Your search keyword '"Espenes A"' showing total 15 results

1. A 1 bp deletion in HACE1 causes ataxia in Norwegian elkhound, black

Author

Kim K. L. Bellamy, Fredrik S. Skedsmo, Josefin Hultman, Ellen F. Arnet, Ole Albert Guttersrud, Hege Kippenes Skogmo, Stein Istre Thoresen, Arild Espenes, Karin Hultin Jäderlund, and Frode Lingaas

Subjects

Medicine, Science

Abstract

A number of inherited ataxias is known in humans, with more than 250 loci implicated, most of which are included in human ataxia screening panels. Anecdotally, cases of ataxia in the Norwegian elkhound black have been known for the last 40 years. Affected puppies from three litters were clinically and neurologically examined, and postmortem samples were collected for morphological studies, including ultrastructural analyses. The puppies displayed vestibulocerebellar neurological signs and had degenerative histopathological alterations in cerebellum and brain stem. Three affected dogs, each from different litters, as well as both parents and one healthy littermate from each litter, were whole genome sequenced. Through variant calling we discovered a disease-associated 1 bp deletion in HACE1 (CFA12), resulting in a frameshift at codon 333 and a premature stop codon at codon 366. The perfect association combined with the predicted significant molecular effect, strongly suggest that we have found the causative mutation for Norwegian elkhound black ataxia. We have identified a novel candidate gene for ataxia where dogs can serve as a spontaneous model for improved understanding of ataxia, also in human.

Published

2022

2. A 1 bp deletion in HACE1 causes ataxia in Norwegian elkhound, black

Author

Bellamy, Kim K. L., primary, Skedsmo, Fredrik S., additional, Hultman, Josefin, additional, Arnet, Ellen F., additional, Guttersrud, Ole Albert, additional, Skogmo, Hege Kippenes, additional, Thoresen, Stein Istre, additional, Espenes, Arild, additional, Jäderlund, Karin Hultin, additional, and Lingaas, Frode, additional

Published

2022

3. A Gly98Val mutation in the N-Myc downstream regulated gene 1 (NDRG1) in Alaskan Malamutes with polyneuropathy.

Author

Camilla S Bruun, Karin H Jäderlund, Mette Berendt, Kristine B Jensen, Eva H Spodsberg, Hanne Gredal, G Diane Shelton, James R Mickelson, Katie M Minor, Hannes Lohi, Inge Bjerkås, Oyvind Stigen, Arild Espenes, Cecilia Rohdin, Rebecca Edlund, Jennie Ohlsson, Sigitas Cizinauskas, Páll S Leifsson, Cord Drögemüller, Lars Moe, Susanna Cirera, and Merete Fredholm

Subjects

Medicine, Science

Abstract

The first cases of early-onset progressive polyneuropathy appeared in the Alaskan Malamute population in Norway in the late 1970s. Affected dogs were of both sexes and were ambulatory paraparetic, progressing to non-ambulatory tetraparesis. On neurologic examination, affected dogs displayed predominantly laryngeal paresis, decreased postural reactions, decreased spinal reflexes and muscle atrophy. The disease was considered eradicated through breeding programmes but recently new cases have occurred in the Nordic countries and the USA. The N-myc downstream-regulated gene (NDRG1) is implicated in neuropathies with comparable symptoms or clinical signs both in humans and in Greyhound dogs. This gene was therefore considered a candidate gene for the polyneuropathy in Alaskan Malamutes. The coding sequence of the NDRG1 gene derived from one healthy and one affected Alaskan Malamute revealed a non-synonymous G>T mutation in exon 4 in the affected dog that causes a Gly98Val amino acid substitution. This substitution was categorized to be "probably damaging" to the protein function by PolyPhen2 (score: 1.000). Subsequently, 102 Alaskan Malamutes from the Nordic countries and the USA known to be either affected (n = 22), obligate carriers (n = 7) or healthy (n = 73) were genotyped for the SNP using TaqMan. All affected dogs had the T/T genotype, the obligate carriers had the G/T genotype and the healthy dogs had the G/G genotype except for 13 who had the G/T genotype. A protein alignment showed that residue 98 is conserved in mammals and also that the entire NDRG1 protein is highly conserved (94.7%) in mammals. We conclude that the G>T substitution is most likely the mutation that causes polyneuropathy in Alaskan Malamutes. Our characterization of a novel candidate causative mutation for polyneuropathy offers a new canine model that can provide further insight into pathobiology and therapy of human polyneuropathy. Furthermore, selection against this mutation can now be used to eliminate the disease in Alaskan Malamutes.

