Your search keyword '"C. Ersdal"' showing total 37 results

1. LPS-induced systemic inflammation reveals an immunomodulatory role for the prion protein at the blood-brain interface

Author

Ø. Salvesen, M. R. Reiten, A. Espenes, M. K. Bakkebø, M. A. Tranulis, and C. Ersdal

Subjects

Cellular prion protein, Systemic inflammation, Lipopolysaccharide (LPS), Innate immunity, Choroid plexus, Hippocampus, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background The cellular prion protein (PrPC) is an evolutionary conserved protein abundantly expressed not only in the central nervous system but also peripherally including the immune system. A line of Norwegian dairy goats naturally devoid of PrPC (PRNP Ter/Ter) provides a novel model for studying PrPC physiology. Methods In order to explore putative roles for PrPC in acute inflammatory responses, we performed a lipopolysaccharide (LPS, Escherichia coli O26:B6) challenge of 16 goats (8 PRNP +/+ and 8 PRNP Ter/Ter) and included 10 saline-treated controls (5 of each PRNP genotype). Clinical examinations were performed continuously, and blood samples were collected throughout the trial. Genome-wide transcription profiles of the choroid plexus, which is at the blood-brain interface, and the hippocampus were analyzed by RNA sequencing, and the same tissues were histologically evaluated. Results All LPS-treated goats displayed clinical signs of sickness behavior, which were of significantly (p

Published

2017

2. Early neonatal lamb mortality: postmortem findings

Author

I.H. Holmøy, S. Waage, E.G. Granquist, T.M. L’Abée-Lund, C. Ersdal, L. Hektoen, and R. Sørby

Subjects

sheep, neonatal, lamb mortality, postmortem, Animal culture, SF1-1100

Abstract

An investigation of stillbirth and early neonatal lamb mortality was conducted in sheep flocks in Norway. Knowledge of actual causes of death are important to aid the interpretation of results obtained during studies assessing the risk factors for lamb mortality, and when tailoring preventive measures at the flock, ewe and individual lamb level. This paper reports on the postmortem findings in 270 liveborn lambs that died during the first 5 days after birth. The lambs were from 17 flocks in six counties. A total of 27% died within 3 h after birth, 41% within 24 h and 80% within 2 days. Most lambs (62%) were from triplet or higher order litters. In 81% of twin and larger litters, only one lamb died. The most frequently identified cause of neonatal death was infectious disease (n=97, 36%); 48% (n=47) of these died from septicaemia, 25% (n=24) from pneumonia, 22% (n=21) from gastrointestinal infections and 5% (n=5) from other infections. Escherichia coli accounted for 65% of the septicaemic cases, and were the most common causal agent obtained from all cases of infection (41%). In total, 14% of neonatal deaths resulted from infection by this bacterium. Traumatic lesions were the primary cause of death in 20% (n=53) of the lambs. A total of 46% of these died within 3 h after birth and 66% within 24 h. Severe congenital malformations were found in 10% (n=27) of the lambs, whereas starvation with no concurrent lesions was the cause of death in 6% (n=17). In 16% (n=43) of the lambs, no specific cause of death was identified, lambs from triplet and higher order litters being overrepresented among these cases. In this study, the main causes of neonatal lamb mortality were infection and traumatic lesions. Most neonatal deaths occurred shortly after birth, suggesting that events related to lambing and the immediate post-lambing period are critical for lamb survival.

Published

2017

3. O-137 Campylobacter as a cause of ovine abortion

Author

C. Ersdal, S. Lystad, S. Loopstra, and S. Rodriguez-Campos

Published

2023

4. O-138 Bilateral otitis media in a six-month-old lamb

Author

C. Ersdal, M. Ruiz De Arcaute Rivero, E. Castells, L.M. Ferrer, M. Climent, M. De Las Heras, and D. Lacasta

Published

2023

5. Additional file 4: of LPS-induced systemic inflammation reveals an immunomodulatory role for the prion protein at the blood-brain interface

Author

Ø. Salvesen, M. Reiten, A. Espenes, M. Bakkebø, M. Tranulis, and C. Ersdal

Abstract

Gene ontology analyses of DEGs after LPS challenge. (PDF 312 kb)

Published

2017

6. Additional file 2: of LPS-induced systemic inflammation reveals an immunomodulatory role for the prion protein at the blood-brain interface

Author

Ø. Salvesen, M. Reiten, A. Espenes, M. Bakkebø, M. Tranulis, and C. Ersdal

Subjects

body regions, nervous system, fungi, lipids (amino acids, peptides, and proteins)

Abstract

Hematology and biochemistry after LPS challenge. (PDF 590 kb)

Published

2017

7. Additional file 5: of LPS-induced systemic inflammation reveals an immunomodulatory role for the prion protein at the blood-brain interface

Author

Ø. Salvesen, M. Reiten, A. Espenes, M. Bakkebø, M. Tranulis, and C. Ersdal

Abstract

Validation of RNAseq data by qPCR. (PDF 484 kb)

Published

2017

8. Additional file 1: of LPS-induced systemic inflammation reveals an immunomodulatory role for the prion protein at the blood-brain interface

Author

Ø. Salvesen, M. Reiten, A. Espenes, M. Bakkebø, M. Tranulis, and C. Ersdal

Abstract

Material and methods. Study groups, experimental protocol, RNA quality control, RNA sequencing quality control and mapping status, and primer sequences. (PDF 395 kb)

Published

2017

9. Additional file 3: of LPS-induced systemic inflammation reveals an immunomodulatory role for the prion protein at the blood-brain interface

Author

Ø. Salvesen, M. Reiten, A. Espenes, M. Bakkebø, M. Tranulis, and C. Ersdal

Subjects

body regions, nervous system, fungi, sense organs, eye diseases

Abstract

List of upregulated and downregulated genes in choroid plexus after LPS challenge. (PDF 458 kb)

Published

2017

10. Early neonatal lamb mortality: postmortem findings

Author

C. Ersdal, T.M. L’Abée-Lund, Steinar Waage, L. Hektoen, Erik Georg Granquist, Ingrid H. Holmøy, and R. Sørby

Subjects

medicine.medical_specialty, 040301 veterinary sciences, animal diseases, Sheep Diseases, SF1-1100, Congenital Abnormalities, 0403 veterinary science, neonatal, Pregnancy, Risk Factors, medicine, Animals, lamb mortality, Cause of death, Starvation, postmortem, Lamb mortality, Sheep, Obstetrics, business.industry, Norway, Domestic sheep reproduction, 0402 animal and dairy science, Congenital malformations, 04 agricultural and veterinary sciences, respiratory system, Stillbirth, medicine.disease, 040201 dairy & animal science, Animal culture, Pneumonia, Animals, Newborn, Animal Science and Zoology, Female, Flock, Neonatal death, medicine.symptom, business

Abstract

An investigation of stillbirth and early neonatal lamb mortality was conducted in sheep flocks in Norway. Knowledge of actual causes of death are important to aid the interpretation of results obtained during studies assessing the risk factors for lamb mortality, and when tailoring preventive measures at the flock, ewe and individual lamb level. This paper reports on the postmortem findings in 270 liveborn lambs that died during the first 5 days after birth. The lambs were from 17 flocks in six counties. A total of 27% died within 3 h after birth, 41% within 24 h and 80% within 2 days. Most lambs (62%) were from triplet or higher order litters. In 81% of twin and larger litters, only one lamb died. The most frequently identified cause of neonatal death was infectious disease (n=97, 36%); 48% (n=47) of these died from septicaemia, 25% (n=24) from pneumonia, 22% (n=21) from gastrointestinal infections and 5% (n=5) from other infections. Escherichia coli accounted for 65% of the septicaemic cases, and were the most common causal agent obtained from all cases of infection (41%). In total, 14% of neonatal deaths resulted from infection by this bacterium. Traumatic lesions were the primary cause of death in 20% (n=53) of the lambs. A total of 46% of these died within 3 h after birth and 66% within 24 h. Severe congenital malformations were found in 10% (n=27) of the lambs, whereas starvation with no concurrent lesions was the cause of death in 6% (n=17). In 16% (n=43) of the lambs, no specific cause of death was identified, lambs from triplet and higher order litters being overrepresented among these cases. In this study, the main causes of neonatal lamb mortality were infection and traumatic lesions. Most neonatal deaths occurred shortly after birth, suggesting that events related to lambing and the immediate post-lambing period are critical for lamb survival.

