Your search keyword '"Brent Race"' showing total 40 results

1. Nature Communications

Author

Li Cui, Pierluigi Gambetti, Byron Caughey, Manuel V. Camacho, Xiaoping Dong, Alise Adornato, Gregory J. Raymond, Nicholas R. Maurer, Baiya Li, Jue Yuan, Brian S. Appleby, Johnny Dang, Aaron Foutz, Zerui Wang, Bin Xu, Katie Williams, Witold K. Surewicz, Brent Race, Yue Lang, Wen-Quan Zou, Christina D. Orrú, Matteo Manca, Qingzhong Kong, Pingping Shen, Robert B. Petersen, and Biochemistry

Subjects

0301 basic medicine, Genetically modified mouse, PrPSc Proteins, Science, Transgene, animal diseases, General Physics and Astronomy, Mice, Transgenic, 02 engineering and technology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Mice, Medicine, Animals, Humans, lcsh:Science, Skin, Multidisciplinary, biology, medicine.diagnostic_test, Mesocricetus, business.industry, Brain biopsy, Antibodies, Monoclonal, Brain, General Chemistry, 021001 nanoscience & nanotechnology, biology.organism_classification, Virology, Publisher Correction, nervous system diseases, Intracerebral inoculation, Disease Models, Animal, 030104 developmental biology, biology.protein, Protein Misfolding Cyclic Amplification, Biomarker (medicine), Feasibility Studies, Biological Assay, Female, lcsh:Q, Antibody, 0210 nano-technology, business, Biomarkers, Scrapie

Abstract

A definitive pre-mortem diagnosis of prion disease depends on brain biopsy for prion detection currently and no validated alternative preclinical diagnostic tests have been reported to date. To determine the feasibility of using skin for preclinical diagnosis, here we report ultrasensitive serial protein misfolding cyclic amplification (sPMCA) and real-time quaking-induced conversion (RT-QuIC) assays of skin samples from hamsters and humanized transgenic mice (Tg40h) at different time points after intracerebral inoculation with 263K and sCJDMM1 prions, respectively. sPMCA detects skin PrPSc as early as 2 weeks post inoculation (wpi) in hamsters and 4 wpi in Tg40h mice; RT-QuIC assay reveals earliest skin prion-seeding activity at 3 wpi in hamsters and 20 wpi in Tg40h mice. Unlike 263K-inoculated animals, mock-inoculated animals show detectable skin/brain PrPSc only after long cohabitation periods with scrapie-infected animals. Our study provides the proof-of-concept evidence that skin prions could be a biomarker for preclinical diagnosis of prion disease. CJD Foundation National Institutes of Health (NIH) [NS062787, NS087588, NS109532, NS088604] Intramural Research Program of the NIAID, NIH Centers for Disease Control and Prevention [UR8/CCU515004] National Natural Science Foundation of China [81671186] We thank Miriam Warren and Diane Kofskey for skillful histologic and immunohistochemical preparations. We thank Andrew Hughson (RML) for providing recombinant hamster prion protein. Supported by the CJD Foundation and the National Institutes of Health (NIH) NS062787 and NS087588 to W.-Q.Z., NS062787 and NS109532 to W.-Q.Z., and Q.K., NS088604 to Q.K., the Intramural Research Program of the NIAID, NIH to B.C., the Centers for Disease Control and Prevention Contract UR8/CCU515004 to B.S.A. as well as the National Natural Science Foundation of China (No. 81671186) to L.C.

Published

2019

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

Author

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

Subjects

0301 basic medicine, Prions, animal diseases, Dynein, Central nervous system, Kinesins, Scrapie, Striatum, Biology, kinesin, Microbiology, Article, Prion Diseases, prion, Mice, 03 medical and health sciences, 0302 clinical medicine, Virology, medicine, Animals, KIF5C, Mice, Knockout, PrP, scrapie, PrPC, Brain, QR1-502, nervous system diseases, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, nervous system, Axoplasmic transport, Kinesin, Immunohistochemistry, Female, 030217 neurology & neurosurgery, Intracellular, PrPSc

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

3. 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

4. Sporadic Creutzfeldt-Jakob disease prion infection of human cerebral organoids

Author

Cathryn L. Haigh, Simote T. Foliaki, Gianluigi Zanusso, Bradley R. Groveman, Brent Race, James A. Carroll, and Christina D. Orrú

Subjects

0301 basic medicine, medicine.medical_specialty, Neurology, animal diseases, Disease, Biology, lcsh:RC346-429, Pathology and Forensic Medicine, Pathogenesis, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Prion infection, Human cerebral organoid, medicine, Organoid, Induced pluripotent stem cell, lcsh:Neurology. Diseases of the nervous system, CJD, Induced pluripotent stem cells, Prion, RT-QuIC, Research, Neurodegeneration, medicine.disease, Virology, nervous system diseases, 030104 developmental biology, Immunohistochemistry, Neurology (clinical), 030217 neurology & neurosurgery

Abstract

For the transmissible, neurogenerative family of prion diseases, few human models of infection exist and none represent structured neuronal tissue. Human cerebral organoids are self-organizing, three-dimensional brain tissues that can be grown from induced pluripotent stem cells. Organoids can model aspects of neurodegeneration in Alzheimer’s Disease and Down’s Syndrome, reproducing tau hyperphosphorylation and amyloid plaque pathology. To determine whether organoids could be used to reproduce human prion infection and pathogenesis, we inoculated organoids with two sporadic Creutzfeldt-Jakob Disease prion subtypes. Organoids showed uptake, followed by clearance, of the infectious inoculum. Subsequent re-emergence of prion self-seeding activity indicated de novo propagation. Organoid health assays, prion titer, prion protein electrophoretic mobility and immunohistochemistry demonstrated inoculum-specific differences. Our study shows, for the first time, that cerebral organoids can model aspects of human prion disease and thus offer a powerful system for investigating different human prion subtype pathologies and testing putative therapeutics. Electronic supplementary material The online version of this article (10.1186/s40478-019-0742-2) contains supplementary material, which is available to authorized users.

Published

2019

5. Transmission studies of chronic wasting disease to transgenic mice overexpressing human prion protein using the RT-QuIC assay

Author

Bruce Chesebro, Brent Race, and Katie Williams

Subjects

0301 basic medicine, Genetically modified mouse, 040301 veterinary sciences, [SDV]Life Sciences [q-bio], animal diseases, Transgene, Immunoblotting, Mice, Transgenic, Disease, Biology, Prion Proteins, 0403 veterinary science, Mice, 03 medical and health sciences, medicine, Animals, Humans, Wasting Syndrome, lcsh:Veterinary medicine, General Veterinary, Transmission (medicine), Inoculation, Deer, Brain, 04 agricultural and veterinary sciences, Chronic wasting disease, medicine.disease, Immunohistochemistry, Virology, 3. Good health, Disease Models, Animal, 030104 developmental biology, Wasting Disease, Chronic, lcsh:SF600-1100, Research Article

Abstract

Chronic wasting disease (CWD) is a fatal prion disease which infects deer, elk and moose. CWD was first described as a wasting syndrome in captive deer in Colorado and Wyoming wildlife facilities from 1967 to 1979. Currently, CWD has been reported in 26 states of the USA, three Canadian provinces, South Korea, Norway and Finland. Since human consumption of cervids is common, it is critical to determine if CWD can infect humans. Published research, including epidemiologic studies and transmission studies using animal models, including transgenic mice that express human prion protein, have suggested existence of a strong species barrier between cervid CWD and humans. In the current study, we tested CWD transmission into two additional strains of transgenic mice (tg66 and tgRM). These mice over-express human prion protein at high levels and are highly sensitive to infection by human-tropic prions. One hundred and eight mice were inoculated intracerebrally with three different sources of CWD. After long periods of observation, brain tissues from CWD-inoculated mice were screened for evidence of prion infection by RT-QuIC, immunohistochemistry (IHC) and immunoblot. No IHC or immunoblot evidence was found to suggest transmission had occurred, and most mice were negative by RT-QuIC assay. However, four mice with inconsistent positive RT-QuIC reactions were detected. The seeding activity detected in these mice may represent a low level of CWD agent, suggesting a possible transfer of CWD infection. Alternatively, these results might be due to false positive reactions or residual CWD inoculum. Electronic supplementary material The online version of this article (10.1186/s13567-019-0626-2) contains supplementary material, which is available to authorized users.

