Your search keyword '"PRION DISEASE"' showing total 2,384 results

201. Generation of human chronic wasting disease in transgenic mice.

Author

Wang, Zerui, Qin, Kefeng, Camacho, Manuel V., Cali, Ignazio, Yuan, Jue, Shen, Pingping, Greenlee, Justin, Kong, Qingzhong, Mastrianni, James A., and Zou, Wen-Quan

Subjects

*PRIONS, *TRANSGENIC mice, *BOVINE spongiform encephalopathy, *PRION diseases, *CHRONIC wasting disease, *CREUTZFELDT-Jakob disease, *ANIMAL diseases, *VACCINATION

Abstract

Chronic wasting disease (CWD) is a cervid prion disease caused by the accumulation of an infectious misfolded conformer (PrPSc) of cellular prion protein (PrPC). It has been spreading rapidly in North America and also found in Asia and Europe. Although bovine spongiform encephalopathy (i.e. mad cow disease) is the only animal prion disease known to be zoonotic, the transmissibility of CWD to humans remains uncertain. Here we report the generation of the first CWD-derived infectious human PrPSc by elk CWD PrPSc-seeded conversion of PrPC in normal human brain homogenates using in vitro protein misfolding cyclic amplification (PMCA). Western blotting with human PrP selective antibody confirmed that the PMCA-generated protease-resistant PrPSc was derived from the human PrPC substrate. Two lines of humanized transgenic mice expressing human PrP with either Val or Met at the polymorphic codon 129 developed clinical prion disease following intracerebral inoculation with the PMCA-generated CWD-derived human PrPSc. Diseased mice exhibited distinct PrPSc patterns and neuropathological changes in the brain. Our study, using PMCA and animal bioassays, provides the first evidence that CWD PrPSc can cross the species barrier to convert human PrPC into infectious PrPSc that can produce bona fide prion disease when inoculated into humanized transgenic mice. [ABSTRACT FROM AUTHOR]

Published

2021

202. Chronic wasting disease: a cervid prion infection looming to spillover.

Author

Otero, Alicia, Velásquez, Camilo Duque, Aiken, Judd, and McKenzie, Debbie

Abstract

The spread of chronic wasting disease (CWD) during the last six decades has resulted in cervid populations of North America where CWD has become enzootic. This insidious disease has also been reported in wild and captive cervids from other continents, threatening ecosystems, livestock and public health. These CWD "hot zones" are particularly complex given the interplay between cervid PRNP genetics, the infection biology, the strain diversity of infectious prions and the long-term environmental persistence of infectivity, which hinder eradication efforts. Here, we review different aspects of CWD including transmission mechanisms, pathogenesis, epidemiology and assessment of interspecies infection. Further understanding of these aspects could help identify "control points" that could help reduce exposure for humans and livestock and decrease CWD spread between cervids. [ABSTRACT FROM AUTHOR]

Published

2021

203. Pneumonia initiates a tauopathy.

Author

Balczon, Ron, Lin, Mike T., Lee, Ji Young, Abbasi, Adeel, Renema, Phoibe, Voth, Sarah B., Zhou, Chun, Koloteva, Anna, Michael Francis, C., Sodha, Neel R., Pittet, Jean‐Francois, Wagener, Brant M., Bell, Jessica, Choi, Chung‐Sik, Ventetuolo, Corey E., and Stevens, Troy

Abstract

Pneumonia causes short‐ and long‐term cognitive dysfunction in a high proportion of patients, although the mechanism(s) responsible for this effect are unknown. Here, we tested the hypothesis that pneumonia‐elicited cytotoxic amyloid and tau variants: (1) are present in the circulation during infection; (2) lead to impairment of long‐term potentiation; and, (3) inhibit long‐term potentiation dependent upon tau. Cytotoxic amyloid and tau species were recovered from the blood and the hippocampus following pneumonia, and they were present in the extracorporeal membrane oxygenation oxygenators of patients with pneumonia, especially in those who died. Introduction of immunopurified blood‐borne amyloid and tau into either the airways or the blood of uninfected animals acutely and chronically impaired hippocampal information processing. In contrast, the infection did not impair long‐term potentiation in tau knockout mice and the amyloid‐ and tau‐dependent disruption in hippocampal signaling was less severe in tau knockout mice. Moreover, the infection did not elicit cytotoxic amyloid and tau variants in tau knockout mice. Therefore, pneumonia initiates a tauopathy that contributes to cognitive dysfunction. [ABSTRACT FROM AUTHOR]

Published

2021

204. Evolution of Transmissible Spongiform Encephalopathies and the Prion Protein Gene (PRNP) in Mammals.

Author

Buchanan, Brittaney L. and Zink, Robert M.

