Pathogenesis and Cross-species Infection of Hepatitis E Virus

Yugo, Danielle Marie

18 January 2019

Hepatitis E Virus (HEV), the causative agent of hepatitis E, is a zoonotic pathogen of worldwide significance. The genus Orthohepevirus A of the family Hepeviridae includes all mammalian strains of HEV and consists of 8 recognized genotypes. Genotypes 1 and 2 HEVs only infect humans and genotypes 3 and 4 infect humans and several other animal species including pigs and rabbits. An ever-expanding host range of genetically-diversified strains of HEV now include bat, fish, rat, ferret, moose, wild boar, mongoose, deer, and camel. Additionally, the ruminant species goats, sheep, and cattle have been implicated as potential reservoirs as well. My dissertation research investigates a novel animal model for HEV, examines the immune dynamics during acute infection, and evaluates the possibility of additional animal reservoirs of HEV. The first project established an immunoglobulin (Ig) heavy chain knock-out JH (-/-) gnotobiotic piglet model that mimics the course of acute HEV infection observed in humans and evaluated the pathogenesis of HEV infection in this novel animal model. The dynamics of acute HEV infection in gnotobiotic pigs were systematically determined with a genotype 3 human strain of HEV. We also investigated the potential role of immunoglobulin heavy-chain JH in HEV pathogenesis and immune dynamics during the acute stage of virus infection. This novel gnotobiotic pig model will aid in future studies into HEV pathogenicity, an aspect which has thus far been difficult to reproduce in the available animal model systems. The objective of the second project for my PhD dissertation was to determine if cattle in the United States are infected with a bovine strain of HEV. We demonstrated serological evidence of an HEV-related agent in cattle populations with a high level of IgG anti-HEV prevalence. We demonstrated that calves from a seropositive cattle herd seroconverted to IgG binding HEV during a prospective study. We also showed that the IgG anti-HEV present in cattle has an ability to neutralize genotype 3 human HEV in vitro. However, our exhaustive attempts to detect HEVrelated sequence from cattle in the United States failed, suggesting that one should be cautious in interpreting the IgG anti-HEV serological results in bovine and other species. Collectively, the work from my PhD dissertation delineated important mechanisms in HEV pathogenesis and established a novel animal model for future HEV research. / Ph. D. / Hepatitis E Virus (HEV), the causative agent of hepatitis E, is a zoonotic pathogen of worldwide significance. According to the World Health Organization, there are approximately 20 million HEV infections annually, which result in 3.3 million cases of acute hepatitis E and >44,000 HEV-related deaths. Hepatitis E is a self-limiting acute disease in general, but carries the ability to cause high mortality in pregnant women and chronic hepatitis in immunocompromised individuals. The underlying mechanisms of HEV host tropism and progression of disease to chronicity are unknown. My dissertation work investigates a novel animal model for HEV, evaluates the possibility of additional animal reservoirs of HEV, and examines the immune dynamics during acute infection. The first project established an immunoglobulin (Ig) heavy chain knock-out JH (-/-) gnotobiotic piglet model that mimics the course of acute HEV infection observed in humans. The dynamics of acute HEV infection were determined in both the knock-out and wild-type piglets with a genotype 3 strain of human HEV. We also investigated the potential role of immunoglobulin heavy-chain JH in HEV pathogenesis and virus infection. In the second project, we determined if cattle in the United States are infected with a bovine strain of HEV. We showed serological evidence of an HEV-related agent in cattle as well as calves born in a seropositive herd. Despite the detection of specific antibodies recognizing HEV in cattle, definitive evidence of virus infection could not be demonstrated. Our exhaustive attempts to detect HEV-related sequence from cattle in the United States failed, suggesting that one should be cautious in interpreting the IgG anti-HEV serological results in bovine and other species. Collectively, the work from my PhD dissertation research delineated important mechanisms in HEV pathogenesis and established a novel animal model for future HEV research.