Published

2019

6. Inactivation of chronic wasting disease prions using sodium hypochlorite

Author

Katie Williams, Andrew G. Hughson, Bruce Chesebro, and Brent Race

Subjects

0301 basic medicine, Bleach, Sodium Hypochlorite, Disinfectant, animal diseases, Scrapie, Biochemistry, Animal Diseases, Prion Diseases, chemistry.chemical_compound, Zoonoses, Medicine and Health Sciences, Decontamination, Mammals, Multidisciplinary, Hypochlorites, Zoonosis, Eukaryota, Brain, Ruminants, Animal Prion Diseases, Chemistry, Infectious Diseases, Sodium hypochlorite, Vertebrates, Physical Sciences, Engineering and Technology, Wasting Disease, Chronic, Medicine, Research Article, Prions, Bovine spongiform encephalopathy, Science, Equines, 030106 microbiology, Equipment, Mules, Biology, 03 medical and health sciences, medicine, Animals, Humans, Deer, Organisms, Chemical Compounds, Biology and Life Sciences, Proteins, Chronic wasting disease, medicine.disease, Virology, 030104 developmental biology, chemistry, Human exposure, Amniotes, Salts, Zoology, Chronic Wasting Disease

Abstract

Chronic wasting disease (CWD) is a fatal prion disease that can infect deer, elk and moose. CWD has now been detected in 26 states of the USA, 3 Canadian provinces, South Korea, Norway, Sweden and Finland. CWD continues to spread from endemic areas, and new foci of infections are frequently detected. As increasing numbers of cervids become infected, the likelihood for human exposure increases. To date, no cases of CWD infection in humans have been confirmed, but experience with the BSE zoonosis in the United Kingdom suggests exposure to CWD should be minimized. Specifically, hunters, meat processors and others in contact with tissues from potentially CWD-infected cervids need a practical method to decontaminate knives, saws and other equipment. Prions are notoriously difficult to inactivate, and most effective methods require chemicals or sterilization processes that are either dangerous, caustic, expensive or not readily available. Although corrosive, sodium hypochlorite (bleach) is widely available and affordable and has been shown to inactivate prion agents including those that cause scrapie, bovine spongiform encephalopathy and Creutzfeldt-Jakob disease. In the current study, we confirm that bleach is an effective disinfectant for CWD prions and establish minimum times and bleach concentrations to eliminate prion seeding activity from stainless steel and infected brain homogenate solutions. We found that a five-minute treatment with a 40% dilution of household bleach was effective at inactivating CWD seeding activity from stainless-steel wires and CWD-infected brain homogenates. However, bleach was not able to inactivate CWD seeding activity from solid tissues in our studies.

Published

2019

7. Interferon Alpha Subtype-Specific Suppression of HIV-1 Infection In Vivo

Author

Ali Gawanbacht, Eric J. Lee, Jacob Piehler, Jens Verheyen, Janis A. Müller, Brent Race, Mario L. Santiago, Sandra Francois, Cara C. Wilson, Kim J. Hasenkrug, Ronald J. Messer, Karin E. Peterson, Michael S. Harper, Kejun Guo, Katie Phillips, Jan Münch, Hartmut Hengel, Ulf Dittmer, Kathrin Gibbert, Erik Van Dis, Tyson A. Woods, Mirko Trilling, and Kerry J. Lavender

Subjects

Myxovirus Resistance Proteins, 0301 basic medicine, Combination therapy, Immunology, Medizin, Antiviral protein, Alpha interferon, HIV Infections, Mice, Transgenic, Viremia, APOBEC-3G Deaminase, CD8-Positive T-Lymphocytes, Biology, GPI-Linked Proteins, Lymphocyte Activation, Virus Replication, Antiviral Agents, Microbiology, Virus, Mice, 03 medical and health sciences, Immune system, Antigens, CD, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, Interferon-alpha, virus diseases, Viral Load, medicine.disease, Immunity, Innate, Killer Cells, Natural, 030104 developmental biology, Viral replication, Insect Science, Disease Progression, HIV-1, Viral load

Abstract

Although all 12 subtypes of human interferon alpha (IFN-α) bind the same receptor, recent results have demonstrated that they elicit unique host responses and display distinct efficacies in the control of different viral infections. The IFN-α2 subtype is currently in HIV-1 clinical trials, but it has not consistently reduced viral loads in HIV-1 patients and is not the most effective subtype against HIV-1 in vitro . We now demonstrate in humanized mice that, when delivered at the same high clinical dose, the human IFN-α14 subtype has very potent anti-HIV-1 activity whereas IFN-α2 does not. In both postexposure prophylaxis and treatment of acute infections, IFN-α14, but not IFN-α2, significantly suppressed HIV-1 replication and proviral loads. Furthermore, HIV-1-induced immune hyperactivation, which is a prognosticator of disease progression, was reduced by IFN-α14 but not IFN-α2. Whereas ineffective IFN-α2 therapy was associated with CD8 + T cell activation, successful IFN-α14 therapy was associated with increased intrinsic and innate immunity, including significantly higher induction of tetherin and MX2, increased APOBEC3G signature mutations in HIV-1 proviral DNA, and higher frequencies of TRAIL + NK cells. These results identify IFN-α14 as a potent new therapeutic that operates via mechanisms distinct from those of antiretroviral drugs. The ability of IFN-α14 to reduce both viremia and proviral loads in vivo suggests that it has strong potential as a component of a cure strategy for HIV-1 infections. The broad implication of these results is that the antiviral efficacy of each individual IFN-α subtype should be evaluated against the specific virus being treated. IMPORTANCE The naturally occurring antiviral protein IFN-α2 is used to treat hepatitis viruses but has proven rather ineffective against HIV in comparison to triple therapy with the antiretroviral (ARV) drugs. Although ARVs suppress the replication of HIV, they fail to completely clear infections. Since IFN-α acts by different mechanism than ARVs and has been shown to reduce HIV proviral loads, clinical trials are under way to test whether IFN-α2 combined with ARVs might eradicate HIV-1 infections. IFN-α is actually a family of 12 distinct proteins, and each IFN-α subtype has different efficacies toward different viruses. Here, we use mice that contain a human immune system, so they can be infected with HIV. With this model, we demonstrate that while IFN-α2 is only weakly effective against HIV, IFN-α14 is extremely potent. This discovery identifies IFN-α14 as a more powerful IFN-α subtype for use in combination therapy trials aimed toward an HIV cure.

Published

2016

8. 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

9. Familial human prion diseases associated with prion protein mutations Y226X and G131V are transmissible to transgenic mice expressing human prion protein

Author

Katie Williams, Annemieke J. M. Rozemuller, Andrew G. Hughson, Casper Jansen, Piero Parchi, Bruce Chesebro, Brent Race, Pathology, Amsterdam Neuroscience - Neurodegeneration, Race, Brent, Williams, Katie, Hughson, Andrew G., Jansen, Casper, Parchi, Piero, Rozemuller, Annemieke J. M., and Chesebro, Bruce

Subjects

0301 basic medicine, Genetically modified mouse, Prion disease, truncating PRNP mutation, prion protein, animal models, brain pathology, prion transmission, amyloid proteins, Amyloid, Transgene, animal diseases, Mutant, Mice, Transgenic, Biology, medicine.disease_cause, lcsh:RC346-429, Prion Proteins, Pathology and Forensic Medicine, Prion Diseases, 03 medical and health sciences, Cellular and Molecular Neuroscience, Mice, 0302 clinical medicine, Glial Fibrillary Acidic Protein, medicine, Animals, Humans, lcsh:Neurology. Diseases of the nervous system, Mutation, Glial fibrillary acidic protein, Research, Brain, Human brain, Virology, nervous system diseases, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Mutant Proteins, Neurology (clinical), 030217 neurology & neurosurgery, Immunostaining