Subjects

*BOVINE spongiform encephalopathy, *BRAIN diseases, *NUCLEOTIDES, *AMINO acids, *GENOTYPES

Abstract

Transmissible spongiform encephalopathies (TSEs) are currently incurable, always fatal, and have the potential to cross species boundaries. The expression of TSEs is thought to be influenced by genetic variation at the prion protein gene (PRNP). Although a wide range of mammals exhibit TSEs, it is currently unclear whether they are evolutionarily clustered or if TSE+ species are randomly distributed phylogenetically. We tested whether mammalian species with TSEs are phylogenetically underdispersed on three phylogenetic trees, one constructed from 20 aligned gene sequences for 102 taxa (a species tree), and PRNP gene trees from nucleotide and from amino acid sequence variation. TSEs were present in a variety of orders excluding Chiroptera, Eulipotyphyla, and Lagomorpha, and cetaceans. The occurrence of TSEs on the PRNP and species trees is non-random (Species tree D-value = 0.291; PRNP tree D-value = 0.273; PRNP amino acid tree D-value = 0.238), and TSEs appears to have arisen independently in the recent history of different mammalian groups. We found no evidence that particular protein motifs segregated between species with or without TSEs. Our findings suggest that the evolution of TSEs develops in groups of species irrespective of PRNP genotype. [ABSTRACT FROM AUTHOR]

Published

2021

205. Use of a 2-aminothiazole to Treat Chronic Wasting Disease in Transgenic Mice

Author

Berry, David, Giles, Kurt, Oehler, Abby, Bhardwaj, Sumita, DeArmond, Stephen J, and Prusiner, Stanley B

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Health Sciences, Rare Diseases, Brain Disorders, Transmissible Spongiform Encephalopathy (TSE), Infectious Diseases, Neurodegenerative, Emerging Infectious Diseases, Neurosciences, Aetiology, 2.1 Biological and endogenous factors, Neurological, Animals, Brain, Cell Line, Deer, Drug Resistance, Female, Kaplan-Meier Estimate, Mice, Mice, Transgenic, Prions, Rabbits, Scrapie, Sheep, Thiazoles, Wasting Disease, Chronic, chronic wasting disease, therapeutic, prion disease, transgenic mice, survival extension, Medical and Health Sciences, Microbiology, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Treatment with the 2-aminothiazole IND24 extended the survival of mice infected with mouse-adapted scrapie but also resulted in the emergence of a drug-resistant prion strain. Here, we determined whether IND24 extended the survival of transgenic mice infected with prions that caused scrapie in sheep or prions that caused chronic wasting disease (CWD; hereafter "CWD prions") in deer, using 2 isolates for each disease. IND24 doubled the incubation times for mice infected with CWD prions but had no effect on the survival of those infected with scrapie prions. Biochemical, neuropathologic, and cell culture analyses were used to characterize prion strain properties following treatment, and results indicated that the CWD prions were not altered by IND24, regardless of survival extension. These results suggest that IND24 may be a viable candidate for treating CWD in infected captive cervid populations and raise questions about why some prion strains develop drug resistance whereas others do not.

Published

2015

206. Epidemiological and Clinical Characteristics of Sporadic Creutzfeldt–Jakob Disease: A Retrospective Study in Eastern China

Author

Shuo Feng, Xinjing Zhao, Xueying Zhou, Xiang Ye, Xiaolin Yu, Wei Jiang, Yu Deng, Shengnian Zhou, Lin Ma, Peiyan Shan, and Guoyu Zhou

Subjects

prion disease, sporadic CJD, clinical, survival time, eastern China, Neurology. Diseases of the nervous system, RC346-429