Hepatitis E Virus (HEV)

gnotobiotic pig

Ig heavy-chain knock-out

novel model

animal reservoir

bovine

seroprevalence

cross-species infection

Effect of circovirus vaccination on immune responses, viral load, and growth performance of pigs under field conditions

Potter, Megan Lynn

January 1900

Doctor of Philosophy / Department of Diagnostic Medicine/Pathobiology / Steven S. Dritz / Vaccination against porcine circovirus type 2 (PCV2) has become a standard practice to improve pig mortality and growth rate in PCV2-affected herds. Unfortunately, there has been little field-based research evaluating factors which affect circovirus vaccination. The focus of this research was on potential vaccination-affecting factors such as age, dosing strategy, pig genetic makeup, and interaction with other vaccines. A total of 6,275 pigs were used to determine factors which affect circovirus vaccination and the effects of vaccination on average daily gain (ADG), immune responses, and viral circulation under field conditions. In the first study evaluating circovirus vaccination effects on PCV2 antibody titer, regardless of age and dose administration protocol, pigs vaccinated with a 2-dose circovirus vaccine had increased (P ≤ 0.008) antibody titers compared with non-vaccinates. In a second study, dosing strategy failed (P = 0.31) to affect antibody titers. However, product and time after vaccination did affect (P = 0.005) antibody titers. In another 130-d study across the nursery and finishing phases, pigs vaccinated with a 2-dose circovirus vaccine had decreased (P < 0.001) serum PCV2 viral load compared with non-vaccinates and ADG of vaccinates was better than non-vaccinates. However, the effect was more pronounced (vaccination-by-genetic interaction, P ≤ 0.05) in Duroc-based compared to Pietrain-based pigs. In a study limited to the nursery phase, vaccination for PCV2 and Mycoplasma hyopneumoniae independently reduced ADG and consumption, but the effect was product-dependent. In a 155-d study across the nursery and finishing phases, vaccination with a 2-dose, 2-vaccine program for PCV2 and Mycoplasma hyopneumoniae decreased (P < 0.001) nursery ADG but tended to increase (P = 0.06) finishing ADG compared to a 1-dose, 2-vaccine program, with no difference (P = 0.66) observed between final pig weights. Finally, circovirus vaccination affected PCV2-circulation in high-health research herds but not in a commercial herd where PCV2 DNA was detected in the environment. These results indicate that finishing performance was improved by a 2-dose circovirus vaccine; however, nursery performance was negatively affected by the same product. Circovirus vaccination responses of growth, viral load, and antibody titer were affected by pig genetic makeup, product, and PCV2-exposure status.

Antibody

Genetics

Growth performance

Nursery pig

Porcine circovirus type 2

Vaccine

Agriculture, Animal Pathology (0476)

Agriculture, General (0473)

Biology, Veterinary Science (0778)

Application of high-throughput sequencing for the analyses of PRRSV-host interactions

Chen, Nanhua

January 1900

Doctor of Philosophy / Department of Diagnostic Medicine and Pathobiology / Raymond R. R. Rowland / Porcine Reproductive and Respiratory Syndrome Virus (PRRSV) is the most costly virus to the swine industry, worldwide. This study explored the application of deep sequencing techniques to understand better the virus-host interaction. On the virus side, PRRSV exists as a quasispecies. The first application of deep sequencing was to investigate amino acid substitutions in hypervariable regions during acute infection and after virus rebound. The appearance and disappearance of mutations, especially the generation of a new N-glycosylation site in GP5, indicated they are likely the result of immune selection. The second application of deep sequencing was to investigate the quasispecies makeup in pigs with severe combined immunodeficiency (SCID) that lack B and T cells. The results showed the same pattern of amino acid substitutions in SCID and normal littermates and no different mutations were identified between SCID and normal littermates. This suggests the mutations that appear during the early stages of infection are the product of the virus becoming adapted to replication in pigs. The third application of deep sequencing was to investigate the locations of recombination events between GFP-expressing PRRSV infectious clones. The results identified different cross-over occurred within three conserved regions between EGFP and GFPm genes. And finally, the fourth goal was applied to develop a set of sequencing tools for analyzing the host antibody repertoire. A simple method was developed to amplify swine VDJ repertoires. Shared and abundant VDJ sequences that are likely expressed by PRRSV-activated B cells were determined in pigs that had different neutralization activities. These sequences are potentially correlated with different antibody responses.