Abstract

Human familial prion diseases are associated with mutations at 34 different prion protein (PrP) amino acid residues. However, it is unclear whether infectious prions are found in all cases. Mutant PrP itself may be neurotoxic, or alternatively, PrP mutation might predispose to spontaneous formation of infectious PrP isoforms. Previous reports demonstrated transmission to animal models by human brain tissue expressing 7 different PrP mutations, but 3 other mutations were not transmissible. In the present work, we tested transmission using brain homogenates from patients expressing 3 untested PrP mutants: G131V, Y226X, and Q227X. Human brain homogenates were injected intracerebrally into tg66 transgenic mice overexpressing human PrP. Mice were followed for nearly 800 days. From 593 to 762 dpi, 4 of 8 mice injected with Y226X brain had PrPSc detectable in brain by immunostaining, immunoblot, and PrP amyloid seeding activity assayed by RT-QuIC. From 531 to 784 dpi, 11 of 11 G131V-injected mice had PrPSc deposition in brain, but none were positive by immunoblot or RT-QuIC assay. In contrast, from 529 to 798 dpi, no tg66 mice injected with Q227X brain had PrPSc or PrP amyloid seeding activity detectable by these methods. Y226X is the only one of 4 known PrP truncations associated with familial disease which has been shown to be transmissible. This transmission of prion infectivity from a patient expressing truncated human PrP may have implications for the spread and possible transmission of other aggregated truncated proteins in prion-like diseases such as Alzheimer’s disease, Parkinson’s disease and tauopathies.

Published

2018

10. PrP P102L and Nearby Lysine Mutations Promote Spontaneous In Vitro Formation of Transmissible Prions

Author

Katrina J. Campbell, Brent Race, Kelsie J. Anson, Gregory J. Raymond, Lynne D. Raymond, Andrew G. Hughson, Byron Caughey, and Allison Kraus

Subjects

0301 basic medicine, Mutation, Transmissible spongiform encephalopathy, animal diseases, Immunology, Scrapie, Protein aggregation, Biology, Fibril, medicine.disease_cause, medicine.disease, Microbiology, Virology, In vitro, nervous system diseases, Cell biology, law.invention, 03 medical and health sciences, 030104 developmental biology, law, Insect Science, Recombinant DNA, medicine, Protein folding

Abstract

Accumulation of fibrillar protein aggregates is a hallmark of many diseases. While numerous proteins form fibrils by prion-like seeded polymerization in vitro , only some are transmissible and pathogenic in vivo . To probe the structural features that confer transmissibility to prion protein (PrP) fibrils, we have analyzed synthetic PrP amyloids with or without the human prion disease-associated P102L mutation. The formation of infectious prions from PrP molecules in vitro has required cofactors and/or unphysiological denaturing conditions. Here, we demonstrate that, under physiologically compatible conditions without cofactors, the P102L mutation in recombinant hamster PrP promoted prion formation when seeded by minute amounts of scrapie prions in vitro . Surprisingly, combination of the P102L mutation with charge-neutralizing substitutions of four nearby lysines promoted spontaneous prion formation. When inoculated into hamsters, both of these types of synthetic prions initiated substantial accumulation of prion seeding activity and protease-resistant PrP without transmissible spongiform encephalopathy (TSE) clinical signs or notable glial activation. Our evidence suggests that PrP's centrally located proline and lysine residues act as conformational switches in the in vitro formation of transmissible PrP amyloids. IMPORTANCE Many diseases involve the damaging accumulation of specific misfolded proteins in thread-like aggregates. These threads (fibrils) are capable of growing on the ends by seeding the refolding and incorporation of the normal form of the given protein. In many cases such aggregates can be infectious and propagate like prions when transmitted from one individual host to another. Some transmitted aggregates can cause fatal disease, as with human iatrogenic prion diseases, while other aggregates appear to be relatively innocuous. The factors that distinguish infectious and pathogenic protein aggregates from more innocuous ones are poorly understood. Here we have compared the combined effects of prion seeding and mutations of prion protein (PrP) on the structure and transmission properties of synthetic PrP aggregates. Our results highlight the influence of specific sequence features in the normally unstructured region of PrP that influence the infectious and neuropathogenic properties of PrP-derived aggregates.

Published

2017

11. Amplified Detection of Prions and Other Amyloids by RT-QuIC in Diagnostics and the Evaluation of Therapeutics and Disinfectants

Author

Matteo Manca, Allison Kraus, Gregory J. Raymond, Lynne D. Raymond, Christina D. Orrú, Byron Caughey, Eri Saijo, Andrew G. Hughson, Brent Race, and Bradley R. Groveman

Subjects

0301 basic medicine, 03 medical and health sciences, Protein Misfolding Diseases, 030104 developmental biology, law, animal diseases, Recombinant DNA, Bioassay, Biology, Prion protein, Virology, nervous system diseases, law.invention

Abstract

Among the most sensitive, specific and practical of methods for detecting prions are the real-time quaking-induced conversion (RT-QuIC) assays. These assays exploit the fundamental self-propagating activity of prions to amplify the presence of prion seeds by as much as a trillion-fold. The reactions can detect most of the known mammalian prion diseases, often with sensitivities greater than those of animal bioassays. RT-QuIC assays are performed in multiwell plates with fluorescence detection and have now reached the sensitivity and practicality required for routine prion disease diagnostics. Some key strains of prions within particular host species, e.g., humans, cattle, and sheep, can be discriminated by comparison of RT-QuIC responses with different recombinant prion protein substrates. The most thoroughly validated diagnostic application of RT-QuIC is in the diagnosis of sporadic Creutzfeldt-Jakob disease (sCJD) using cerebrospinal fluid. Diagnostic sensitivities as high as 96% can be achieved in less than 24h with specificities of 98%-100%. The ability, if needed, to also test nasal swab samples can increase the RT-QuIC sensitivity for sCJD to virtually 100%. In addition to diagnostic applications, RT-QuIC has also been used in the testing of prion disinfectants and potential therapeutics. Mechanistically related assays are also now being developed for other protein misfolding diseases.

Published

2017

12. 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

13. Inactivation of Prions and Amyloid Seeds with Hypochlorous Acid

Author

Allison Kraus, Byron Caughey, Laura Sangaré, Bradley R. Groveman, Jeffrey Francis Williams, Luis Contreras, Katie Phillips, Brent Race, Andrew G. Hughson, Eri Saijo, Daniel S. Terry, Gianluigi Zanusso, Matteo Manca, Lori I. Robins, and Virkamal K. Dhaliwal

Subjects

0301 basic medicine, Bleach, Scrapie, Biochemistry, protein amyloid seeds, Animal Diseases, Prion Diseases, chemistry.chemical_compound, Zoonoses, Medicine and Health Sciences, Bioassay, prion decontamination, lcsh:QH301-705.5, Mammals, Hypochlorites, Hypochlorous acid, prions, prion inactivation, Neurodegenerative diseases, 3. Good health, Animal Prion Diseases, Chemistry, Infectious Diseases, Neurology, Sodium hypochlorite, Vertebrates, Physical Sciences, Metallurgy, Hamsters, Research Article, lcsh:Immunologic diseases. Allergy, Amyloid, Prions, Bovine spongiform encephalopathy, Immunology, Materials Science, Biology, Microbiology, Rodents, 03 medical and health sciences, In vivo, Virology, Genetics, medicine, Alloys, Animals, Molecular Biology, Organisms, Chemical Compounds, Biology and Life Sciences, Proteins, medicine.disease, Stainless Steel, Creutzfeldt-Jakob disease, 030104 developmental biology, lcsh:Biology (General), chemistry, Steel, Amniotes, Amyloid Proteins, Parasitology, Salts, lcsh:RC581-607, Zoology