Published

2016

11. Intestinal adenocarcinomas in three generations of sheep

Author

T. Løken, C. Ersdal, and E. R. Bjørnstad

Subjects

Pathology, medicine.medical_specialty, Sheep, General Veterinary, Thoracic cavity, Sheep Diseases, Ileum, General Medicine, Biology, Adenocarcinoma, Breed, Jejunum, Lymphatic system, medicine.anatomical_structure, Fatal Outcome, Intestinal Neoplasms, medicine, Abdomen, Animals, Female, Genetic Predisposition to Disease, Flock, Clostridial infection

Abstract

INTESTINAL adenocarcinomas are the most frequently reported type of tumours in sheep (Ross 1980) and have also been reported in other domestic animal species and in human beings (Johnstone and others 1983, Hamir 1985, McCoy and others 2009). In sheep, these tumours have a low incidence (Else 2007), although an incidence of up to 6 per cent in some populations has been documented (Simpson and Jolly 1974). In Norway, intestinal adenocarcinomas were described in 2.9 per cent of 1256 adult sheep submitted for postmortem examination over a period of eight-and-a-half years at a research institute (Ulvund 1983). The tumour presents as a stenotic, often annular, firm tissue 3 to 5 cm in length, typically situated in the jejunum or ileum (Georgsson and Vigfusson 1973, Tontis 2006, Munday and others 2006). The neoplastic tissue has a tendency to grow via the intestinal wall to the mesentery and along the serosal lymphatics to the regional lymph node (Munday and others 2006, Brown and others 2007). Metastatic implantations on the peritoneum are common, and the tumour may occasionally spread to the serosal surfaces in the thoracic cavity. In a few cases, haematogenous metastasis to the liver and/or the lungs have been demonstrated (Ross 1980, Ulvund 1983). Accumulation of fluid in the abdomen and thorax is frequent in amounts of up to 35 litres (Ulvund 1983). This short communication describes scirrhous jejunal adenocarcinomas in three closely related ewes in a sheep flock. The flock consisted of approximately 120 winter-fed sheep in eastern Norway. The animals were of the Norwegian White breed, demonstrated high quality and production, and were routinely treated for endoparasites and vaccinated against clostridial infections. During the six-month winter season, the sheep were kept indoors on a slatted wooden floor and fed hay silage and commercial …

Published

2011

12. Abnormal prion protein is associated with changes of plasma membranes and endocytosis in bovine spongiform encephalopathy (BSE)-affected cattle brains

Author

Marion Simmons, Martin Jeffrey, C. Ersdal, Gillian McGovern, and Caroline M. Goodsir

Subjects

Pathology, medicine.medical_specialty, Histology, Prions, animal diseases, Bovine spongiform encephalopathy, Encephalopathy, Scrapie, Endosomes, Biology, Endocytosis, Pathology and Forensic Medicine, Physiology (medical), medicine, Neuropil, Animals, Microscopy, Immunoelectron, Neurodegeneration, Cell Membrane, Brain, Immunogold labelling, Dendrites, medicine.disease, Immunohistochemistry, nervous system diseases, Encephalopathy, Bovine Spongiform, medicine.anatomical_structure, Neurology, Gliosis, Astrocytes, Vacuoles, Cattle, Neurology (clinical), medicine.symptom

Abstract

Aims: Transmissible spongiform encephalopathies (TSEs) or prion diseases are fatal neurodegenerative diseases of man and animals characterized by vacuolation and gliosis of neuropil and the accumulation of abnormal isoforms of a host protein known as prion protein (PrP). It is widely assumed that the abnormal isoforms of PrP (PrPd, disease-specific form of PrP) are the proximate cause of neurodegeneration. Methods: To determine the nature of subcellular changes and their association with PrPd we perfusion-fixed brains of eight bovine spongiform encephalopathy (BSE)-affected cows and three control cattle for immunogold electron microscopy at two different neuroanatomical sites. Results: All affected cattle presented plasma membrane alterations of dendrites and astrocytes that were labelled for PrPd. PrPd on membranes of dendrites and occasionally of neuronal perikarya was associated with abnormal endocytotic events, including bizarre coated pits and invagination of the plasma membrane. BSE-affected cattle also presented excess and abnormal multivesicular bodies, sometimes associated to the plasma membrane perturbations. In contrast, two TSE-specific lesions, vacuolation and rare tubulovesicular bodies, were not labelled for PrPd as were a number of other nonspecific lesions, such as autophagy and dystrophic neurites. At least two different morphological pathways to vacuoles were recognized. Conclusions: When compared with other TSEs, these changes are common to those of sheep and rodent scrapie and shows that there are consistent membrane toxicity properties of PrPd. This toxicity involves an aberration of endocytosis. However, it is by no means clear that the lesions are of sufficient severity to result in clinical deficits.

Published

2009

13. Lethal Gram-negative sepsis in healthy pigs during anaesthesia with contaminated propofol.

Author

Maaland MG, Oropeza-Moe M, Nes SK, Myrland F, Ersdal C, and Oveland NP

Subjects

Animals, Swine, Drug Contamination, Fatal Outcome, Cross Infection veterinary, Cross Infection microbiology, Gram-Negative Bacterial Infections veterinary, Gram-Negative Bacterial Infections microbiology, Klebsiella drug effects, Klebsiella Infections veterinary, Female, Propofol adverse effects, Propofol administration & dosage, Sepsis veterinary, Sepsis microbiology, Sepsis etiology, Swine Diseases chemically induced, Swine Diseases microbiology, Anesthetics, Intravenous adverse effects, Anesthetics, Intravenous administration & dosage

Abstract

Two healthy Landrace pigs anaesthetized with propofol suffered rapid onset of fatal sepsis. Clinical signs included severe arterial hypotension, loss of peripheral oxygenation, low end-tidal CO 2 , clinical onset of pulmonary oedema and cardiac dysfunction. Gross and histopathological examination revealed loss of vascular integrity with severe lung oedema and congestion, haemorrhages in several organs and fluid leakage into body cavities. Large numbers of Gram-negative bacteria, primarily Klebsiella sp., were present in the anaesthetic infusion containing propofol and were also cultured from internal organs of both pigs. The propofol was likely contaminated by bacteria after inappropriate handling and storage in the operating room. This report illustrates the potential for severe nosocomial infection when applying propofol in animals and humans and may serve as a reminder of the importance of strict aseptic practice in general, and specifically in the handling of this anaesthetic agent., Competing Interests: Declaration of conflicting interestsThe authors have no conflicts of interest to declare.

Published

2024

14. Transmission of Norwegian reindeer CWD to sheep by intracerebral inoculation results in an unusual phenotype and prion distribution.

Author

Harpaz E, Cazzaniga FA, Tran L, Vuong TT, Bufano G, Salvesen Ø, Gravdal M, Aldaz D, Sun J, Kim S, Celauro L, Legname G, Telling GC, Tranulis MA, Benestad SL, Espenes A, Moda F, and Ersdal C

Subjects

Animals, Sheep, Norway, Brain metabolism, Phenotype, Sheep Diseases transmission, Wasting Disease, Chronic transmission, Reindeer, Prions metabolism

Abstract

Chronic wasting disease (CWD), a prion disease affecting cervids, has been known in North America (NA) since the 1960s and emerged in Norway in 2016. Surveillance and studies have revealed that there are different forms of CWD in Fennoscandia: contagious CWD in Norwegian reindeer and sporadic CWD in moose and red deer. Experimental studies have demonstrated that NA CWD prions can infect various species, but thus far, there have been no reports of natural transmission to non-cervid species. In vitro and laboratory animal studies of the Norwegian CWD strains suggest that these strains are different from the NA strains. In this work, we describe the intracerebral transmission of reindeer CWD to six scrapie-susceptible sheep. Detection methods included immunohistochemistry (IHC), western blot (WB), enzyme-linked immunosorbent assay (ELISA), real-time quaking-induced conversion (RT-QuIC) and protein misfolding cyclic amplification (PMCA). In the brain, grey matter vacuolation was limited, while all sheep exhibited vacuolation of the white matter. IHC and WB conventional detection techniques failed to detect prions; however, positive seeding activity with the RT-QuIC and PMCA amplification techniques was observed in the central nervous system of all but one sheep. Prions were robustly amplified in the lymph nodes of all animals, mainly by RT-QuIC. Additionally, two lymph nodes were positive by WB, and one was positive by ELISA. These findings suggest that sheep can propagate reindeer CWD prions after intracerebral inoculation, resulting in an unusual disease phenotype and prion distribution with a low amount of detectable prions., (© 2024. The Author(s).)