Abstract

Objective: We aimed to characterize the epidemiological and clinical characteristics of sporadic Creutzfeldt–Jakob disease (sCJD) in eastern China in this retrospective study.Methods: This study enrolled 67 patients with sCJD hospitalized in a grade-A tertiary hospital in eastern China from January 2010 to January 2020. Demographic data, clinical symptoms, brain magnetic resonance imaging (MRI), electroencephalogram (EEG), cerebrospinal fluid (CSF) 14-3-3 protein test, polymerase chain reaction (PCR), and DNA sequence determination of genes were collected and analyzed.Results: There were 62 patients with probable sCJD and 5 patients with possible sCJD. Male (28 cases) to female (39 cases) ratio was 1:1.39. Mean age at disease onset was 64.42 ± 9.00 years (range: 29–88 years), and mean survival time was 9.39 ± 12.58 months (range: 1–60 months for patients who received the follow-ups). The most common onset symptoms were dementia (49.25%), movement disorder (44.78%), and visual disturbance (22.39%), while the most frequent clinical manifestations were language disorders (74.63%), ataxia (70.15%), and myoclonus (70.15%). The positive rates of brain MRI abnormalities, 14-3-3 protein in CSF, and periodic sharp wave complexes (PSWCs) on EEG were 84.90, 68.00, and 46.03%, respectively. The 14-3-3 protein positive (p = 0.033) and PSWCs on EEG (p = 0.020) acted as the favorable and unfavorable factor for over 1 year of survival time, respectively.Conclusions: There were some differences in epidemiological and clinical characteristics among patients in China and those of other countries. The prognosis and its influencing factors were relatively unexplored in China. The mean survival time of Chinese patients was longer than that of Caucasian patients but shorter than that of Japanese patients. The 14-3-3 protein in CSF and PSWCs on EEG were both closely related to the survival time. It is necessary to promote autopsy or biopsy to better understand sCJD in China.

Published

2021

207. Amino Acid Substitution within Seven-Octapeptide Repeat Insertions in the Prion Protein Gene Associated with Short-Term Course

Author

Zhongyun Chen, Haitian Nan, Yu Kong, Min Chu, Li Liu, Jing Zhang, Lin Wang, and Liyong Wu

Subjects

Creutzfeldt–Jakob disease, genetics, prion disease, octapeptide repeat insertion, amino acid substitution, Microbiology, QR1-502

Abstract

The majority of seven-octapeptide repeat insertion (7-OPRI) carriers exhibit relatively early onset and a slowly progressive course. We have presented three cases of 7-OPRI, including two that are rapidly progressing, and compared the clinical and ancillary characteristics of the short-term and long-term disease course, as well as factors that influence disease course. The clinical and ancillary features of three new 7-OPRI patients in a Chinese pedigree were analyzed. Global data on 7-OPRI cases were then collected by reviewing the literature, and the cases were grouped according to clinical duration as per the WHO sCJD criteria, with a two-year cut-off. A Chinese pedigree has a glycine-to-glutamate substitution within the 7-OPRI insertion, which enhances the hydrophilicity of the prion protein. Two cases in this pedigree had a short disease course (consistent with the typical clinical and ancillary features of sCJD). In addition, the members of this pedigree had a later onset (p < 0.001) and shorter disease course (p < 0.001) compared to previously reported 7-OPRI cases with 129 cis-M and a similar age of onset and disease course to that of cases with 129 cis-V. The 7-OPRI cases with a shorter clinical course (n = 4) had a later onset (p = 0.021), higher rate of hyperintensity on MRI (p = 0.029) and higher frequency of 129 cis-V (p = 0.066) compared to those with a longer clinical course (n = 13). The clinical presentation of 7-OPRI is significantly heterogeneous. Codon 129 cis-V and amino acid substitution within repeat insertions are possible contributors to the short-term disease course of 7-OPRI.