Abstract

Hypochlorous acid (HOCl) is produced naturally by neutrophils and other cells to kill conventional microbes in vivo. Synthetic preparations containing HOCl can also be effective as microbial disinfectants. Here we have tested whether HOCl can also inactivate prions and other self-propagating protein amyloid seeds. Prions are deadly pathogens that are notoriously difficult to inactivate, and standard microbial disinfection protocols are often inadequate. Recommended treatments for prion decontamination include strongly basic (pH ≥~12) sodium hypochlorite bleach, ≥1 N sodium hydroxide, and/or prolonged autoclaving. These treatments are damaging and/or unsuitable for many clinical, agricultural and environmental applications. We have tested the anti-prion activity of a weakly acidic aqueous formulation of HOCl (BrioHOCl) that poses no apparent hazard to either users or many surfaces. For example, BrioHOCl can be applied directly to skin and mucous membranes and has been aerosolized to treat entire rooms without apparent deleterious effects. Here, we demonstrate that immersion in BrioHOCl can inactivate not only a range of target microbes, including spores of Bacillus subtilis, but also prions in tissue suspensions and on stainless steel. Real-time quaking-induced conversion (RT-QuIC) assays showed that BrioHOCl treatments eliminated all detectable prion seeding activity of human Creutzfeldt-Jakob disease, bovine spongiform encephalopathy, cervine chronic wasting disease, sheep scrapie and hamster scrapie; these findings indicated reductions of ≥103- to 106-fold. Transgenic mouse bioassays showed that all detectable hamster-adapted scrapie infectivity in brain homogenates or on steel wires was eliminated, representing reductions of ≥~105.75-fold and >104-fold, respectively. Inactivation of RT-QuIC seeding activity correlated with free chlorine concentration and higher order aggregation or destruction of proteins generally, including prion protein. BrioHOCl treatments had similar effects on amyloids composed of human α-synuclein and a fragment of human tau. These results indicate that HOCl can block the self-propagating activity of prions and other amyloids., Author Summary Many serious diseases have been linked to pathogenic states of various proteins. These naturally occurring proteins can be corrupted to form aggregates such as prions and amyloids that propagate in and between tissues by acting as seeds that convert the normal form of the protein into more of the pathological form. For example, corrupted prion protein can cause fatal transmissible neurodegenerative diseases such as Creutzfeldt-Jakob disease in humans, chronic wasting disease in cervids and bovine spongiform encephalopathy. Other amyloid-forming protein aggregates are pathogenic in Parkinson’s, Alzheimer’s, and other diseases. The fact that prions and amyloids are composed predominantly of tough, tightly packed proteins makes them unusually resistant to conventional microbial disinfection procedures. Infectious prions can persist indefinitely in, or on, a variety of materials such as tissues, fluids, tools, instruments, and environmental surfaces, making it important to identify decontaminants that are effective without being dangerous or damaging. Here we show that hypochlorous acid, a disinfectant that is produced naturally by certain cells within the body, has strong anti-prion and anti-amyloid activity. We find that a non-irritating and broadly applicable hypochlorous acid preparation can disinfect prions in tissue homogenates and on stainless steel wires serving as surrogates for surgical instruments.

Published

2016

14. 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

15. In Vivo Comparison of Chronic Wasting Disease Infectivity from Deer with Variation at Prion Protein Residue 96

Author

Kimberly Meade-White, Michael W. Miller, Bruce Chesebro, Karen A. Fox, and Brent Race

Subjects

Genetically modified mouse, Prions, animal diseases, Transgene, Immunology, Mice, Transgenic, Biology, Microbiology, Mice, In vivo, Virology, Genotype, medicine, Animals, Point Mutation, Peptide sequence, Infectivity, Deer, Neurodegeneration, Chronic wasting disease, medicine.disease, nervous system diseases, Insect Science, Disease Progression, Wasting Disease, Chronic, Pathogenesis and Immunity

Abstract

Chronic wasting disease (CWD) is a prion disease of cervids that causes neurodegeneration and death. Susceptibility to prion infections, including CWD, can be dependent on the amino acid sequence of the host prion protein (PrP). Here, CWD agent obtained from a deer expressing the 96SS genotype, associated with partial resistance to CWD, was used to infect transgenic (tg) mice expressing either 96GG or 96SS deer PrP. Transgenic mice expressing 96GG deer PrP succumbed to this agent, but tg mice expressing 96SS deer PrP did not. Additional studies using inocula from 96GG deer showed no transmission to 96SS PrP mice and delayed disease in 96GS mice. Thus, 96S PrP played an inhibitory role in disease progression in tg mice.

Published

2011

16. 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

17. 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

18. Characteristics of 263K Scrapie Agent in Multiple Hamster Species

Author

Richard E. Race, Kimberly Meade-White, Don Gardner, Kent D. Barbian, Brent Race, Lara M. Taubner, Cynthia Favara, and Stephen F. Porcella

Subjects

Microbiology (medical), PrPSc Proteins, Epidemiology, Prions, animal diseases, Molecular Sequence Data, Hamster, lcsh:Medicine, Scrapie, Prion Diseases, lcsh:Infectious and parasitic diseases, Species Specificity, species barriers, Serial passage, Cricetinae, medicine, Animals, TSE, lcsh:RC109-216, Amino Acid Sequence, Serial Passage, biochemical profile, Peptide sequence, Transmissible spongiform encephalopathy, Strain (chemistry), biology, Research, scrapie, lcsh:R, hamsters, Sequence Analysis, DNA, Proteinase K, medicine.disease, Virology, Immunohistochemistry, PRNP amino acid sequence, Infectious Diseases, biology.protein, prnp nucleotide sequence, Endopeptidase K, molecular profile

Abstract

Characteristics correlated better with host factors than with agent strain., Transmissible spongiform encephalopathy (TSE) diseases are known to cross species barriers, but the pathologic and biochemical changes that occur during transmission are not well understood. To better understand these changes, we infected 6 hamster species with 263K hamster scrapie strain and, after each of 3 successive passages in the new species, analyzed abnormal proteinase K (PK)–resistant prion protein (PrPres) glycoform ratios, PrPres PK sensitivity, incubation periods, and lesion profiles. Unique 263K molecular and biochemical profiles evolved in each of the infected hamster species. Characteristics of 263K in the new hamster species seemed to correlate best with host factors rather than agent strain. Furthermore, 2 polymorphic regions of the prion protein amino acid sequence correlated with profile differences in these TSE-infected hamster species.

Published

2009

19. 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

20. 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

21. Capillaries in the olfactory bulb but not the cortex are highly susceptible to virus-induced vascular leak and promote viral neuroinvasion

Author

Katie Phillips, Brent Race, Clayton W. Winkler, and Karin E. Peterson

Subjects

viruses, Viral pathogenesis, Central nervous system, Mice, Transgenic, Biology, Blood–brain barrier, Virus, Pathology and Forensic Medicine, Capillary Permeability, Cellular and Molecular Neuroscience, Bacterial Proteins, Encephalitis, California, La Crosse virus, medicine, Animals, Cytoskeleton, Cerebral Cortex, Viral encephalitis, Viral Load, Virus Internalization, medicine.disease, Virology, Olfactory Bulb, Olfactory bulb, Capillaries, Mice, Inbred C57BL, Disease Models, Animal, Luminescent Proteins, medicine.anatomical_structure, Axoplasmic transport, Neurology (clinical), Viral load

Abstract

Viral neuroinvasion is a critical step in the pathogenesis of viral encephalitis. Multiple mechanisms of neuroinvasion have been identified, but their relative contribution to central nervous system (CNS) infection remains unclear for many viruses. In this study, we examined neuroinvasion of the mosquito-borne bunyavirus La Crosse (LACV), the leading cause of pediatric viral encephalitis in the USA. We found that the olfactory bulb (OB) and tract were the initial areas of CNS virus infection in mice. Removal of the OB reduced the incidence of LACV-induced disease demonstrating the importance of this area to neuroinvasion. However, we determined that infection of the OB was not due to axonal transport of virus from olfactory sensory neurons as ablation of these cells did not affect viral pathogenesis. Instead, we found that OB capillaries were compromised allowing leakage of virus-sized particles into the brain. Analysis of OB capillaries demonstrated specific alterations in cytoskeletal and Rho GTPase protein expression not observed in capillaries from other brain areas such as the cortex where leakage did not occur. Collectively, these findings indicate that LACV neuroinvasion occurs through hematogenous spread in specific brain regions where capillaries are prone to virus-induced activation such as the OB. Capillaries in these areas may be “hot spots” that are more susceptible to neuroinvasion not only for LACV, but other neurovirulent viruses as well.