High-throughput sequencing

Quasispecies

Antibody repertoire

Recombination

Veterinary Medicine (0778)

Virology (0720)

Klonierung und funktionelle Charakterisierung des pOAT1 in ok-Zellen / Cloning and functional characterization of the pOAT1 in ok-cells

Sendler, Mark Florian

25 November 2015

No description available.

610

pOAT1

organische Anionen Transporter

ok-Zellen

slc22 Familie

Schwein

pOAT1

organic anion transporter

ok cells

slc22 family

pig

Medizin (PPN619874732)

Showmanship of Project Animals

Sprinkle, Jim, Fish, Dean

03 1900

8 pp. / Information to help reduce the occurrence of show ring fiascos. Focus is on proper preparation, selection, and the necessary time commitment that youth participants can expect.

show

project

animal

horse

cattle

beef

equine

show ring

showing

showmanship

project animals

4-h

4-H

FFA

ffa

judging

youth

swine

pig

goat

lamb

livestock

livestock project

Potential pathogenicity and antimicrobial resistance of Escherichia coli from pig and poultry feces on-farm and carcasses at the abattoir in Vietnam

Pham, Thu Minh

12 1900

E. coli avec potentiel zoonotique pourrait éclore dans les réservoirs porcins et avicoles. Cette étude consiste à examiner la présence de souches E. coli porteuses de gènes virulents associés aux STEC (E. coli producteurs de Shiga-toxines), EPEC (E. coli entéropathogène), et ExPEC (E. coli pathogène extra-intestinal) chez les porcs et volailles élevés au Vietnam. Des prélèvements d’excréments et de carcasses ont été effectués dans des fermes et abattoirs porcins et avicoles sélectionnés où les animaux ont été suivis de l’élevage à l’abattage. Un total de 13,1% des souches, toutes sources confondues, ont été catégorisées comme potentiellement contaminées par ExPEC, possédant un ou plusieurs gènes de virulence iucD, tsh, papC et cnf. Peu d’isolats d’autres pathotypes ont été observés. Tous les gènes de virulence ExPEC, à l’exception de cnf, ont été identifiés plus fréquemment dans les isolats de fèces et carcasses avicoles que dans les isolats porcins. Même constatation pour le groupe du phylogénétique D. Une multirésistance aux médicaments a été régulièrement observée chez les deux isolats ExPEC. Les isolats de fèces de volailles ont souvent été associés à une résistance à l’acide nalidixique et à la ciprofloxacine (P<0.05), de même qu’au gène blaTEM, alors que les gènes qnr et aac(6’)-Ib ont peu été rencontrés des deux côtés. Cette étude démontre que les isolats ExPEC avicoles sont potentiellement plus pathogèniques que ceux porcins et que les isolats ExPEC de carcasses porcines et avicoles peuvent provenir de leurs excréments par la contamination associée au processus d'abattage. Ainsi, la volaille, particulièrement, serait un facteur de transmission de souches ExPEC zoonotiques. / Zoonotic potential pathogenic Escherichia coli could arise from poultry and pig reservoirs. The aim of this study is to investigate the occurrence of E. coli strains carrying virulence genes associated with STEC (Shiga toxin-producing E. coli), EPEC (Enteropathogenic E. coli), and ExPEC (Extraintestinal pathogenic E. coli) in pigs and poultry on-farm and at abattoirs in Vietnam. Samples of feces and carcasses were collected at selected pig and poultry farms and abattoirs, in which animals were traced from farms to the abattoir. A total of 13.1% strains from all sources were classified as potential ExPEC, possessing one or more virulence genes iucD, tsh, papC and cnf. Few isolates of other pathotypes were observed. All ExPEC virulence genes, except cnf, were more frequently found in isolates from poultry than in isolates from pigs. A higher proportion of ExPEC isolates belonging to phylogenetic group D was observed in poultry. Multi-drug resistance was frequently observed in ExPEC isolates from both pigs and poultry. Nalidixic acid and ciprofloxacin resistance were significantly associated with poultry feces isolates (P<0.05). blaTEM gene was more frequently associated with poultry isolates, whereas qnr and aac(6’)-Ib genes were present at low prevalence in pig and poultry isolates. This study demonstrates that poultry ExPEC isolates are potentially more pathogenic than pig ExPEC isolates, and ExPEC isolates in pig and poultry carcasses may originate from pig and poultry feces, due to contamination associated to slaughtering process. Thus, meats particularly from poultry, might be a vehicle for transmission of zoonotic ExPEC strains.