Published

2022

208. Biochemical and Neuropathological Findings in a Creutzfeldt–Jakob Disease Patient with the Rare Val180Ile-129Val Haplotype in the Prion Protein Gene

Author

Gianluigi Zanusso, Elisa Colaizzo, Anna Poleggi, Carlo Masullo, Raffaello Romeo, Sergio Ferrari, Matilde Bongianni, Michele Fiorini, Dorina Tiple, Luana Vaianella, Marco Sbriccoli, Flavia Porreca, Michele Equestre, Maurizio Pocchiari, Franco Cardone, and Anna Ladogana

Subjects

Creutzfeldt–Jakob disease, prion disease, neuropathology, prion protein, Val180Ile mutation, RT-QuIC assay, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Genetic Creutzfeldt–Jakob disease (gCJD) associated with the V180I mutation in the prion protein (PrP) gene (PRNP) in phase with residue 129M is the most frequent cause of gCJD in East Asia, whereas it is quite uncommon in Caucasians. We report on a gCJD patient with the rare V180I-129V haplotype, showing an unusually long duration of the disease and a characteristic pathological PrP (PrPSc) glycotype. Family members carrying the mutation were fully asymptomatic, as commonly observed with this mutation. Neuropathological examination showed a lesion pattern corresponding to that commonly reported in Japanese V180I cases with vacuolization and gliosis of the cerebral cortexes, olfactory areas, hippocampus and amygdala. PrP was deposited with a punctate, synaptic-like pattern in the cerebral cortex, amygdala and olfactory tract. Western blot analyses of proteinase-K-resistant PrP showed the characteristic two-banding pattern of V180I gCJD, composed of mono- and un-glycosylated isoforms. In line with reports on other V180I cases in the literature, Real-Time Quaking Induced Conversion (RT-QuIC) analyses did not demonstrate the presence of seeding activity in the cerebrospinal fluid and olfactory mucosa, suggesting that this haplotype also may result in a reduced seeding efficiency of the pathological PrP. Further studies are required to understand the origin, penetrance, disease phenotype and transmissibility of 180I-129V haplotype in Caucasians.

Published

2022

209. Impairment of Neuronal Mitochondrial Quality Control in Prion-Induced Neurodegeneration

Author

Mo-Jong Kim, Hee-Jun Kim, Byungki Jang, Hyun-Ji Kim, Mohd Najib Mostafa, Seok-Joo Park, Yong-Sun Kim, and Eun-Kyoung Choi

Subjects

prion disease, dynamin-related protein 1, mitochondrial quality control, mitochondrial fission, mitophagy, neurodegeneration, Cytology, QH573-671

Abstract

Mitochondrial dynamics continually maintain cell survival and bioenergetics through mitochondrial quality control processes (fission, fusion, and mitophagy). Aberrant mitochondrial quality control has been implicated in the pathogenic mechanism of various human diseases, including cancer, cardiac dysfunction, and neurological disorders, such as Alzheimer’s disease, Parkinson’s disease, and prion disease. However, the mitochondrial dysfunction-mediated neuropathological mechanisms in prion disease are still uncertain. Here, we used both in vitro and in vivo scrapie-infected models to investigate the involvement of mitochondrial quality control in prion pathogenesis. We found that scrapie infection led to the induction of mitochondrial reactive oxygen species (mtROS) and the loss of mitochondrial membrane potential (ΔΨm), resulting in enhanced phosphorylation of dynamin-related protein 1 (Drp1) at Ser616 and its subsequent translocation to the mitochondria, which was followed by excessive mitophagy. We also confirmed decreased expression levels of mitochondrial oxidative phosphorylation (OXPHOS) complexes and reduced ATP production by scrapie infection. In addition, scrapie-infection-induced aberrant mitochondrial fission and mitophagy led to increased apoptotic signaling, as evidenced by caspase 3 activation and poly (ADP-ribose) polymerase cleavage. These results suggest that scrapie infection induced mitochondrial dysfunction via impaired mitochondrial quality control processes followed by neuronal cell death, which may have an important role in the neuropathogenesis of prion diseases.

Published

2022

210. Prion strains associated with iatrogenic CJD in French and UK human growth hormone recipients.

Author

Douet, Jean-Yves, Huor, Alvina, Cassard, Hervé, Lugan, Séverine, Aron, Naïma, Mesic, Chloé, Vilette, Didier, Barrio, Tomás, Streichenberger, Nathalie, Perret-Liaudet, Armand, Delisle, Marie-Bernadette, Péran, Patrice, Deslys, Jean-Philippe, Comoy, Emmanuel, Vilotte, Jean-Luc, Goudarzi, Katayoun, Béringue, Vincent, Barria, Marcelo A., Ritchie, Diane L., and Ironside, James W.