Published

2015

22. 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

23. Poor Vector Competence of Fleas and the Evolution of Hypervirulence inYersinia pestis

Author

Brent Race, Florent Sebbane, B. Joseph Hinnebusch, and Ellen A Lorange

Subjects

Infectivity, Plague, Flea, Virulence, biology, Yersinia pestis, bacterial infections and mycoses, medicine.disease, biology.organism_classification, Biological Evolution, Virology, Bubonic plague, Insect Vectors, Microbiology, Infectious Diseases, Susceptible individual, Vector (epidemiology), medicine, Animals, Siphonaptera, Immunology and Allergy, Xenopsylla, Arthropod Vector

Abstract

Population genetics and comparative genomics analyses of the pathogenic Yersinia species have indicated that arthropodborne transmission is an evolutionarily recent adaptation in Yersinia pestis, the agent of plague. We show that the infectivity of Y. pestis to its most proficient vector, the rat flea Xenopsylla cheopis, and subsequent transmission efficiency are both low. The poor vector competence of fleas likely imposed selective pressure that favored the emergence and continued maintenance of a hypervirulent Y. pestis clone. In particular, the rapidly fatal gram-negative sepsis that typifies plague is a consequence of the high threshold bacteremia level that must be attained to complete the transmission cycle. Epidemiological modeling predicts that, to compensate for a relatively short period of infectivity of the mammalian host for the arthropod vector, plague epizootics require a high flea burden per host, even when the susceptible host population density is high.

Published

2005

24. Temporal Effects of Gamma Interferon Deficiency on the Course of Friend Retrovirus Infection in Mice

Author

Karin E. Peterson, Koen Schepers, Ingunn M. Stromnes, Kim J. Hasenkrug, Ronald J. Messer, Ton N. Schumacher, Leonard H. Evans, Brent Race, and Ulf Dittmer

Subjects

Immunology, Spleen, CD8-Positive T-Lymphocytes, Antibodies, Viral, Antiviral Agents, Polymerase Chain Reaction, Microbiology, Virus, Immunoglobulin G, Interferon-gamma, Mice, Neutralization Tests, Virology, medicine, Animals, Interferon gamma, Mice, Knockout, Leukemia, Experimental, biology, Friend virus, Antibody titer, Flow Cytometry, biology.organism_classification, Recombinant Proteins, Friend murine leukemia virus, Mice, Inbred C57BL, Tumor Virus Infections, medicine.anatomical_structure, Insect Science, DNA, Viral, biology.protein, RNA, Viral, Pathogenesis and Immunity, Leukemia, Erythroblastic, Acute, Bone marrow, Antibody, Retroviridae Infections, medicine.drug

Abstract

The current studies demonstrate complex and seemingly contradictory effects by gamma interferon (IFN-γ) on Friend virus (FV) infection. Both temporal and tissue-specific effects were observed. During the first week of infection, IFN-γ-deficiency caused increased levels of FV infection in multiple tissues. Surprisingly, however, by 2 weeks postinfection, IFN-γ-deficient mice had significantly lower levels of infection in both the spleen and bone marrow compared to wild-type mice. The rapid reduction of virus in the IFN-γ-deficient mice correlated with a more rapid virus-neutralizing antibody response than was observed in the wild-type mice. Furthermore, the virus-neutralizing antibody response in wild-type mice could be accelerated by ablation of their IFN-γ response. Although the IFN-γ-deficient mice developed an accelerated virus-neutralizing antibody response, they did not class-switch to immunoglobulin G class immunoglobulins nor could they maintain long-term virus-neutralizing antibody titers. Eventually, all of the IFN-γ-deficient mice failed to keep persistent virus in check and developed fatal FV-induced erythroleukemia.

Published

2002

25. Prion Infectivity in Fat of Deer with Chronic Wasting Disease

Author

Kimberly Meade-White, Bruce Chesebro, Richard E. Race, and Brent Race

Subjects

animal diseases, Bovine spongiform encephalopathy, Immunology, Central nervous system, Adipose tissue, Animals, Wild, Food Contamination, Disease, Biology, Microbiology, Prion Diseases, Prion infectivity, Virology, medicine, Animals, Humans, Tissue Distribution, Infectivity, Deer, Ruminants, Chronic wasting disease, medicine.disease, nervous system diseases, Titer, medicine.anatomical_structure, Adipose Tissue, Insect Science, Wasting Disease, Chronic, Pathogenesis and Immunity, Disease Susceptibility

Abstract

Chronic wasting disease (CWD) is a neurodegenerative prion disease of cervids. Some animal prion diseases, such as bovine spongiform encephalopathy, can infect humans; however, human susceptibility to CWD is unknown. In ruminants, prion infectivity is found in central nervous system and lymphoid tissues, with smaller amounts in intestine and muscle. In mice, prion infectivity was recently detected in fat. Since ruminant fat is consumed by humans and fed to animals, we determined infectivity titers in fat from two CWD-infected deer. Deer fat devoid of muscle contained low levels of CWD infectivity and might be a risk factor for prion infection of other species.

Published

2009

26. 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

27. Prion Seeding Activities of Mouse Scrapie Strains with Divergent PrPSc Protease Sensitivities and Amyloid Plaque Content Using RT-QuIC and eQuIC

Author

Rona Barron, Brent Race, Gerald S. Baron, Byron Caughey, Andrew G. Hughson, Christina D. Orrú, Alessandra Pani, Declan King, Sarah Vascellari, and Jason M. Wilham

Subjects

Time Factors, PrPSc Proteins, Glycosylphosphatidylinositols, medicine.medical_treatment, animal diseases, lcsh:Medicine, Scrapie, Plaque, Amyloid, law.invention, Prion Diseases, Mice, law, lcsh:Science, Medicine(all), Infectivity, Multidisciplinary, Transmissible spongiform encephalopathy, Agricultural and Biological Sciences(all), Zoonotic Diseases, Titrimetry, Brain, Neurodegenerative Diseases, Adaptation, Physiological, Infectious Diseases, Neurology, Veterinary Diseases, Recombinant DNA, Medicine, Biological Assay, Research Article, Genetically modified mouse, Amyloid, Prions, Immunoblotting, Biology, Bovine Spongiform Encephalopathy, Prion Proteins, medicine, Animals, Veterinary Prion Diseases, Protease, Biochemistry, Genetics and Molecular Biology(all), lcsh:R, medicine.disease, Virology, nervous system diseases, Mice, Inbred C57BL, Disease Models, Animal, lcsh:Q, Veterinary Science, Peptide Hydrolases, Synaptosomes

Abstract

Different transmissible spongiform encephalopathy (TSE)-associated forms of prion protein (e.g. PrP(Sc)) can vary markedly in ultrastructure and biochemical characteristics, but each is propagated in the host. PrP(Sc) propagation involves conversion from its normal isoform, PrP(C), by a seeded or templated polymerization mechanism. Such a mechanism is also the basis of the RT-QuIC and eQuIC prion assays which use recombinant PrP (rPrP(Sen)) as a substrate. These ultrasensitive detection assays have been developed for TSE prions of several host species and sample tissues, but not for murine models which are central to TSE pathogenesis research. Here we have adapted RT-QuIC and eQuIC to various murine prions and evaluated how seeding activity depends on glycophosphatidylinositol (GPI) anchoring and the abundance of amyloid plaques and protease-resistant PrP(Sc) (PrP(Res)). Scrapie brain dilutions up to 10(-8) and 10(-13) were detected by RT-QuIC and eQuIC, respectively. Comparisons of scrapie-affected wild-type mice and transgenic mice expressing GPI anchorless PrP showed that, although similar concentrations of seeding activity accumulated in brain, the heavily amyloid-laden anchorless mouse tissue seeded more rapid reactions. Next we compared seeding activities in the brains of mice with similar infectivity titers, but widely divergent PrP(Res) levels. For this purpose we compared the 263K and 139A scrapie strains in transgenic mice expressing P101L PrP(C). Although the brains of 263K-affected mice had little immunoblot-detectable PrP(Res), RT-QuIC indicated that seeding activity was comparable to that associated with a high-PrP(Res) strain, 139A. Thus, in this comparison, RT-QuIC seeding activity correlated more closely with infectivity than with PrP(Res) levels. We also found that eQuIC, which incorporates a PrP(Sc) immunoprecipitation step, detected seeding activity in plasma from wild-type and anchorless PrP transgenic mice inoculated with 22L, 79A and/or RML scrapie strains. Overall, we conclude that these new mouse-adapted prion seeding assays detect diverse types of PrP(Sc).

