Your search keyword '"James F. Striebel"' showing total 36 results

1. Second passage experiments of chronic wasting disease in transgenic mice overexpressing human prion protein

Author

Brent Race, Chase Baune, Katie Williams, James F. Striebel, Andrew G. Hughson, and Bruce Chesebro

Subjects

RT-QuIC, prion, cross-species transmission, barrier, chronic wasting disease, transgenic mice, Veterinary medicine, SF600-1100

Abstract

Abstract Chronic wasting disease (CWD) is a prion disease of cervids including deer, elk, reindeer, and moose. Human consumption of cervids is common, therefore assessing the risk potential of CWD transmission to humans is critical. In a previous study, we tested CWD transmission via intracerebral inoculation into transgenic mice (tg66 and tgRM) that over-expressed human prion protein. Mice screened by traditional prion detection assays were negative. However, in a group of 88 mice screened by the ultrasensitive RT-QuIC assay, we identified 4 tg66 mice that produced inconsistent positive RT-QuIC reactions. These data could be false positive reactions, residual input inoculum or indicative of subclinical infections suggestive of cross species transmission of CWD to humans. Additional experiments were required to understand the nature of the prion seeding activity in this model. In this manuscript, second passage experiments using brains from mice with weak prion seeding activity showed they were not infectious to additional recipient tg66 mice. Clearance experiments showed that input CWD prion seeding activity was eliminated by 180 days in tg66 mice and PrPKO mice, which are unable to replicate prion protein, indicating that the weak positive levels of seeding activity detected at later time points was not likely residual inoculum. The failure of CWD prions to cause disease in tg66 after two sequential passages suggested that a strong species barrier prevented CWD infection of mice expressing human prion protein.

Published

2022

2. CD11c is not required by microglia to convey neuroprotection after prion infection

Author

James A. Carroll, James F. Striebel, Chase Baune, Bruce Chesebro, and Brent Race

Subjects

Medicine, Science

Published

2023

3. Innate immune responses after stimulation with Toll-like receptor agonists in ex vivo microglial cultures and an in vivo model using mice with reduced microglia

Author

James A. Carroll, Brent Race, Katie Williams, James F. Striebel, and Bruce Chesebro

Subjects

Microglia, Neuroinflammation, Innate immunity, PLX5622, CSF1R, Toll-like receptor, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Past experiments studying innate immunity in the central nervous system (CNS) utilized microglia obtained from neonatal mouse brain, which differ developmentally from adult microglia. These differences might impact our current understanding of the role of microglia in CNS development, function, and disease. Methods Cytokine protein secretion was compared in ex vivo P3 and adult microglial cultures after exposure to agonists for three different toll-like receptors (TLR4, lipopolysaccharide [LPS]; TLR7, imiquimod [IMQ]; and TLR9, CpG Oligodeoxynucleotide [CpG-ODN] 1585). In addition, changes in inflammatory gene expression in ex vivo adult microglia in response to the TLR agonists was assessed. Furthermore, in vivo experiments evaluated changes in gene expression associated with inflammation and TLR signaling in brains of mice with or without treatment with PLX5622 to reduce microglia. Results Ex vivo adult and P3 microglia increased cytokine secretion when exposed to TLR4 agonist LPS and to TLR7 agonist IMQ. However, adult microglia decreased expression of numerous genes after exposure to TLR 9 agonist CpG-ODN 1585. In contrast, in vivo studies indicated a core group of inflammatory and TLR signaling genes increased when each of the TLR agonists was introduced into the CNS. Reducing microglia in the brain led to decreased expression of various inflammatory and TLR signaling genes. Mice with reduced microglia showed extreme impairment in upregulation of genes after exposure to TLR7 agonist IMQ. Conclusions Cultured adult microglia were more reactive than P3 microglia to LPS or IMQ exposure. In vivo results indicated microglial influences on neuroinflammation were agonist specific, with responses to TLR7 agonist IMQ more dysregulated in mice with reduced microglia. Thus, TLR7-mediated innate immune responses in the CNS appeared more dependent on the presence of microglia. Furthermore, partial responses to TLR4 and TLR9 agonists in mice with reduced microglia suggested other cell types in the CNS can compensate for their absence.

Published

2021

4. Prion-induced photoreceptor degeneration begins with misfolded prion protein accumulation in cones at two distinct sites: cilia and ribbon synapses

Author

James F. Striebel, Brent Race, Jacqueline M. Leung, Cindi Schwartz, and Bruce Chesebro

Subjects

Prion, Prion-like, Ribbon synapses, Retinitis pigmentosa, Alzheimer, Parkinson, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Accumulation of misfolded host proteins is central to neuropathogenesis of numerous human brain diseases including prion and prion-like diseases. Neurons of retina are also affected by these diseases. Previously, our group and others found that prion-induced retinal damage to photoreceptor cells in mice and humans resembled pathology of human retinitis pigmentosa caused by mutations in retinal proteins. Here, using confocal, epifluorescent and electron microscopy we followed deposition of disease-associated prion protein (PrPSc) and its association with damage to critical retinal structures following intracerebral prion inoculation. The earliest time and place of retinal PrPSc deposition was 67 days post-inoculation (dpi) on the inner segment (IS) of cone photoreceptors. At 104 and 118 dpi, PrPSc was associated with the base of cilia and swollen cone inner segments, suggesting ciliopathy as a pathogenic mechanism. By 118 dpi, PrPSc was deposited in both rods and cones which showed rootlet damage in the IS, and photoreceptor cell death was indicated by thinning of the outer nuclear layer. In the outer plexiform layer (OPL) in uninfected mice, normal host PrP (PrPC) was mainly associated with cone bipolar cell processes, but in infected mice, at 118 dpi, PrPSc was detected on cone and rod bipolar cell dendrites extending into ribbon synapses. Loss of ribbon synapses in cone pedicles and rod spherules in the OPL was observed to precede destruction of most rods and cones over the next 2–3 weeks. However, bipolar cells and horizontal cells were less damaged, indicating high selectivity among neurons for injury by prions. PrPSc deposition in cone and rod inner segments and on the bipolar cell processes participating in ribbon synapses appear to be critical early events leading to damage and death of photoreceptors after prion infection. These mechanisms may also occur in human retinitis pigmentosa and prion-like diseases, such as AD.

Published

2021

5. Prion-associated cerebral amyloid angiopathy is not exacerbated by human phosphorylated tau aggregates in scrapie-infected mice expressing anchorless prion protein

Author

Brent Race, Katie Williams, James F. Striebel, and Bruce Chesebro

Subjects

Tau, Human tau, Amyloid, Neurodegeneration, Anchorless prion protein, GPI-anchored prion protein, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Tau aggregates consisting of hyperphosphorylated tau fibrils are associated with many neurodegenerative diseases, including Alzheimer's disease, Pick's disease, frontotemporal dementia, and progressive supranuclear palsy. Tau may contribute to the pathogenesis of these diseases, collectively referred to as tauopathies. In human genetic prion diseases, tau aggregates are detected in association with amyloid plaques consisting of prion protein (PrP). However, the role of abnormal tau aggregates in PrP amyloid disease remains unclear. Previously we inoculated scrapie prions into transgenic mice expressing human tau, mouse tau, glycophosphatidylinositol (GPI) anchored PrP, and anchorless PrP. These mice developed both spongiform vacuolar pathology and PrP amyloid pathology, and human tau was detected near PrP amyloid plaques. However, the presence of human tau did not alter the disease tempo or prion-induced neuropathology. In the present study, we tested mice which more closely modeled familial human prion disease. These mice expressed human tau but lacked both mouse tau and GPI-anchored PrP. However, they did produce anchorless PrP, resulting in perivascular PrP amyloid plaques, i.e. cerebral amyloid angiopathy (CAA), without spongiform degeneration. Typical of PrP amyloid disease, the clinical course was very slow in this model. Nevertheless, the accumulation of aggregated, phosphorylated human tau and its association with PrP amyloid plaques failed to alter the timing or course of the clinical disease observed. These data suggest that human tau does not contribute to the pathogenesis of mouse PrP amyloid brain disease and raise the possibility that tau may also not be pathogenic in human PrP amyloid disease.

Published

2020

6. Microglia are not required for prion-induced retinal photoreceptor degeneration

Author

James F. Striebel, Brent Race, Katie Williams, James A. Carroll, Mikael Klingeborn, and Bruce Chesebro

Subjects

Retina, Degeneration, Photoreceptors, Gliosis, Microglia, Macrophages, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Degeneration of photoreceptors in the retina is a major cause of blindness in humans. Often retinal degeneration is due to inheritance of mutations in genes important in photoreceptor (PR) function, but can also be induced by other events including retinal trauma, microvascular disease, virus infection or prion infection. The onset of apoptosis and degeneration of PR neurons correlates with invasion of the PR cellular areas by microglia or monocytes, suggesting a causal role for these cells in pathogenesis of PR degenerative disease. To study the role of microglia in prion-induced retinal disease, we fed prion-infected mice a CSF-1 receptor blocking drug, PLX5622, to eliminate microglia in vivo, and the effects on retinal degeneration were analyzed over time. In mice not receiving drug, the main inflammatory cells invading the degenerating PR areas were microglia, not monocytes. Administration of PLX5622 was highly effective at ablating microglia in retina. However, lack of microglia during prion infection did not prevent degeneration of PR cells. Therefore, microglia were not required for the PR damage process during prion infection. Indeed, mice lacking microglia had slightly faster onset of PR damage. Similar results were seen in C57BL/10 mice and transgenic mice expressing GFP or RFP on microglia and monocytes, respectively. These results were supported by experiments using prion-infected Cx3cr1 knockout mice without PLX5622 treatment, where microglial expansion in retina was delayed, but PR degeneration was not. Contrary to predictions, microglia were not a causative factor in retinal damage by prion infection. Instead, newly generated PrPSc accumulated around the inner segment region of the PR cells and appeared to correlate with initiation of the pathogenic process in the absence of microglia.