Published

2013

4. Exosome-producing follicle associated epithelium is not involved in uptake of PrPd from the gut of sheep (Ovis aries): an ultrastructural study.

Author

Caroline Piercey Åkesson, Gillian McGovern, Mark P Dagleish, Arild Espenes, Charles McL Press, Thor Landsverk, and Martin Jeffrey

Subjects

Medicine, Science

Abstract

In natural or experimental oral scrapie infection of sheep, disease associated prion protein (PrP(d)) often first accumulates in Peyer's patch (PP) follicles. The route by which infectivity reaches the follicles is unknown, however, intestinal epithelial cells may participate in intestinal antigenic presentation by delivering exosomes as vehicles of luminal antigens. In a previous study using an intestinal loop model, following inoculation of scrapie brain homogenate, inoculum associated PrP(d) was detected by light microscopy shortly (15 minutes to 3.5 hours) after inoculation in the villous lacteals and sub-mucosal lymphatics. No PrP(d) was located within the follicle-associated epithelium (FAE), sub-FAE domes or the PP follicles. To evaluate this gut loop model and the transportation routes in more detail, we used electron microscopy (EM) to study intestinal tissues exposed to scrapie or control homogenates for 15 minutes to 10 days. In addition, immuno-EM was used to investigate whether exosomes produced in the FAE may possess small amounts of PrP(d) that were not detectable by light microscopy. This study showed that the integrity of the intestinal epithelium was sustained in the intestinal loop model. Despite prominent transcytotic activity and exosome release from the FAE of the ileal PP in sheep, these structures were not associated with transportation of PrP(d) across the mucosa. The study did not determine how infectivity reaches the follicles of PPs. The possibility that the infectious agent is transported across the FAE remains a possibility if it occurs in a form that is undetectable by the methods used in this study. Infectivity may also be transported via lymph to the blood and further to all other lymphoid tissues including the PP follicles, but the early presence of PrP(d) in the PP follicles during scrapie infection argues against such a mechanism.

Published

2011

5. PrP expression, PrPSc accumulation and innervation of splenic compartments in sheep experimentally infected with scrapie.

Author

Randi Sørby, Lars Austbø, Charles McL Press, Grethe Skretting, Thor Landsverk, and Arild Espenes

Subjects

Medicine, Science

Abstract

BACKGROUND: In prion disease, the peripheral expression of PrP(C) is necessary for the transfer of infectivity to the central nervous system. The spleen is involved in neuroinvasion and neural dissemination in prion diseases but the nature of this involvement is not known. The present study undertook the investigation of the spatial relationship between sites of PrP(Sc) accumulation, localisation of nerve fibres and PrP(C) expression in the tissue compartments of the spleen of scrapie-inoculated and control sheep. METHODOLOGY/PRINCIPAL FINDINGS: Laser microdissection and quantitative PCR were used to determine PrP mRNA levels and results were compared with immunohistochemical protocols to distinguish PrP(C) and PrP(Sc) in tissue compartments of the spleen. In sheep experimentally infected with scrapie, the major sites of accumulation of PrP(Sc) in the spleen, namely the lymphoid nodules and the marginal zone, expressed low levels of PrP mRNA. Double immunohistochemical labelling for PrP(Sc) and the pan-nerve fibre marker, PGP, was used to evaluate the density of innervation of splenic tissue compartments and the intimacy of association between PrP(Sc) and nerves. Some nerve fibres were observed to accompany blood vessels into the PrP(Sc)-laden germinal centres. However, the close association between nerves and PrP(Sc) was most apparent in the marginal zone. Other sites of close association were adjacent to the wall of the central artery of PALS and the outer rim of germinal centres. CONCLUSIONS/SIGNIFICANCE: The findings suggest that the degree of PrP(Sc) accumulation does not depend on the expression level of PrP(C). Though several splenic compartments may contribute to neuroinvasion, the marginal zone may play a central role in being the compartment with most apparent association between nerves and PrP(Sc).