Published

2012

28. Isolation of novel synthetic prion strains by amplification in transgenic mice coexpressing wild-type and anchorless prion proteins

Author

Lynne D. Raymond, Rebecca Rosenke, Gerald S. Baron, Brent Race, Ravindra Kodali, David W. Dorward, Gregory J. Raymond, Jason R. Hollister, Andrew G. Hughson, Dan Long, Roger A. Moore, and Danielle K. Offerdahl

Subjects

Gene isoform, Genetically modified mouse, Prions, animal diseases, Immunology, Scrapie, Mice, Transgenic, Biology, Microbiology, law.invention, Mice, law, Virology, mental disorders, medicine, Animals, Transmissible spongiform encephalopathy, Wild type, medicine.disease, Phenotype, Molecular biology, In vitro, Recombinant Proteins, nervous system diseases, Mice, Inbred C57BL, Insect Science, Recombinant DNA

Abstract

Mammalian prions are thought to consist of misfolded aggregates (protease-resistant isoform of the prion protein [PrP res ]) of the cellular prion protein (PrP C ). Transmissible spongiform encephalopathy (TSE) can be induced in animals inoculated with recombinant PrP (rPrP) amyloid fibrils lacking mammalian posttranslational modifications, but this induction is inefficient in hamsters or transgenic mice overexpressing glycosylphosphatidylinositol (GPI)-anchored PrP C . Here we show that TSE can be initiated by inoculation of misfolded rPrP into mice that express wild-type (wt) levels of PrP C and that synthetic prion strain propagation and selection can be affected by GPI anchoring of the host's PrP C . To create prions de novo , we fibrillized mouse rPrP in the absence of molecular cofactors, generating fibrils with a PrP res -like protease-resistant banding profile. These fibrils induced the formation of PrP res deposits in transgenic mice coexpressing wt and GPI-anchorless PrP C (wt/GPI − ) at a combined level comparable to that of PrP C expression in wt mice. Secondary passage into mice expressing wt, GPI − , or wt plus GPI − PrP C induced TSE disease with novel clinical, histopathological, and biochemical phenotypes. Contrary to laboratory-adapted mouse scrapie strains, the synthetic prion agents exhibited a preference for conversion of GPI − PrP C and, in one case, caused disease only in GPI − mice. Our data show that novel TSE agents can be generated de novo solely from purified mouse rPrP after amplification in mice coexpressing normal levels of wt and anchorless PrP C . These observations provide insight into the minimal elements required to create prions in vitro and suggest that the PrP C GPI anchor can modulate the propagation of synthetic TSE strains.

Published

2012

29. Reply to Karapetyan: Viral synthesis and assembly is unlikely to occur under cell-free PMCA conditions

Author

Bruce Chesebro, Brent Race, and Mikael Klingeborn

Subjects

Infectivity, Multidisciplinary, Transmissible spongiform encephalopathy, viruses, Poliovirus, Scrapie, Biology, medicine.disease_cause, medicine.disease, Virology, Virus, Nucleic acid, medicine, Protein Misfolding Cyclic Amplification, Letters, Energy source

Abstract

The letter to the editor by Karapetyan (1) takes issue with our conclusion in PNAS (2) that the generation of transmissible spongiform encephalopathy (TSE) infectivity in cell-free conditions is against the concept that the TSE infectious agent is a virus. Karapetyan's main point is that poliovirus has been shown to “replicate in a cell-free system” by Wimmer and colleagues (3). We would disagree with the interpretation that these poliovirus experiments are analogous to our protein misfolding cyclic amplification (PMCA) reactions. The divalent cations (Mg2+) and energy sources (ATP and GTP) required for synthesis of viral proteins and nucleic acids, as well as virus assembly (3, 4), should not be present at appropriate concentrations in the crude 1% Triton X-100 brain homogenates made in PBS with EDTA that were used for PMCA reactions. Furthermore, in scrapie PMCA experiments, we and others were able to passage and amplify infectivity serially over multiple reactions, whereas in the poliovirus experiments, serial cell-free passage of the assembled infectious viruses was not demonstrated and would probably not be possible without a mechanism for gently uncoating the viral RNA packaged within the particles. For all these reasons, the generation of new scrapie infectivity in the amounts we detected in PMCA reactions (up to 3 × 105 LD50/0.050 mL reaction mix) is not likely to represent viral synthesis and assembly into infectious TSE virus particles.

Published

2012

30. Time course of prion seeding activity in cerebrospinal fluid of scrapie-infected hamsters after intratongue and intracerebral inoculations

Author

Byron Caughey, Christina D. Orrú, Brent Race, Andrew G. Hughson, and Gregory J. Raymond

Subjects

Microbiology (medical), Pathology, medicine.medical_specialty, Amyloid, Inoculation, Prions, Brain, Scrapie, Biology, Virology, Intracerebral inoculation, Kinetics, Cerebrospinal fluid, Tongue, Limit of Detection, Cricetinae, Time course, medicine, Animals, Seeding

Abstract

To assess prospects for early diagnosis of prion disease based on prion seeding activity in cerebrospinal fluid (CSF), we measured the activity over time in scrapie-infected hamsters by r eal- t ime qu aking- i nduced c onversion (RT-QuIC). After intracerebral inoculation, activity appeared in CSF within 1 day and plateaued weeks before the onset of clinical signs. However, after intratongue inoculation, activity first appeared in CSF with the onset of clinical signs, well after higher-level accumulation of seeding activity in brain.

Published

2012

31. Lower specific infectivity of protease-resistant prion protein generated in cell-free reactions

Author

Kimberly Meade-White, Bruce Chesebro, Brent Race, and Mikael Klingeborn

Subjects

Protein Denaturation, Protein Folding, Prions, Immunoblotting, Mice, Transgenic, Scrapie, Biology, Virus, Incubation period, Cell-free system, Mice, Cricetinae, medicine, Animals, Letters, Infectivity, Multidisciplinary, Transmissible spongiform encephalopathy, Cell-Free System, Brain, Nucleic acid amplification technique, medicine.disease, Immunohistochemistry, Virology, Titer, PNAS Plus, Nucleic Acid Amplification Techniques

Abstract

Prions are unconventional infectious agents that cause transmissible spongiform encephalopathy (TSE) diseases, or prion diseases. The biochemical nature of the prion infectious agent remains unclear. Previously, using a protein misfolding cyclic amplification (PMCA) reaction, infectivity and disease-associated protease-resistant prion protein (PrPres) were both generated under cell-free conditions, which supported a nonviral hypothesis for the agent. However, these studies lacked comparative quantitation of both infectivity titers and PrPres, which is important both for biological comparison with in vivo-derived infectivity and for excluding contamination to explain the results. Here during four to eight rounds of PMCA, end-point dilution titrations detected a >320-fold increase in infectivity versus that in controls. These results provide strong support for the hypothesis that the agent of prion infectivity is not a virus. PMCA-generated samples caused the same clinical disease and neuropathology with the same rapid incubation period as the input brain-derived scrapie samples, providing no evidence for generation of a new strain in PMCA. However, the ratio of the infectivity titer to the amount of PrPres (specific infectivity) was much lower in PMCA versus brain-derived samples, suggesting the possibility that a substantial portion of PrPres generated in PMCA might be noninfectious.