Published

2019

7. Deletion of Kif5c Does Not Alter Prion Disease Tempo or Spread in Mouse Brain

Author

Brent Race, Katie Williams, Chase Baune, James F. Striebel, Clayton W. Winkler, James A. Carroll, Sandra E. Encalada, and Bruce Chesebro

Subjects

scrapie, prion, PrP, PrPC, PrPSc, kinesin, Microbiology, QR1-502

Abstract

In prion diseases, the spread of infectious prions (PrPSc) is thought to occur within nerves and across synapses of the central nervous system (CNS). However, the mechanisms by which PrPSc moves within axons and across nerve synapses remain undetermined. Molecular motors, including kinesins and dyneins, transport many types of intracellular cargo. Kinesin-1C (KIF5C) has been shown to transport vesicles carrying the normal prion protein (PrPC) within axons, but whether KIF5C is involved in PrPSc axonal transport is unknown. The current study tested whether stereotactic inoculation in the striatum of KIF5C knock-out mice (Kif5c−/−) with 0.5 µL volumes of mouse-adapted scrapie strains 22 L or ME7 would result in an altered rate of prion spreading and/or disease timing. Groups of mice injected with each strain were euthanized at either pre-clinical time points or following the development of prion disease. Immunohistochemistry for PrP was performed on brain sections and PrPSc distribution and tempo of spread were compared between mouse strains. In these experiments, no differences in PrPSc spread, distribution or survival times were observed between C57BL/6 and Kif5c−/− mice.

Published

2021

8. Prion-induced photoreceptor degeneration begins with misfolded prion protein accumulation in cones at two distinct sites: cilia and ribbon synapses

Author

Bruce Chesebro, Brent Race, James F. Striebel, Cindi L. Schwartz, and Jacqueline M. Leung

Subjects

0301 basic medicine, PrPSc Proteins, genetic structures, animal diseases, Apoptosis, Ribbon synapse, Photoreceptor cell, lcsh:RC346-429, chemistry.chemical_compound, Mice, 0302 clinical medicine, Retinal Rod Photoreceptor Cells, Parkinson, Prion-like, Microscopy, Confocal, Cell Death, Chemistry, Cell biology, Retinitis pigmentosa, medicine.anatomical_structure, Disease Progression, Retinal Cone Photoreceptor Cells, Prion, Retinal Bipolar Cells, Ciliopathy, Outer plexiform layer, Pathology and Forensic Medicine, 03 medical and health sciences, Cellular and Molecular Neuroscience, Necrosis, Ribbon synapses, medicine, Animals, Retinal Photoreceptor Cell Inner Segment, Outer nuclear layer, Photoreceptor Connecting Cilium, lcsh:Neurology. Diseases of the nervous system, Retina, Research, Retinal, medicine.disease, Retinal Photoreceptor Cell Outer Segment, nervous system diseases, Microscopy, Electron, 030104 developmental biology, Microscopy, Fluorescence, Alzheimer, Neurology (clinical), sense organs, 030217 neurology & neurosurgery, Scrapie

Abstract

Accumulation of misfolded host proteins is central to neuropathogenesis of numerous human brain diseases including prion and prion-like diseases. Neurons of retina are also affected by these diseases. Previously, our group and others found that prion-induced retinal damage to photoreceptor cells in mice and humans resembled pathology of human retinitis pigmentosa caused by mutations in retinal proteins. Here, using confocal, epifluorescent and electron microscopy we followed deposition of disease-associated prion protein (PrPSc) and its association with damage to critical retinal structures following intracerebral prion inoculation. The earliest time and place of retinal PrPSc deposition was 67 days post-inoculation (dpi) on the inner segment (IS) of cone photoreceptors. At 104 and 118 dpi, PrPSc was associated with the base of cilia and swollen cone inner segments, suggesting ciliopathy as a pathogenic mechanism. By 118 dpi, PrPSc was deposited in both rods and cones which showed rootlet damage in the IS, and photoreceptor cell death was indicated by thinning of the outer nuclear layer. In the outer plexiform layer (OPL) in uninfected mice, normal host PrP (PrPC) was mainly associated with cone bipolar cell processes, but in infected mice, at 118 dpi, PrPSc was detected on cone and rod bipolar cell dendrites extending into ribbon synapses. Loss of ribbon synapses in cone pedicles and rod spherules in the OPL was observed to precede destruction of most rods and cones over the next 2–3 weeks. However, bipolar cells and horizontal cells were less damaged, indicating high selectivity among neurons for injury by prions. PrPSc deposition in cone and rod inner segments and on the bipolar cell processes participating in ribbon synapses appear to be critical early events leading to damage and death of photoreceptors after prion infection. These mechanisms may also occur in human retinitis pigmentosa and prion-like diseases, such as AD.

Published

2021

9. Microglia have limited influence on early prion pathogenesis, clearance, or replication

Author

Brent Race, Katie Williams, Chase Baune, James F. Striebel, Dan Long, Tina Thomas, Lori Lubke, Bruce Chesebro, and James A. Carroll

Subjects

Mice, Inbred C57BL, Mice, Multidisciplinary, Prions, Animals, Brain, Microglia, Prion Diseases

Abstract

Microglia (MG) are critical to host defense during prion infection, but the mechanism(s) of this neuroprotection are poorly understood. To better examine the influence of MG during prion infection, we reduced MG in the brains of C57BL/10 mice using PLX5622 and assessed prion clearance and replication using multiple approaches that included bioassay, immunohistochemistry, and Real-Time Quaking Inducted Conversion (RT-QuIC). We also utilized a strategy of intermittent PLX5622 treatments to reduce MG and allow MG repopulation to test whether new MG could alter prion disease progress. Lastly, we investigated the influence of MG using tga20 mice, a rapid prion model that accumulates fewer pathological features and less PrPres in the infected brain. In C57BL/10 mice we found that MG were excluded from the inoculation site early after infection, but Iba1 positive infiltrating monocytes/macrophage were present. Reducing MG in the brain prior to prion inoculation did not increase susceptibility to prion infection. Short intermittent treatments with PLX5622 in prion infected C57BL/10 mice after 80 dpi were unsuccessful at altering the MG population, gliosis, or survival. Additionally, MG depletion using PLX5622 in tga20 mice had only a minor impact on prion pathogenesis, indicating that the presence of MG might be less important in this fast model with less prion accumulation. In contrast to the benefits of MG against prion disease in late stages of disease, our current experiments suggest MG do not play a role in early prion pathogenesis, clearance, or replication.

Published

2022

10. Innate immune responses after stimulation with Toll-like receptor agonists in ex vivo microglial cultures and an in vivo model using mice with reduced microglia

Author

Bruce Chesebro, Brent Race, James F. Striebel, Katie Williams, and James A. Carroll

Subjects

Agonist, LPS, medicine.drug_class, Immunology, Biology, CpG-ODN, Cellular and Molecular Neuroscience, Mice, Neuroinflammation, In vivo, Toll-like receptor, medicine, Animals, RC346-429, Innate immunity, Imiquimod, Microglia, General Neuroscience, Research, Toll-Like Receptors, CSF1R, Immunity, Innate, Mice, Inbred C57BL, Toll-Like Receptor 4, PLX5622, medicine.anatomical_structure, Neurology, Toll-Like Receptor 7, Toll-Like Receptor 9, TLR4, Cytokines, Cytokine secretion, Neurology. Diseases of the nervous system, Ex vivo

Abstract

BackgroundPast experiments studying innate immunity in the central nervous system (CNS) utilized microglia obtained from neonatal mouse brain, which differ developmentally from adult microglia. These differences might impact our current understanding of the role of microglia in CNS development, function, and disease.MethodsCytokine protein secretion was compared in ex vivo P3 and adult microglial cultures after exposure to agonists for three different toll-like receptors (TLR4, lipopolysaccharide [LPS]; TLR7, imiquimod [IMQ]; and TLR9, CpG Oligodeoxynucleotide [CpG-ODN] 1585). In addition, changes in inflammatory gene expression in ex vivo adult microglia in response to the TLR agonists was assessed. Furthermore, in vivo experiments evaluated changes in gene expression associated with inflammation and TLR signaling in brains of mice with or without treatment with PLX5622 to reduce microglia.ResultsEx vivo adult and P3 microglia increased cytokine secretion when exposed to TLR4 agonist LPS and to TLR7 agonist IMQ. However, adult microglia decreased expression of numerous genes after exposure to TLR 9 agonist CpG-ODN 1585. In contrast, in vivo studies indicated a core group of inflammatory and TLR signaling genes increased when each of the TLR agonists was introduced into the CNS. Reducing microglia in the brain led to decreased expression of various inflammatory and TLR signaling genes. Mice with reduced microglia showed extreme impairment in upregulation of genes after exposure to TLR7 agonist IMQ.ConclusionsCultured adult microglia were more reactive than P3 microglia to LPS or IMQ exposure. In vivo results indicated microglial influences on neuroinflammation were agonist specific, with responses to TLR7 agonist IMQ more dysregulated in mice with reduced microglia. Thus, TLR7-mediated innate immune responses in the CNS appeared more dependent on the presence of microglia. Furthermore, partial responses to TLR4 and TLR9 agonists in mice with reduced microglia suggested other cell types in the CNS can compensate for their absence.

Published

2021

11. Prion-associated cerebral amyloid angiopathy is not exacerbated by human phosphorylated tau aggregates in scrapie-infected mice expressing anchorless prion protein

Author

James F. Striebel, Katie Williams, Bruce Chesebro, and Brent Race

Subjects

0301 basic medicine, Genetically modified mouse, Pathology, medicine.medical_specialty, Amyloid, animal diseases, GPI-anchored prion protein, Scrapie, Mice, Transgenic, Plaque, Amyloid, tau Proteins, Neuropathology, Biology, Prion Proteins, Progressive supranuclear palsy, lcsh:RC321-571, 03 medical and health sciences, Amyloid disease, Mice, Protein Aggregates, 0302 clinical medicine, mental disorders, medicine, Animals, Humans, Neurodegeneration, Phosphorylation, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Brain, Human tau, medicine.disease, nervous system diseases, Cerebral Amyloid Angiopathy, 030104 developmental biology, Neurology, Anchorless prion protein, Disease Progression, Cerebral amyloid angiopathy, Tau, 030217 neurology & neurosurgery

Abstract

Tau aggregates consisting of hyperphosphorylated tau fibrils are associated with many neurodegenerative diseases, including Alzheimer's disease, Pick's disease, frontotemporal dementia, and progressive supranuclear palsy. Tau may contribute to the pathogenesis of these diseases, collectively referred to as tauopathies. In human genetic prion diseases, tau aggregates are detected in association with amyloid plaques consisting of prion protein (PrP). However, the role of abnormal tau aggregates in PrP amyloid disease remains unclear. Previously we inoculated scrapie prions into transgenic mice expressing human tau, mouse tau, glycophosphatidylinositol (GPI) anchored PrP, and anchorless PrP. These mice developed both spongiform vacuolar pathology and PrP amyloid pathology, and human tau was detected near PrP amyloid plaques. However, the presence of human tau did not alter the disease tempo or prion-induced neuropathology. In the present study, we tested mice which more closely modeled familial human prion disease. These mice expressed human tau but lacked both mouse tau and GPI-anchored PrP. However, they did produce anchorless PrP, resulting in perivascular PrP amyloid plaques, i.e. cerebral amyloid angiopathy (CAA), without spongiform degeneration. Typical of PrP amyloid disease, the clinical course was very slow in this model. Nevertheless, the accumulation of aggregated, phosphorylated human tau and its association with PrP amyloid plaques failed to alter the timing or course of the clinical disease observed. These data suggest that human tau does not contribute to the pathogenesis of mouse PrP amyloid brain disease and raise the possibility that tau may also not be pathogenic in human PrP amyloid disease.

