Concentrations and deficiencies of minerals in cattle submitted to a diagnostic laboratory in Saskatchewan from 2003-2012: A retrospective study.

Trace mineral analyses of samples submitted to Prairie Diagnostic Services laboratory from Saskatchewan cattle between 2003 and 2012 were examined, with the objective of describing trends and reporting concentrations and deficiencies of minerals. Deficiencies were observed with copper, iron, manganese, magnesium, zinc, and cobalt. Deficiency was most commonly seen in copper, followed by iron, manganese, and magnesium accounting for 47.2%, 15.1%, 13.0%, and 10.8% of deficiencies, respectively. Deficiency in cobalt was least common followed by zinc accounting for 4.2% and 9.7% of deficiencies, respectively. The following minerals were also analyzed: barium, beryllium, bismuth, cadmium, chromium, antimony, tin, molybdenum, strontium, thallium, and vanadium. Submissions from 1434 animals were reviewed and a diagnosis of mineral deficiency was made for 509 animals with 92 of these having multiple deficiencies. There were significant differences in the number of deficient animals by year (P = 0.001), age group (P = 0.01), but not month (P = 0.109) or soil type (P = 0.172).

Concentrations et déficiences en minéraux dans des échantillons bovins soumis à un laboratoire de diagnostic en Saskatchewan entre 2003­2012 : une étude rétrospective. Les résultats d'analyse pour les oligo-éléments dans des échantillons provenant de bovins en Saskatchewan soumis au laboratoire de Prairie Diagnostic Services entre 2003 et 2012 furent examinés, avec comme objectif de décrire les tendances et rapporter les concentrations et déficiences en minéraux. Des déficiences furent observées pour le cuivre, le fer, le manganèse, le magnésium, le zinc, et le cobalt. Les déficiences étaient les plus fréquemment rencontrées avec le cuivre, suivi du fer, manganèse, et magnésium représentant 47,2 %, 15,1 %, 13,0 %, et 10,8 % des déficiences, respectivement. La déficience en cobalt était moins fréquente suivie par le zinc et représentant 4,2 % et 9,7 % des déficiences, respectivement. Les minéraux suivants furent également analysés : barium, béryllium, bismuth, cadmium, chromium, antimoine, étain, molybdène, strontium, thallium, et vanadium. Les soumissions provenant de 1434 animaux furent revues et un diagnostic de déficience en minéraux fut posé chez 509 animaux, avec 92 de ceux-ci ayant des déficiences multiples. Il y avait des différences significatives dans le nombre d'animaux déficients par année (P = 0,001), les groupes d'âge (P = 0,01), mais pas pour les mois (P = 0,109) ou le type de sol (P = 0,172).(Traduit par Dr Serge Messier).

Feline infectious peritonitis in a cat presented because of papular skin lesions.

A 19-week-old neutered male domestic shorthair cat was examined because of multiple raised pruritic skin lesions along the dorsal head and back. Histopathology of biopsies of the lesions detected nodular pyogranulomatous dermatitis with vasculitis and necrosis, leading to a suspicion of feline infectious peritonitis (FIP). Postmortem examination revealed gross lesions consistent with FIP. Histopathologic lesions and positive immunohistochemical staining for feline coronavirus in multiple tissues, including the skin, confirmed the diagnosis of FIP. The current case was similar to previous cases, except for the initial presentation with cutaneous lesions and no other clinical signs, which had not been reported previously.

Péritonite infectieuse féline chez un chat présenté pour des lésions cutanées papuleuses. Un chat domestique commun mâle stérilisé âgé de 19 semaines a été examiné en raison de multiples lésions cutanées prurigineuses épaisses le long de la tête dorsale et du dos. L'histopathologie des biopsies des lésions a détecté une dermatite pyogranulomateuse nodulaire avec vasculite et nécrose, ce qui a soulevé des soupçons de péritonite infectieuse féline (PIF). L'examen post mortem a révélé des lésions macroscopiques conformes à la PIF. Les lésions histopathologiques et la coloration immunohistochimique positive pour le coronavirus félin dans plusieurs tissus, y compris la peau, ont confirmé le diagnostic de PIF. Le cas actuel est semblable aux cas antérieurs, sauf pour la présentation initiale avec des lésions cutanées et aucun autre signe clinique, ce qui n'avait pas été signalé précédemment.(Traduit par Isabelle Vallières).