Published

2011

32. 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

33. Rapid end-point quantitation of prion seeding activity with sensitivity comparable to bioassays

Author

Kimberly Meade-White, Ryuichiro Atarashi, Kazunori Sano, Christina D. Orrú, Byron Caughey, Brent Race, Andrew Timmes, Richard A. Bessen, Jason M. Wilham, and Lara M. Taubner

Subjects

lcsh:Immunologic diseases. Allergy, Amyloid, Serial dilution, Endpoint Determination, Prions, Immunology, Scrapie, Biology, Microbiology, Biochemistry, Protein Structure, Secondary, Biochemistry/Protein Chemistry, Infectious Diseases/Prion Diseases, Virology, Cricetinae, High-Throughput Screening Assays, Genetics, medicine, Methods, Bioassay, Animals, Humans, Molecular Biology, lcsh:QH301-705.5, Cerebrospinal Fluid, Transmissible mink encephalopathy, Sheep, Deer, Brain, Chronic wasting disease, medicine.disease, Molecular biology, Neurological Disorders/Prion Diseases, Infectious Diseases, lcsh:Biology (General), Mink, Protein Misfolding Cyclic Amplification, Parasitology, lcsh:RC581-607, Research Article

Abstract

A major problem for the effective diagnosis and management of prion diseases is the lack of rapid high-throughput assays to measure low levels of prions. Such measurements have typically required prolonged bioassays in animals. Highly sensitive, but generally non-quantitative, prion detection methods have been developed based on prions' ability to seed the conversion of normally soluble protease-sensitive forms of prion protein to protease-resistant and/or amyloid fibrillar forms. Here we describe an approach for estimating the relative amount of prions using a new prion seeding assay called real-time quaking induced conversion assay (RT-QuIC). The underlying reaction blends aspects of the previously described quaking-induced conversion (QuIC) and amyloid seeding assay (ASA) methods and involves prion-seeded conversion of the alpha helix-rich form of bacterially expressed recombinant PrPC to a beta sheet-rich amyloid fibrillar form. The RT-QuIC is as sensitive as the animal bioassay, but can be accomplished in 2 days or less. Analogous to end-point dilution animal bioassays, this approach involves testing of serial dilutions of samples and statistically estimating the seeding dose (SD) giving positive responses in 50% of replicate reactions (SD50). Brain tissue from 263K scrapie-affected hamsters gave SD50 values of 1011-1012/g, making the RT-QuIC similar in sensitivity to end-point dilution bioassays. Analysis of bioassay-positive nasal lavages from hamsters affected with transmissible mink encephalopathy gave SD50 values of 103.5–105.7/ml, showing that nasal cavities release substantial prion infectivity that can be rapidly detected. Cerebral spinal fluid from 263K scrapie-affected hamsters contained prion SD50 values of 102.0–102.9/ml. RT-QuIC assay also discriminated deer chronic wasting disease and sheep scrapie brain samples from normal control samples. In principle, end-point dilution quantitation can be applied to many types of prion and amyloid seeding assays. End point dilution RT-QuIC provides a sensitive, rapid, quantitative, and high throughput assay of prion seeding activity., Author Summary Prion diseases are deadly infectious neurodegenerative disorders of mammals which involve the misfolding of host prion protein. To better manage these diseases, we need to be able to detect and quantify the infectious particles, or prions, in biological samples. However, current tests lack the sensitivity, speed and/or quantitative capabilities required for many important applications in medicine, agriculture, wildlife biology and research. To address this problem, we have developed a new prion assay that is highly sensitive, rapid, and quantitative. This assay takes advantage of the ability of miniscule amounts of infectious prions to seed the misfolding of large excesses of normal prion protein in test tube reactions. Quantitation is achieved by testing a range of sample dilutions and determining loss of seeding activity, i.e. the end-point dilution. Similar analyses have long been used to quantify prions by inoculation into animals; however, such bioassays take months or years to perform and are both animal-intensive and expensive. Our new method provides a more practical means of detecting and quantifying prions. So far, we have applied this assay to prions from sheep, deer, and hamsters, and have found surprisingly high levels of prions in the nasal and cerebral spinal fluids of infected hamsters.

Published

2010

34. Detection of prion infectivity in fat tissues of scrapie-infected mice

Author

Richard E. Race, Kimberly Meade-White, Bruce Chesebro, Brent Race, and Michael B. A. Oldstone

Subjects

lcsh:Immunologic diseases. Allergy, PrPSc Proteins, Adipose Tissue, White, animal diseases, Immunology, Immunoblotting, Public Health and Epidemiology/Infectious Diseases, Scrapie, Mice, Transgenic, Biology, Disease pathogenesis, Microbiology, 03 medical and health sciences, Mice, 0302 clinical medicine, Prion infection, Adipose Tissue, Brown, Prion infectivity, Infectious Diseases/Prion Diseases, Virology, Genetics, Animals, Tissue Distribution, Tissue distribution, Molecular Biology, lcsh:QH301-705.5, 030304 developmental biology, 2. Zero hunger, Infectivity, 0303 health sciences, Transmission (medicine), Immunohistochemistry, 3. Good health, nervous system diseases, lcsh:Biology (General), Parasitology, lcsh:RC581-607, 030217 neurology & neurosurgery, Research Article

Abstract

Distribution of prion infectivity in organs and tissues is important in understanding prion disease pathogenesis and designing strategies to prevent prion infection in animals and humans. Transmission of prion disease from cattle to humans resulted in banning human consumption of ruminant nervous system and certain other tissues. In the present study, we surveyed tissue distribution of prion infectivity in mice with prion disease. We show for the first time detection of infectivity in white and brown fat. Since high amounts of ruminant fat are consumed by humans and also incorporated into animal feed, fat-containing tissues may pose a previously unappreciated hazard for spread of prion infection., Author Summary Prion diseases, also known as transmissible spongiform encephalopathies, are infectious progressive fatal neurodegenerative diseases which affect humans as well as wild and domestic animals. Distribution of prion infectivity in organs and tissues is important in understanding prion disease pathogenesis and designing strategies to prevent prion infection in animals and humans. We show for the first time the presence of prion infectivity in white fat and brown fat tissues of mice with prion disease. Our results suggest that fat tissues of domestic or wild animals infected with prions may pose an unappreciated hazard for spread of infection to humans or domestic animals. The presence of prion infectivity in fat suggests that additional consideration may be required to eliminate from the food chain any fat from ruminants suspected of exposure to or infection with prions. Thus, this finding has implications for public health, food safety, and prion disease prevention strategies.

Published

2008

35. Prion protein on astrocytes or in extracellular fluid impedes neurodegeneration induced by truncated prion protein

Author

Bruce Chesebro, Brent Race, Adriano Aguzzi, Richard E. Race, Frank Baumann, Kimberly Meade-White, University of Zurich, and Race, B

Subjects

Genetically modified mouse, Central Nervous System, Male, Cell signaling, Prions, animal diseases, Central nervous system, 10208 Institute of Neuropathology, 610 Medicine & health, Mice, Transgenic, Cell Communication, Hippocampal formation, Biology, Article, Prion Diseases, 2806 Developmental Neuroscience, Mice, Developmental Neuroscience, medicine, Animals, chemistry.chemical_classification, Mice, Knockout, Neurons, Neurodegeneration, Extracellular Fluid, Genetic Therapy, medicine.disease, Virology, Peptide Fragments, Cell biology, nervous system diseases, Molecular Weight, medicine.anatomical_structure, Neurology, chemistry, 2808 Neurology, Astrocytes, Nerve Degeneration, Neuroglia, 570 Life sciences, biology, Female, Glycoprotein, Astrocyte

Abstract

Prion protein (PrP) is a host-encoded membrane-anchored glycoprotein which is required for susceptibility to prion disease. PrP may also be important for normal brain functions such as hippocampal spatial memory. Previously transgenic mice expressing amino terminally truncated mouse PrP (Delta32-134) spontaneously developed a fatal disease associated with degeneration of cerebellar granular neurons as well as vacuolar degeneration of deep cerebellar and brain stem white matter. This disease could be prevented by co-expression of wild-type (WT) mouse PrP on neurons or oligodendroglia. In the present experiments we studied Delta32-134 PrP transgenic mice with WT PrP expression restricted to astroglia, an abundant CNS cell-type important for neuronal viability. Expression of WT PrP in astroglia was sufficient to rescue 50% of mice from disease and prolonged survival by 200 days in the other 50%. We also found that transgenic mice expressing full-length soluble anchorless PrP had increased survival by 100 days. Together these two results indicated that rescue from neurodegeneration induced by Delta32-134 PrP might involve interactions between neurons expressing truncated PrP and nearby astrocytes expressing WT PrP or extracellular fluid containing soluble WT PrP.