Published

2020

12. Statins are ineffective at reducing neuroinflammation or prolonging survival in scrapie-infected mice

Author

James A. Carroll, Bruce Chesebro, Katie Phillips, James F. Striebel, and Brent Race

Subjects

0301 basic medicine, Simvastatin, Statin, medicine.drug_class, Atorvastatin, Biology, Pharmacology, Mice, 03 medical and health sciences, 0302 clinical medicine, Virology, Hyperlipidemia, medicine, Animals, Humans, cardiovascular diseases, Neuroinflammation, Pravastatin, Multiple sclerosis, nutritional and metabolic diseases, Neurodegenerative Diseases, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Gliosis, Immunology, lipids (amino acids, peptides, and proteins), medicine.symptom, 030217 neurology & neurosurgery, Scrapie, Research Article, medicine.drug

Abstract

Neuroinflammation is a prominent component of several neurodegenerative diseases, including multiple sclerosis, Alzheimer’s disease, Parkinson’s disease, tauopathies, amyotrophic lateral sclerosis and prion diseases. In such conditions, the ability to decrease neuroinflammation by drug therapy may influence disease progression. Statins have been used to treat hyperlipidemia as well as reduce neuroinflammation and oxidative stress in various tissues. In previous studies, treatment of scrapie-infected mice with the type 1 statins, simvastatin or pravastatin, showed a small beneficial effect on survival time. In the current study, to increase the effectiveness of statin therapy, we treated infected mice with atorvastatin, a type 2 statin that has improved pharmacokinetics over many type 1 statins. Treatments with either simvastatin or pravastatin were tested for comparison. We evaluated scrapie-infected mice for protease-resistant PrP (PrPres) accumulation, gliosis, neuroinflammation and time until advanced clinical disease requiring euthanasia. All three statin treatments reduced total serum cholesterol ≥40 % in mice. However, gliosis and PrPres deposition were similar in statin-treated and untreated infected mice. Time to euthanasia due to advanced clinical signs was not changed in statin-treated mice relative to untreated mice, a finding at odds with previous reports. Expression of 84 inflammatory genes involved in neuroinflammation was also quantitated. Seven genes were reduced by pravastatin, and one gene was reduced by atorvastatin. In contrast, simvastatin therapy did not reduce any of the tested genes, but did slightly increase the expression of Ccl2 and Cxcl13. Our studies indicate that none of the three statins tested were effective in reducing scrapie-induced neuroinflammation or neuropathogenesis.

Published

2017

13. RNA-seq and network analysis reveal unique glial gene expression signatures during prion infection

Author

James A. Carroll, James F. Striebel, Katie Williams, Bruce Chesebro, and Brent Race

Subjects

0301 basic medicine, Male, Scrapie, Apoptosis, lcsh:RC346-429, Prion Diseases, Mice, 0302 clinical medicine, Gene expression, Cluster Analysis, Gliosis, RNA-Seq, Organic Chemicals, In Situ Hybridization, CD18, Microglia, Neurodegeneration, Brain, Neurodegenerative Diseases, Immunohistochemistry, Cell biology, Astrogliosis, medicine.anatomical_structure, Prion, Female, medicine.symptom, Astrocyte, Neuroglia, Signal Transduction, Prions, CD11c, Biology, 03 medical and health sciences, Cellular and Molecular Neuroscience, medicine, Animals, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, Research, medicine.disease, nervous system diseases, CD11c Antigen, Mice, Inbred C57BL, PLX5622, 030104 developmental biology, Gene Ontology, Gene Expression Regulation, Astrocytes, CD18 Antigens, Transcriptome, 030217 neurology & neurosurgery

Abstract

Background Prion diseases and prion-like disorders, including Alzheimer’s disease and Parkinson’s disease, are characterized by gliosis and accumulation of misfolded aggregated host proteins. Ablating microglia in prion-infected brain by treatment with the colony-stimulating factor-1 receptor (CSF-1R) inhibitor, PLX5622, increased accumulation of misfolded prion protein and decreased survival time. Methods To better understand the role of glia during neurodegeneration, we used RNA-seq technology, network analysis, and hierarchical cluster analysis to compare gene expression in brains of prion-infected versus mock-inoculated mice. Comparisons were also made between PLX5622-treated prion-infected mice and untreated prion-infected mice to assess mechanisms involved in disease acceleration in the absence of microglia. Results RNA-seq and network analysis suggested that microglia responded to prion infection through activation of integrin CD11c/18 and did not adopt the expression signature associated with other neurodegenerative disease models. Instead, microglia acquired an alternative molecular signature late in the disease process. Furthermore, astrocytes expressed a signature pattern of genes which appeared to be specific for prion diseases. Comparisons were also made with prion-infected mice treated with PLX5622 to assess the impact of microglia ablation on astrocyte gene expression during prion infection. In the presence of microglia, a unique mix of transcripts associated with A1- and A2-reactive astrocytes was increased in brains of prion-infected mice. After ablation of microglia, this reactive astrocyte expression pattern was enhanced. Thus, after prion infection, microglia appeared to decrease the overall A1/A2-astrocyte responses which might contribute to increased survival after infection. Conclusions RNA-seq analysis indicated dysregulation of over 300 biological processes within the CNS during prion disease. Distinctive microglia- and astrocyte-associated expression signatures were identified during prion infection. Furthermore, astrogliosis and the unique astrocyte-associated expression signature were independent of microglial influences. Astrogliosis and the unique astrocyte-associated gene expression pattern were increased when microglia were ablated. Our findings emphasize the potential existence of alternative pathways for activating the A1/A2 paradigm in astrocytes during neurodegenerative disease.

Published

2020

14. Knockout of fractalkine receptor Cx3cr1 does not alter disease or microglial activation in prion-infected mice

Author

Katie Phillips, Bruce Chesebro, James F. Striebel, Brent Race, and James A. Carroll

Subjects

0301 basic medicine, Chemokine, medicine.medical_treatment, CX3C Chemokine Receptor 1, Scrapie, Prion Diseases, Mice, 03 medical and health sciences, Receptors, HIV, Virology, CX3CR1, medicine, Animals, Receptors, Cytokine, CX3CL1, Mice, Knockout, biology, Microglia, Animal, Brain, medicine.disease, 030104 developmental biology, Cytokine, medicine.anatomical_structure, Immunology, biology.protein, Receptors, Chemokine, Signal transduction, Signal Transduction, Spongiosis

Abstract

Microglial activation is a hallmark of the neuroimmunological response to Alzheimer's disease, Parkinson's disease, amyotrophic lateral sclerosis and prion disease. The CX3C chemokine axis consists of fractalkine (CX3CL1) and its receptor (CX3CR1); these are expressed by neurons and microglia respectively, and are known to modulate microglial activation. In prion-infected mice, both Cx3cr1 and Cx3cl1 are altered, suggesting a role in disease. To investigate the influence of CX3C axis signalling on prion disease, we infected Cx3cr1 knockout (Cx3cr1-KO) and control mice with scrapie strains 22L and RML. Deletion of Cx3cr1 had no effect on development of clinical signs or disease incubation period. In addition, comparison of brain tissue from Cx3cr1-KO and control mice revealed no significant differences in cytokine levels, spongiosis, deposition of disease-associated prion protein or microglial activation. Thus, microglial activation during prion infection did not require CX3C axis signalling.

Published

2016

15. Microglia Are Critical in Host Defense against Prion Disease

Author

Bruce Chesebro, Brent Race, James A. Carroll, James F. Striebel, and Katie Williams

Subjects

0301 basic medicine, Male, PrPSc Proteins, medicine.drug_class, Prions, Immunology, Central nervous system, Administration, Oral, Scrapie, Apoptosis, Disease, Biology, Microbiology, Severity of Illness Index, Tyrosine-kinase inhibitor, 03 medical and health sciences, Mice, 0302 clinical medicine, Virology, medicine, Animals, Organic Chemicals, Receptor, Neuroinflammation, Microglia, medicine.disease, Astrogliosis, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, nervous system, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, Insect Science, Female, 030217 neurology & neurosurgery

Abstract

Microglial cells in the central nervous system play important roles in neurodevelopment and resistance to infection, yet microglia can become neurotoxic under some conditions. An early event during prion infection is the activation of microglia and astrocytes in the brain prior to damage or death of neurons. Previous prion disease studies using two different strategies to manipulate signaling through the microglial receptor CSF-1R reported contrary effects on survival from prion disease. However, in these studies, reductions of microglial numbers and function were variable, thus confounding interpretation of the results. In the present work, we used oral treatment with a potent inhibitor of CSF-1R, PLX5622, to eliminate 78 to 90% of microglia from cortex early during the course of prion infection. Oral drug treatment early after infection with the RML scrapie strain significantly accelerated vacuolation, astrogliosis, and deposition of disease-associated prion protein. Furthermore, drug-treated mice had advanced clinical disease requiring euthanasia 31 days earlier than untreated control mice. Similarly, PLX5622 treatment during the preclinical phase at 80 days postinfection with RML scrapie also accelerated disease and resulted in euthanasia of mice 33 days earlier than infected controls. PLX5622 also accelerated clinical disease after infection with scrapie strains ME7 and 22L. Thus, microglia are critical in host defense during prion disease. The early accumulation of PrPSc in the absence of microglia suggested that microglia may function by clearing PrPSc, resulting in longer survival.IMPORTANCE Microglia contribute to many aspects of health and disease. When activated, microglia can be beneficial by repairing damage in the central nervous system (CNS) or they can turn harmful by becoming neurotoxic. In prion and prionlike diseases, the involvement of microglia in disease is unclear. Previous studies suggest that microglia can either speed up or slow down disease. In this study, we infected mice with prions and depleted microglia from the brains of mice using PLX5622, an effective CSF-1R tyrosine kinase inhibitor. Microglia were markedly reduced in brains, and prion disease was accelerated, so that mice needed to be euthanized 20 to 33 days earlier than infected control mice due to advanced clinical disease. Similar results occurred when mice were treated with PLX5622 at 80 days after infection, which was just prior to the start of clinical signs. Thus, microglia are important for removing prions, and the disease is faster when microglia are depleted.