Subjects

*CREUTZFELDT-Jakob disease, *HUMAN growth hormone, *PRIONS, *LABORATORY mice, *IATROGENIC diseases

Abstract

Treatment with human pituitary-derived growth hormone (hGH) was responsible for a significant proportion of iatrogenic Creutzfeldt–Jakob disease (iCJD) cases. France and the UK experienced the largest case numbers of hGH-iCJD, with 122 and 81 cases respectively. Differences in the frequency of the three PRNP codon 129 polymorphisms (MM, MV and VV) and the estimated incubation periods associated with each of these genotypes in the French and the UK hGH-iCJD cohorts led to the suggestion that the prion strains responsible for these two hGH-iCJD cohorts were different. In this study, we characterized the prion strains responsible for hGH-iCJD cases originating from UK (n = 11) and France (n = 11) using human PrP expressing mouse models. The cases included PRNP MM, MV and VV genotypes from both countries. UK and French sporadic CJD (sCJD) cases were included as controls. The prion strains identified following inoculation with hGH-iCJD homogenates corresponded to the two most frequently observed sCJD prion strains (M1CJD and V2CJD). However, in clear contradiction to the initial hypothesis, the prion strains that were identified in the UK and the French hGH-iCJD cases were not radically different. In the vast majority of the cases originating from both countries, the V2CJD strain or a mixture of M1CJD + V2CJD strains were identified. These data strongly support the contention that the differences in the epidemiological and genetic profiles observed in the UK and France hGH-iCJD cohorts cannot be attributed only to the transmission of different prion strains. [ABSTRACT FROM AUTHOR]

Published

2021

211. Volatile Anesthetic Sevoflurane Precursor 1,1,1,3,3,3-Hexafluoro-2-Propanol (HFIP) Exerts an Anti-Prion Activity in Prion-Infected Culture Cells.

Author

Shimizu, Takuto, Nogami, Emiko, Ito, Yuka, Morikawa, Kazuo, Nagane, Masaki, Yamashita, Tadashi, Ogawa, Tsuyoshi, Kametani, Fuyuki, Yagi, Hisashi, and Hachiya, Naomi

Subjects

*CELL culture, *PRION diseases, *PRIONS, *SEVOFLURANE, *ANESTHETICS, *SYMPTOMS

Abstract

Prion disease is a neurodegenerative disorder with progressive neurologic symptoms and accelerated cognitive decline. The causative protein of prion disease is the prion protein (PrP), and structural transition of PrP from the normal helix rich form (PrPC) to the abnormal β-sheet rich form (PrPSc) occurs in prion disease. While so far numerous therapeutic agents for prion diseases have been developed, none of them are still useful. A fluorinated alcohol, hexafluoro isopropanol (HFIP), is a precursor to the inhalational anesthetic sevoflurane and its metabolites. HFIP is also known as a robust α-helix inducer and is widely used as a solvent for highly aggregated peptides. Here we show that the α-helix-inducing activity of HFIP caused the conformational transformation of the fibrous structure of PrP into amorphous aggregates in vitro. HFIP added to the ScN2a cell medium, which continuously expresses PrPSc, reduced PrPSc protease resistance after 24-h incubation. It was also clarified that ScN2a cells are more susceptible to HFIP than any of the cells being compared. Based on these findings, HFIP is expected to develop as a therapeutic agent for prion disease. [ABSTRACT FROM AUTHOR]

Published

2021

212. Prion disease in Indigenous Australians.

Author

Panegyres, Peter K., Stehmann, Christiane, Klug, Genevieve M., Masters, Colin L., and Collins, Steven

Subjects

*INDIGENOUS Australians, *PRION diseases, *CONFIDENCE intervals, *CREUTZFELDT-Jakob disease, *TERMINALLY ill, *DISEASE incidence, *DESCRIPTIVE statistics, *DISEASE duration, *PHENOTYPES