Published

2024

15. Inter- and intra-species conversion efficacies of Norwegian prion isolates estimated by serial protein misfolding cyclic amplification.

Author

Harpaz E, Vuong TT, Tran L, Tranulis MA, Benestad SL, and Ersdal C

Subjects

Animals, Sheep, Prion Proteins genetics, Prion Proteins metabolism, Norway epidemiology, Goats metabolism, Prions genetics, Reindeer metabolism, Scrapie, Deer, Prion Diseases veterinary, Wasting Disease, Chronic genetics, Goat Diseases, Sheep Diseases

Abstract

Prion diseases, including chronic wasting disease (CWD) in cervids, are fatal neurodegenerative disorders caused by the misfolding of cellular prion proteins. CWD is known to spread among captive and free-ranging deer in North America. In 2016, an outbreak of contagious CWD was detected among wild reindeer in Norway, marking the first occurrence of the disease in Europe. Additionally, new sporadic forms of CWD have been discovered in red deer in Norway and moose in Fennoscandia. We used serial protein misfolding cyclic amplification to study the ability of Norwegian prion isolates from reindeer, red deer, and moose (two isolates), as well as experimental classical scrapie from sheep, to convert a panel of 16 brain homogenates (substrates) from six different species with various prion protein genotypes. The reindeer CWD isolate successfully converted substrates from all species except goats. The red deer isolate failed to convert sheep and goat substrates but exhibited amplification in all cervid substrates. The two moose isolates demonstrated lower conversion efficacies. The wild type isolate propagated in all moose substrates and in the wild type red deer substrate, while the other isolate only converted two of the moose substrates. The experimental classical scrapie isolate was successfully propagated in substrates from all species tested. Thus, reindeer CWD and classical sheep scrapie isolates were similarly propagated in substrates from different species, suggesting the potential for spillover of these contagious diseases. Furthermore, the roe deer substrate supported conversion of three isolates suggesting that this species may be vulnerable to prion disease., (© 2023. L’Institut National de Recherche en Agriculture, Alimentation et Environnement (INRAE).)

Published

2023

16. Selenium Speciation Analysis Reveals Improved Antioxidant Status in Finisher Pigs Fed L-Selenomethionine, Alone or Combined with Sodium Selenite, and Vitamin E.

Author

Reinoso-Maset E, Falk M, Bernhoft A, Ersdal C, Framstad T, Fuhrmann H, Salbu B, and Oropeza-Moe M

Subjects

Animals, Dietary Supplements, Lipopolysaccharides, Selenomethionine pharmacology, Sodium Selenite pharmacology, Swine, Vitamin E, Antioxidants metabolism, Selenium

Abstract

Conditions associated with selenium (Se) and/or vitamin E (VitE) deficiency are still being reported in high-yielding pigs fed the recommended amounts. Here, the dietary effects of Se source (sodium selenite, NaSe, 0.40 or 0.65 mg Se/kg; L-selenomethionine, SeMet, 0.19 or 0.44 mg Se/kg; a NaSe-SeMet mixture, SeMix, 0.44-0.46 mg Se/kg) and VitE concentration (27, 50-53 or 101 mg/kg) on the antioxidant status of finisher pigs were compared with those in pigs fed non-Se-supplemented diets (0.08-0.09 mg Se/kg). Compared to NaSe-enriched diets, SeMet-supplemented diets resulted in significantly (p < 0.0018) higher plasma concentrations of total Se (14-27%) and selenospecies (GPx3, SelP, SeAlb; 7-83%), significantly increased the total Se accumulation in skeletal muscles, myocardium, liver and brain (10-650%), and enhanced the VitE levels in plasma (15-74%) and tissues (8-33%) by the end of the 80-day trial, proving better Se distribution and retention in pigs fed organic Se. Injecting lipopolysaccharide (LPS) intravenously half-way into the trial provoked a pyrogenic response in the pigs followed by a rapid increase of inorganic Se after 5-12 h, a drastic drop of SeMet levels between 12 and 24 h that recovered by 48 h, and a small increase of SeCys by 24-48 h, together with a gradual rise of GPx3, SelP and SeAlb in plasma up to 48 h. These changes in Se speciation in plasma were particularly significant (0.0024 > p > 0.00007) in pigs receiving SeMet- (0.44 mg Se/kg, above EU-legislated limits) or SeMix-supplemented (SeMet and NaSe both at 0.2 mg Se/kg, within EU-legislated limits) diets, which demonstrates Se metabolism upregulation to counteract the LPS-induced oxidative stress and a strengthened antioxidant capacity in these pigs. Overall, a Se source combination (without exceeding EU-legislated limits) and sufficient VitE supplementation (≥ 50 mg/kg) improved the pigs' antioxidant status, while doubling the allowed dietary organic Se increased the Se in tissues up to sixfold without compromising the animal's health due to toxicity. This study renders valuable results for revising the current dietary SeMet limits in swine rations., (© 2022. The Author(s).)

Published

2023

17. Fasciolosis-An Increasing Challenge in the Sheep Industry.

Author

Stuen S and Ersdal C

Abstract

The liver fluke Fasciola hepatica may cause severe infection in several mammalian species, including sheep and humans. Fasciolosis is a parasitic disease occurring worldwide in temperate climates and involves intermediate lymnaeid snails as vectors, in Europe the pond snail Galba truncatula in particular. In the sheep industry, the disease is a serious welfare and health problem. Fasciolosis is usually classified as acute, subacute or chronic according to the number and stage of flukes present in the liver, but with a considerable overlap. Acute disease, associated with a large number of migrating larvae, often results in sudden death due to acute and massive hemorrhage, while chronic fasciolosis is characterized by anemia, hypoalbuminaemia and weight loss. The management of fasciolosis is an increasing challenge in the sheep industry. Early diagnostic tests are limited. Protective immunity against liver flukes in sheep is low or lacking, and vaccines are not yet available. Treatment and control possibilities are challenging, and resistance to flukicide drugs is increasing. In addition, climate change with warmer and more humid weather will have a substantial effect on the establishment of both flukes and snails and will most likely increase the future distribution of F. hepatica .