Antimicrobial resistance

E. coli

Virulence genes

Pig

Poultry

Farm

Abattoir

Résistance antimicrobienne

Gènes virulents

Porc

Volaille

Ferme

Évaluation in vivo de l’efficacité thérapeutique, de la résistance et la pharmacocinétique de la colistine sulfate lors du traitement de la diarrhée colibacillaire post sevrage chez le porc

Rhouma, Mohamed

08 1900

La diarrhée colibacillaire post-sevrage (DCPS) est une infection intestinale endémique dans les fermes porcines à l’échelle mondiale. Cette maladie est causée principalement par la présence et la multiplication au niveau de l’intestin des porcelets d’un pathotype d’Escherchia coli, nommé E. coli entérotoxinogène (ETEC) et en particulier celui qui exprime l’adhésine F4 (K88) (ETEC: F4). Le sérogroupe ETEC: O149 a été le plus isolé à partir des cas de DCPS à travers le monde. Plusieurs études ont rapporté un taux de résistance important des souches O149: F4 contre les antibiotiques qui sont classiquement utilisés pour traiter cette infection et en particulier les aminoglycosides. Ainsi, pour remédier aux échecs thérapeutiques observés dans les fermes porcines au Canada, les vétérinaires ont commencé à utiliser, sous leurs responsabilités, un antibiotique, la colistine sulfate (CS), qui n’est pas homologué en production animale au Canada. Cette étude avait pour buts d’étudier la pharmacocinétique de la CS in vitro et in vivo, de développer une technique sensible pour une quantification plasmatique de la CS, de déterminer son efficacité thérapeutique in vivo dans un modèle d’infection expérimentale de DCPS et de caractériser la résistance d’E. coli consécutive à l’utilisation thérapeutique de la CS chez le porc. Une simulation du liquide gastrique (SLG) a été préparée, et après l’ajout de la CS et de la pepsine à cette solution, les concentrations de la CS ont été mesurées par chromatographie liquide à haute performance couplée à la spectrométrie de masse en tandem (HPLC-MS/MS). Une dégradation rapide de CS a été constatée dans la SLG et a été accompagnée par la formation de produits de dégradation qui ont démontré une activité microbienne plus importante par comparaison avec la molécule mère (CS). Dans un volet in vivo, l’infection expérimentale des porcelets sevrés par une souche ETEC: F4 n’a pas augmenté l’absorption digestive de la CS dans un modèle subclinique de DCPS chez le porc. L’administration orale de la CS à la dose thérapeutique de 50,000 UI/kg à raison de 2 fois par jour pendant 5 jours pour traiter la DCPS dans des conditions expérimentales a entraîné une réduction significative de l’excrétion fécale de la souche infectieuse (ETEC : F4), de la population totale d’E. coli et des scores de diarrhée, uniquement pendant la période du traitement. Cependant, ces résultats ont été accompagnés par une légère augmentation dans l’excrétion fécale des E. coli résistants à la colistine, et le traitement n'a pas empêché la perte de poids des porcs infectés. En revanche, l’infection expérimentale des porcelets par ETEC: F4 a augmenté l’absorption digestive de la CS dans un modèle clinique de diarrhée colibacillaire chez le porc. Cette étude a permis de générer pour la première fois des données scientifiques