Abstract

Background: Indigenous Australians are at increased risk of developing dementia – Alzheimer disease and mixed dementia diagnoses are the most common. While prion diseases have been reported in Indigenous peoples of Papua New Guinea and the United States, the occurrence and phenotype of prion disease in Indigenous Australians is hitherto unreported. Aim: To report the incidence rate and clinical phenotype of Creutzfeldt‐Jakob disease (CJD) in Indigenous Australians. Method: Crude sporadic CJD (sCJD) incidence rates and indirect age standardisation of all CJD were assessed to calculate the standardised mortality ratio (SMR) of the Indigenous Australian population in comparison to the all‐resident Australian population, along with analysis of clinical phenotypes. Results: We report an illustrative case of an Indigenous Australian from regionally remote Western Australia dying from typical 'probable' sCJD 2 months after disease onset, with Australian National CJD Registry (ANCJDR) surveillance overall demonstrating eight Indigenous Australians dying from sCJD (five post‐mortem confirmed, three classified as 'probable') with a clinical phenotype similar to non‐indigenous people, including median age at death of 61 years (interquartile range IQR = 16 years) and median duration of illness of 3 months (IQR = 1.6 months). Indigenous Australians with sCJD were geographically dispersed throughout Australia. The calculated overall crude annual rate of sCJD in Indigenous Australians compared to the remainder of the Australian population was not significantly different (0–3.87/million for Indigenous Australians; 0.94–1.83/million for non‐indigenous). The overall indirect age‐standardised CJD mortality ratio for the indigenous population for the years 2006–2018 was 1.49 (95% CI, 0.75–2.98), also not significantly different to the all‐resident Australian population. Conclusion: CJD occurs in Indigenous Australians with clinical phenotype and occurrence rates similar to non‐Indigenous Australians. These findings contrast with a previous report where the incidence rate of CJD in a non‐Australian indigenous population was reported to be decreased. [ABSTRACT FROM AUTHOR]

Published

2021

213. Place de la biologie dans les maladies de Creutzfeldt-Jakob et apparentées.

Author

Kaczorowski, Flora, Perret-Liaudet, Armand, Verdurand, Mathieu, and Quadrio, Isabelle

Abstract

Les maladies à prions sont des maladies neurodégénératives rares d'issue toujours fatale. Elles sont caractérisées par l'accumulation principalement cérébrale d'une isoforme pathologique (PrPsc) d'une protéine cellulaire normale, la PrPc. Du fait de leur caractère transmissible d'homme à homme et animal-homme, ces maladies sont étroitement surveillées par les autorités de santé et à déclaration obligatoire dès leur suspicion. Leur diagnostic est donc un enjeu majeur de santé publique alors même que le diagnostic de certitude reste l'examen neuropathologique, très majoritairement réalisé en post-mortem. Les marqueurs biologiques jouent un rôle important dans la démarche diagnostique du vivant du patient et dans la surveillance de ces maladies. En effet, la détection de la protéine 1433 dans le liquide cérébrospinal (LCS), marqueur non étiologique, permet d'augmenter la probabilité diagnostique. De nombreux efforts ont été menés pour mesurer directement la PrPsc dans les fluides biologiques. Seuls des progrès technologiques récents reposant sur des méthodes innovantes d'amplification des protéines ont permis de la mesurer dans le LCS. Cependant, ces technologies nécessitent une mise en œuvre dans des environnements de sécurité microbiologique de niveau 3. Ces techniques d'avenir, réservées à des centres de référence experts, sont de réalisation délicate, manquent de robustesse et de standardisation avant de pouvoir être proposées comme outils diagnostiques en pratique courante. Prion diseases are fatal neurodegenerative disorders which are characterized by aggregations of a misfolded protein (called PrPsc) coming from its cellular isoform PrPc, mainly in brain tissue. Due to the transmissibility of this agent, every suspected case has to be monitored and reported to health authorities. Prion diseases diagnosis is a major public health issue, while the definite diagnostic is still based on post-mortem neuropathological examination. CSF biomarkers are an integral part of the diagnostic criteria and are important for the disease surveillance. The 14-3-3 detection is the first CSF surrogate biomarker helping in probable CJD classification. Despite many efforts for specific PrPsc detection, only recent technological development of assays based on protein amplification allowed to detect it in the CSF. However, reference centers have to manage this innovative technology in high security facilities (level 3). Then, nowadays, these protein amplification assays need to be optimized and standardized before their use in current practice. [ABSTRACT FROM AUTHOR]

Published

2021

214. Sporadic Creutzfeldt-Jakob disease: a case report of long disease duration and difficulties in confirming the diagnosis with short literature review.