Published

2018

16. Chronic Wasting Disease Agents in Nonhuman Primates

Author

Kimberly Meade-White, Bruce Chesebro, Katie Phillips, Richard E. Race, Brent Race, and James F. Striebel

Subjects

Primates, Microbiology (medical), Genotype, Prions, Epidemiology, animal diseases, lcsh:Medicine, non-human primate, Disease, lcsh:Infectious and parasitic diseases, prion, biology.animal, squirrel monkey, species barrier, medicine, Animals, lcsh:RC109-216, Primate, Saimiri, transmissible spongiform encephalopathy, Transmissible spongiform encephalopathy, biology, Transmission (medicine), Monkey Diseases, lcsh:R, Squirrel monkey, Dispatch, transmission, Brain, Chronic wasting disease, medicine.disease, biology.organism_classification, Virology, Infectious Diseases, Immunology, Macaca, Wasting Disease, Chronic, Disease Susceptibility, cynomolgus macaque

Abstract

Chronic wasting disease is a prion disease of cervids. Assessment of its zoonotic potential is critical. To evaluate primate susceptibility, we tested monkeys from 2 genera. We found that 100% of intracerebrally inoculated and 92% of orally inoculated squirrel monkeys were susceptible, but cynomolgus macaques were not, suggesting possible low risk for humans.

Published

2014

17. Lack of influence of prion protein gene expression on kainate-induced seizures in mice: Studies using congenic, coisogenic and transgenic strains

Author

Melissa Pathmajeyan, Alejandra Rangel, Bruce Chesebro, Brent Race, and James F. Striebel

Subjects

Kainic acid, animal diseases, General Neuroscience, Transgene, Congenic, Kainate receptor, Biology, Molecular biology, nervous system diseases, PRNP, Complementation, chemistry.chemical_compound, chemistry, Gene expression, Gene

Abstract

Prion protein (PrP) is a glycosylphosphatidylinositol (GPI) anchored cell surface protein expressed by many cells, including those of the mammalian nervous system. At present the physiologic functions of PrP remain unclear. Deletion of Prnp, the gene encoding PrP in mice, has been shown to alter normal synaptic and electrophysiologic activities, indicating a potential role in seizure susceptibility. However, published efforts to link PrP with seizures, using both in vivo and in vitro models, are conflicting and difficult to interpret due to use of various mouse backgrounds and seizure induction techniques. Here we investigated the role of PrP in kainic acid (KA)-induced seizure sensitivity, using three types of mice. In contrast to previous published results, Prnp−/− mice on the C57BL/10SnJ background had a significant decrease in KA-induced seizure susceptibility. In genetic complementation experiments using a PrP-expressing transgene, genes derived from strain 129/Ola, which flanked the Prnp−/− locus in C57BL/10SnJ mice, rather than Prnp itself, appeared to account for this effect. Furthermore, using coisogenic 129/Ola mice differing only at Prnp, this difference was not reproduced when comparing PrP-negative and PrP-positive mice. In contrast, substrains of PrP-expressing C57BL mice, showed large variations in KA-induced seizure sensitivity. The magnitude of these differences in susceptibility was larger than that associated with the presence of the Prnp gene, suggesting extensive influence of genes other than Prnp on seizure sensitivity in this system.

Published

2013

18. Non-amyloid and amyloid prion protein deposits in prion-infected mice differ in blockage of interstitial brain fluid

Author

Bruce Chesebro, Brent Race, Alejandra Rangel, and James F. Striebel

Subjects

Genetically modified mouse, Pathology, medicine.medical_specialty, Histology, Amyloid, animal diseases, PrPSc Proteins, Colocalization, Biology, medicine.disease, nervous system diseases, Pathology and Forensic Medicine, Neurology, Interstitial fluid, Physiology (medical), mental disorders, Extracellular fluid, medicine, Extracellular, Neurology (clinical), Cerebral amyloid angiopathy

Abstract

Aims Prion diseases are characterized by brain deposits of misfolded aggregated protease-resistant prion protein (PrP), termed PrPres. In humans and animals, PrPres is found as either disorganized non-amyloid aggregates or organized amyloid fibrils. Both PrPres forms are found in extracellular spaces of the brain. Thus, both might block drainage of brain interstitial fluid (ISF). The present experiments studied whether ISF blockage occurred during amyloid and/or non-amyloid prion diseases. Methods Various-sized fluorescein-labelled ISF tracers were stereotactically inoculated into the striatum of adult mice. At times from 5 min to 77 h, uninfected and scrapie-infected mice were compared. C57BL/10 mice expressing wild-type anchored PrP, which develop non-amyloid PrPres similar to humans with sporadic Creutzfeldt–Jakob disease, were compared with Tg44+/+ mice (transgenic mice secreting anchorless PrP) expressing anchorless PrP, which develop amyloid PrPres similar to certain human familial prion diseases. Results In C57BL/10 mice, extensive non-amyloid PrPres aggregate deposition was not associated with abnormal clearance kinetics of tracers. In contrast, scrapie-infected Tg44+/+ mice showed blockage of tracer clearance and colocalization of tracer with perivascular PrPres amyloid. Conclusions As tracer localization and clearance was normal in infected C57BL/10 mice, ISF blockage was not an important pathogenic mechanism in this model. Therefore, ISF blockage is unlikely to be a problem in non-amyloid human prion diseases such as sporadic Creutzfeldt–Jakob disease. In contrast, partial ISF blockage appeared to be a possible pathogenic mechanism in Tg44+/+ mice. Thus this mechanism might also influence human amyloid prion diseases where expression of anchorless or mutated PrP results in perivascular amyloid PrPres deposition and cerebral amyloid angiopathy.

Published

2013

19. Early Cytokine Elevation, PrPres Deposition, and Gliosis in Mouse Scrapie: No Effect on Disease by Deletion of Cytokine Genes IL-12p40 and IL-12p35

Author

Bruce Chesebro, Brent Race, James A. Carroll, Déborah Tribouillard-Tanvier, James F. Striebel, and Katie Phillips

Subjects

Prions, Chemokine CXCL1, medicine.medical_treatment, Interleukin-1beta, Immunology, Scrapie, Biology, Microbiology, Interleukin-12 Subunit p35, Mice, Virology, medicine, Animals, CXCL10, Gliosis, Neuroinflammation, Chemokine CCL3, Inflammation, Mice, Knockout, Interleukin-12 Subunit p40, Brain, medicine.disease, Astrogliosis, Mice, Inbred C57BL, CXCL1, Cytokine, Insect Science, Knockout mouse, Cytokines, Female, medicine.symptom, Gene Deletion

Abstract

Neurodegenerative diseases are typically associated with an activation of glia and an increased level of cytokines. In our previous studies of prion disease, the cytokine response in the brains of clinically sick scrapie-infected mice was restricted to a small group of cytokines, of which IL-12p40, CCL2, and CXCL10 were present at the highest levels. The goal of our current research was to determine the relationship between cytokine responses, gliosis, and neuropathology during prion disease. Here, in time course studies of C57BL/10 mice intracerebrally inoculated with 22L scrapie, abnormal protease-resistant prion protein (PrPres), astrogliosis, and microgliosis were first detected at 40 days after intracerebral scrapie inoculation. In cytokine studies, IL-12p40 was first elevated by 60 days; CCL3, IL-1β, and CXCL1 were elevated by 80 days; and CCL2 and CCL5 were elevated by 115 days. IL-12p40 showed the most extensive increase throughout disease and was 30-fold above control levels at the terminal stage. Because of the early onset and dramatic elevation of IL-12p40 during scrapie, we investigated whether IL-12p40 contributed to the development of prion disease neuropathogenesis by using three different scrapie strains (22L, RML, 79A) to infect knockout mice in which the gene encoding IL-12p40 was deleted. We also studied knockout mice lacking IL-12p35, which combines with IL-12p40 to form active IL-12 heterodimers. In all instances, knockout mice did not differ from control mice in survival time, clinical tempo, or levels of spongiosis, gliosis, or PrPres in the brain. Thus, neither IL-12p40 nor IL-12p35 molecules were required for prion disease-associated neurodegeneration or neuroinflammation.

Published

2012

20. Role of Cyclophilin A from Brains of Prion-infected Mice in Stimulation of Cytokine Release by Microglia and Astroglia in Vitro

Author

Roger A. Moore, James A. Carroll, James F. Striebel, Déborah Tribouillard-Tanvier, and Bruce Chesebro

Subjects

Prions, medicine.medical_treatment, Nerve Tissue Proteins, Scrapie, Cypa, Stimulation, CCL2, Biology, Biochemistry, Antibodies, Prion Diseases, Mice, medicine, Animals, Molecular Biology, Chemokine CCL2, Transmissible spongiform encephalopathy, Microglia, Interleukin-12 Subunit p40, Brain, Molecular Bases of Disease, Cell Biology, biology.organism_classification, medicine.disease, Virology, Cell biology, Cytokine, medicine.anatomical_structure, nervous system, Gliosis, Astrocytes, medicine.symptom, Cyclophilin A

Abstract

Prion diseases or transmissible spongiform encephalopathy diseases are typically characterized by deposition of abnormally folded partially protease-resistant host-derived prion protein (PrPres), which is associated with activated glia and increased release of cytokines. This neuroinflammatory response may play a role in transmissible spongiform encephalopathy pathogenesis. We previously reported that brain homogenates from prion-infected mice induced cytokine protein release in primary astroglial and microglial cell cultures. Here we measured cytokine release by cultured glial cells to determine what factors in infected brain contributed to activation of microglia and astroglia. In assays analyzing IL-12p40 and CCL2 (MCP-1), glial cells were not stimulated in vitro by either PrPres purified from infected mouse brains or prion protein amyloid fibrils produced in vitro. However, significant glial stimulation was induced by clarified scrapie brain homogenates lacking PrPres. This stimulation was greatly reduced both by antibody to cyclophilin A (CyPA), a known mediator of inflammation in peripheral tissues, and by cyclosporine A, a CyPA inhibitor. In biochemical studies, purified truncated CyPA fragments stimulated a pattern of cytokine release by microglia and astroglia similar to that induced by scrapie-infected brain homogenates, whereas purified full-length CyPA was a poor stimulator. This requirement for CyPA truncation was not reported in previous studies of stimulation of peripheral macrophages, endothelial cell cardiomyocytes, and vascular smooth muscle cells. Therefore, truncated CyPA detected in brain following prion infection may have an important role in the activation of brain-derived primary astroglia and microglia in prion disease and perhaps other neurodegenerative or neuroinflammatory diseases.