concernant l’efficacité thérapeutique, la pharmacocinétique et la résistance à la colistine dans un modèle de DCPS chez le porc. Elle a également remis en doute la pertinence économique d’augmenter la dose de CS pour accélérer le rétablissement clinique des porcs. Finalement, elle a indiqué que des conditions d’élevage optimales, sans autres facteurs prédisposants, étaient aussi efficaces que la CS dans l’amélioration des symptômes cliniques de la DCPS. / Post-weaning diarrhea (PWD) caused by Escherichia coli is an endemic intestinal infection in pig farms worldwide. This disease is mostly the consequence of the presence and the multiplication in piglet’s gut of an Escherchia pathotype, named enterotoxigenic E. coli (ETEC) and in particular those that express the F4 (K88) fimbrial adhesin (ETEC: F4). The predominant serogroup of E. coli isolated from piglets with PWD worldwide is O149. Several studies have reported a significant resistance rate of O149 ETEC strains against commonly used antibiotics for the treatment of PWD, particularly, aminoglycosides. Thereby, to address therapeutic failures observed in pig farms during PWD treatment, veterinarians in Canada started using, under their responsibilities, the colistin sulfate (CS), an antibiotic not approved for farm animals in Canada. The objectives of this thesis were: to study the pharmacokinetics of CS in vitro and in vivo, to develop a sensitive method for the quantification of CS plasma concentrations in pigs, to determine the therapeutic efficacy of CS in an experimental model of PWD, and to characterize the resistance of E. coli to colistin consecutive to its therapeutic use in pigs. Simulated gastric fluid (SGF) was prepared, and after the addition of CS and pepsin to this solution, the concentrations of CS were followed by liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS). A rapid degradation of CS in the SGF was observed, and the degradation products showed a greater antimicrobial activity compared to the native CS. On the other hand, the experimental challenge of piglets with an ETEC: F4 strain has not increased the CS intestinal absorption in a subclinical model of PWD in pigs. The oral administration of a therapeutic dose of CS at 50,000 IU/kg twice a day for 5 successive days to treat an experimental PWD in pigs, resulted in a significant reduction of fecal ETEC: F4 and total E. coli shedding, and in diarrhea scores but only during the treatment period. However, CS treatment resulted in a slight increase in fecal shedding of CS resistant E. coli and did not prevent weight loss in challenged pigs. In addition, challenge with ETEC: F4 resulted in an increase of CS intestinal absorption in a clinical model of PWD. This study has generated, for the first time, scientific data regarding CS therapeutic efficacy, its pharmacokinetic and the selection of E. coli colistin resistant in an experimental model of PWD in pigs. It also challenged the economic relevance of increasing CS oral doses to accelerate the clinical recovery of pigs. Finally, it indicated that optimal housing conditions were without other predisposing factors, effective as CS in improving clinical symptoms of experimental PWD in pigs.