Author

Stanowska, Anna Karolina, Wach, Barbara, Herman-Sucharska, Izabela, and Adamek, Dariusz

Abstract

Creutzfeldt-Jakob disease (CJD) is a spongiform encephalopathy with the fatal outcome, caused by the accumulation of pathological prion protein in the central nervous system (CNS). CJD is classified into four types: sporadic (sCJD), familial or genetic (fCJD), iatrogenic (iCJD) and variant form (vCJD). The recognition of CJD is based on the clinical presentation, neuroimaging, electroencephalography and biochemical tests. The hyperintense signals in basal ganglia on brain magnetic resonance imaging (MRI), periodic sharp and slow wave complexes (PSWCs) in the electroencephalogram as well as presence of neuronal proteins such as protein 14-3-3 in the cerebrospinal fluid (CSF) support the diagnosis. The definite diagnosis of CJD still demands neuropathological confirmation. We report the case of a 56-year-old woman with the rapidly progressive cognitive impairment, motor dysfunctions and the fulminant neurological deterioration to akinetic mutism during the five weeks' hospitalisation. The probable diagnosis of sCJD was based on medical history and characteristic findings in MRI. The positive result of the real-time quaking-induced conversion (RT-QuIC) test and presence of protein 14-3-3 were obtained post-mortem and definite diagnosis was confirmed by neuropathological examination. In this paper we would like to emphasize the difficulties in reaching the diagnosis and the need for a series of diagnostic examinations in different points of time to obtain the confirming results. [ABSTRACT FROM AUTHOR]

Published

2021

215. The role of macrophage scavenger receptor 1 (Msr1) in prion pathogenesis.

Author

Li, Bei, Chen, Meiling, Aguzzi, Adriano, and Zhu, Caihong

Subjects

*PRIONS, *MACROPHAGES, *PRION diseases, *PHAGOCYTOSIS, *DISEASE progression

Abstract

The progression of prion diseases is accompanied by the accumulation of prions in the brain. Ablation of microglia enhances prion accumulation and accelerates disease progression, suggesting that microglia play a neuroprotective role by clearing prions. However, the mechanisms underlying the phagocytosis and clearance of prion are largely unknown. The macrophage scavenger receptor 1 (Msr1) is an important phagocytic receptor expressed by microglia in the brain and is involved in the uptake and clearance of soluble amyloid-β. We therefore asked whether Msr1 might play a role in prion clearance and assessed the scavenger function of Msr1 in prion pathogenesis. We found that Msr1 expression was upregulated in prion-infected mouse brains. However, Msr1 deficiency did not change prion disease progression or lesion patterns. Prion deposition in Msr1 deficient mice was similar to their wild-type littermates. In addition, prion-induced neuroinflammation was not affected by Msr1 ablation. We conclude that Msr1 does not play a major role in prion pathogenesis. Key messages: Msr1 expression is upregulated in prion-infected mouse brains at the terminal stage Msr1 deficiency does not affect prion disease progression Msr1 does not play a major role in prion clearance or prion pathogenesis Microglia-mediated phagocytosis and clearance of Aβ and prion may adopt distinct molecular pathways [ABSTRACT FROM AUTHOR]

Published

2021

216. An individual-based model for direct and indirect transmission of chronic wasting disease in free-ranging white-tailed deer.

Author

Thompson, Noelle E, Butts, David J, Murillo, Michael S, O'Brien, Daniel J, Christensen, Sonja A, Porter, William F, and Roloff, Gary J

Subjects

*CHRONIC wasting disease, *WHITE-tailed deer, *DEER populations, *PRION diseases, *DEER behavior, *CERVIDAE