Metallothionein Expression in Horses With Chronic Liver Disease and Its Correlation With Ki-67 Immunoreactivity.

Chronic liver disease is an important cause of illness in horses, and treatment is mainly supportive. Research into new treatment modalities for humans has shown promising data regarding metallothionein (MT), which has been shown to possess regenerative, antifibrotic, and anti-inflammatory properties. This study aimed to examine the relationship between hepatic MT expression and the histopathologic markers of hepatic inflammation, fibrosis and bile duct proliferation, as well as cellular regeneration in 77 selected cases of chronic liver disease in horses. We hypothesized that higher MT expression would be associated with increased heptocellular proliferation and decreased fibrosis, inflammation, and bile duct proliferation. Hepatocellular MT expression was evaluated with immunohistochemistry. Additionally, cellular regeneration was evaluated with immunohistochemistry for Ki-67, a protein expressed during all active stages of the cell cycle. The severity of inflammation and fibrosis was scored, and bile duct proliferation was assessed by counting bile duct profiles. MT expression was observed in 73 of 77 (94.8%) cases of chronically diseased livers. Ki-67 expression was seen in resident Kupffer cells ( n = 42, 54.6%), lymphocytes ( n = 39, 50.7%), bile duct epithelium ( n = 10, 13.0%), and hepatocytes ( n = 8, 10.4%). MT expression was significantly associated with Ki-67 staining in bile duct epithelium and Kupffer cells. Additionally, median MT expression was higher in cases containing lymphocytic infiltrates as compared with cases with no lymphocytic infiltrate ( P < .05). These findings are the first known report of MT expression within chronic equine hepatic disease.

Accidental selenium toxicosis in lambs.

Acute selenium toxicosis occurred in 3-week-old lambs after accidental over-supplementation by intramuscular injection and caused dyspnea, cyanosis, and sudden death. Pathological lesions included myocardial necrosis, skeletal muscle necrosis, pulmonary edema, hydrothorax, and hydropericardium.

Toxicose accidentelle au sélénium chez des agneaux. Une toxicose aiguë au sélénium s'est produite chez des agneaux âgés de 3 semaines après une supplémentation excédentaire accidentelle par injection intramusculaire et elle a causé des signes de dyspnée, de cyanose et de mort soudaine. Les lésions pathologiques incluaient une nécrose du myocarde, une nécrose du muscle squelettique, un œdème pulmonaire, de l'hydrothorax et de l'hydropéricarde.(Traduit par Isabelle Vallières).

Primary intranasal melanoma with brain invasion in a dog.

A 6-year-old castrated male boxer dog with right-sided dark purulent nasal discharge and acute bilateral blindness was diagnosed on magnetic resonance imaging (MRI) and then on necropsy with primary nasal malignant melanoma that extended into the brain, as well as concurrent ocular melanosis. There was no evidence of metastasis in other organs.

Un cas de mélanome primitif des fosses nasales avec invasion cérébrale chez un chien. Un boxer mâle castré de 6 ans a été présenté pour écoulement nasal purulent et de couleur foncée à droite et perte de vision bilatérale aiguë. Un mélanome malin nasal primaire qui s'étendait dans le cerveau, ainsi qu'une mélanose oculaire, ont été diagnostiqués par imagerie à résonnance magnétique (IRM) puis nécropsie. Il n'y avait pas d'évidence de métastases dans les autres organes.(Traduit par les auteurs).

Relationships of CD163 and CD169 positive cell numbers in the endometrium and fetal placenta with type 2 PRRSV RNA concentration in fetal thymus.