Published

2022

18. No evidence of uptake or propagation of reindeer CWD prions in environmentally exposed sheep.

Author

Harpaz E, Salvesen Ø, Rauset GR, Mahmood A, Tran L, Ytrehus B, Benestad SL, Tranulis MA, Espenes A, and Ersdal C

Subjects

Animals, Norway, Sheep, Deer, Prions, Reindeer, Sheep Diseases, Wasting Disease, Chronic diagnosis, Wasting Disease, Chronic epidemiology

Abstract

Background: Chronic wasting disease (CWD) is a prion disease of cervids first reported in North America in the 1960s. In Europe, CWD was first diagnosed in 2016 in a wild reindeer in Norway. Detection of two more cases in the same mountain area led to the complete culling of this partially confined reindeer population of about 2400 animals. A total of 19 CWD positive animals were identified. The affected area is extensively used for the grazing of sheep during summers. There are many mineral licks intended for sheep in the area, but these have also been used by reindeer. This overlap in area use raised concerns for cross-species prion transmission between reindeer and sheep. In this study, we have used global positioning system (GPS) data from sheep and reindeer, including tracking one of the CWD positive reindeer, to investigate spatial and time-relevant overlaps between these two species. Since prions can accumulate in lymphoid follicles following oral uptake, samples of gut-associated lymphoid tissue (GALT) from 425 lambs and 78 adult sheep, which had grazed in the region during the relevant timeframe, were analyzed for the presence of prions. The recto-anal mucosa associated lymphoid tissue (RAMALT) from all the animals were examined by histology, immunohistochemistry (IHC) and enzyme-linked immunosorbent assay (ELISA), and the ileal Peyer's patch (IPP) from a subsample of 37 lambs were examined by histology and IHC, for the detection of prions., Results: GPS data showed an overlap in area use between the infected reindeer herd and the sheep. In addition, the GPS positions of an infected reindeer and some of the sampled sheep showed temporospatial overlap. No prions were detected in the GALT of the investigated sheep even though the mean lymphoid follicle number in RAMALT and IPP samples were high., Conclusion: The absence of prions in the GALT of sheep that have shared pasture with CWD-infected reindeer, may suggest that transmission of this novel CWD strain to sheep does not easily occur under the conditions found in these mountains. We document that the lymphoid follicle rich RAMALT could be a useful tool to screen for prions in sheep., (© 2022. The Author(s).)

Published

2022

19. DNA glycosylase Neil2 contributes to genomic responses in the spleen during clinical prion disease.

Author

Scheffler K, Jalland CMO, Benestad SL, Moldal T, Ersdal C, Gunnes G, Suganthan R, Bjørås M, and Tranulis MA

Subjects

Animals, DNA Repair, Genomics, Mice, Spleen metabolism, DNA Glycosylases genetics, DNA Glycosylases metabolism, Prion Diseases

Abstract

The DNA glycosylase Neil2 is a member of the base excision repair (BER) family of enzymes, which are important for repair of oxidative DNA damage. Specifically, Neil2 participates in repair of oxidized bases in single-stranded DNA of transcriptionally active genes. Mice with genetic ablation of Neil2 (Neil2 -/- ) display no overt phenotypes, but an age-dependent accumulation of oxidative DNA damage and increased inflammatory responsiveness. In young mice intra-cerebrally inoculated with prions, vigorous prion propagation starts rapidly in the germinal follicles of the spleen due to inoculum spillover. Here, we compare experimental prion disease in Neil2 -/- mice with that in wild-type mice at disease onset and end-stage. Specifically, we investigated disease progression, accumulation of DNA damage, and mitochondrial respiratory complex activity in brain and spleen. We used genome-wide RNA sequencing of the spleen to compare the immune responses to prion propagation between the two groups of mice, at both onset and end-stage prion disease. The Neil2 -/- mice deteriorated more rapidly than wild-type mice after onset of clinical signs. Levels of DNA damage in brain increased in both mouse groups, slightly more in the Neil2 -/- mice. Transcriptome data from spleen at disease onset were similar between the mouse groups with moderate genomic responses. However, at end-stage a substantial response was evident in the wild-type mice but not in Neil2 -/- mice. Our data show that Neil2 counteracts toxic signaling in clinical prion disease, and this is separate from gross pathological manifestations and PrP Sc accumulation., Competing Interests: Declaration of competing interest The authors declare no competing financial interests., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

20. Demyelinating polyneuropathy in goats lacking prion protein.

Author

Skedsmo FS, Malachin G, Våge DI, Hammervold MM, Salvesen Ø, Ersdal C, Ranheim B, Stafsnes MH, Bartosova Z, Bruheim P, Jäderlund KH, Matiasek K, Espenes A, and Tranulis MA

Subjects

Animals, Demyelinating Diseases pathology, Macrophages immunology, Macrophages pathology, Mice, Myelin Sheath pathology, Polyneuropathies pathology, PrPC Proteins immunology, T-Lymphocytes immunology, T-Lymphocytes pathology, Demyelinating Diseases immunology, Goats immunology, Myelin Sheath immunology, Polyneuropathies immunology, PrPC Proteins deficiency

Abstract

Studies in mice with ablation of Prnp, the gene that encodes the cellular prion protein (PrP C ), have led to the hypothesis that PrP C is important for peripheral nerve myelin maintenance. Here, we have used a nontransgenic animal model to put this idea to the test; namely, goats that, due to a naturally occurring nonsense mutation, lack PrP C . Teased nerve fiber preparation revealed a demyelinating pathology in goats without PrP C . Affected nerves were invaded by macrophages and T cells and displayed vacuolated fibers, shrunken axons, and onion bulbs. Peripheral nerve lipid composition was similar in young goats with or without PrP C , but markedly different between corresponding groups of adult goats, reflecting the progressive nature of the neuropathy. This is the first report of a subclinical demyelinating polyneuropathy caused by loss of PrP C function in a nontransgenic mammal., (© 2019 Norwegian University of Life Sciences. The FASEB Journal published by John Wiley & Sons Ltd on behalf of The FASEB Journal.)

Published

2020

21. Goats naturally devoid of PrP C are resistant to scrapie.

Author

Salvesen Ø, Espenes A, Reiten MR, Vuong TT, Malachin G, Tran L, Andréoletti O, Olsaker I, Benestad SL, Tranulis MA, and Ersdal C

Subjects

Animals, Female, Goats, Disease Resistance genetics, Goat Diseases genetics, PrPC Proteins deficiency, Scrapie genetics

Abstract

Prion diseases are progressive and fatal, neurodegenerative disorders described in humans and animals. According to the "protein-only" hypothesis, the normal host-encoded prion protein (PrP C ) is converted into a pathological and infectious form (PrP Sc ) in these diseases. Transgenic knockout models have shown that PrP C is a prerequisite for the development of prion disease. In Norwegian dairy goats, a mutation (Ter) in the prion protein gene (PRNP) effectively blocks PrP C synthesis. We inoculated 12 goats (4 PRNP +/+ , 4 PRNP +/Ter , and 4 PRNP Ter/Ter ) intracerebrally with goat scrapie prions. The mean incubation time until clinical signs of prion disease was 601 days post-inoculation (dpi) in PRNP +/+ goats and 773 dpi in PRNP +/Ter goats. PrP Sc and vacuolation were similarly distributed in the central nervous system (CNS) of both groups and observed in all brain regions and segments of the spinal cord. Generally, accumulation of PrP Sc was limited in peripheral organs, but all PRNP +/+ goats and 1 of 4 PRNP +/Ter goats were positive in head lymph nodes. The four PRNP Ter/Ter goats remained healthy, without clinical signs of prion disease, and were euthanized 1260 dpi. As expected, no accumulation of PrP Sc was observed in the CNS or peripheral tissues of this group, as assessed by immunohistochemistry, enzyme immunoassay, and real-time quaking-induced conversion. Our study shows for the first time that animals devoid of PrP C due to a natural mutation do not propagate prions and are resistant to scrapie. Clinical onset of disease is delayed in heterozygous goats expressing about 50% of PrP C levels.