Published

2012

21. Increased excitatory amino acid transport into murine prion protein knockout astrocytes cultured in vitro

Author

James A. Carroll, James F. Striebel, Todd Seib, Bruce Chesebro, Sarjubhai A. Patel, Richard J. Bridges, and Melissa Pathmajeyan

Subjects

Cell Survival, Prions, Blotting, Western, Excitotoxicity, Glutamic Acid, Glutamate Plasma Membrane Transport Proteins, Biology, Neurotransmission, Real-Time Polymerase Chain Reaction, medicine.disease_cause, Article, Mice, Cellular and Molecular Neuroscience, Glutamatergic, medicine, Animals, RNA, Messenger, Cells, Cultured, Mice, Knockout, Neurons, Aspartic Acid, Sodium, Flow Cytometry, Immunohistochemistry, Molecular biology, Coculture Techniques, Excitatory Amino Acid Transporter 1, Mice, Inbred C57BL, medicine.anatomical_structure, Excitatory Amino Acid Transporter 2, Neurology, Astrocytes, Excitatory postsynaptic potential, NMDA receptor, Glutamatergic synapse, Astrocyte

Abstract

Prion protein (PrP) is expressed on a wide variety of cells and plays an important role in the pathogenesis of transmissible spongiform encephalopathies. However, its normal function remains unclear. Mice that do not express PrP exhibit deficits in spatial memory and abnormalities in excitatory neurotransmission suggestive that PrP may function in the glutamatergic synapse. Here, we show that transport of D-aspartate, a nonmetabolized L-glutamate analog, through excitatory amino acid transporters (EAATs) was faster in astrocytes from PrP knockout (PrPKO) mice than in astrocytes from C57BL/10SnJ wild-type (WT) mice. Experiments using EAAT subtype-specific inhibitors demonstrated that in both WT and PrPKO astrocytes, the majority of transport was mediated by EAAT1. Furthermore, PrPKO astrocytes were more effective than WT astrocytes at alleviating L-glutamate-mediated excitotoxic damage in both WT and PrPKO neuronal cultures. Thus, in this in vitro model, PrPKO astrocytes exerted a functional influence on neuronal survival and may therefore influence regulation of glutamatergic neurotransmission in vivo.

Published

2011

22. Crucial Role for Prion Protein Membrane Anchoring in the Neuroinvasion and Neural Spread of Prion Infection

Author

Bruce Chesebro, James F. Striebel, Brent Race, Kimberly Meade-White, Mikael Klingeborn, and Rebecca Rosenke

Subjects

Central Nervous System, Gene isoform, PrPSc Proteins, Prions, animal diseases, Transgene, Immunology, Central nervous system, Mice, Transgenic, Scrapie, Biology, Microbiology, Prion Diseases, Mice, Tongue, Virology, medicine, Animals, Cell Membrane, Brain, Sciatic Nerve, nervous system diseases, Mice, Inbred C57BL, Membrane glycoproteins, medicine.anatomical_structure, Spinal Cord, Membrane protein, Insect Science, biology.protein, Pathogenesis and Immunity, Sciatic nerve

Abstract

In nature prion diseases are usually transmitted by extracerebral prion infection, but clinical disease results only after invasion of the central nervous system (CNS). Prion protein (PrP), a host-encoded glycosylphosphatidylinositol (GPI)-anchored membrane glycoprotein, is necessary for prion infection and disease. Here, we investigated the role of the anchoring of PrP on prion neuroinvasion by studying various inoculation routes in mice expressing either anchored or anchorless PrP. In control mice with anchored PrP, intracerebral or sciatic nerve inoculation resulted in rapid CNS neuroinvasion and clinical disease (154 to 156 days), and after tongue, ocular, intravenous, or intraperitoneal inoculation, CNS neuroinvasion was only slightly slower (193 to 231 days). In contrast, in anchorless PrP mice, these routes resulted in slow and infrequent CNS neuroinvasion. Only intracerebral inoculation caused brain PrPres, a protease-resistant isoform of PrP, and disease in both types of mice. Thus, anchored PrP was an essential component for the rapid neural spread and CNS neuroinvasion of prion infection.

Published

2011

23. Susceptibilities of Nonhuman Primates to Chronic Wasting Disease

Author

Richard Rubenstein, Donald J. Gardner, Kent D. Barbian, Elizabeth S. Williams, Giuseppe LaFauci, Kimberly Meade-White, Michael J. Parnell, Larisa Cervenakova, Michael W. Miller, Cynthia Favara, James F. Striebel, Suzette A. Priola, Richard E. Race, Bruce Chesebro, Brent Race, Anne Ward, and Dan Long

Subjects

Microbiology (medical), TSE diseases, Prions, Epidemiology, animal diseases, lcsh:Medicine, Mice, Transgenic, Spleen, Disease, Biology, intracerebral transmission, Prion Diseases, lcsh:Infectious and parasitic diseases, Mice, Species Specificity, oral transmission, medicine, Animals, Humans, lcsh:RC109-216, Wasting Syndrome, Saimiri, Transmissible spongiform encephalopathy, Research, lcsh:R, Brain, Chronic wasting disease, Clinical disease, medicine.disease, Virology, prions and related diseases, Disease Models, Animal, Macaca fascicularis, Infectious Diseases, medicine.anatomical_structure, Immunology, squirrel monkeys, Wasting Disease, Chronic, Disease Susceptibility, Lymph Nodes, Lymph, Spongiform encephalopathy, cynomolgus macaques, Peptide Hydrolases

Abstract

A species barrier may protect humans from this disease., Chronic wasting disease (CWD) is a transmissible spongiform encephalopathy, or prion disease, that affects deer, elk, and moose. Human susceptibility to CWD remains unproven despite likely exposure to CWD-infected cervids. We used 2 nonhuman primate species, cynomolgus macaques and squirrel monkeys, as human models for CWD susceptibility. CWD was inoculated into these 2 species by intracerebral and oral routes. After intracerebral inoculation of squirrel monkeys, 7 of 8 CWD isolates induced a clinical wasting syndrome within 33–53 months. The monkeys’ brains showed spongiform encephalopathy and protease-resistant prion protein (PrPres) diagnostic of prion disease. After oral exposure, 2 squirrel monkeys had PrPres in brain, spleen, and lymph nodes at 69 months postinfection. In contrast, cynomolgus macaques have not shown evidence of clinical disease as of 70 months postinfection. Thus, these 2 species differed in susceptibility to CWD. Because humans are evolutionarily closer to macaques than to squirrel monkeys, they may also be resistant to CWD.

Published

2009

24. Prion Protein Expression Differences in Microglia and Astroglia Influence Scrapie-Induced Neurodegeneration in the Retina and Brain of Transgenic Mice

Author

Rachel A. LaCasse, Bruce Chesebro, Cynthia Favara, James F. Striebel, and Lisa Kercher

Subjects

Retinal degeneration, Genetically modified mouse, Chemokine, PrPSc Proteins, Immunology, Mice, Transgenic, Scrapie, Microbiology, Retina, Mice, chemistry.chemical_compound, Virology, medicine, Animals, Microglia, biology, Neurodegeneration, Brain, Neurodegenerative Diseases, Retinal, medicine.disease, Up-Regulation, Cell biology, medicine.anatomical_structure, chemistry, Astrocytes, Insect Science, biology.protein, Pathogenesis and Immunity, Chemokines

Abstract

Activated microglia and astroglia are known to be involved in a variety of neurodegenerative diseases, including prion diseases. In the present experiments, we studied activation of astroglia and microglia after intraocular scrapie infection in transgenic mice expressing prion protein (PrP) in multiple cell types (tg7 mice) or in neurons only (tgNSE mice). In this model, scrapie infection and protease-resistant PrP deposition occurs in the retinas of both strains of mice, but retinal degeneration is observed only in tg7 mice. Our results showed that the retinas of tg7 and tgNSE mice both had astroglial activation with increased chemokine expression during the course of infection. However, only tg7 retinas exhibited strong microglial activation compared to tgNSE retinas, which showed little microglial activation by biochemical or morphological criteria. Therefore, microglial PrP expression might be required for scrapie-induced retinal microglial activation and damage. Furthermore, microglial activation preceded retinal neurodegeneration in tg7 mice, suggesting that activated microglia might contribute to the degenerative process, rather than being a response to the damage. Surprisingly, brain differed from retina in that an altered profile of microglial activation markers was upregulated, and the profiles in the two mouse strains were indistinguishable. Microglial activation in the brain was associated with severe brain vacuolation and neurodegeneration, leading to death. Thus, retinal and brain microglia appeared to differ in their requirements for activation, suggesting that different activation pathways occur in the two tissues.

Published

2007

25. Early Generation of New PrPSc on Blood Vessels after Brain Microinjection of Scrapie in Mice

Author

Byron Caughey, Bruce Chesebro, Brent Race, Katie Phillips, Alejandra Rangel, James F. Striebel, and Andrew G. Hughson

Subjects

Pathology, medicine.medical_specialty, Time Factors, Microinjections, PrPSc Proteins, animal diseases, Immunoblotting, Central nervous system, Scrapie, Biology, Microbiology, Chemistry Techniques, Analytical, Interstitial fluid, In vivo, Virology, medicine, Animals, Microinjection, Basement membrane, Immunohistochemistry, QR1-502, nervous system diseases, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, Blood Vessels, Research Article, Blood vessel

Abstract

Aggregation of misfolded host proteins in the central nervous system is believed to be important in the pathogenic process in several neurodegenerative diseases of humans, including prion diseases, Alzheimer’s disease, and Parkinson’s disease. In these diseases, protein misfolding and aggregation appear to expand through a process of seeded polymerization. Prion diseases occur in both humans and animals and are experimentally transmissible orally or by injection, thus providing a controllable model of other neurodegenerative protein misfolding diseases. In rodents and ruminants, prion disease has a slow course, lasting months to years. Although prion infectivity has been detected in brain tissue at 3 to 4 weeks postinfection (p.i.), the details of early prion replication in the brain are not well understood. Here we studied the localization and quantitation of PrPSc generation in vivo starting at 30 min postmicroinjection of scrapie into the brain. In C57BL mice at 3 days p.i., generation of new PrPSc was detected by immunohistochemistry and immunoblot assays, and at 7 days p.i., new generation was confirmed by real-time quaking-induced conversion assay. The main site of new PrPSc generation was near the outer basement membrane of small and medium blood vessels. The finding and localization of replication at this site so early after injection have not been reported previously. This predominantly perivascular location suggested that structural components of the blood vessel basement membrane or perivascular astrocytes might act as cofactors in the initial generation of PrPSc. The location of PrPSc replication at the basement membrane also implies a role for the brain interstitial fluid drainage in the early infection process., IMPORTANCE Neurodegenerative diseases, including Alzheimer’s disease, Parkinson’s disease, and prion diseases, of humans are characterized by misfolding and aggregation of certain proteins, resulting in the destruction of brain tissue. In these diseases, the damage process spreads progressively within the central nervous system, but only prion diseases are known to be transmissible between individuals. Here we used microinjection of infectious prion protein (PrPSc) into the mouse brain to model early events of iatrogenic prion transmission via surgical instruments or tissue grafts. At 3 and 7 days postinjection, we detected the generation of new PrPSc, mostly on the outer walls of blood vessels near the injection site. This location and very early replication were surprising and unique. Perivascular prion replication suggested the transport of injected PrPSc via brain interstitial fluid to the basement membranes of blood vessels, where interactions with possible cofactors made by astrocytes or endothelia might facilitate the earliest cycles of prion infection.