Several routes of porcine reproductive and respiratory virus PRRSV transmission across the porcine diffuse epitheliochorial placentation have been proposed, but none have been proven. The objectives of this study were to investigate associations between numbers of CD163 and CD169 positive macrophages, cathepsin positive areolae, and type 2 PRRSV load at the maternal-fetal interface in order to examine important factors related to transplacental infection. On gestation day 85 ± 1, naïve pregnant gilts were inoculated with PRRSV (n = 114) or were sham inoculated (n = 19). At 21 days post-inoculation (dpi), dams and their litters were humanely euthanized and necropsied. Samples of the maternal-fetal interface (uterus with fully attached placenta) and fetal thymus were collected for analysis by RT-qPCR to quantify PRRSV RNA concentration. The corresponding paraffin-embedded uterine tissue sections were subjected to immunohistochemistry for PRRSV nucleocapsid N protein, CD163, CD169, and cathepsin. Our findings confirm significant increases in the numbers of PRRSV, CD163 and CD169 positive cells at the maternal-fetal interface during type 2 PRRSV infection in pregnant gilts. PRRSV load in fetal thymus was positively related to CD163(+) cell count in endometrium and negatively related to CD163(+) cell count in placenta, but unrelated to CD169 counts or cathepsin positive areolae. The endometrium:placenta ratio of CD163 cells, and to a lesser extent CD169 cells, was significantly associated with an increase fetal viral load in thymus. These findings suggest a more important role for CD163(+) cells following trans-placental PRRSV infection, but dichotomous responses in endometrium and placenta for both CD163 and CD169 cells.

Toxicology for the Equine Practitioner.

A wide variety of toxins cause diseases in the horse and are investigated routinely by veterinarians and veterinary pathologists to identify the cause of illness and death. A complete investigation involves performing a thorough necropsy and requires macroscopic and microscopic examination of lesions and a variety of laboratory testing to obtain an accurate diagnosis. The identification of gross lesions by equine practitioners is often the first step in formulating a diagnostic plan. This article provides a description of selected common toxins producing detectable gross lesions in horses in North America. The article is useful to equine practitioners and veterinary pathologists investigating a toxicology-related death.

The C-8-S-isomers of ergot alkaloids - a review of biological and analytical aspects.

Ergot alkaloids are secondary metabolites that are produced by fungi and contaminate cereal crops and grasses. The ergot alkaloids produced by Claviceps purpurea are the most abundant worldwide. The metabolites exist in two configurations, the C-8-R-isomer (R-epimer) and the C-8-S-isomer (S-epimer). These two configurations can interconvert to one another. Ergot alkaloids cause toxic effects after consumption of ergot-contaminated food and feed at various concentrations. For bioactivity reasons, the C-8-R-isomers have been studied to a greater extent than the C-8-S-isomer since the C-8-S-isomers were considered biologically inactive. However, recent studies suggest the contrary. Analytical assessment of ergot alkaloids now includes the C-8-S-isomers and high concentrations of specific C-8-S-isomers have been identified. The inclusion of the C-8-S-isomer in regulatory standards is reviewed. This review has identified that further research into the C-8-S-isomers of ergot alkaloids is warranted. In addition, the inclusion of the C-8-S-isomers into regulatory recommendations worldwide for food and feed should be implemented. The objectives of this review are to provide an overview of historic and current studies that have assessed the C-8-S-isomers. Specifically, this review will compare the C-8-R-isomers to the C-8-S-isomers with an emphasis on the biological activity and analytical assessment.

An in vitro testicular organoid model for the study of testis morphogenesis, somatic cell maturation, endocrine function, and toxicological assessment of endocrine disruptors.

Male reproductive capacity has fallen considerably in recent decades; in addition, the incidence of testicular cancer has increased in many developed countries. The cause of this phenomenon is unknown, but environmental toxicants are considered a major contributing factor. To study potential reproductive toxicants, robust in vitro testis models are needed. We have recently established a porcine testis organoid system with a high resemblance to the architectures of innate testis tissue. Here, we further investigated the testis morphogenesis, cell maturation, and endocrine function of the testis organoids. We also challenged this system with abiraterone, a steroidogenic inhibitor, to validate its suitability as an in vitro platform for endocrine toxicology tests. Our results showed that the testis cells in the organoids reorganize into testis cordal structures, and the cordal relative areas increase in the organoids over time of culture. Moreover, the diameters and cell numbers per cross-section of the cordal structures increased over time. Interestingly, Sertoli cells in the organoids gradually underwent maturational changes by showing increased expression of androgen receptors, decreased expression of the anti-müllerian hormone, and formation of the blood-testis barrier. Next, we confirmed that the organoids respond to hormonal stimulation and release multiple sex hormones, including testosterone, estradiol, and progesterone. Finally, we showed that the production of testosterone and estradiol in this system can be inhibited in response to the steroidogenic inhibitor. Taken together, our organoid system provides a promising in vitro platform for male reproductive toxicology studies on testis morphogenesis, somatic cell maturation, and endocrine production.

