Comparison of virulence gene profiles of Escherichia coli strains isolated from healthy and diarrheic swine

A combination of uni- and multiplex PCR assays targeting 58 virulence genes (VGs) associated with Escherichia coli strains causing intestinal and extraintestinal disease in humans and other mammals was used to analyze the VG repertoire of 23 commensal E. coli isolates from healthy pigs and 52 clinical isolates associated with porcine neonatal diarrhea (ND) and postweaning diarrhea (PWD). The relationship between the presence and absence of VGs was interrogated using three statistical methods. According to the generalized linear model, 17 of 58 VGs were found to be significant (P < 0.05) in distinguishing between commensal and clinical isolates. Nine of the 17 genes represented by iha, hlyA, aidA, east1, aah, fimH, iroN(E).(coli), traT, and saa have not been previously identified as important VGs in clinical porcine isolates in Australia. The remaining eight VGs code for fimbriae (F4, F5, F18, and F41) and toxins (STa, STh, LT, and Stx2), normally associated with porcine enterotoxigenic E. coli. Agglomerative hierarchical algorithm analysis grouped E. coli strains into subclusters based primarily on their serogroup. Multivariate analyses of clonal relationships based on the 17 VGs were collapsed into two-dimensional space by principal coordinate analysis. PWD clones were distributed in two quadrants, separated from ND and commensal clones, which tended to cluster within one quadrant. Clonal subclusters within quadrants were highly correlated with serogroups. These methods of analysis provide different perspectives in our attempts to understand how commensal and clinical porcine enterotoxigenic E. coli strains have evolved and are engaged in the dynamic process of losing or acquiring VGs within the pig population.

Pathotypes and serogroups of enterotoxigenic Escherichia coli isolated from pre-weaning pigs in north Vietnam

The contribution of enterotoxigenic Escherichia coli (ETEC) to pre-weaning diarrhoea was investigated over a 6 month period at five selected commercial piggeries (CPs) in north Vietnam with at least 100 sows each. Diarrhoea was found to affect 71(.)5% of the litters born during the period of study. Of 406 faecal specimens submitted for bacteriological culture, 200 (49(.)3%) yielded a heavy pure culture of E coli and 126(31 %)were confirmed by PCR to carry at least one of eight porcine ETEC virulence genes. ETEC was responsible for 43% of cases of diarrhoea in neonatal pigs during the first 4 days of life and 23(.)9% of the remaining cases up until the age of weaning. Pathotypes were determined by PCR for the 126 ETEC isolates together with 44 ETEC isolates obtained from village pigs (VPs) raised by smallholder farmers. The CP isolates belonged to five pathotypes, four of which were also identified in VP isolates. Haemolytic serogroup O149: K91 isolates that belonged to F4/STa/STb/LT were most commonly identified in both CPs (33 % of isolates) and VPs (45(.)5%). Other combinations identified in both production systems included O64 (F5/STa), O101 (F4/STa/STb) and O-nontypable (F-/STb). A high proportion of CP isolates (22(.)3 %) possessed all three enterotoxins (STa/STWLT), lacked the genes for all five tested fimbriae (F4, F5, F6, F41 and F18) and belonged to serogroup O8. These unusual 08 F- isolates were haemolytic and were isolated from all ages of diarrhoeic piglets at each CP, suggesting that they have pathogenic potential.

No bastó con los derechos humanos : Sin límites II

Fondo Margaritainés Restrepo

Las píldoras de la felicidad, tranquilizantes : la pequeña química del confort masivo

Fondo Margaritainés Restrepo

Camajanes de perica y a las siete a la camita : sesenta revoluciones por segundo 3