Published

2020

22. Controlled efficacy trial confirming toltrazuril resistance in a field isolate of ovine Eimeria spp.

Author

Odden A, Enemark HL, Ruiz A, Robertson LJ, Ersdal C, Nes SK, Tømmerberg V, and Stuen S

Subjects

Administration, Oral, Animals, Coccidiosis epidemiology, Diarrhea epidemiology, Diarrhea parasitology, Eimeria isolation & purification, Eimeria pathogenicity, Europe epidemiology, Feces parasitology, Norway epidemiology, Parasite Egg Count methods, Sheep, Sheep Diseases epidemiology, Sheep Diseases parasitology, Triazines administration & dosage, Triazines adverse effects, Weight Gain, Coccidiosis veterinary, Eimeria drug effects, Oocysts drug effects, Sheep Diseases drug therapy, Triazines pharmacology, Triazines therapeutic use

Abstract

Background: Coccidiosis due to Eimeria spp. infections in lambs causes increased mortality and substantial production losses, and anticoccidials are important for control of the infection. Anticoccidial resistance has been reported in poultry and swine, and we recently described reduced toltrazuril efficacy in ovine Eimeria spp. in some Norwegian sheep farms using a newly developed faecal oocyst count reduction test (FOCRT). The aim of the present study was to use a controlled efficacy trial to assess the efficacy of toltrazuril against a field isolate suspected of being resistant., Methods: Twenty lambs, 17-22 days old and raised protected against exposure to coccidia, were infected with a field isolate of 100,000 Eimeria spp. oocysts. This isolate was obtained from a farm with a previously calculated drug efficacy of 56% (95% confidence interval: -433.9 to 96.6%). At day 7 post-infection, 10 of the lambs were orally treated with 20 mg/kg toltrazuril (Baycox Sheep vet., Bayer Animal Health), while the other 10 lambs (controls) were given physiological saline. Clinical examinations were conducted, and weight gains recorded. Daily faecal samples were scored for diarrhoea on a scale from 1 to 5, and oocyst excretion was determined using a modified McMaster technique. Oocysts were morphologically identified to species level. At 17-24 days post-infection, the lambs were euthanized and necropsied., Results: The tested Eimeria isolate was resistant against toltrazuril, and resistance was seen in both pathogenic and non-pathogenic species. In addition, no significant differences in faecal score, growth, gross pathology or histological changes were identified between the two groups. The pathogenic E. ovinoidalis was the dominant species, and no significant difference in the individual prevalence of E. ovinoidalis post-treatment was found between treated (66.9%) and control lambs (61.9%). Other species identified included E. crandallis/weybridgensis, E. parva, E. marsica, E. faurei, E. pallida, E. ahsata and E. bakuensis., Conclusions: This study confirms toltrazuril resistance in ovine Eimeria spp.; in addition, the data support the use of FOCRT as an appropriate tool for field evaluation of anticoccidial efficacy. Due to limited anticoccidial treatment alternatives, these findings may have important implications for the sheep industry, particularly in northern Europe.

Published

2018

23. Goats without Prion Protein Display Enhanced Proinflammatory Pulmonary Signaling and Extracellular Matrix Remodeling upon Systemic Lipopolysaccharide Challenge.

Author

Salvesen Ø, Reiten MR, Kamstra JH, Bakkebø MK, Espenes A, Tranulis MA, and Ersdal C

Abstract

A naturally occurring mutation in the PRNP gene of Norwegian dairy goats terminates synthesis of the cellular prion protein (PrP C ), rendering homozygous goats ( PRNP Ter/Ter ) devoid of the protein. Although PrP C has been extensively studied, particularly in the central nervous system, the biological role of PrP C remains incompletely understood. Here, we examined whether loss of PrP C affects the initial stage of lipopolysaccharide (LPS)-induced acute lung injury (ALI). Acute pulmonary inflammation was induced by intravenous injection of LPS ( Escherichia coli O26:B6) in 16 goats (8 PRNP Ter/Ter and 8 PRNP +/+ ). A control group of 10 goats (5 PRNP Ter/Ter and 5 PRNP +/+ ) received sterile saline. Systemic LPS challenge induced sepsis-like clinical signs including tachypnea and respiratory distress. Microscopic examination of lungs revealed multifocal areas with alveolar hemorrhages, edema, neutrophil infiltration, and higher numbers of alveolar macrophages, with no significant differences between PRNP genotypes. A total of 432 ( PRNP +/+ ) and 596 ( PRNP Ter/Ter ) genes were differentially expressed compared with the saline control of the matching genotype. When assigned to gene ontology categories, biological processes involved in remodeling of the extracellular matrix (ECM), were exclusively enriched in PrP C -deficient goats. These genes included a range of collagen-encoding genes, and proteases such as matrix metalloproteinases ( MMP1, MMP2, MMP14, ADAM15 ) and cathepsins. Several proinflammatory upstream regulators (TNF-α, interleukin-1β, IFN-γ) showed increased activation scores in goats devoid of PrP C . In conclusion, LPS challenge induced marked alterations in the lung tissue transcriptome that corresponded with histopathological and clinical findings in both genotypes. The increased activation of upstream inflammatory regulators and enrichment of ECM components could reflect increased inflammation in the absence of PrP C . Further studies are required to elucidate whether these alterations may affect the later reparative phase of ALI.

Published

2017

24. Loss of prion protein induces a primed state of type I interferon-responsive genes.

Author

Malachin G, Reiten MR, Salvesen Ø, Aanes H, Kamstra JH, Skovgaard K, Heegaard PMH, Ersdal C, Espenes A, Tranulis MA, and Bakkebø MK

Subjects

Animals, Cell Line, Female, Gene Expression, Gene Expression Profiling, Gene Knockout Techniques, Homeodomain Proteins genetics, Humans, Leukocytes immunology, Male, Mice, PrPC Proteins genetics, PrPC Proteins immunology, Goats genetics, Goats immunology, Interferon Type I genetics, PrPC Proteins deficiency

Abstract

The cellular prion protein (PrPC) has been extensively studied because of its pivotal role in prion diseases; however, its functions remain incompletely understood. A unique line of goats has been identified that carries a nonsense mutation that abolishes synthesis of PrPC. In these animals, the PrP-encoding mRNA is rapidly degraded. Goats without PrPC are valuable in re-addressing loss-of-function phenotypes observed in Prnp knockout mice. As PrPC has been ascribed various roles in immune cells, we analyzed transcriptomic responses to loss of PrPC in peripheral blood mononuclear cells (PBMCs) from normal goat kids (n = 8, PRNP+/+) and goat kids without PrPC (n = 8, PRNPTer/Ter) by mRNA sequencing. PBMCs normally express moderate levels of PrPC. The vast majority of genes were similarly expressed in the two groups. However, a curated list of 86 differentially expressed genes delineated the two genotypes. About 70% of these were classified as interferon-responsive genes. In goats without PrPC, the majority of type I interferon-responsive genes were in a primed, modestly upregulated state, with fold changes ranging from 1.4 to 3.7. Among these were ISG15, DDX58 (RIG-1), MX1, MX2, OAS1, OAS2 and DRAM1, all of which have important roles in pathogen defense, cell proliferation, apoptosis, immunomodulation and DNA damage response. Our data suggest that PrPC contributes to the fine-tuning of resting state PBMCs expression level of type I interferon-responsive genes. The molecular mechanism by which this is achieved will be an important topic for further research into PrPC physiology.

Published

2017

25. Neil3 induced neurogenesis protects against prion disease during the clinical phase.

Author

Jalland CM, Scheffler K, Benestad SL, Moldal T, Ersdal C, Gunnes G, Suganthan R, Bjørås M, and Tranulis MA

Subjects

Animals, Biomarkers metabolism, DNA Damage, Dentate Gyrus metabolism, Disease Models, Animal, Doublecortin Protein, Gene Knockout Techniques, Lateral Ventricles metabolism, Male, Mice, N-Glycosyl Hydrolases metabolism, Oxidative Stress, Prion Diseases metabolism, N-Glycosyl Hydrolases genetics, Neurogenesis, Prion Diseases genetics, Prion Diseases pathology

Abstract

Base excision repair (BER) is the major pathway for repair of oxidative DNA damage. Mice with genetic knockout of the BER enzyme Neil3 display compromised neurogenesis in the sub-ventricular zone of the lateral ventricle and sub-granular layer of the dentate gyrus of the hippocampus. To elucidate the impact of oxidative DNA damage-induced neurogenesis on prion disease we applied the experimental prion disease model on Neil3-deficient mice. The incubation period for the disease was similar in both wild type and Neil3 -/- mice and the overall neuropathology appeared unaffected by Neil3 function. However, disease in the Neil3 -/- mice was of shorter clinical duration. We observed a mildly reduced astrogliosis in the hippocampus and striatum in the Neil3-deficient mice. Brain expression levels of neuronal progenitor markers, nestin (Nestin), sex determining region Box 2 (Sox2), Class III beta-tubulin (Tuj1) decreased towards end-stage prion disease whereas doublecortin (Dcx) levels were less affected. Neuronal nuclei (NeuN), a marker for mature neurons declined during prion disease and more pronounced in the Neil3 -/- group. Microglial activation was prominent and appeared unaffected by loss of Neil3. Our data suggest that neurogenesis induced by Neil3 repair of oxidative DNA damage protects against prion disease during the clinical phase.