Time-course of oral toxicity to contaminated groundwater in male Sprague Dawley rats.

Assessing toxicity of complex mixtures of contaminants from industrial sites with historic and ongoing contamination remains a challenge for risk assessors. Groundwater from a pesticide packaging site in Canada containing a complex mixture of known and unknown contaminants was examined in male rats to determine the target organ toxicity. This study determined the time-course of toxicity (7, 14, 28, and 60 days) following ad libitum oral exposure to 0.05% v/v contaminated groundwater compared to tap water (control) in male Sprague Dawley rats (n=5 /group/time). Exposure to groundwater resulted in inflammation, indicated by a statistically significant increase in plasma lymphocyte and neutrophil counts on days 7 and 60, respectively, but a reduction in the plasma alpha 2 macroglobulin levels by day 60. Gonadotoxicity was indicated by a reduced Johnsen score (grading spermatogenesis) in all exposed groups at all time points, while seminiferous epithelial height was reduced on days 7, 14, and 28 compared to controls. Plasma testosterone was reduced in exposed groups on days 7 and 28, accompanied by elevated testicular lipid peroxidation at all time points compared to control. In contrast, lipid peroxidation in the lungs from exposed rats was elevated on days 7, 14, and 28. Plasma symmetric dimethylarginine was elevated on day 14 in the exposed group indicating renal impairment. Taken together, these results indicate that testes, kidney, immune and lung are target organs for the contaminated groundwater from this industrial site. The current study highlights the challenge in hazard assessment for complex mixtures and highlights the need for effects-directed analysis and the continued, albeit limited, use of animal models in toxicity testing.

Correlation between E-cadherin expression and tumor grade, proliferation, microvascular density, and apoptosis in canine cutaneous squamous cell carcinoma.

E-cadherin is an adhesion molecule expressed on epithelial surfaces. Loss of its expression is described in cancerous tissues. Here, we examined the expression of E-cadherin in canine cutaneous squamous cell carcinoma (SCC) and determined its association with tumor grade (TG), proliferation index (PI), apoptosis index (AI), and intra-tumoral microvascular density (iMVD) in archived samples. Thirty-six cutaneous SCC samples (archived from 2014 to 2019) were graded and E-cadherin level, Ki67 (PI), von Willebrand factor (iMVD), and apoptosis (AI) were determined immunohistochemically. Tumor grades were assigned as Grade 1 (n = 18), Grade 2 (n = 16), and Grade 3 (n = 2). Of the 36 tumors, 21 were digital and 15 were from other locations, including the tail, neck, ear, and elbow. The median E-cadherin score decreased statistically (P = 0.03) with an increase in TG. There was a negative association between median E-cadherin score and TG (r = -0.445, P = 0.013), AI (r = -0.342, P = 0.08), and PI (r = -0.459, P = 0.016). The median E-cadherin score was significantly higher in digital SCC compared to SCC from other locations (P = 0.035). In conclusion, a negative association was observed between TG, PI, AI, and E-cadherin.