Published

2009

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

Author

Malachin, Giulia, primary, Reiten, Malin R., additional, Salvesen, Øyvind, additional, Aanes, Håvard, additional, Kamstra, Jorke H., additional, Skovgaard, Kerstin, additional, Heegaard, Peter M. H., additional, Ersdal, Cecilie, additional, Espenes, Arild, additional, Tranulis, Michael A., additional, and Bakkebø, Maren K., additional

Published

2017

7. A Gly98Val Mutation in the N-Myc Downstream Regulated Gene 1 (NDRG1) in Alaskan Malamutes with Polyneuropathy

Author

Bruun, Camilla S., primary, Jäderlund, Karin H., additional, Berendt, Mette, additional, Jensen, Kristine B., additional, Spodsberg, Eva H., additional, Gredal, Hanne, additional, Shelton, G. Diane, additional, Mickelson, James R., additional, Minor, Katie M., additional, Lohi, Hannes, additional, Bjerkås, Inge, additional, Stigen, Øyvind, additional, Espenes, Arild, additional, Rohdin, Cecilia, additional, Edlund, Rebecca, additional, Ohlsson, Jennie, additional, Cizinauskas, Sigitas, additional, Leifsson, Páll S., additional, Drögemüller, Cord, additional, Moe, Lars, additional, Cirera, Susanna, additional, and Fredholm, Merete, additional

Published

2013

8. A Gly98Val Mutation in the N-Myc Downstream Regulated Gene 1 (NDRG1) in Alaskan Malamutes with Polyneuropathy

Author

G. Diane Shelton, Katie M. Minor, Lars Moe, Camilla S. Bruun, James R. Mickelson, Pall S. Leifsson, Inge Bjerkås, Jennie Ohlsson, Cecilia Rohdin, Rebecca Edlund, Kristine B. Jensen, Sigitas Cizinauskas, Hanne Gredal, Merete Fredholm, Cord Drögemüller, Hannes Lohi, Karin Hultin Jäderlund, Øyvind Stigen, Mette Berendt, Eva H. Spodsberg, Arild Espenes, Susanna Cirera, Departments of Faculty of Veterinary Medicine, Research Programs Unit, Research Programme of Molecular Medicine, Veterinary Biosciences, and Veterinary Genetics

Subjects

Male, Candidate gene, HEREDITARY MOTOR, Alaskan malamute, Cell Cycle Proteins, medicine.disease_cause, Exon, 0302 clinical medicine, Neurobiology of Disease and Regeneration, Genotype, Dog Diseases, BRAIN, Small Animals, MARIE-TOOTH DISEASE, Animal Management, media_common, Genetics, 0303 health sciences, Mutation, education.field_of_study, Multidisciplinary, 630 Agriculture, GYPSIES, Intracellular Signaling Peptides and Proteins, 3. Good health, 590 Animals (Zoology), Medicine, Female, Polyneuropathy, Veterinary Pathology, Research Article, Veterinary Medicine, Animal Types, Science, education, Population, SENSORY NEUROPATHY-LOM, Biology, Veterinary Neurology, Polyneuropathies, 03 medical and health sciences, Dogs, Genetic Mutation, medicine, Animals, media_common.cataloged_instance, 030304 developmental biology, Point mutation, Human Genetics, medicine.disease, DEMYELINATING NEUROPATHY, Genetics of Disease, Immunology, 1182 Biochemistry, cell and molecular biology, Veterinary Science, 3111 Biomedicine, Gene Function, Animal Genetics, 030217 neurology & neurosurgery, Neuroscience