Published

2015

26. Increased Infectivity of Anchorless Mouse Scrapie Prions in Transgenic Mice Overexpressing Human Prion Protein

Author

Kimberly Meade-White, Katie Phillips, James F. Striebel, Bruce Chesebro, and Brent Race

Subjects

Genetically modified mouse, Glycosylation, Prions, Transgene, animal diseases, Immunology, Scrapie, Mice, Transgenic, Biology, Microbiology, Prion Diseases, chemistry.chemical_compound, In vivo, Virology, Animals, Humans, Transgenes, Peptide sequence, chemistry.chemical_classification, Infectivity, Cell biology, nervous system diseases, Mice, Inbred C57BL, Disease Models, Animal, chemistry, Insect Science, lipids (amino acids, peptides, and proteins), Glycoprotein

Abstract

Prion protein (PrP) is found in all mammals, mostly as a glycoprotein anchored to the plasma membrane by a C-terminal glycosylphosphatidylinositol (GPI) linkage. Following prion infection, host protease-sensitive prion protein (PrPsen or PrPC) is converted into an abnormal, disease-associated, protease-resistant form (PrPres). Biochemical characteristics, such as the PrP amino acid sequence, and posttranslational modifications, such as glycosylation and GPI anchoring, can affect the transmissibility of prions as well as the biochemical properties of the PrPres generated. Previous in vivo studies on the effects of GPI anchoring on prion infectivity have not examined cross-species transmission. In this study, we tested the effect of lack of GPI anchoring on a species barrier model using mice expressing human PrP. In this model, anchorless 22L prions derived from tg44 mice were more infectious than 22L prions derived from C57BL/10 mice when tested in tg66 transgenic mice, which expressed wild-type anchored human PrP at 8- to 16-fold above normal. Thus, the lack of the GPI anchor on the PrPres from tg44 mice appeared to reduce the effect of the mouse-human PrP species barrier. In contrast, neither source of prions induced disease in tgRM transgenic mice, which expressed human PrP at 2- to 4-fold above normal. IMPORTANCE Prion protein (PrP) is found in all mammals, usually attached to cells by an anchor molecule called GPI. Following prion infection, PrP is converted into a disease-associated form (PrPres). While most prion diseases are species specific, this finding is not consistent, and species barriers differ in strength. The amino acid sequence of PrP varies among species, and this variability affects prion species barriers. However, other PrP modifications, including glycosylation and GPI anchoring, may also influence cross-species infectivity. We studied the effect of PrP GPI anchoring using a mouse-to-human species barrier model. Experiments showed that prions produced by mice expressing only anchorless PrP were more infectious than prions produced in mice expressing anchored PrP. Thus, the lack of the GPI anchor on prions reduced the effect of the mouse-human species barrier. Our results suggest that prion diseases that produce higher levels of anchorless PrP may pose an increased risk for cross-species infection.

Published

2015

27. Prion infection of mouse brain reveals multiple new upregulated genes involved in neuroinflammation or signal transduction

Author

Katie Phillips, Bruce Chesebro, James A. Carroll, Brent Race, and James F. Striebel

Subjects

Genetically modified mouse, Prions, Immunology, Scrapie, Inflammation, Mice, Transgenic, Biology, Microbiology, Virology, Gene expression, medicine, Animals, Gliosis, Neuroinflammation, Gene Expression Profiling, Brain, Neurodegenerative Diseases, Mice, Inbred C57BL, Disease Models, Animal, Insect Science, STAT protein, Female, medicine.symptom, Signal transduction, Signal Transduction

Abstract

Gliosis is often a preclinical pathological finding in neurodegenerative diseases, including prion diseases, but the mechanisms facilitating gliosis and neuronal damage in these diseases are not understood. To expand our knowledge of the neuroinflammatory response in prion diseases, we assessed the expression of key genes and proteins involved in the inflammatory response and signal transduction in mouse brain at various times after scrapie infection. In brains of scrapie-infected mice at pre- and postclinical stages, we identified 15 previously unreported differentially expressed genes related to inflammation or activation of the STAT signal transduction pathway. Levels for the majority of differentially expressed genes increased with time postinfection. In quantitative immunoblotting experiments of STAT proteins, STAT1α, phosphorylated-STAT1α (pSTAT1α), and pSTAT3 were increased between 94 and 131 days postinfection (p.i.) in brains of mice infected with strain 22L. Furthermore, a select group of STAT-associated genes was increased preclinically during scrapie infection, suggesting early activation of the STAT signal transduction pathway. Comparison of inflammatory markers between mice infected with scrapie strains 22L and RML indicated that the inflammatory responses and gene expression profiles in the brains were strikingly similar, even though these scrapie strains infect different brain regions. The endogenous interleukin-1 receptor antagonist (IL-1Ra), an inflammatory marker, was newly identified as increasing preclinically in our model and therefore might influence scrapie pathogenesis in vivo . However, in IL-1Ra-deficient or overexpressor transgenic mice inoculated with scrapie, neither loss nor overexpression of IL-1Ra demonstrated any observable effect on gliosis, protease-resistant prion protein (PrPres) formation, disease tempo, pathology, or expression of the inflammatory genes analyzed. IMPORTANCE Prion infection leads to PrPres deposition, gliosis, and neuroinflammation in the central nervous system before signs of clinical illness. Using a scrapie mouse model of prion disease to assess various time points postinoculation, we identified 15 unreported genes that were increased in the brains of scrapie-infected mice and were associated with inflammation and/or JAK-STAT activation. Comparison of mice infected with two scrapie strains (22L and RML), which have dissimilar neuropathologies, indicated that the inflammatory responses and gene expression profiles in the brains were similar. Genes that increased prior to clinical signs might be involved in controlling scrapie infection or in facilitating damage to host tissues. We tested the possible role of the endogenous IL-1Ra, which was increased at 70 days p.i. In scrapie-infected mice deficient in or overexpressing IL-1Ra, there was no observable effect on gliosis, PrPres formation, disease tempo, pathology, or expression of inflammatory genes analyzed.

Published

2014

28. Distinct patterns of spread of prion infection in brains of mice expressing anchorless or anchored forms of prion protein

Author

Katie Phillips, Bruce Chesebro, James F. Striebel, Nancy Kurtz, Brent Race, and Alejandra Rangel

Subjects

Basement membrane, Pathology, medicine.medical_specialty, Microinjections, PrPSc Proteins, Amyloid, Prions, animal diseases, Glycophosphatidylinositol anchor, Mice, Transgenic, Scrapie, Biology, Prion Diseases, Pathology and Forensic Medicine, Amyloid beta-Protein Precursor, Mice, Cellular and Molecular Neuroscience, Glial Fibrillary Acidic Protein, medicine, Subependymal zone, Transgenic mice, Animals, Humans, Cerebral amyloid angiopathy, Amyloid beta-Peptides, Glial fibrillary acidic protein, Research, Calcium-Binding Proteins, Microfilament Proteins, Brain, Human brain, medicine.disease, nervous system diseases, Mice, Inbred C57BL, Platelet Endothelial Cell Adhesion Molecule-1, Disease Models, Animal, medicine.anatomical_structure, Gene Expression Regulation, Gliosis, Brain interstitial fluid, Prion, biology.protein, Neurology (clinical), medicine.symptom

Abstract

Background In humans and animals, prion protein (PrP) is usually expressed as a glycophosphatidylinositol (GPI)-anchored membrane protein, but anchorless PrP may be pathogenic in humans with certain familial prion diseases. Anchored PrP expressed on neurons mediates spread of prions along axons in the peripheral and central nervous systems. However, the mechanism of prion spread in individuals expressing anchorless PrP is poorly understood. Here we studied prion spread within brain of mice expressing anchorless or anchored PrP. Results To create a localized initial point of infection, we microinjected scrapie in a 0.5 microliter volume in the striatum. In this experiment, PrPres and gliosis were first detected in both types of mice at 40 days post-inoculation near the needle track. In mice with anchored PrP, PrPres appeared to spread via neurons to distant connected brain areas by the clinical endpoint at 150 days post-inoculation. This PrPres was rarely associated with blood vessels. In contrast, in mice with anchorless PrP, PrPres spread did not follow neuronal circuitry, but instead followed a novel slower pattern utilizing the drainage system of the brain interstitial fluid (ISF) including perivascular areas adjacent to blood vessels, subependymal areas and spaces between axons in white matter tracts. Conclusions In transgenic mice expressing anchorless PrP small amyloid-seeding PrPres aggregates appeared to be transported in the ISF, thus spreading development of cerebral amyloid angiopathy (CAA) throughout the brain. Spread of amyloid seeding by ISF may also occur in multiple human brain diseases involving CAA.