La E-cadhérine est une molécule d'adhésion exprimée sur les surfaces épithéliales. La perte de son expression est décrite dans les tissus cancéreux. Ici, nous avons examiné l'expression de la E-cadhérine dans le carcinome épidermoïde cutané canin (SCC) et déterminé son association avec le grade de la tumeur (TG), l'indice de prolifération (PI), l'indice d'apoptose (AI) et la densité microvasculaire intra-tumorale (iMVD) dans des échantillons archivés. Trente-six échantillons de SCC cutanés (archivés de 2014 à 2019) ont été classés et le niveau d'E-cadhérine, Ki67 (PI), le facteur von Willebrand (iMVD) et l'apoptose (AI) ont été déterminés par immunohistochimie. Les grades de tumeur ont été attribués au grade 1 (n = 18), au grade 2 (n = 16) et au grade 3 (n = 2). Sur les 36 tumeurs, 21 étaient digitales et 15 provenaient d'autres localisations, notamment la queue, le cou, l'oreille et le coude. Le score médian de la E-cadhérine a diminué statistiquement (P = 0,03) avec une augmentation des TG. Il y avait une association négative entre le score médian de la E-cadhérine et TG (r = −0,445, P = 0,013), AI (r = −0,342, P = 0,08) et PI (r = −0,459, P = 0,016). Le score médian de la E-cadhérine était significativement plus élevé dans les SCC des doigts par rapport au SCC provenant d'autres sites (P = 0,035). En conclusion, une association négative a été observée entre TG, PI, AI et E-cadhérine.(Traduit par Docteur Serge Messier).

Examining the subchronic (28-day) effects of aqueous Cd-BaP co-exposure on detoxification capacity and cardiac function in adult zebrafish (Danio rerio).

The present study aimed to examine the effects of environmentally relevant concentrations of cadmium (Cd) and Benzo[a]Pyrene (BaP) in the adult zebrafish (Danio rerio). To this end, fish were exposed to either 1 or 10 µg/L Cd or 0.1 or 1 µg/L BaP in isolation, or a co-exposure containing a mixture of the two toxicants. Our results showed extensive modulation of the expression of key antioxidant genes (GPx, SOD1, catalase), detoxifying genes (MT1, MT2, CYP1A1) and a stress biomarker (HSP70) differing between control, single toxicant groups and co-exposure groups. We additionally carried out histopathological analysis of the gills, liver, and hearts of exposed animals, noting no differences in tissue necrosis or apoptosis. Finally, we carried out ultrasonographic analysis of cardiac function, noting a significant decrease of E-wave peak velocity and end diastolic volume in exposed fish. This in turn was accompanied by a decrease in stroke volume and ejection fraction, but not cardiac output in co-exposed fish. The present study is the first to demonstrate that a subchronic aqueous exposure to a Cd-BaP mixture can extensively modulate detoxification capacity and cardiac function in adult zebrafish in a tissue-specific manner.

Investigation of the relationship between ergocristinine and vascular receptors.

Ergot alkaloids are secondary metabolites that exist in two configurations, the C-8-R-isomer (R-epimer), and the C-8-S-isomer (S-epimer). Toxic effects of ergot, such as vasoconstriction, have been primarily attributed to the R-epimer bioactivity, as compared to the S-epimer. Recent studies demonstrated potential bioactivity of S-epimers. Therefore, further cost-effective investigations of the S-epimers are needed. The present study investigated the S-epimer - vascular receptor binding relationship. An in silico molecular docking approach, utilizing AutoDock Vina and DockThor, was used to determine if the S-epimer (ergocristinine) binds to vascular receptors and to compare the binding affinity and interactions to the corresponding R-epimer (ergocristine) and a structural analogue (lysergic acid amide). The binding energy (kcal/mol) of ergocristinine was - 9.7 or - 11.0 to the serotonin (5-HT) 2 A receptor and - 8.7 or - 11.4 to the alpha 2 A adrenergic receptor, depending on the software used. A hydrogen bond was formed between ergocristinine and amino acid residues of the 5-HT 2 A and alpha 2 A adrenergic receptor binding sites, with bond lengths of 3.10 Å and 3.28 Å, respectively. Binding affinities and molecular interactions among the ligands to each receptor differed. Different affinities and interactions may relate to differences in the chemical structures. The binding affinities and strong molecular interactions of the S-epimer to vascular receptors may contribute to the observed physiological manifestations that occur after ergot alkaloid exposure. The results of the present study suggest further investigation on the receptor binding of the S-epimers of ergot alkaloids.

The Impact of Storage Temperature and Time on Ergot Alkaloid Concentrations.

