Barfod, Patrik G, Flammer, Martin C J, Maiden, and Adrian L, Smith

Subjects

Molecular Epidemiology, Base Sequence, Genotype, animal diseases, food and beverages, Porins, Campylobacter, Article, Bacterial Typing Techniques, Applied microbiology, Bacterial Proteins, Animals, Microbiome, Animal Husbandry, Bacterial infection, Chickens, Poultry Diseases

Abstract

Chicken meat represents an important source of Campylobacter infections of humans world-wide. A better understanding of Campylobacter epidemiology in commercial chicken flocks will facilitate the development of more effective intervention strategies. We developed a gene-specific parallel sequencing approach that efficiently indicated genetic diversity in farm-derived samples and revealed Campylobacter genotypes that would not be detected using microbiological culture. Parallel sequencing of the porA nucleotide fragment identified a different pattern of diversity in broiler flocks compared with broiler-breeder flocks at both individual bird and flock levels. Amongst the flocks tested, broiler flocks and individual birds were dominated by one or two porA fragment types whereas co-dominance with up to six porA fragment types was evident in breeder birds. A high proportion (83.6–93.3%) of porA variants were shared between broiler and breeder flocks. The porA-based diversity profiling could be a useful addition to the repertoire of tools employed to attribute potential sources of contamination for broiler flocks, including the environment, wild animals or other chickens. This approach can be extended to include other loci within Campylobacter and developed for molecular epidemiology studies of other bacterial species.

Published

2018

12. Molecular archaeoparasitology identifies cultural changes in the Medieval Hanseatic trading centre of Lübeck

Author

Patrik G, Flammer, Simon, Dellicour, Stephen G, Preston, Dirk, Rieger, Sylvia, Warren, Cedric K W, Tan, Rebecca, Nicholson, Renáta, Přichystalová, Niels, Bleicher, Joachim, Wahl, Nuno R, Faria, Oliver G, Pybus, Mark, Pollard, and Adrian L, Smith

Subjects

parasitology, History, 17th Century, Feces, Cultural Evolution, Germany, Helminths, parasitic diseases, Animals, Humans, genetics, Trichuriasis, Cities, DNA, Ancient, Parasite Egg Count, ancient DNA, History, Ancient, History, 15th Century, Genetic Variation, archaeology, History, Medieval, Trichuris, History, 16th Century, Palaeobiology, diet, trade, Research Article

Abstract

Throughout history, humans have been afflicted by parasitic worms, and eggs are readily detected in archaeological deposits. This study integrated parasitological and ancient DNA methods with a large sample set dating between Neolithic and Early Modern periods to explore the utility of molecular archaeoparasitology as a new approach to study the past. Molecular analyses provided unequivocal species-level parasite identification and revealed location-specific epidemiological signatures. Faecal–oral transmitted nematodes (Ascaris lumbricoides and Trichuris trichiura) were ubiquitous across time and space. By contrast, high numbers of food-associated cestodes (Diphyllobothrium latum and Taenia saginata) were restricted to medieval Lübeck. The presence of these cestodes and changes in their prevalence at approximately 1300 CE indicate substantial alterations in diet or parasite availability. Trichuris trichiura ITS-1 sequences grouped into two clades; one ubiquitous and one restricted to medieval Lübeck and Bristol. The high sequence diversity of T.t.ITS-1 detected in Lübeck is consistent with its importance as a Hanseatic trading centre. Collectively, these results introduce molecular archaeoparasitology as an artefact-independent source of historical evidence.

Published

2018

13. Badger macrophages fail to produce nitric oxide, a key anti-mycobacterial effector molecule

Author

Kirstin, Bilham, Amy C, Boyd, Stephen G, Preston, Christina D, Buesching, Chris, Newman, David W, Macdonald, and Adrian L, Smith

Subjects

Lipopolysaccharides, Tumor Necrosis Factor-alpha, Macrophages, Interleukin-1beta, Imidazoles, Nitric Oxide Synthase Type II, Nitric Oxide, Immunity, Innate, Recombinant Proteins, Article, Mycobacterium, Up-Regulation, Interferon-gamma, Toll-Like Receptor 9, Mustelidae, Animals, Cattle, Tuberculosis, Bovine, Phylogeny