Fondo Margaritainés Restrepo

Exposição à radiação em exames de corpo inteiro de 18F-FDG PET-TC

O sistema de PET-TC resulta da combinação de duas modalidades de imagem médica: a Tomografia Computorizada (TC), que permite obter imagens anatómicas precisas, e a Tomografia por Emissão de Positrões (PET), que oferece imagens moleculares do corpo humano. Num exame hibrido de PET-TC, para além da exposição interna, o doente é também submetido a uma exposição externa devida à irradiação do mesmo por uma fonte externa, referente à aquisição dos dados de TC. Como tal, o exame de PET-TC tem associado um aumento da exposição para o doente [Huang, 2009], pelo que normalmente os scans de TC são adquiridos com baixa dose [Nunes,2011]. Pretende-se com este trabalho, estabelecer um método capaz de estimar a dose efetiva em exames de corpo inteiro de 18F-FDG PET-TC, uma vez que existem diversos métodos para realizar análise dosimétrica dos exames individuais de PET e de TC, e comparar os valores obtidos com os valores utilizados em outros países. Foram recolhidos dados de 24 pacientes que efetuaram exames de corpo inteiro de PET-TC com 18F-FDG no ICNAS, por questões de saúde e por necessidade própria, com o intuito de estimar a dose efetiva associada a esses exames. Para estimar a dose efetiva referente ao exame de TC recorreu-se ao valor de DLP, fornecido pelo equipamento de TC com controlo de qualidade em dia, e ao método dos coeficicientes de dose efetiva normalizados, proposto pela CE, obtendo-se um valor de dose de 4.75 mSv. A dose efetiva do exame de PET foi calculada com base nos valores da atividade no momento de aquisição das imagens e em coeficientes de dose para a PET, obtendo-se um valor de dose de 4.77 mSv. Concluiu-se que para os pacientes sujeitos ao exame de corpo inteiro de 18F-FDG PET-TC, foi registado um valor de dose de 9.47 mSv de dose efetiva. Este valor de dose efetiva para os exames de PET-TC é significativamente mais baixo comparativamente aos valores registados em vários estudos internacionais (13.65 mSv, 14.3 mSv, 18.85 mSv, 24.8 mSv, 25 mSv, 32.18 mSv), dos quais apenas no estudo de Brix um dos hospitais estudados regista um valor ligeiramente inferior, de 8.5 mSv. Com este estudo foi possível determinar o valor de exposição à radiação a que os pacientes do ICNAS se encontram sujeitos em exames de corpo inteiro de 18F-FDG PET-TC considerando as duas modalidades de imagem médica.

Los mejillones del fantasma de Molly : a las 10 : 30 de la noche

Fondo Margaritainés Restrepo

Feeding the Gut Microbiome and Immune Maturation to Manage Weaned Piglets

This thesis reports five studies that may contribute to understand how weaning affects the immune and intestinal microbiota maturation of the piglet and proposes some possible nutritional strategies to attenuate its negative effects. The first study showed that weaning is associated in Payer’s patches with the activation of MHC response against class I antigens and that related to the stimulation to IFN-γ and showed, for the first time, that their blood at weaning remains dominated by immature blood cells. In the second study we tested if the use of a live vaccine against a conditionally but also genetically based intestinal disease, like PWD, could have an impact on the growth performance of pigs and their intestinal microbiota and if it could provide a model to test the response to nutritional strategies under conditions of an immune and intestinal stimulation for animals susceptible to ETEC type. In this study, we demonstrated how a vaccinal strain of F4/F18 E. coli can affect the gut microbial composition of piglets, regardless of their genetic susceptibility to ETEC infection. In the third study we evidenced how a nucleotide supplementation can favor the proliferation of jejunal Peyer patches and anticipate the maturation of the fecal microbiota. In the fourth study we reported how xylanase can favor the proliferation of Lactobacillus reuteri. Finally, we showed some first results on the muscles fiber development in fast- and slow-growing suckling pigs and the relationship with the intestinal microbiota. Taken together, the results presented in this thesis provide new insight about the interplay between the host-genetics, gut microbial composition, and host physiological status. Furthermore, it provides confirmation that the use of known genetic markers for ETEC F4 and F18 could represent a potential tool to stratify the animals in the trials both in healthy or challenge-based protocols.