Ergot sclerotia produce toxic secondary metabolites, ergot alkaloids, that infect cereal crops and grasses. Ergot alkaloids have two isomeric configurations: the C-8-R-isomer (R-epimer), and the C-8-S-isomer (S-epimer). Ergot contaminated matrices, such as cereal grains or grasses, may be stored for extended periods at various temperatures before being analyzed, utilized, or consumed. This study assessed the concentration of six common ergot alkaloids in both configurations found in naturally contaminated wheat over time (one, two, and four months) at different temperatures (room temperature, +4 °C, and -20 °C) using ultra-high-performance liquid chromatography-tandem mass spectrometry. The data indicate that the total ergot concentration within a natural contaminated sample varies over time at room temperature, +4 °C, and -20 °C. The total ergot concentration increased until month two, and decreased at month four, independent of temperature (p < 0.05). The total R-epimer concentration appeared to be less stable over time than the total S-epimer concentration. The changes in the total R and total S-epimer concentrations may have been caused by changes in the ergocristine and ergocristinine concentrations, respectively. Time and temperature should be considered when storing potentially contaminated matrices in a laboratory or practical agriculture situations. Quantification of ergot contaminated matrices should occur prior to their use to ensure the most reliable estimates of the concentration of ergot.

Correlation of hepatic copper levels, rhodanine scores and histological diagnosis in archived canine liver samples.

The liver is the main storage site for copper. Excess copper accumulation, however, is a risk factor for the development of chronic hepatitis in dogs. Mass spectrometry or rhodanine staining are frequently used methods to assess copper levels in the liver. The association was studied between analytic hepatic copper levels and rhodanine scores in archived canine formalin-fixed-paraffinembedded liver sections from 2014 to 2021 with various diagnoses. Thirty-six (N = 36) liver samples with analytic interpretation of toxic (n = 12), high normal (n = 17), and normal (n = 7) copper levels were selected for the study. Rhodanine staining for each of these samples was graded (scale: 1 to 5), and the association was determined between actual liver copper levels and rhodanine scores and histological diagnoses (chronic hepatitis or other diagnoses). The analytic copper level and rhodanine scores were significantly higher (P < 0.05) in samples designated as toxic compared to normal. There was a significant association between hepatic copper levels and rhodanine scores (P < 0.05). Rhodanine score, but not the actual liver copper levels were significantly (P < 0.05) associated with chronic hepatitis versus other diagnoses. Rhodanine scores of ≥ 1.89 were statistically significant predictors of chronic hepatitis. It was concluded from this study that actual liver copper levels are positively associated with rhodanine scores and rhodanine scores can be a useful predictor of chronic hepatitis.

Le foie est le principal site de stockage du cuivre. Cependant, une accumulation excessive de cuivre est un facteur de risque pour le développement d'une hépatite chronique chez le chien. La spectrométrie de masse ou la coloration à la rhodanine sont des méthodes fréquemment utilisées pour évaluer les niveaux de cuivre dans le foie. L'association entre les niveaux analytiques de cuivre hépatique et les scores de rhodanine a été étudiée dans des sections de foie de chien archivées fixées au formol et incluses dans de la paraffine de 2014 à 2021 avec divers diagnostics. Trente-six (N = 36) échantillons de foie avec interprétation analytique des niveaux de cuivre toxiques (n = 12), normaux élevés (n = 17) et normaux (n = 7) ont été sélectionnés pour l'étude. La coloration à la rhodanine de chacun de ces échantillons a été évaluée (échelle : 1 à 5) et l'association a été déterminée entre les niveaux réels de cuivre dans le foie et les scores de rhodanine et les diagnostics histologiques (hépatite chronique ou autres diagnostics). Les niveaux analytiques de cuivre et les scores de rhodanine étaient significativement plus élevés (P < 0,05) dans les échantillons désignés comme toxiques par rapport à la normale. Il y avait une association significative entre les niveaux de cuivre hépatique et les scores de rhodamine (P < 0,05). Le score de rhodanine, mais pas les niveaux réels de cuivre dans le foie, était significativement (P < 0,05) associé à l'hépatite chronique par rapport à d'autres diagnostics. Les scores de rhodanine ≥ 1,89 étaient des prédicteurs statistiquement significatifs de l'hépatite chronique. Il a été conclu à partir de cette étude que les niveaux réels de cuivre dans le foie sont positivement associés aux scores de rhodanine et que les scores de rhodanine peuvent être un prédicteur utile de l'hépatite chronique.(Traduit par Docteur Serge Messier).