Abstract

The European badger is recognised as a wildlife reservoir for bovine tuberculosis (bTB); the control of which is complex, costly and controversial. Despite the importance of badgers in bTB and the well-documented role for macrophages as anti-mycobacterial effector cells, badger macrophage (bdMφ) responses remain uncharacterised. Here, we demonstrate that bdMφ fail to produce nitric oxide (NO) or upregulate inducible nitric oxide synthase (iNOS) mRNA following Toll-like receptor (TLR) agonist treatment. BdMφ also failed to make NO after stimulation with recombinant badger interferon gamma (bdIFNγ) or a combination of bdIFNγ and lipopolysaccharide. Exposure of bdMφ to TLR agonists and/or bdIFNγ resulted in upregulated cytokine (IL1β, IL6, IL12 and TNFα) mRNA levels indicating that these critical pathways were otherwise intact. Although stimulation with most TLR agonists resulted in strong cytokine mRNA responses, weaker responses were evident after exposure to TLR9 agonists, potentially due to very low expression of TLR9 in bdMφ. Both NO and TLR9 are important elements of innate immunity to mycobacteria, and these features of bdMφ biology would impair their capacity to resist bTB infection. These findings have significant implications for the development of bTB management strategies, and support the use of vaccination to reduce bTB infection in badgers.

Published

2016

14. Particulate inorganic adjuvants: recent developments and future outlook

Author

Charlotte N Maughan, Gareth R. Williams, and Stephen G. Preston

Subjects

Pharmacology, Immunity, Cellular, Vaccines, Th2 response, business.industry, medicine.medical_treatment, Pharmaceutical Science, Biology, Biotechnology, Vaccine adjuvant, Adjuvants, Immunologic, Metals, Neoplasms, Immunology, medicine, Alum Compounds, Humans, business, Adjuvant

Abstract

Objectives To review the state of the art and assess future potential in the use of inorganic particulates as vaccine adjuvants. Key findings An adjuvant is an entity added to a vaccine formulation to ensure that robust immunity to the antigen is inculcated. The inclusion of an adjuvant is typically vital for the efficacy of vaccines using inactivated organisms, subunit and DNA antigens. With increasing research efforts being focused on subunit and DNA antigens because of their improved safety profiles, the development of appropriate adjuvants is becoming ever more crucial. Despite this, very few adjuvants are licensed for use in humans (four by the FDA, five by the European Medicines Agency). The most widely used adjuvant, alum, has been used for nearly 90 years, yet its mechanism of action remains poorly understood. In addition, while alum produces a powerful antibody Th2 response, it does not provoke the cellular immune response required for the elimination of intracellular infections or cancers. New adjuvants are therefore needed, and inorganic systems have attracted much attention in this regard. Summary In this review, the inorganic adjuvants currently in use are considered, and the efforts made to date to understand their mechanisms of action are summarised. We then move on to survey the literature on inorganic particulate adjuvants, focusing on the most interesting recent developments in this area and their future potential.

Published

2014

15. Novel immunomodulators from hard ticks selectively reprogramme human dendritic cell responses

Author

Chrisoula Kouremenou, Lena F. Burger, Oliwia Rysnik, Juraj Majtan, Alejandro Cabezas Cruz, Stephen G. Preston, Miles A. Nunn, Guido C. Paesen, Jonathan M. Austyn, Maylin Chiong Guzman, Patricia A. Nuttall, Nuffield Department of Surgical Sciences, University of Oxford [Oxford], John Radcliffe Hospital, Department of Zoology, Eszterházy Károly College, Institute of Zoology, Ilia State University [Tbilisi], Nuffield Department of Clinical Medicine [Oxford], Institute of Parisitology, University of South Bohemia, Institute of Parasitology, Animal Biotechnology Division, National Dairy Research Institute, Centre for Ecology and Hydrology, Natural Environment Research Council (NERC), Division of Structural Biology, Henry Wellcome Building for Genomic Medicine, Wellcome Trust Centre for Human Genetics, Natural Environment Research Council (CEH010021 ), European Union (LSHB-CT-2004-512074), and Austyn, Jonathan M

Subjects

tique, Cellular differentiation, [SDV]Life Sciences [q-bio], Antigen Processing and Recognition, Adaptive Immunity, Monocytes, 0302 clinical medicine, Ticks, Cytotoxic T cell, Biology (General), Immune Response, 0303 health sciences, biology, Cell Differentiation, immunomodulator, Acquired immune system, Innate Immunity, Recombinant Proteins, 3. Good health, Cell biology, Rhipicephalus, Host-Pathogen Interaction, medicine.anatomical_structure, Cytokines, Research Article, QH301-705.5, T cell, Immune Cells, Immunology, Antigen-Presenting Cells, Immune Suppression, Microbiology, Vector Biology, Arthropod Proteins, Cell Line, Immune Activation, 03 medical and health sciences, Immune system, immunomodulateur, Virology, Genetics, medicine, Animals, Humans, Immunologic Factors, Salivary Proteins and Peptides, Molecular Biology, Biology, Immunity to Infections, 030304 developmental biology, Inflammation, Innate immune system, Immunity, Immunoregulation, Immune Defense, Dendritic cell, Dendritic Cells, RC581-607, biology.organism_classification, Biology and Microbiology, Gene Expression Regulation, Immune System, Parasitology, Immunologic diseases. Allergy, 030215 immunology