Published

2014

29. Prion protein and susceptibility to kainate-induced seizures: genetic pitfalls in the use of PrP knockout mice

Author

Bruce Chesebro, Brent Race, and James F. Striebel

Subjects

kainate, Prions, Transgene, animal diseases, Gene Expression, Mice, Transgenic, Biology, Biochemistry, Article, PRNP, Mice, Cellular and Molecular Neuroscience, Species Specificity, Seizures, mental disorders, Genotype, Gene expression, Prnp knockout, Animals, flanking genes, Genetic Predisposition to Disease, Gene, Genetics, Neurons, Kainic Acid, Extra View, Cell Biology, Phenotype, Molecular biology, nervous system diseases, Complementation, Infectious Diseases, Knockout mouse, Prnp deletion

Abstract

Prion protein (PrP) is a glycosylphosphatidylinositol (GPI) anchored cell surface protein expressed by many cells, including those of the mammalian nervous system. At present the physiologic functions of PrP remain unclear. Deletion of Prnp, the gene encoding PrP in mice, has been shown to alter normal synaptic and electrophysiologic activities, indicating a potential role in seizure susceptibility. However, published efforts to link PrP with seizures, using both in vivo and in vitro models, are conflicting and difficult to interpret due to use of various mouse backgrounds and seizure induction techniques. Here we investigated the role of PrP in kainic acid (KA)-induced seizure sensitivity, using three types of mice. In contrast to previous published results, Prnp-/- mice on the C57BL/10SnJ background had a significant decrease in KA-induced seizure susceptibility. In genetic complementation experiments using a PrP-expressing transgene, genes derived from strain 129/Ola, which flanked the Prnp-/- locus in C57BL/10SnJ mice, rather than Prnp itself, appeared to account for this effect. Furthermore, using coisogenic 129/Ola mice differing only at Prnp, this difference was not reproduced when comparing PrP-negative and PrP-positive mice. In contrast, substrains of PrP-expressing C57BL mice, showed large variations in KA-induced seizure sensitivity. The magnitude of these differences in susceptibility was larger than that associated with the presence of the Prnp gene, suggesting extensive influence of genes other than Prnp on seizure sensitivity in this system.

Published

2013

30. Prion Strain Differences in Accumulation of PrPSc on Neurons and Glia Are Associated with Similar Expression Profiles of Neuroinflammatory Genes: Comparison of Three Prion Strains

Author

Karin E. Peterson, Bruce Chesebro, James A. Carroll, Katie Phillips, Brent Race, James F. Striebel, Alejandra Rangel, and Tyson A. Woods

Subjects

0301 basic medicine, Neuropil, PrPSc Proteins, Physiology, Scrapie, Animal Diseases, Prion Diseases, Pathogenesis, Mice, Thalamus, Animal Cells, Zoonoses, Immune Physiology, Medicine and Health Sciences, lcsh:QH301-705.5, Neurons, Innate Immune System, Microglia, Reverse Transcriptase Polymerase Chain Reaction, Chemotaxis, Brain, Immunohistochemistry, Animal Prion Diseases, Cell Motility, Infectious Diseases, medicine.anatomical_structure, Cytokines, Neuroglia, Chemokines, Anatomy, Cellular Types, Research Article, lcsh:Immunologic diseases. Allergy, Immunoblotting, Immunology, Glial Cells, Substantia nigra, Biology, Microbiology, 03 medical and health sciences, Virology, Genetics, medicine, Animals, Microglial Cells, Molecular Biology, Neuroinflammation, Interleukins, Biology and Life Sciences, Cell Biology, Molecular Development, Molecular biology, Mice, Inbred C57BL, 030104 developmental biology, lcsh:Biology (General), nervous system, Cellular Neuroscience, Immune System, Parasitology, lcsh:RC581-607, Zoology, Neuroscience, Developmental Biology

Abstract

Misfolding and aggregation of host proteins are important features of the pathogenesis of neurodegenerative diseases including Alzheimer’s disease, Parkinson’s disease, frontotemporal dementia and prion diseases. In all these diseases, the misfolded protein increases in amount by a mechanism involving seeded polymerization. In prion diseases, host prion protein is misfolded to form a pathogenic protease-resistant form, PrPSc, which accumulates in neurons, astroglia and microglia in the CNS. Here using dual-staining immunohistochemistry, we compared the cell specificity of PrPSc accumulation at early preclinical times post-infection using three mouse scrapie strains that differ in brain regional pathology. PrPSc from each strain had a different pattern of cell specificity. Strain 22L was mainly associated with astroglia, whereas strain ME7 was mainly associated with neurons and neuropil. In thalamus and cortex, strain RML was similar to 22L, but in substantia nigra, RML was similar to ME7. Expression of 90 genes involved in neuroinflammation was studied quantitatively using mRNA from thalamus at preclinical times. Surprisingly, despite the cellular differences in PrPSc accumulation, the pattern of upregulated genes was similar for all three strains, and the small differences observed correlated with variations in the early disease tempo. Gene upregulation correlated with activation of both astroglia and microglia detected in early disease prior to vacuolar pathology or clinical signs. Interestingly, the profile of upregulated genes in scrapie differed markedly from that seen in two acute viral CNS diseases (LaCrosse virus and BE polytropic Friend retrovirus) that had reactive gliosis at levels similar to our prion-infected mice., Author Summary Accumulation of aggregates of misfolded protein in brain is a common feature of the damage seen in several neurodegenerative diseases including prion disease, Alzheimer’s disease and Parkinson’s disease. In the present work three strains of prion disease differed in accumulation of the disease-associated prion protein (PrPSc) on neurons and astroglial cells. These patterns were first detectable in the thalamus at 40–60 days after inoculation. This coincided with initial detection of gliosis and PrPSc deposition, but was far in advance of clinical signs or spongiform pathology. In spite of the different patterns of cellular PrPSc deposition, these three strains had similar patterns of expression of a large number of genes known to be active during neuroinflammatory responses and gliosis. However, the gene upregulation in scrapie differed markedly from that seen in two neurovirulent viral diseases, which also had abundant glial responses similar to those observed with prion infection.

Published

2016

31. Strain specific resistance to murine scrapie associated with a naturally occurring human prion protein polymorphism at residue 171

Author

Rachel LaCasse, James F. Striebel, Kimberly Meade-White, Bruce Chesebro, and Brent Race

Subjects

Genetically modified mouse, lcsh:Immunologic diseases. Allergy, Protein Folding, Mouse, Prions, animal diseases, Immunology, Mice, Transgenic, Scrapie, Neuropathology, Biology, Polymorphism, Single Nucleotide, Microbiology, Prion Diseases, Transgenic Model, Mice, Model Organisms, Species Specificity, In vivo, Virology, Neurobiology of Disease and Regeneration, Genetics, Animals, Humans, Molecular Biology, lcsh:QH301-705.5, Human Genetics, Neurodegenerative Diseases, Animal Models, In vitro, nervous system diseases, Infectious Diseases, Neurology, lcsh:Biology (General), Medicine, Protein Misfolding Cyclic Amplification, Parasitology, Protein folding, lcsh:RC581-607, Research Article, Neuroscience

Abstract

Transmissible spongiform encephalopathies (TSE) or prion diseases are neurodegenerative disorders associated with conversion of normal host prion protein (PrP) to a misfolded, protease-resistant form (PrPres). Genetic variations of prion protein in humans and animals can alter susceptibility to both familial and infectious prion diseases. The N171S PrP polymorphism is found mainly in humans of African descent, but its low incidence has precluded study of its possible influence on prion disease. Similar to previous experiments of others, for laboratory studies we created a transgenic model expressing the mouse PrP homolog, PrP-170S, of human PrP-171S. Since PrP polymorphisms can vary in their effects on different TSE diseases, we tested these mice with four different strains of mouse-adapted scrapie. Whereas 22L and ME7 scrapie strains induced typical clinical disease, neuropathology and accumulation of PrPres in all transgenic mice at 99-128 average days post-inoculation, strains RML and 79A produced clinical disease and PrPres formation in only a small subset of mice at very late times. When mice expressing both PrP-170S and PrP-170N were inoculated with RML scrapie, dominant-negative inhibition of disease did not occur, possibly because interaction of strain RML with PrP-170S was minimal. Surprisingly, in vitro PrP conversion using protein misfolding cyclic amplification (PMCA), did not reproduce the in vivo findings, suggesting that the resistance noted in live mice might be due to factors or conditions not present in vitro. These findings suggest that in vivo conversion of PrP-170S by RML and 79A scrapie strains was slow and inefficient. PrP-170S mice may be an example of the conformational selection model where the structure of some prion strains does not favor interactions with PrP molecules expressing certain polymorphisms., Author Summary Transmissible spongiform encephalopathies (TSE) or prion diseases are infectious fatal neurological diseases that affect many mammals, including humans. In these diseases a misfolded form of host prion protein (PrP) leads to brain degeneration and death. The genetic code of PrP in individual animals or humans has minor variations, which in some cases are associated with altered susceptibility to disease. In humans a variation at residue 171 (N171S) has been found in people mainly of African descent. However, due to the low incidence of the variation and difficult accessibility of these individuals, studies of prion diseases in these populations have not been carried out. Therefore, to create a laboratory animal model to study the effect of this variation on prion diseases, we generated transgenic mice expressing the mouse version of the human PrP variation at residue 171. We then studied the susceptibility of these mice to 4 strains of mouse-adapted scrapie. In our experiments these transgenic mice were uniquely resistant to two scrapie strains, but showed high sensitivity to two others. This resistance appeared to be related to a slow or inefficient generation of the aggregated disease-associated form of PrP in these mice, and was not duplicated using in vitro assays. In summary, transgenic mice expressing this variant PrP provide an interesting model to study differences among prion strains and their interactions with PrP in vivo.

Published

2011

32. Analysis of Protein Levels of 24 Cytokines in Scrapie Agent-Infected Brain and Glial Cell Cultures from Mice Differing in Prion Protein Expression Levels ▿

Author

Bruce Chesebro, James F. Striebel, Karin E. Peterson, and Déborah Tribouillard-Tanvier

Subjects

PrPSc Proteins, Prions, medicine.medical_treatment, Immunology, CCL3, Scrapie, Mice, Transgenic, Biology, Microbiology, CCL5, Mice, Virology, medicine, CXCL10, Animals, Humans, RNA, Messenger, Cells, Cultured, Microglia, Brain, CXCL1, Mice, Inbred C57BL, medicine.anatomical_structure, Cytokine, nervous system, Insect Science, Neuroglia, Pathogenesis and Immunity, Cytokines

Abstract

Activation of microglia and astroglia is seen in many neurodegenerative diseases including prion diseases. Activated glial cells produce cytokines as a protective response against certain pathogens and as part of the host inflammatory response to brain damage. In addition, cytokines might also exacerbate tissue damage initiated by other processes. In the present work using multiplex assays to analyze protein levels of 24 cytokines in scrapie agent-infected C57BL/10 mouse brains, we observed elevation of CCL2, CCL5, CXCL1, CXCL10, granulocyte-macrophage colony-stimulating factor (GM-CSF), gamma interferon (IFN-γ), interleukin 1α (IL-1α), IL-1β, IL-6, and IL-12p40. Scrapie agent-infected wild-type mice and transgenic mice expressing anchorless prion protein (PrP) had similar cytokine responses in spite of extensive differences in neuropathology. Therefore, these responses may be primarily a reaction to brain damage induced by prion infection rather than specific inducers of a particular type of pathology. To study the roles of astroglia and microglia in these cytokine responses, primary glial cultures were exposed to scrapie agent-infected brain homogenates. Microglia produced only IL-12p40 and CXCL10, whereas astroglia produced these cytokines plus CCL2, CCL3, CCL5, CXCL1, G-CSF, IL-1β, IL-6, IL-12p70, and IL-13. Glial cytokine responses from wild-type mice and transgenic mice expressing anchorless PrP differed only slightly, but glia from PrP-null mice produced only IL-12p40, indicating that PrP expression was required for scrapie agent induction of other cytokines detected. The difference in cytokine response between microglia and astroglia correlated with 20-fold-higher levels of PrP expression in astroglia versus microglia, suggesting that high-level PrP expression on astroglia might be important for induction of certain cytokines.