Abstract

The first cases of early-onset progressive polyneuropathy appeared in the Alaskan Malamute population in Norway in the late 1970s. Affected dogs were of both sexes and were ambulatory paraparetic, progressing to non-ambulatory tetraparesis. On neurologic examination, affected dogs displayed predominantly laryngeal paresis, decreased postural reactions, decreased spinal reflexes and muscle atrophy. The disease was considered eradicated through breeding programmes but recently new cases have occurred in the Nordic countries and the USA. The N-myc downstream-regulated gene (NDRG1) is implicated in neuropathies with comparable symptoms or clinical signs both in humans and in Greyhound dogs. This gene was therefore considered a candidate gene for the polyneuropathy in Alaskan Malamutes. The coding sequence of the NDRG1 gene derived from one healthy and one affected Alaskan Malamute revealed a non-synonymous G>T mutation in exon 4 in the affected dog that causes a Gly98Val amino acid substitution. This substitution was categorized to be "probably damaging" to the protein function by PolyPhen2 (score: 1.000). Subsequently, 102 Alaskan Malamutes from the Nordic countries and the USA known to be either affected (n = 22), obligate carriers (n = 7) or healthy (n = 73) were genotyped for the SNP using TaqMan. All affected dogs had the T/T genotype, the obligate carriers had the G/T genotype and the healthy dogs had the G/G genotype except for 13 who had the G/T genotype. A protein alignment showed that residue 98 is conserved in mammals and also that the entire NDRG1 protein is highly conserved (94.7%) in mammals. We conclude that the G>T substitution is most likely the mutation that causes polyneuropathy in Alaskan Malamutes. Our characterization of a novel candidate causative mutation for polyneuropathy offers a new canine model that can provide further insight into pathobiology and therapy of human polyneuropathy. Furthermore, selection against this mutation can now be used to eliminate the disease in Alaskan Malamutes.

Published

2013

9. Exosome-Producing Follicle Associated Epithelium Is Not Involved in Uptake of PrPd from the Gut of Sheep (Ovis aries): An Ultrastructural Study

Author

Åkesson, Caroline Piercey, primary, McGovern, Gillian, additional, Dagleish, Mark P., additional, Espenes, Arild, additional, McL Press, Charles, additional, Landsverk, Thor, additional, and Jeffrey, Martin, additional

Published

2011

10. Exosome-Producing Follicle Associated Epithelium Is Not Involved in Uptake of PrPd from the Gut of Sheep (Ovis aries): An Ultrastructural Study

Author

Martin Jeffrey, Caroline Piercey Åkesson, Mark P. Dagleish, Charles McL. Press, Arild Espenes, Thor Landsverk, and Gillian McGovern

Subjects

Veterinary Medicine, Pathology, medicine.medical_specialty, Prions, lcsh:Medicine, Scrapie, Biology, Exosomes, Exosome, Veterinary Immunology, Epithelium, Absorption, Peyer's Patches, Molecular Cell Biology, Glial Fibrillary Acidic Protein, medicine, Animals, lcsh:Science, Veterinary Prion Diseases, Infectivity, Sheep, Multidisciplinary, Microvilli, lcsh:R, Epithelial Cells, Intestinal epithelium, Molecular biology, Gastrointestinal Tract, medicine.anatomical_structure, Lymphatic system, Veterinary Diseases, Ultrastructure, Veterinary Science, lcsh:Q, Lymph, Cellular Types, Veterinary Pathology, Research Article

Abstract

In natural or experimental oral scrapie infection of sheep, disease associated prion protein (PrP(d)) often first accumulates in Peyer's patch (PP) follicles. The route by which infectivity reaches the follicles is unknown, however, intestinal epithelial cells may participate in intestinal antigenic presentation by delivering exosomes as vehicles of luminal antigens. In a previous study using an intestinal loop model, following inoculation of scrapie brain homogenate, inoculum associated PrP(d) was detected by light microscopy shortly (15 minutes to 3.5 hours) after inoculation in the villous lacteals and sub-mucosal lymphatics. No PrP(d) was located within the follicle-associated epithelium (FAE), sub-FAE domes or the PP follicles. To evaluate this gut loop model and the transportation routes in more detail, we used electron microscopy (EM) to study intestinal tissues exposed to scrapie or control homogenates for 15 minutes to 10 days. In addition, immuno-EM was used to investigate whether exosomes produced in the FAE may possess small amounts of PrP(d) that were not detectable by light microscopy. This study showed that the integrity of the intestinal epithelium was sustained in the intestinal loop model. Despite prominent transcytotic activity and exosome release from the FAE of the ileal PP in sheep, these structures were not associated with transportation of PrP(d) across the mucosa. The study did not determine how infectivity reaches the follicles of PPs. The possibility that the infectious agent is transported across the FAE remains a possibility if it occurs in a form that is undetectable by the methods used in this study. Infectivity may also be transported via lymph to the blood and further to all other lymphoid tissues including the PP follicles, but the early presence of PrP(d) in the PP follicles during scrapie infection argues against such a mechanism.