Abstract

Hard ticks subvert the immune responses of their vertebrate hosts in order to feed for much longer periods than other blood-feeding ectoparasites; this may be one reason why they transmit perhaps the greatest diversity of pathogens of any arthropod vector. Tick-induced immunomodulation is mediated by salivary components, some of which neutralise elements of innate immunity or inhibit the development of adaptive immunity. As dendritic cells (DC) trigger and help to regulate adaptive immunity, they are an ideal target for immunomodulation. However, previously described immunoactive components of tick saliva are either highly promiscuous in their cellular and molecular targets or have limited effects on DC. Here we address the question of whether the largest and globally most important group of ticks (the ixodid metastriates) produce salivary molecules that specifically modulate DC activity. We used chromatography to isolate a salivary gland protein (Japanin) from Rhipicephalus appendiculatus ticks. Japanin was cloned, and recombinant protein was produced in a baculoviral expression system. We found that Japanin specifically reprogrammes DC responses to a wide variety of stimuli in vitro, radically altering their expression of co-stimulatory and co-inhibitory transmembrane molecules (measured by flow cytometry) and their secretion of pro-inflammatory, anti-inflammatory and T cell polarising cytokines (assessed by Luminex multiplex assays); it also inhibits the differentiation of DC from monocytes. Sequence alignments and enzymatic deglycosylation revealed Japanin to be a 17.7 kDa, N-glycosylated lipocalin. Using molecular cloning and database searches, we have identified a group of homologous proteins in R. appendiculatus and related species, three of which we have expressed and shown to possess DC-modulatory activity. All data were obtained using DC generated from at least four human blood donors, with rigorous statistical analysis. Our results suggest a previously unknown mechanism for parasite-induced subversion of adaptive immunity, one which may also facilitate pathogen transmission., Author Summary Dendritic cells (DC) are specialised cells of the vertebrate immune system. DC can sense different types of infectious agents and parasites, and both trigger and help regulate the specific types of immunity needed to eliminate them. We have discovered that the largest and globally most important group of hard ticks produce a unique family of proteins in their saliva that selectively targets DC, radically altering functions that would otherwise induce robust immune responses; these proteins also prevent DC developing from precursor cells. The production of these salivary molecules may help to explain two highly unusual features of these hard ticks compared with other blood-feeding parasites: their ability to feed continuously on their vertebrate hosts for considerable lengths of time (7 days or more) without eliciting potentially damaging immune responses, and their capacity to transmit possibly the greatest variety of pathogens of any type of invertebrate.

Published

2013

16. DNA fusion vaccines incorporating IL-23 or RANTES for use in immunization against influenza

Author

Puiyi Pang, Jonathan M. Austyn, Lynn Slobbe, G.S. Buchan, Margaret A. Baird, Sarah L. Young, Stephen G. Preston, Michelle Wilson, and Jonathan Williman

Subjects

Chemokine, Recombinant Fusion Proteins, Hemagglutinin (influenza), Hemagglutinin Glycoproteins, Influenza Virus, Biology, Interleukin-23, Virus, Gene gun, DNA vaccination, Mice, Th2 Cells, Immune system, Orthomyxoviridae Infections, Antigen, Vaccines, DNA, Animals, Chemokine CCL5, Mice, Inbred BALB C, General Veterinary, General Immunology and Microbiology, Immunogenicity, Public Health, Environmental and Occupational Health, Th1 Cells, Virology, Specific Pathogen-Free Organisms, Infectious Diseases, Influenza A virus, Influenza Vaccines, Immunology, biology.protein, Molecular Medicine, Female, Immunization

Abstract

The incorporation of RANTES or IL-23 into DNA vaccines may improve their immunogenicity by the recruitment and activation of dendritic cells. This may also select for a TH1 response counteracting the TH2 response which can predominate when a DNA vaccine is delivered by gene gun. We have immunized mice with various DNA constructs encoding APR/8/34 influenza virus hemagglutinin (HA), either fused to or separate from, IL-23 or RANTES using a gene gun. Those immunized with IL-23/HA fusion constructs and challenged with influenza 27 weeks post-vaccination, tended to have cleared more virus than those vaccinated with HA DNA. Mice immunized with the RANTES/HA fusion construct produced a mixed TH1/TH2 response whereas in HA-vaccinated mice, a TH2 response predominated. Immunization with a plasmid in which HA and RANTES were under the control of separate promoters, failed to generate a mixed TH1/TH2 response suggesting that enhanced antigen uptake via RANTES receptors may contribute to the mixed immune response generated to the fusion construct. Overall these findings provide further evidence that Type 1 cytokines or chemokines, fused to antigen in a DNA vaccine, can influence the nature and the longevity of the immune response and ultimately, its protective capacity.