Published

2008

36. Resistance to Chronic Wasting Disease in Transgenic Mice Expressing a Naturally Occurring Allelic Variant of Deer Prion Protein▿

Author

Kimberly Meade-White, Rachel LaCasse, Elizabeth S. Williams, Alex Bossers, Bruce Chesebro, Richard E. Race, Brent Race, Michael B. A. Oldstone, Michael W. Miller, Matthew J. Trifilo, and Cynthia Favara

Subjects

Genetically modified mouse, Prions, Transgene, animal diseases, Immunology, Immunoblotting, Molecular Sequence Data, Oligonucleotides, mule deer, Scrapie, Spleen, Mice, Transgenic, Biology, in-vitro, transmissible spongiform encephalopathies, Microbiology, susceptibility, Transgenic Model, Pathogenesis, Mice, Virology, cervus-elaphus-nelsoni, medicine, Animals, CIDC - Divisie Bacteriologie en TSE's, creutzfeldt-jakob-disease, elk, Transmissible spongiform encephalopathy, Polymorphism, Genetic, Base Sequence, Deer, scrapie, Brain, Chronic wasting disease, medicine.disease, Immunity, Innate, nervous system diseases, white-tailed deer, medicine.anatomical_structure, Insect Science, Pathogenesis and Immunity, Wasting Disease, Chronic, prp knockout mice

Abstract

Prion protein (PrP) is a required factor for susceptibility to transmissible spongiform encephalopathy or prion diseases. In transgenic mice, expression of prion protein (PrP) from another species often confers susceptibility to prion disease from that donor species. For example, expression of deer or elk PrP in transgenic mice has induced susceptibility to chronic wasting disease (CWD), the prion disease of cervids. In the current experiments, transgenic mice expressing two naturally occurring allelic variants of deer PrP with either glycine (G) or serine (S) at residue 96 were found to differ in susceptibility to CWD infection. G96 mice were highly susceptible to infection, and disease appeared starting as early as 160 days postinfection. In contrast, S96 mice showed no evidence of disease or generation of disease-associated protease-resistant PrP (PrPres) over a 600-day period. At the time of clinical disease, G96 mice showed typical vacuolar pathology and deposition of PrPres in many brain regions, and in some individuals, extensive neuronal loss and apoptosis were noted in the hippocampus and cerebellum. Extraneural accumulation of PrPres was also noted in spleen and intestinal tissue of clinically ill G96 mice. These results demonstrate the importance of deer PrP polymorphisms in susceptibility to CWD infection. Furthermore, this deer PrP transgenic model is the first to demonstrate extraneural accumulation of PrPres in spleen and intestinal tissue and thus may prove useful in studies of CWD pathogenesis and transmission by oral or other natural routes of infection.

Published

2007

37. Essential roles for CD8+ T cells and gamma interferon in protection of mice against retrovirus-induced immunosuppression

Author

Brent Race, Kim J. Hasenkrug, Karin E. Peterson, Ulf Dittmer, Ronald J. Messer, and Ingunn M. Stromnes

Subjects

medicine.medical_treatment, Immunology, CD8-Positive T-Lymphocytes, Major histocompatibility complex, Microbiology, Interferon-gamma, Mice, Immune system, Antigen, Virology, medicine, Cytotoxic T cell, Animals, Immunosuppression Therapy, biology, Friend virus, Immunologic Deficiency Syndromes, Immunosuppression, biology.organism_classification, Disease Models, Animal, Cytokine, Retroviridae, Insect Science, biology.protein, Pathogenesis and Immunity, CD8, Retroviridae Infections

Abstract

It is known that both animal and human retroviruses typically cause immunosuppression in their respective hosts, but the mechanisms by which this occurs are poorly understood. The present study uses Friend virus (FV) infections of mice as a model to determine how major histocompatibility complex (MHC) genes influence immunosuppression. Previously, MHC-I genes were shown to influence antibody responses to potent antigenic challenges given during acute FV infection. The mapping of an immune response to an MHC-I gene implicated CD8+T cells in the mechanism, so we directly tested for their role by using in vivo CD8+T-cell depletions. Mice resistant to FV-induced immunosuppression became susceptible when they were depleted of CD8+T cells. Resistance also required gamma interferon (IFN-γ), as in vivo neutralization of IFN-γ converted mice from a resistant to susceptible phenotype. On the other hand, susceptibility to FV-induced immunosuppression was dependent on the immunosuppressive cytokine, interleukin-10 (IL-10), as antibody responses were restored in susceptible mice when IL-10 function was blocked in vivo. Thus, FV-induced immunosuppression of antibody responses involves complex mechanisms controlled at least in part by CD8+T cells.

Published

2001

38. Kinetics of the Development of Protective Immunity in Mice Vaccinated with a Live Attenuated Retrovirus

Author

Brent Race, Kim J. Hasenkrug, and Ulf Dittmer

Subjects

Immunology, Spleen, Biology, Microbiology, Virus, Mice, Immunity, Virology, Vaccines and Antiviral Agents, medicine, Cytotoxic T cell, Animals, B-Lymphocytes, Attenuated vaccine, Viral Vaccine, Viral Vaccines, Vaccination, CTL, medicine.anatomical_structure, Retroviridae, Insect Science, Female, Retroviridae Infections, T-Lymphocytes, Cytotoxic

Abstract

Vaccination of mice with a live attenuated vaccine virus induces potent protection against subsequent challenge with pathogenic Friend retroviral complex. The kinetic studies presented here demonstrate protection from acute splenomegaly as early as 1 week postvaccination. At this time point virus-specific cytotoxic T lymphocytes (CTL) were demonstrable in direct chromium release assays. However, during the first 2 weeks after vaccination protection was incomplete since the mice were not protected against establishment of low-level persistent infections in the spleen. By 3 weeks postvaccination the animals were protected against the establishment of persistent virus as well as acute splenomegaly. The timing of this complete protection correlated with the presence of both virus-neutralizing antibodies and primed CTL in the immunized mice. Within 3 days of virus challenge, vaccinated mice showed high levels of activated B cells and CD4 + and CD8 + T cells, indicating an efficient priming of all lymphocyte subsets. Despite very limited replication of the vaccine virus, the protective effect was long lived and was still present 6 months after immunization.

Published

1999

39. 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

40. Levels of Abnormal Prion Protein in Deer and Elk with Chronic Wasting Disease

Author

Kimberly Meade-White, Elizabeth S. Williams, Anne Ward, Jean E. Jewell, Michael W. Miller, Richard E. Race, Bruce Chesebro, and Brent Race

Subjects

Microbiology (medical), Colorado, CWD, Prions, Epidemiology, animal diseases, Palatine Tonsil, lcsh:Medicine, Scrapie, Spleen, Disease, Biology, immunoblot analysis, lcsh:Infectious and parasitic diseases, Pathogenesis, prion, fluids and secretions, parasitic diseases, medicine, Animals, lcsh:RC109-216, Prion protein, cervids, lymphoid tissue, elk, Montana, Transmission (medicine), Research, pathogenesis, chronic wasting disease, lcsh:R, Brain, Chronic wasting disease, medicine.disease, Virology, Infectious Diseases, medicine.anatomical_structure, Animals, Domestic, Tonsil, Immunology, surveillance, deer, Wasting Disease, Chronic, Lymph Nodes

Abstract

Infected deer may pose a higher risk than elk for disease transmission., Chronic wasting disease (CWD) of deer and elk is a widespread health concern because its potential for cross-species transmission is undetermined. CWD prevalence in wild elk is much lower than its prevalence in wild deer, and whether CWD-infected deer and elk differ in ability to infect other species is unknown. Because lymphoid tissues are important in the pathogenesis of some transmissible spongiform encephalopathies such as sheep scrapie, we investigated whether CWD-affected elk and deer differ in distribution or quantity of disease-associated prion protein (PrPres) in lymphoid tissues. Immunoblot quantification of PrPres from tonsil and retropharyngeal lymph nodes showed much higher levels of PrPres in deer than in elk. This difference correlated with the natural prevalence of CWD in these species and suggested that CWD-infected deer may be more likely than elk to transmit the disease to other cervids and have a greater potential to transmit CWD to noncervids.

Published

2007