Prolonged absorption and susceptibility to enterohepatic circulation after oral administration of ergot alkaloids in ewes.

The objective of this study was to evaluate the pharmacokinetics profile of ergot alkaloids when administered to sheep orally. Although ergot alkaloids frequently contaminate animal feed, current understanding of their pharmacokinetics in animals cannot adequately predict toxicity. Blood samples were collected from ewes at 0.5, 1, 3, 5, and 12 h after oral exposure to 4 ergot alkaloids: ergocornine, ergocristine, ergocryptine, and ergosine, followed by serum analysis of these alkaloids using high performance liquid chromatography and tandem mass spectrometry. The alkaloids showed extended absorption time, in addition to clear signs of enterohepatic circulation. This pharmacokinetic profile suggests potential enhanced toxicity in animals with disorders related to secretion of bile acid. It may also explain the high susceptibility of sheep to ergot poisoning compared to other species. An extended sampling protocol (> 12 h) is necessary, however, to identify the pharmacokinetic properties of ergot alkaloids in ewes. In conclusion, ewes exposed to ergot alkaloids showed a prolonged absorption phase and enterohepatic circulation, which is in contrast with human ergot pharmacokinetics.

L'objectif de cette étude était d'évaluer le profil pharmacocinétique des alcaloïdes de l'ergot lorsqu'ils sont administrés à des moutons par voie orale. Bien que les alcaloïdes de l'ergot contaminent fréquemment les aliments pour animaux, la compréhension actuelle de leur pharmacocinétique chez les animaux ne permet pas de prédire de manière adéquate la toxicité. Des échantillons de sang ont été prélevés chez les brebis à 0,5, 1, 3, 5 et 12 h après exposition orale à quatre alcaloïdes de l'ergot : ergocornine, ergocristine, ergocryptine et ergosine, suivi d'une analyse sérique de ces alcaloïdes par chromatographie liquide à haute performance et spectrométrie de masse en tandem. Les alcaloïdes ont montré un temps d'absorption prolongé, en plus de signes évidents de circulation entérohépatique. Ce profil pharmacocinétique suggère une toxicité potentiellement accrue chez les animaux présentant des troubles liés à la sécrétion d'acide biliaire. Cela peut également expliquer la forte sensibilité des moutons à l'empoisonnement par l'ergot par rapport aux autres espèces. Un protocole de prélèvement étendu (> 12 h) est cependant nécessaire pour identifier les propriétés pharmacocinétiques des alcaloïdes de l'ergot chez les brebis. En conclusion, les brebis exposées aux alcaloïdes ont montré une phase d'absorption prolongée et une circulation entérohépatique, ce qui contraste avec la pharmacocinétique de l'ergot chez l'humain.(Traduit par Docteur Serge Messier).

Sustained vascular contractile response induced by an R- and S-epimer of the ergot alkaloid ergocristine and attenuation by a noncompetitive antagonist.