Published

2008

17. Epidemiological insights from a large-scale investigation of intestinal helminths in Medieval Europe.

Author

Patrik G Flammer, Hannah Ryan, Stephen G Preston, Sylvia Warren, Renáta Přichystalová, Rainer Weiss, Valerie Palmowski, Sonja Boschert, Katarina Fellgiebel, Isabelle Jasch-Boley, Madita-Sophie Kairies, Ernst Rümmele, Dirk Rieger, Beate Schmid, Ben Reeves, Rebecca Nicholson, Louise Loe, Christopher Guy, Tony Waldron, Jiří Macháček, Joachim Wahl, Mark Pollard, Greger Larson, and Adrian L Smith

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

Helminth infections are among the World Health Organization's top neglected diseases with significant impact in many Less Economically Developed Countries. Despite no longer being endemic in Europe, the widespread presence of helminth eggs in archaeological deposits indicates that helminths represented a considerable burden in past European populations. Prevalence of infection is a key epidemiological feature that would influence the elimination of endemic intestinal helminths, for example, low prevalence rates may have made it easier to eliminate these infections in Europe without the use of modern anthelminthic drugs. To determine historical prevalence rates we analysed 589 grave samples from 7 European sites dated between 680 and 1700 CE, identifying two soil transmitted nematodes (Ascaris spp. and Trichuris trichiura) at all locations, and two food derived cestodes (Diphyllobothrium latum and Taenia spp.) at 4 sites. The rates of nematode infection in the medieval populations (1.5 to 25.6% for T. trichiura; 9.3-42.9% for Ascaris spp.) were comparable to those reported within modern endemically infected populations. There was some evidence of higher levels of nematode infection in younger individuals but not at all sites. The genetic diversity of T. trichiura ITS-1 in single graves was variable but much lower than with communal medieval latrine deposits. The prevalence of food derived cestodes was much lower (1.0-9.9%) than the prevalence of nematodes. Interestingly, sites that contained Taenia spp. eggs also contained D. latum which may reflect local culinary practices. These data demonstrate the importance of helminth infections in Medieval Europe and provide a baseline for studies on the epidemiology of infection in historical and modern contexts. Since the prevalence of medieval STH infections mirror those in modern endemic countries the factors affecting STH decline in Europe may also inform modern intervention campaigns.

Published

2020

18. Novel immunomodulators from hard ticks selectively reprogramme human dendritic cell responses.

Author

Stephen G Preston, Juraj Majtán, Chrisoula Kouremenou, Oliwia Rysnik, Lena F Burger, Alejandro Cabezas Cruz, Maylin Chiong Guzman, Miles A Nunn, Guido C Paesen, Patricia A Nuttall, and Jonathan M Austyn

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Hard ticks subvert the immune responses of their vertebrate hosts in order to feed for much longer periods than other blood-feeding ectoparasites; this may be one reason why they transmit perhaps the greatest diversity of pathogens of any arthropod vector. Tick-induced immunomodulation is mediated by salivary components, some of which neutralise elements of innate immunity or inhibit the development of adaptive immunity. As dendritic cells (DC) trigger and help to regulate adaptive immunity, they are an ideal target for immunomodulation. However, previously described immunoactive components of tick saliva are either highly promiscuous in their cellular and molecular targets or have limited effects on DC. Here we address the question of whether the largest and globally most important group of ticks (the ixodid metastriates) produce salivary molecules that specifically modulate DC activity. We used chromatography to isolate a salivary gland protein (Japanin) from Rhipicephalus appendiculatus ticks. Japanin was cloned, and recombinant protein was produced in a baculoviral expression system. We found that Japanin specifically reprogrammes DC responses to a wide variety of stimuli in vitro, radically altering their expression of co-stimulatory and co-inhibitory transmembrane molecules (measured by flow cytometry) and their secretion of pro-inflammatory, anti-inflammatory and T cell polarising cytokines (assessed by Luminex multiplex assays); it also inhibits the differentiation of DC from monocytes. Sequence alignments and enzymatic deglycosylation revealed Japanin to be a 17.7 kDa, N-glycosylated lipocalin. Using molecular cloning and database searches, we have identified a group of homologous proteins in R. appendiculatus and related species, three of which we have expressed and shown to possess DC-modulatory activity. All data were obtained using DC generated from at least four human blood donors, with rigorous statistical analysis. Our results suggest a previously unknown mechanism for parasite-induced subversion of adaptive immunity, one which may also facilitate pathogen transmission.

Published

2013