Colistine sulfate

E. coli

Diarrhée post-sevrage

Porc

Pharmacocinétique

Résistance

Colistin sulphate

Post-weaning diarrhea

Pig

Pharmacokinetics

THE ROLE OF DIETARY STARCH AND NON-STARCH POLYSACCHARIDE IN SWINE PERFORMANCE AND NUTRIENT RECEPTORS GENE EXPRESSION

RZEPUS, MARCIN MATEUSZ

28 January 2015

The present work has been divided into two parts. At first, research projects attempt to evaluate technologies that increase digestibility of energy and other nutrients in cereal grains and their co-products. Differences in starch digestibility have been attributed to various factors, including the the type of corn endosperm, the presence of proteins and prolamins, the presence of lipids, the amylose-amylopectin ratio, the starch granule structure, the particle size, the conservation and processing methods. Second part of my work was dedicated to investigate the sensors of diet compounds which could be considered as potential markers to monitor nutrition status of organism. Activation of these receptors is believed to influence the hunger-satiety cycle, and their expression levels may be altered by dietary composition. Thus, the aim was to investigate for the first time the effect of arabinoxylans (AX) and β-glucans (BG) on the relative level of expression of carbohydrates, amino and fatty acid nutrient sensors genes in porcine oral and non-oral tissues. / The present work has been divided into two parts. At first, research projects attempt to evaluate technologies that increase digestibility of energy and other nutrients in cereal grains and their co-products. Differences in starch digestibility have been attributed to various factors, including the the type of corn endosperm, the presence of proteins and prolamins, the presence of lipids, the amylose-amylopectin ratio, the starch granule structure, the particle size, the conservation and processing methods. Second part of my work was dedicated to investigate the sensors of diet compounds which could be considered as potential markers to monitor nutrition status of organism. Activation of these receptors is believed to influence the hunger-satiety cycle, and their expression levels may be altered by dietary composition. Thus, the aim was to investigate for the first time the effect of arabinoxylans (AX) and β-glucans (BG) on the relative level of expression of carbohydrates, amino and fatty acid nutrient sensors genes in porcine oral and non-oral tissues.

BIO/11: BIOLOGIA MOLECOLARE

AGR/15: SCIENZE E TECNOLOGIE ALIMENTARI

Valorisation de lisier de porc dans une plantation de saules à croissance rapide

Cavanagh, Annie

02 1900

Le but de cette étude est de mieux comprendre l’effet d’une fertilisation en lisier de porc sur la productivité d’une plantation de saule tout en évaluant les risques d’impact négatif sur l’environnement. Nous avons évalué la réponse des plants à des quantités croissantes de lisiers en plus de la comparer à celle d’une fertilisation minérale. Nous avons aussi vérifié l’impact du lisier sur les teneurs nutritionnelles du sol ainsi que sur les concentrations en nitrates et phosphore de la solution du sol. Bien que l’azote du lisier soit moins efficace que celui des engrais minéraux, les résultats de notre étude montrent que le lisier est un bon engrais pour les plantations de saules. En effet, les rendements sur deux ans des parcelles ayant reçu les quantités croissantes de lisier étaient de l’ordre de 30,3 à 32,9 t/ha. Nous avons observé l’augmentation des teneurs en nitrate, cuivre et zinc dans le sol en fonction des apports croissants de lisier. Ces teneurs ont d’ailleurs diminué lors de la deuxième saison de croissance, ce qui pourrait être dû au prélèvement par les saules. Les concentrations printanières des eaux de lysimètres indiquent que la quantité maximale de lisier telle que testée lors de nos essais comporte un certain facteur de risque de lessivage des nitrates. Nous n’avons pas analysé la solution du sol des parcelles fertilisées avec des quantités plus faibles de lisier, mais nous pouvons croire qu’elles auraient induit des concentrations en nitrate comportant moins de risque de lessivage tout en assurant une productivité considérable. / The aim of this study is to investigate the effect of the use of pig slurry as fertilizer on the productivity of a willow plantation, while evaluating the risk of a negative impact on the environment. We evaluated plant response to increasing slurry amounts and compared this response to the effect of mineral fertilization. We also verified the impact of slurry on soil nutritional content as well as on nitrate and phosphorus concentrations in the soil. Although slurry nitrogen was less efficient than mineral fertilizer, the results of our study show that slurry constitutes an effective fertilizer for willow plantations. In fact, yields over two years on plots that received increasing amounts of slurry were on the order of 30.0 to 32.9 t/ha. We observed an increase in soil levels of nitrates, copper and zinc as a function of increasing slurry amounts. These levels actually decreased during the second growing season, possibly due to uptake by the willows. Springtime concentrations of water in lysimeters indicated that the maximum amount of slurry tested in our experiments was accompanied by a certain risk of nitrates leaching into the soil. We did not analyze the soil solution of plots fertilized with lower amounts of slurry, but it seems likely that these nitrate concentrations would have had a lower risk of leaching while still ensuring considerable productivity.