Published

2011

11. PrP Expression, PrPSc Accumulation and Innervation of Splenic Compartments in Sheep Experimentally Infected with Scrapie

Author

Sørby, Randi, primary, Austbø, Lars, additional, Press, Charles McL., additional, Skretting, Grethe, additional, Landsverk, Thor, additional, and Espenes, Arild, additional

Published

2009

12. PrP Expression, PrPSc Accumulation and Innervation of Splenic Compartments in Sheep Experimentally Infected with Scrapie

Author

Charles McL. Press, Arild Espenes, Thor Landsverk, Randi Sørby, Lars Austbø, and Grethe Skretting

Subjects

Pathology/Histopathology, Pathology, medicine.medical_specialty, PrPSc Proteins, Lymphoid Tissue, animal diseases, lcsh:Medicine, Spleen, Scrapie, In situ hybridization, Biology, Models, Biological, Polymerase Chain Reaction, Prion Diseases, Infectious Diseases/Prion Diseases, medicine, Animals, PrPC Proteins, RNA, Messenger, lcsh:Science, In Situ Hybridization, Laser capture microdissection, Sheep, Multidisciplinary, lcsh:R, Brain, Germinal center, Genetics and Genomics/Gene Expression, Marginal zone, Immunohistochemistry, nervous system diseases, medicine.anatomical_structure, Lymphatic system, nervous system, Gene Expression Regulation, Splenic Tissue, lcsh:Q, Research Article

Abstract

BACKGROUND: In prion disease, the peripheral expression of PrP(C) is necessary for the transfer of infectivity to the central nervous system. The spleen is involved in neuroinvasion and neural dissemination in prion diseases but the nature of this involvement is not known. The present study undertook the investigation of the spatial relationship between sites of PrP(Sc) accumulation, localisation of nerve fibres and PrP(C) expression in the tissue compartments of the spleen of scrapie-inoculated and control sheep. METHODOLOGY/PRINCIPAL FINDINGS: Laser microdissection and quantitative PCR were used to determine PrP mRNA levels and results were compared with immunohistochemical protocols to distinguish PrP(C) and PrP(Sc) in tissue compartments of the spleen. In sheep experimentally infected with scrapie, the major sites of accumulation of PrP(Sc) in the spleen, namely the lymphoid nodules and the marginal zone, expressed low levels of PrP mRNA. Double immunohistochemical labelling for PrP(Sc) and the pan-nerve fibre marker, PGP, was used to evaluate the density of innervation of splenic tissue compartments and the intimacy of association between PrP(Sc) and nerves. Some nerve fibres were observed to accompany blood vessels into the PrP(Sc)-laden germinal centres. However, the close association between nerves and PrP(Sc) was most apparent in the marginal zone. Other sites of close association were adjacent to the wall of the central artery of PALS and the outer rim of germinal centres. CONCLUSIONS/SIGNIFICANCE: The findings suggest that the degree of PrP(Sc) accumulation does not depend on the expression level of PrP(C). Though several splenic compartments may contribute to neuroinvasion, the marginal zone may play a central role in being the compartment with most apparent association between nerves and PrP(Sc).

Published

2009

13. A Gly98Val Mutation in the N-Myc Downstream Regulated Gene 1 (NDRG1) in Alaskan Malamutes with Polyneuropathy.

Author

Bruun, Camilla S., Jäderlund, Karin H., Berendt, Mette, Jensen, Kristine B., Spodsberg, Eva H., Gredal, Hanne, Shelton, G. Diane, Mickelson, James R., Minor, Katie M., Lohi, Hannes, Bjerkås, Inge, Stigen, Øyvind, Espenes, Arild, Rohdin, Cecilia, Edlund, Rebecca, Ohlsson, Jennie, Cizinauskas, Sigitas, Leifsson, Páll S., Drögemüller, Cord, and Moe, Lars

Subjects

VETERINARY neurology, DISEASE progression, GENETIC mutation, ENTRAPMENT neuropathies, VETERINARY medicine, SPINAL reflexes, GENOTYPE-environment interaction