Vasoconstriction is a known effect associated with ergot alkaloid consumption. The vascular contractile responses are often sustained for an extended period after exposure. Ergot alkaloids exist in two molecular configurations, the C-8-(R)-isomer (R-epimer) and the C-8-(S)-isomer (S-epimer). The sustained vascular contractile response to the R-epimers has been studied previously, unlike the S-epimers which are thought to be biologically inactive. Additionally, antagonists have been utilized to attenuate the vascular contraction associated with the R-epimers of ergot alkaloids utilizing ex vivo techniques. This study utilized an arterial tissue bath to examine and compare the sustained vascular contractile response attributed to ergocristine (R) and ergocristinine (S) using dissected bovine metatarsal arteries. The contractile blocking effect of a noncompetitive alpha-adrenergic antagonist, phenoxybenzamine (POB), was also investigated in precontracted arteries. Arteries (n = 6/epimer) were exposed to a single dose of ergocristine or ergocristinine (1 × 10-6 M in buffer). Each of the epimer doses was followed by a POB (1 × 10-3 M) or methanol (control) treatment at 90 min and the response was observed for another 90 min. Both epimers produced a sustained contractile response over the 180-min incubation period in the control groups. The R-epimer caused a greater sustained contractile response from 60 to 180 min post epimer exposure, compared to the S-epimer (P < 0.05, generalized estimating equations, independent t-test). Phenoxybenzamine caused a decrease in the contractile response induced by ergocristine and ergocristinine from 105 to 180 min, compared to the control (P < 0.05, generalized estimating equations, paired t-test). Overall, these results demonstrate the presence of a sustained vascular contractile response attributed to the R- and S-epimer of an ergot alkaloid with differences in contractile response between the epimers, suggesting differences in receptor binding mechanisms. Furthermore, this study demonstrated that a noncompetitive antagonist could attenuate the sustained arterial contractile effects of both ergot configurations ex vivo. Additional investigation into S-epimers of ergot alkaloids is needed. This research contributes to the understanding of the ergot epimer-vascular receptor binding mechanisms, which may support the investigation of different approaches of minimizing ergot toxicity in livestock.

Ergot alkaloids cause blood vessels to contract when contaminated feed is consumed by animals. Vascular contraction often remains for a prolonged period and involves the binding of ergot to specific receptors in the blood vessels. This study assessed and compared the sustained contraction of cow arteries after exposure to two forms of an ergot alkaloid, namely, ergocristine and ergocristinine. The effects of a specific receptor blocker, phenoxybenzamine, on the vascular contraction induced by these forms were also examined. This study showed that both forms of ergot caused a sustained contraction of cow arteries but to different magnitudes. Differences in contraction could be related to differences in how each form of ergot binds to receptors. The receptor blocker decreased the sustained contractile response of both forms of ergot. Further understanding of how the different forms of ergot bind to receptors, and how to decrease the adverse effects, may help mitigate the toxic effects of ergotism.

Ammonization of the R- and S-Epimers of Ergot Alkaloids to Assess Detoxification Potential.

Detoxification of ergot-contaminated feed by ammonia would be a practical application, given that ammonia is routinely used in the agriculture industry. To assess the effects of ammonia on ergot alkaloids, natural ergot-contaminated wheat was ammoniated. The total concentration of ergot alkaloids (R- and S-epimers) decreased after exposure to ammonia (8-29%). Separately, the total R-epimers decreased in concentration (40-66%), whereas the total S-epimers increased (21-81%). Specific ergot alkaloids demonstrated degradation and/or epimerization after exposure to ammonia, potentially associated with structural differences, and influenced the total concentrations observed. Ammonization of ergot standards resulted in potential degradation products and epimerization, supporting the above results. The use of ultrahigh-performance liquid chromatography-tandem mass spectrometry provides an updated assessment of the detoxification potential of ammonia for ergot alkaloids and the quantification of the S-epimers. Ammonia alters the R- and S-epimers of ergot alkaloids, which may lead to a potential practical detoxification process of ergot-contaminated feed.

A case of biphasic mesothelioma with osseous and chondromatous differentiation in a cat.

An 11-year-old domestic short hair cat with dyspnea, cyanosis, and pleural effusion died. Necropsy revealed several nodules and masses on the parietal pleura, pericardium, and diaphragm. The tumor contained epithelial and mesenchymal components and displayed osseous and chondromatous differentiation. Tumors cells were positive for pancytokeratin and vimentin. This is the first report of a biphasic mesothelioma with osseous and chondromatous differentiation in this species.

Selenium toxicosis in a white-tailed deer herd.

Chronic selenium (Se) toxicosis was found in a herd of white-tailed deer showing signs of anorexia, weight loss, and lameness. Concentration of Se in the liver ranged from 2.7 to 8.97 mg/kg wet weight. Myocardial necrosis, mineralization, and fibroplasia were seen histologically. This is the first report of this toxicosis in white-tailed deer.