Saules à croissance rapide

Fast growing willow

CICR

SRIC

Lisier de porc

Pig slurry

Fertilisation

Fertilization

Nitrate

Nitrate

Phosphore

Phosphorus

Potential pathogenicity and antimicrobial resistance of Escherichia coli from pig and poultry feces on-farm and carcasses at the abattoir in Vietnam

Pham, Thu Minh

12 1900

E. coli avec potentiel zoonotique pourrait éclore dans les réservoirs porcins et avicoles. Cette étude consiste à examiner la présence de souches E. coli porteuses de gènes virulents associés aux STEC (E. coli producteurs de Shiga-toxines), EPEC (E. coli entéropathogène), et ExPEC (E. coli pathogène extra-intestinal) chez les porcs et volailles élevés au Vietnam. Des prélèvements d’excréments et de carcasses ont été effectués dans des fermes et abattoirs porcins et avicoles sélectionnés où les animaux ont été suivis de l’élevage à l’abattage. Un total de 13,1% des souches, toutes sources confondues, ont été catégorisées comme potentiellement contaminées par ExPEC, possédant un ou plusieurs gènes de virulence iucD, tsh, papC et cnf. Peu d’isolats d’autres pathotypes ont été observés. Tous les gènes de virulence ExPEC, à l’exception de cnf, ont été identifiés plus fréquemment dans les isolats de fèces et carcasses avicoles que dans les isolats porcins. Même constatation pour le groupe du phylogénétique D. Une multirésistance aux médicaments a été régulièrement observée chez les deux isolats ExPEC. Les isolats de fèces de volailles ont souvent été associés à une résistance à l’acide nalidixique et à la ciprofloxacine (P<0.05), de même qu’au gène blaTEM, alors que les gènes qnr et aac(6’)-Ib ont peu été rencontrés des deux côtés. Cette étude démontre que les isolats ExPEC avicoles sont potentiellement plus pathogèniques que ceux porcins et que les isolats ExPEC de carcasses porcines et avicoles peuvent provenir de leurs excréments par la contamination associée au processus d'abattage. Ainsi, la volaille, particulièrement, serait un facteur de transmission de souches ExPEC zoonotiques. / Zoonotic potential pathogenic Escherichia coli could arise from poultry and pig reservoirs. The aim of this study is to investigate the occurrence of E. coli strains carrying virulence genes associated with STEC (Shiga toxin-producing E. coli), EPEC (Enteropathogenic E. coli), and ExPEC (Extraintestinal pathogenic E. coli) in pigs and poultry on-farm and at abattoirs in Vietnam. Samples of feces and carcasses were collected at selected pig and poultry farms and abattoirs, in which animals were traced from farms to the abattoir. A total of 13.1% strains from all sources were classified as potential ExPEC, possessing one or more virulence genes iucD, tsh, papC and cnf. Few isolates of other pathotypes were observed. All ExPEC virulence genes, except cnf, were more frequently found in isolates from poultry than in isolates from pigs. A higher proportion of ExPEC isolates belonging to phylogenetic group D was observed in poultry. Multi-drug resistance was frequently observed in ExPEC isolates from both pigs and poultry. Nalidixic acid and ciprofloxacin resistance were significantly associated with poultry feces isolates (P<0.05). blaTEM gene was more frequently associated with poultry isolates, whereas qnr and aac(6’)-Ib genes were present at low prevalence in pig and poultry isolates. This study demonstrates that poultry ExPEC isolates are potentially more pathogenic than pig ExPEC isolates, and ExPEC isolates in pig and poultry carcasses may originate from pig and poultry feces, due to contamination associated to slaughtering process. Thus, meats particularly from poultry, might be a vehicle for transmission of zoonotic ExPEC strains.

Antimicrobial resistance

E. coli

Virulence genes

Pig

Poultry

Farm

Abattoir

Résistance antimicrobienne

Gènes virulents

Porc

Volaille

Ferme