Published

2016

26. Activation of innate immune genes in caprine blood leukocytes after systemic endotoxin challenge.

Author

Salvesen Ø, Reiten MR, Heegaard PM, Tranulis MA, Espenes A, Skovgaard K, and Ersdal C

Subjects

Animals, Female, Goats, Interferons metabolism, Endotoxins immunology, Immunity, Innate genetics, Leukocytes immunology

Abstract

Background: Sepsis is a serious health problem associated with a range of infectious diseases in animals and humans. Early events of this syndrome can be mimicked by experimental administration of lipopolysaccharides (LPS). Compared with mice, small ruminants and humans are highly sensitive to LPS, making goats valuable in inflammatory models. We performed a longitudinal study in eight Norwegian dairy goats that received LPS (0.1 μg/kg, Escherichia coli O26:B6) intravenously. A control group of five goats received corresponding volumes of sterile saline. Clinical examinations were performed continuously, and blood samples were collected throughout the trial., Results: Characteristic signs of acute sepsis, such as sickness behavior, fever, and leukopenia were observed within 1 h of LPS administration. A high-throughput longitudinal gene expression analysis of circulating leukocytes was performed, and genes associated with the acute phase response, type I interferon signaling, LPS cascade and apoptosis, in addition to cytokines and chemokines were targeted. Pro-inflammatory genes, such as IL1B, CCL3 and IL8, were significantly up-regulated. Interestingly, increased mRNA levels of seven interferon stimulated genes (ISGs) were observed peaking at 2 h, corroborating the increasing evidence that ISGs respond immediately to bacterial endotoxins. A slower response was manifested by four extrahepatic acute phase proteins (APP) (SAA3, HP, LF and LCN2) reaching maximum levels at 5 h., Conclusions: We report an immediate induction of ISGs in leukocytes in response to LPS supporting a link between the interferon system and defense against bacterial infections. The extrahepatic expression of APPs suggests that leukocytes contribute to synthesis of these proteins at the beginning of a systemic inflammation. Taken together, these findings provide insights into the dynamic regulation of innate immune genes, as well as raising new questions regarding the importance of ISGs and extrahepatic APPs in leukocytes after systemic endotoxin challenge.

Published

2016

27. Acute and Chronic Erysipelothrix rhusiopathiae Infection in Lambs.

Author

Ersdal C, Jørgensen HJ, and Lie KI

Subjects

Animals, Arthritis epidemiology, Arthritis pathology, Communicable Diseases epidemiology, Communicable Diseases pathology, Electrophoresis, Gel, Pulsed-Field veterinary, Erysipelothrix isolation & purification, Erysipelothrix Infections pathology, Glomerulonephritis epidemiology, Glomerulonephritis pathology, Real-Time Polymerase Chain Reaction veterinary, Sheep, Sheep Diseases pathology, Arthritis veterinary, Communicable Diseases veterinary, Disease Outbreaks veterinary, Erysipelothrix Infections epidemiology, Glomerulonephritis veterinary, Sheep Diseases epidemiology

Abstract

Polyarthritis caused by Erysipelothrix rhusiopathiae is a relatively common infection in lambs characterized by low mortality and high morbidity. E. rhusiopathiae is a ubiquitous Gram-positive bacterium that is both a commensal and a pathogen of vertebrates. The disease was studied during an outbreak in a Norwegian Spæl sheep flock. In the acute phase, 48 of 230 (20%) lambs developed clinical signs and 4 died (1.7%). One acute case was necropsied and E. rhusiopathiae was cultured from all major organs investigated and from joints. There was a fibrinous polyarthritis, increased presence of monocytes in vessels, and necrosis of Purkinje cells. Sixteen of the diseased animals (33%) developed a chronic polyarthritis. Eight of these lambs were necropsied; all had lesions in major limb joints, and 3 of 8 also had lesions in the atlanto-occipital joint. At this stage, E. rhusiopathiae was cultured only from the joints in 7 of 8 (87.5%) lambs, but by real-time polymerase chain reaction, we showed persistence of the bacterium in several organs. Pulsed-field gel electrophoresis typing of the bacterial isolates indicated that the same strain caused the acute and chronic disease. Five of 6 (83%) chronically affected animals had amyloidosis of the spleen, and 6 of 8 (75%) had amyloidosis of the liver. All chronically affected animals had a glomerulonephritis, and 6 of 8 (75%) had sparse degeneration in the brain. Ceruloplasmin and haptoglobin were significantly increased in the chronically diseased lambs. These results show that chronic ovine erysipelas is not restricted to joints but is a multisystemic disease., (© The Author(s) 2014.)

Published

2015

28. Accelerated clinical course of prion disease in mice compromised in repair of oxidative DNA damage.

Author

Jalland CM, Benestad SL, Ersdal C, Scheffler K, Suganthan R, Nakabeppu Y, Eide L, Bjørås M, and Tranulis MA

Subjects

Animals, DNA Damage genetics, DNA Glycosylases metabolism, DNA Repair genetics, Disease Models, Animal, Guanine analogs & derivatives, Guanine metabolism, Humans, Mice, Mice, Knockout, Oxidative Stress genetics, Prion Diseases metabolism, Prion Diseases pathology, Prions metabolism, Reactive Oxygen Species, Scrapie pathology, DNA Glycosylases genetics, Prion Diseases genetics, Prions genetics, Scrapie genetics

Abstract

The detailed mechanisms of prion-induced neurotoxicity are largely unknown. Here, we have studied the role of DNA damage caused by reactive oxygen species in a mouse scrapie model by characterizing prion disease in the ogg1(-/-)mutyh(-/-) double knockout, which is compromised in oxidative DNA base excision repair. Ogg1 initiates removal of the major oxidation product 8-oxoguanine (8-oxoG) in DNA, and Mutyh initiates removal of adenine that has been misincorporated opposite 8-oxoG. Our data show that the onset of clinical signs appeared unaffected by Mutyh and Ogg1 expression. However, the ogg1(-/-)mutyh(-/-) mice displayed a significantly shorter clinical phase of the disease. Thus, accumulation of oxidative DNA damage might be of particular importance in the terminal clinical phase of prion disease. The prion-induced pathology and lesion profile were similar between knockout mice and controls. The fragmentation pattern of protease-resistant PrP as revealed in Western blots was also identical between the groups. Our data show that the fundamentals of prion propagation and pathological manifestation are not influenced by the oxidative DNA damage repair mechanisms studied here, but that progressive accumulation of oxidative lesions may accelerate the final toxic phase of prion disease., (© 2013 Elsevier Inc. All rights reserved.)

Published

2014

29. Intestinal adenocarcinomas in three generations of sheep.

Author

Løken T, Bjørnstad ER, and Ersdal C

Subjects

Adenocarcinoma epidemiology, Adenocarcinoma etiology, Adenocarcinoma genetics, Animals, Fatal Outcome, Female, Genetic Predisposition to Disease, Intestinal Neoplasms epidemiology, Intestinal Neoplasms etiology, Intestinal Neoplasms genetics, Sheep, Sheep Diseases epidemiology, Sheep Diseases etiology, Adenocarcinoma veterinary, Intestinal Neoplasms veterinary, Sheep Diseases genetics

Published

2012

30. Large outbreak of blackleg in housed cattle.

Author

Groseth PK, Ersdal C, Bjelland AM, and Stokstad M

Subjects

Animal Husbandry methods, Animals, Cattle, Clostridium Infections epidemiology, Female, Male, Myositis epidemiology, Norway epidemiology, Cattle Diseases epidemiology, Clostridium Infections veterinary, Clostridium chauvoei, Disease Outbreaks veterinary, Housing, Animal, Myositis veterinary

Published

2011

31. Abnormal prion protein is associated with changes of plasma membranes and endocytosis in bovine spongiform encephalopathy (BSE)-affected cattle brains.