Abstract

The first cases of early-onset progressive polyneuropathy appeared in the Alaskan Malamute population in Norway in the late 1970s. Affected dogs were of both sexes and were ambulatory paraparetic, progressing to non-ambulatory tetraparesis. On neurologic examination, affected dogs displayed predominantly laryngeal paresis, decreased postural reactions, decreased spinal reflexes and muscle atrophy. The disease was considered eradicated through breeding programmes but recently new cases have occurred in the Nordic countries and the USA. The N-myc downstream-regulated gene (NDRG1) is implicated in neuropathies with comparable symptoms or clinical signs both in humans and in Greyhound dogs. This gene was therefore considered a candidate gene for the polyneuropathy in Alaskan Malamutes. The coding sequence of the NDRG1 gene derived from one healthy and one affected Alaskan Malamute revealed a non-synonymous G>T mutation in exon 4 in the affected dog that causes a Gly98Val amino acid substitution. This substitution was categorized to be “probably damaging” to the protein function by PolyPhen2 (score: 1.000). Subsequently, 102 Alaskan Malamutes from the Nordic countries and the USA known to be either affected (n = 22), obligate carriers (n = 7) or healthy (n = 73) were genotyped for the SNP using TaqMan. All affected dogs had the T/T genotype, the obligate carriers had the G/T genotype and the healthy dogs had the G/G genotype except for 13 who had the G/T genotype. A protein alignment showed that residue 98 is conserved in mammals and also that the entire NDRG1 protein is highly conserved (94.7%) in mammals. We conclude that the G>T substitution is most likely the mutation that causes polyneuropathy in Alaskan Malamutes. Our characterization of a novel candidate causative mutation for polyneuropathy offers a new canine model that can provide further insight into pathobiology and therapy of human polyneuropathy. Furthermore, selection against this mutation can now be used to eliminate the disease in Alaskan Malamutes. [ABSTRACT FROM AUTHOR]

Published

2013

14. PrP Expression, PrPSc Accumulation and Innervation of Splenic Compartments in Sheep Experimentally Infected with Scrapie.

Author

Sørby, Randi, Austbø, Lars, Press, Charles McL., Skretting, Grethe, Landsverk, Thor, and Espenes, Arild

Subjects

PRION diseases, CENTRAL nervous system, SPLEEN, METASTASIS, MESSENGER RNA, NERVES

Abstract

Background: In prion disease, the peripheral expression of PrPC is necessary for the transfer of infectivity to the central nervous system. The spleen is involved in neuroinvasion and neural dissemination in prion diseases but the nature of this involvement is not known. The present study undertook the investigation of the spatial relationship between sites of PrPSc accumulation, localisation of nerve fibres and PrPC expression in the tissue compartments of the spleen of scrapieinoculated and control sheep. Methodology/Principal Findings: Laser microdissection and quantitative PCR were used to determine PrP mRNA levels and results were compared with immunohistochemical protocols to distinguish PrPC and PrPSc in tissue compartments of the spleen. In sheep experimentally infected with scrapie, the major sites of accumulation of PrPSc in the spleen, namely the lymphoid nodules and the marginal zone, expressed low levels of PrP mRNA. Double immunohistochemical labelling for PrPSc and the pan-nerve fibre marker, PGP, was used to evaluate the density of innervation of splenic tissue compartments and the intimacy of association between PrPSc and nerves. Some nerve fibres were observed to accompany blood vessels into the PrPSc-laden germinal centres. However, the close association between nerves and PrPSc was most apparent in the marginal zone. Other sites of close association were adjacent to the wall of the central artery of PALS and the outer rim of germinal centres. Conclusions/Significance: The findings suggest that the degree of PrPSc accumulation does not depend on the expression level of PrPC. Though several splenic compartments may contribute to neuroinvasion, the marginal zone may play a central role in being the compartment with most apparent association between nerves and PrPSc. [ABSTRACT FROM AUTHOR]

Published

2009

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

Author

Giulia Malachin, Malin R Reiten, Øyvind Salvesen, Håvard Aanes, Jorke H Kamstra, Kerstin Skovgaard, Peter M H Heegaard, Cecilie Ersdal, Arild Espenes, Michael A Tranulis, and Maren K Bakkebø

Subjects

Medicine, Science

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