Published

2009

33. Role of Erk1/2 Activation in Prion Disease Pathogenesis: Absence of CCR1 Leads to Increased Erk1/2 Activation and Accelerated Disease Progression

Author

Lisa Kercher, James F. Striebel, Bruce Chesebro, Rachel A. LaCasse, and Cynthia Favara

Subjects

CCR1, PrPSc Proteins, Receptors, CCR5, Immunology, Receptors, CCR1, Scrapie, Biology, Article, Prion Diseases, Pathogenesis, Mice, Downregulation and upregulation, Glial Fibrillary Acidic Protein, medicine, Immunology and Allergy, Animals, Mice, Knockout, Mitogen-Activated Protein Kinase 3, Neurodegeneration, Calcium-Binding Proteins, Microfilament Proteins, Brain, medicine.disease, Enzyme Activation, Mice, Inbred C57BL, Disease Models, Animal, Neurology, Gliosis, Gene Expression Regulation, Knockout mouse, Disease Progression, Cytokines, Neurology (clinical), medicine.symptom

Abstract

Prion diseases are neurodegenerative infections with gliosis and vacuolation. The mechanisms of degeneration remain unclear, but chemokines may be important. In current experiments CCR1 knock-out (KO) mice succumbed more rapidly to scrapie infection than WT controls. Infected KO mice had upregulation of CCL3, a CCR1 ligand, and CCR5, a receptor with specificity for CCL3. Both infected KO and WT mice had upregulation of CCR5-mediated signaling involving activation of Erk1/2 in astrocytes; however, activation was earlier in KO mice suggesting a role in pathogenesis. In both mouse strains activation of the Erk1/2 pathway may lead to astrocyte dysfunction resulting in neurodegeneration.

Published

2008

34. Fatal Transmissible Amyloid Encephalopathy: A New Type of Prion Disease Associated with Lack of Prion Protein Membrane Anchoring

Author

David W. Dorward, Rachel LaCasse, Martin Jeffrey, Gillian McGovern, Richard E. Race, Bruce Chesebro, Brent Race, Mikael Klingeborn, James F. Striebel, and Kimberly Meade-White

Subjects

lcsh:Immunologic diseases. Allergy, Genetically modified mouse, Protein Folding, Amyloid, Prions, Immunology, Encephalopathy, Mice, Transgenic, Scrapie, Neuropathology, Biology, Microbiology, Basement Membrane, Prion Diseases, Mice, Infectious Diseases/Prion Diseases, Cerebellum, Virology, Neurites, Genetics, medicine, Animals, Brain Tissue Transplantation, Microscopy, Immunoelectron, lcsh:QH301-705.5, Molecular Biology, Cerebral Cortex, Neurons, Amyloidosis, Cell Membrane, medicine.disease, nervous system diseases, Mice, Inbred C57BL, Neurological Disorders/Prion Diseases, lcsh:Biology (General), Pathology/Neuropathology, Parasitology, Cerebral amyloid angiopathy, lcsh:RC581-607, Neuroglia, Research Article, Spongiosis

Abstract

Prion diseases are fatal neurodegenerative diseases of humans and animals characterized by gray matter spongiosis and accumulation of aggregated, misfolded, protease-resistant prion protein (PrPres). PrPres can be deposited in brain in an amyloid-form and/or non-amyloid form, and is derived from host-encoded protease-sensitive PrP (PrPsen), a protein normally anchored to the plasma membrane by glycosylphosphatidylinositol (GPI). Previously, using heterozygous transgenic mice expressing only anchorless PrP, we found that PrP anchoring to the cell membrane was required for typical clinical scrapie. However, in the present experiments, using homozygous transgenic mice expressing two-fold more anchorless PrP, scrapie infection induced a new fatal disease with unique clinical signs and altered neuropathology, compared to non-transgenic mice expressing only anchored PrP. Brain tissue of transgenic mice had high amounts of infectivity, and histopathology showed dense amyloid PrPres plaque deposits without gray matter spongiosis. In contrast, infected non-transgenic mice had diffuse non-amyloid PrPres deposits with significant gray matter spongiosis. Brain graft studies suggested that anchored PrPsen expression was required for gray matter spongiosis during prion infection. Furthermore, electron and light microscopic studies in infected transgenic mice demonstrated several pathogenic processes not seen in typical prion disease, including cerebral amyloid angiopathy and ultrastructural alterations in perivascular neuropil. These findings were similar to certain human familial prion diseases as well as to non-prion human neurodegenerative diseases, such as Alzheimer's disease., Author Summary Prion diseases, also known as transmissible spongiform encephalopathies, are infectious fatal neurodegenerative diseases of humans and animals. A major feature of prion diseases is the refolding and aggregation of a normal host protein, prion protein (PrP), into a disease-associated form which may contribute to brain damage. In uninfected individuals, normal PrP is anchored to the outer cell membrane by a sugar-phosphate-lipid linker molecule. In the present report we show that prion infection of mice expressing PrP lacking the anchor can result in a new type of fatal neurodegenerative disease. This disease displays mechanisms of damage to brain cells and brain blood vessels found in Alzheimer's disease and in familial amyloid brain diseases. In contrast, the typical sponge-like brain damage seen in prion diseases was not observed. These results suggest that presence or absence of PrP membrane anchoring can influence the type of neurodegeneration seen after prion infection.

Published

2010

35. Unusual cerebral vascular prion protein amyloid distribution in scrapie-infected transgenic mice expressing anchorless prion protein

Author

Mikael Klingeborn, Alejandra Rangel, Bruce Chesebro, James F. Striebel, and Brent Race

Subjects

Male, Genetically modified mouse, Basement membrane, Amyloid, Pathology, medicine.medical_specialty, PrPSc Proteins, Ovalbumin, Glycophosphatidylinositol anchor, Fluorescent Antibody Technique, Mice, Transgenic, Scrapie, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, Interstitial fluid, Animals, Medicine, Cerebral amyloid angiopathy, biology, business.industry, Research, Brain, Extracellular Fluid, Cerebral Arteries, medicine.disease, Cerebral Veins, Immunohistochemistry, Actins, Capillaries, Mice, Inbred C57BL, medicine.anatomical_structure, Brain interstitial fluid, Prion, biology.protein, Neurology (clinical), business, Blood vessel

Abstract

Background In some prion diseases, misfolded aggregated protease-resistant prion protein (PrPres) is found in brain as amyloid, which can cause cerebral amyloid angiopathy. Small diffusible precursors of PrPres amyloid might flow with brain interstitial fluid (ISF), possibly accounting for the perivascular and intravascular distribution of PrPres amyloid. We previously reported that PrPres amyloid in scrapie-infected transgenic mice appeared to delay clearance of microinjected brain ISF tracer molecules. Results Here we studied distribution of PrPres amyloid on capillaries, arteries and veins to test whether vascular specificity of PrPres corresponded to distribution of ISF tracer molecules. To distinguish PrPres-positive arteries from veins and capillaries, scrapie-infected mouse brains were studied by immunodetection of alpha smooth muscle actin. ISF was studied using fluorescein-labeled ovalbumin microinjected into brain as a tracer. In infected preclinical or clinical mice, PrPres was found mostly on capillaries (73-78%). Lower levels were found on arteries (11-14%) and veins (11-13%). Compared to PrPres, ISF tracer was found at higher levels on capillaries (96-97%), and the remaining tracer was found at a skewed ratio of 4 to 1 on arteries and veins respectively. Conclusions PrPres association with blood vessels suggested that ISF flow might transport diffusible PrPres precursor molecules to perivascular sites. However, the different vascular specificity of PrPres and ISF tracer indicated that ISF flow did not alone control PrPres dissemination. Possibly blood vessel basement membrane (BM) components, such as glucosaminoglycans, might concentrate small PrPres aggregates and serve as scaffolds for PrP conversion on multiple vessel types.

36. Strain specific resistance to murine scrapie associated with a naturally occurring human prion protein polymorphism at residue 171.

Author

James F Striebel, Brent Race, Kimberly D Meade-White, Rachel LaCasse, and Bruce Chesebro

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Transmissible spongiform encephalopathies (TSE) or prion diseases are neurodegenerative disorders associated with conversion of normal host prion protein (PrP) to a misfolded, protease-resistant form (PrPres). Genetic variations of prion protein in humans and animals can alter susceptibility to both familial and infectious prion diseases. The N171S PrP polymorphism is found mainly in humans of African descent, but its low incidence has precluded study of its possible influence on prion disease. Similar to previous experiments of others, for laboratory studies we created a transgenic model expressing the mouse PrP homolog, PrP-170S, of human PrP-171S. Since PrP polymorphisms can vary in their effects on different TSE diseases, we tested these mice with four different strains of mouse-adapted scrapie. Whereas 22L and ME7 scrapie strains induced typical clinical disease, neuropathology and accumulation of PrPres in all transgenic mice at 99-128 average days post-inoculation, strains RML and 79A produced clinical disease and PrPres formation in only a small subset of mice at very late times. When mice expressing both PrP-170S and PrP-170N were inoculated with RML scrapie, dominant-negative inhibition of disease did not occur, possibly because interaction of strain RML with PrP-170S was minimal. Surprisingly, in vitro PrP conversion using protein misfolding cyclic amplification (PMCA), did not reproduce the in vivo findings, suggesting that the resistance noted in live mice might be due to factors or conditions not present in vitro. These findings suggest that in vivo conversion of PrP-170S by RML and 79A scrapie strains was slow and inefficient. PrP-170S mice may be an example of the conformational selection model where the structure of some prion strains does not favor interactions with PrP molecules expressing certain polymorphisms.

Published

2011