Author

Ersdal C, Goodsir CM, Simmons MM, McGovern G, and Jeffrey M

Subjects

Animals, Astrocytes metabolism, Astrocytes pathology, Astrocytes ultrastructure, Brain ultrastructure, Cattle, Cell Membrane metabolism, Cell Membrane ultrastructure, Dendrites metabolism, Dendrites pathology, Dendrites ultrastructure, Encephalopathy, Bovine Spongiform metabolism, Endosomes metabolism, Endosomes pathology, Endosomes ultrastructure, Immunohistochemistry, Microscopy, Immunoelectron, Vacuoles metabolism, Vacuoles pathology, Vacuoles ultrastructure, Brain pathology, Cell Membrane pathology, Encephalopathy, Bovine Spongiform pathology, Endocytosis, Prions metabolism

Abstract

Aims: Transmissible spongiform encephalopathies (TSEs) or prion diseases are fatal neurodegenerative diseases of man and animals characterized by vacuolation and gliosis of neuropil and the accumulation of abnormal isoforms of a host protein known as prion protein (PrP). It is widely assumed that the abnormal isoforms of PrP (PrP(d), disease-specific form of PrP) are the proximate cause of neurodegeneration., Methods: To determine the nature of subcellular changes and their association with PrP(d) we perfusion-fixed brains of eight bovine spongiform encephalopathy (BSE)-affected cows and three control cattle for immunogold electron microscopy at two different neuroanatomical sites., Results: All affected cattle presented plasma membrane alterations of dendrites and astrocytes that were labelled for PrP(d). PrP(d) on membranes of dendrites and occasionally of neuronal perikarya was associated with abnormal endocytotic events, including bizarre coated pits and invagination of the plasma membrane. BSE-affected cattle also presented excess and abnormal multivesicular bodies, sometimes associated to the plasma membrane perturbations. In contrast, two TSE-specific lesions, vacuolation and rare tubulovesicular bodies, were not labelled for PrP(d) as were a number of other nonspecific lesions, such as autophagy and dystrophic neurites. At least two different morphological pathways to vacuoles were recognized., Conclusions: When compared with other TSEs, these changes are common to those of sheep and rodent scrapie and shows that there are consistent membrane toxicity properties of PrP(d). This toxicity involves an aberration of endocytosis. However, it is by no means clear that the lesions are of sufficient severity to result in clinical deficits.

Published

2009

32. Proteolytic processing of the ovine prion protein in cell cultures.

Author

Tveit H, Lund C, Olsen CM, Ersdal C, Prydz K, Harbitz I, and Tranulis MA

Subjects

Amino Acid Sequence, Animals, Cell Line, Cell Line, Tumor, Dogs, Enzyme Inhibitors pharmacology, Green Fluorescent Proteins genetics, Humans, Macrolides pharmacology, Mice, Molecular Sequence Data, Mutagenesis, Site-Directed, Prions genetics, Protein Transport, Recombinant Fusion Proteins metabolism, Sheep metabolism, Vacuolar Proton-Translocating ATPases antagonists & inhibitors, Prions metabolism

Abstract

The cellular compartment and purpose of the proteolytic processing of the prion protein (PrP) are still under debate. We have studied ovine PrP constructs expressed in four cell lines; murine neuroblastoma cells (N2a), human neuroblastoma cells (SH-SY5Y), dog kidney epithelial cells (MDCK), and human furin-deficient colon cancer cells (LoVo). Cleavage of PrP in LoVo cells indicates that the processing is furin independent. Neither is it reduced by some inhibitors of lysosomal proteinases, proteasomes or zinc-metalloproteinases, but incubation with bafilomycin A1, an inhibitor of vacuolar H+/ATPases, increases the amount of uncleaved PrP in the apical medium of MDCK cells. Mutations affecting the putative cleavage site near amino acid 113 reveal that the cleavage is independent of primary structure at this site. Absence of glycosylphosphatidylinositol anchor and glycan modifications does not influence the proteolytic processing of PrP. Our data indicate that PrP is cleaved during transit to the cell membrane.

Published

2005

33. Mapping PrPSc propagation in experimental and natural scrapie in sheep with different PrP genotypes.

Author

Ersdal C, Ulvund MJ, Espenes A, Benestad SL, Sarradin P, and Landsverk T

Subjects

Amino Acid Substitution genetics, Animals, Blotting, Western, Enzyme-Linked Immunosorbent Assay, Female, Genotype, Immunohistochemistry, Male, Protein Transport physiology, Sheep, Lymphatic System metabolism, Nervous System metabolism, PrPSc Proteins genetics, PrPSc Proteins metabolism, Scrapie metabolism

Abstract

Twenty-one orally inoculated and seven naturally infected sheep with scrapie were examined for PrP(Sc) in peripheral tissues and in the central nervous system (CNS), using immunohistochemistry. In the inoculated group, VRQ (valine at codon 136, arginine at codon 154 and glutamine at codon 171)/VRQ sheep generally had a greater accumulation of the pathologic form of prion protein (PrP(Sc)) in peripheral tissues, as compared with VRQ/ARQ (alanine at codon 136, arginine at codon 154, and glutamine at codon 171) animals at corresponding time points after inoculation. PrP(Sc) was not detected in the ileal Peyer's patch, the spleen, the superficial cervical lymph node, and peripheral nervous tissues of several inoculated VRQ/ARQ animals. All inoculated VRQ/VRQ sheep, but only one of eight inoculated VRQ/ARQ animals, were PrP(Sc)-positive in the CNS. Thus, the propagation of PrP(Sc) seemed slower and more limited in VRQ/ARQ animals. Tissue and cellular localization of PrP(Sc) suggested that PrP(Sc) was disseminated through three different routes. PrP(Sc)-positive cells in lymph node sinuses and in lymphatics indicated spreading by lymph. The sequential appearance of PrP(Sc) in the peripheral nervous system and the CNS, with satellite cells as early targets, suggested the periaxonal transportation of PrP(Sc) through supportive cells. Focal areas of vascular amyloid-like PrP(Sc) in the brain of five sheep, suggested the hematogenous dissemination of PrP(Sc). There was a poor correlation between the amount of PrP(Sc) in the CNS and clinical signs. One subclinically affected sheep showed widespread PrP(Sc) accumulation in the CNS, whereas three sheep had early clinical signs without detectable PrP(Sc) in the CNS. A VV(136) (homozygous for valine at codon 136) sheep inoculated with ARQ/ARR (alanine at codon 136, arginine at codon 154, and arginine at codon 171) tissue succumbed to disease, demonstrating successful heterologous transmission. Less susceptible sheep receiving VRQ/VRQ or ARQ/ARR material were PrP(Sc)-negative by immunohistochemistry, enzyme-linked immunosorbent assay, and western blot.

Published

2005

34. Relationships between ultrastructural scrapie pathology and patterns of abnormal prion protein accumulation.

Author

Ersdal C, Simmons MM, González L, Goodsir CM, Martin S, and Jeffrey M

Subjects

Animals, Extracellular Space, Immunohistochemistry methods, Microscopy, Electron methods, Neuroglia metabolism, Neuroglia pathology, Neuroglia ultrastructure, Neurons pathology, Neurons ultrastructure, Phenotype, Prions ultrastructure, Sheep, Subcellular Fractions metabolism, Subcellular Fractions pathology, Subcellular Fractions ultrastructure, Vacuoles metabolism, Vacuoles pathology, Vacuoles ultrastructure, Medulla Oblongata pathology, Neurons metabolism, Prions metabolism, Scrapie metabolism, Scrapie pathology

Abstract

On immunohistochemical examination several morphological types of disease-specific prion protein (PrP(d)) accumulation are recognised in the brain of sheep suffering from scrapie. The present study examined the relationship between the type of PrP(d) deposits seen by light microscopy and ultrastructural changes in the olivary nuclei and the dorsal motor nucleus of the vagus (DMNV) in naturally infected sheep with clinical scrapie. The nature and magnitude of sub-cellular morphological changes found in the olivary nuclei differed from the patterns of degeneration previously described in the DMNV. In the olivary nuclei, lamellar bodies in the neuronal perikaryon were found to correlate with marked intraneuronal PrP(d) accumulation. Bizarre, coated, spiral invaginations of the plasmalemma were only found in A(136) homozygous sheep in this nucleus, where few coated pits were usually observed. Neuropil vacuolation in the olivary nuclei was mild and correlated with sparse extracellular PrP(d) deposition. In the DMNV, the magnitude of extracellular immunolabelling in the neuropil was prominent. These extracellular PrP(d )aggregates coincided with intense neuropil vacuolation, increased numbers of coated pits, and with the presence of pre-amyloid changes and infrequent short fibrils in the extracellular space. Scrapie-infected neurons in the two neuroanatomic sites examined, therefore, appear to process and respond to the presence of PrP(d) differently. We hypothesise that vacuolation, coated pits and spiral invaginations of the plasmalemma may be responses to extracellular PrP(d) molecules, and that lamellar bodies are changes associated with the high levels of intraneuronal PrP(d).

Published

2004

35. Sub-cellular pathology of scrapie: coated pits are increased in PrP codon 136 alanine homozygous scrapie-affected sheep.

Author

Ersdal C, Simmons MM, Goodsir C, Martin S, and Jeffrey M

Subjects

ATP-Binding Cassette Transporters genetics, ATP-Binding Cassette Transporters ultrastructure, Animals, Coated Pits, Cell-Membrane pathology, Coated Pits, Cell-Membrane ultrastructure, Homozygote, Immunohistochemistry, Microscopy, Electron methods, Myelin Sheath metabolism, Myelin Sheath pathology, Myelin Sheath ultrastructure, Neuroglia metabolism, Neuroglia pathology, Neuroglia ultrastructure, Neurons metabolism, Neurons pathology, Neurons ultrastructure, Neuropil metabolism, Neuropil pathology, Neuropil ultrastructure, Olivary Nucleus metabolism, Olivary Nucleus pathology, Olivary Nucleus ultrastructure, Peptide Fragments immunology, Peptide Fragments metabolism, Peptide Fragments ultrastructure, Scrapie genetics, Sheep, Subcellular Fractions metabolism, Subcellular Fractions pathology, Subcellular Fractions ultrastructure, Vacuoles metabolism, Vacuoles pathology, Vacuoles ultrastructure, ATP-Binding Cassette Transporters metabolism, Alanine genetics, Coated Pits, Cell-Membrane metabolism, Scrapie pathology, Sheep Diseases pathology

Abstract

Sub-cellular studies of transmissible spongiform encephalopathies (TSEs) have been carried out on several animal species and human beings. However, studies of optimal perfusion-fixed tissues have largely been confined to examination of rodents. Using a recently developed technique, heads of scrapie-affected sheep and controls were perfusion fixed with mixed aldehydes. The obexes were immunohistochemically labelled with PrP antibodies, and the dorsal motor nucleus of the vagal nerve was examined by electron microscopy. Irregular neuritic profiles with highly invaginated membranes, associated with coated pits were found in all scrapie-affected sheep, but not in controls. Interestingly, they were consistently more frequent in the homozygous A(136) sheep. This is the first report describing sub-cellular differences in pathology associated with different PrP genotypes. Rarely, amorphous material, or sparse fibrillar structures, were present in the extracellular space. The changes were often associated with irregular plasmalemma and frequent coated pits. Vacuolation typical of TSEs, dystrophic neurites and variable gliosis were present. Herniation of membranes and organelles from apparently healthy processes into adjacent vacuoles and dendrites was also observed. We suggest that the increase in coated pits and plasmalemma invagination is related to an attempted internalisation of aggregated disease-specific PrP, or protofilaments, from the extracellular space.

Published

2003

36. Accumulation of pathogenic prion protein (PrPSc) in nervous and lymphoid tissues of sheep with subclinical scrapie.

Author

Ersdal C, Ulvund MJ, Benestad SL, and Tranulis MA

Subjects

Animals, Cerebellum pathology, Female, Genetic Predisposition to Disease, Genotype, Immunohistochemistry veterinary, In Situ Hybridization veterinary, Lymphoid Tissue pathology, Mutation, PrPSc Proteins genetics, Scrapie genetics, Scrapie pathology, Sheep, Cerebellum metabolism, Lymphoid Tissue metabolism, PrPSc Proteins metabolism, Scrapie metabolism

Abstract

All sheep older than 1 year of age from a flock of the Rygja breed in which clinical scrapie was detected for the first time in two animals (4%) were examined for accumulation of pathogenic prion protein (PrPSc) by immunohistochemistry in the obex, the cerebellum, and the medial retrophayngeal lymph node. In addition, six lambs, 2-3 months old, all offspring of PrPSc-positive dams, were examined for PrPSc in the ileal Peyers' patch (IPP), the distal jejunal lymph node, the spleen, and the medial retropharyngeal lymph node (RPLN). In this flock, 35% (17/48) of the adult sheep showed accumulation of PrPSc, an eightfold increase compared with clinical disease. All positives carried susceptible PrP genotypes. Three sheep had deposits of PrPSc in the RPLN and not in the brain, suggesting that this organ, easily accessible at slaughter, is suitable for screening purposes. Two 7-year-old clinically healthy homozygous V136Q171 ewes showed sparse immunostaining in the central nervous system and may have been infected as adults. Further, two littermates, 86-days-old, showed PrPSc in the IPP. Interestingly, one of these lambs had the intermediate susceptible PrP genotype, VA136QR171. In addition to early immunolabeling in the dorsal motor nucleus of the vagal nerve, a few of the sheep had early involvement of the cerebellum. In fact, a 2-year-old sheep had sparse deposits of PrPSc in the cerebellum only. Because experimental bovine spongiform encephalopathy (BSE) in sheep seems to behave in a similar manner as natural scrapie, these results, particularly regarding spread of infectivity, may have implications for the handling of BSE should it be diagnosed in sheep.

Published

2003

37. An epidemiological study of cataracts in seawater farmed Atlantic salmon Salmo salar.

Author

Ersdal C, Midtlyng PJ, and Jarp J

Subjects

Animals, Body Weight, Cataract epidemiology, Cataract pathology, Cross-Sectional Studies, Fish Diseases pathology, Fisheries, Norway epidemiology, Otoscopes veterinary, Prevalence, Seasons, Seawater, Surveys and Questionnaires, Cataract veterinary, Fish Diseases epidemiology, Salmo salar

Abstract

Cataracts in farmed Atlantic salmon have been known for many years, but the aetiology and importance of the disease have not been clarified. A cross-sectional field study of 51 cages of Atlantic salmon at 49 randomly selected sea sites was performed during the summer of 1998. The target population was spring and autumn entry groups of the 1997 generation salmon. Approximately 15 fish from each cage, altogether 777 fish, were autopsied by the same person. Each eye of the fish was scored for cataracts on a scale from 0 to 4 using an otoscope lamp with magnification. The weight and length of each fish were measured. The prevalence of cataracts was 83 % and 79% in spring entry groups and autumn entry groups, respectively. The overall mean cataract index (mean score of both eyes) was 1.23, being significantly higher in the spring entry groups (1.36) than the autumn entry groups (0.85). The final results in the spring entry groups showed that the fish groups with higher weight at sea transfer also had a higher cataract index at inspection. The risk of development of cataracts varied significantly among the offspring from the 5 strains represented in the study. Fish from sites located in 2 counties in the southern part of Norway had a significantly higher cataract index than fish farmed in the northernmost county in the study. For the autumn entry groups none of the explanatory variables was significant. In the spring entry groups a significant negative relationship was observed between the cataract score and the weight of the fish at the time of inspection (Pearson's r = -0.17), while the corresponding correlation for the autumn released groups was r = -0.10. Among the spring entry groups the average weight of the fish with the highest cataract score was estimated to about a third of the weight of the fish with no visible cataracts.

Published

2001