Abstract

• Our model reproduced trends in prevalence reported by state wildlife agencies. • One infected deer led to an outbreak of CWD in 29 % of introduction events. • CWD outbreaks are likely to persist once prevalence reaches 1.5 %. • CWD prevalence is most sensitive to female yearling and adult deer harvest rates. • Deer population parameters are more influential than disease parameters on CWD. Chronic wasting disease (CWD) is an infectious prion disease that infects members of the Cervidae family (i.e., deer) resulting in widespread ecological, economic, and recreational ramifications. We introduce a spatially explicit individual-based model (IBM) that integrates individual deer movement and behavior with population and disease dynamics to forecast CWD in populations of free-ranging white-tailed deer (Odocoileus virginianus). We use a Susceptible-Exposed-Infectious-Dead (S-E-I-D) epidemiological framework to explore spatiotemporal dynamics of CWD within an agriculturally dominated area in Michigan, USA. The IBM results closely mimicked documented short- and long-term dynamics of white-tailed deer populations and CWD in the Midwestern, USA. We applied pattern-oriented modeling using annual apparent CWD prevalence rates reported by Midwestern state wildlife agencies to validate the disease model. The introduction of a single infected deer to the modeled landscape (93 km2) led to an outbreak of CWD in 100 out of 350 model simulations (29 %); prevalence never exceeded 1.47 % for repetitions where the outbreak ended. For the 100 simulations where disease persisted, the deer population declined by 87 % by year 50 following initial introduction of CWD. Mean (±SD) prevalence after 5, 10, 25, and 50 years was 1.1 % (±1.0 %), 3.4 % (±3.3 %), 46.5 % (±18.8 %), and 51.8 % (±18.1 %), respectively, which highly correlated (r = 0.99) with annual CWD prevalence reported in Wisconsin white-tailed deer populations for years 1–21 post initial detection. Combined with a global sensitivity analysis, the IBM indicated that prevalence of CWD at year 20 was most sensitive to harvest rate of yearling and adult female deer and least sensitive to prion shedding rate, prion half-life, and deer group numbers, indicating that deer population parameters were more influential than disease parameters on CWD dynamics. Our IBM serves as a tool to explore and better understand indirect and direct transmission of CWD within free-ranging cervid populations. Users of this model can adjust parameter values to explore how interactions among individual deer and between deer and their environment affect CWD dynamics. This IBM also serves as a framework for applying and assessing spatially and temporally explicit management scenarios. [ABSTRACT FROM AUTHOR]

Published

2024

217. Application of quantitative DTI metrics in sporadic CJD.

Author

Caverzasi, E, Henry, RG, Vitali, P, Lobach, IV, Kornak, J, Bastianello, S, Dearmond, SJ, Miller, BL, Rosen, HJ, Mandelli, ML, and Geschwind, MD

Subjects

Brain, Humans, Creutzfeldt-Jakob Syndrome, Image Interpretation, Computer-Assisted, Sensitivity and Specificity, Reproducibility of Results, Aging, Algorithms, Middle Aged, Female, Male, Diffusion Tensor Imaging, Gray Matter, Atrophy, Creutzfeldt–Jakob disease, DWI, MD, Prion disease, sCJD, Creutzfeldt-Jakob disease, Brain Disorders, Clinical Research, Infectious Diseases, Rare Diseases, Acquired Cognitive Impairment, Neurodegenerative, Dementia, Neurosciences, Biomedical Imaging, Transmissible Spongiform Encephalopathy (TSE), Neurological

Abstract

Diffusion Weighted Imaging is extremely important for the diagnosis of probable sporadic Jakob-Creutzfeldt disease, the most common human prion disease. Although visual assessment of DWI MRI is critical diagnostically, a more objective, quantifiable approach might more precisely identify the precise pattern of brain involvement. Furthermore, a quantitative, systematic tracking of MRI changes occurring over time might provide insights regarding the underlying histopathological mechanisms of human prion disease and provide information useful for clinical trials. The purposes of this study were: 1) to describe quantitatively the average cross-sectional pattern of reduced mean diffusivity, fractional anisotropy, atrophy and T1 relaxation in the gray matter (GM) in sporadic Jakob-Creutzfeldt disease, 2) to study changes in mean diffusivity and atrophy over time and 3) to explore their relationship with clinical scales. Twenty-six sporadic Jakob-Creutzfeldt disease and nine control subjects had MRIs on the same scanner; seven sCJD subjects had a second scan after approximately two months. Cortical and subcortical gray matter regions were parcellated with Freesurfer. Average cortical thickness (or subcortical volume), T1-relaxiation and mean diffusivity from co-registered diffusion maps were calculated in each region for each subject. Quantitatively on cross-sectional analysis, certain brain regions were preferentially affected by reduced mean diffusivity (parietal, temporal lobes, posterior cingulate, thalamus and deep nuclei), but with relative sparing of the frontal and occipital lobes. Serial imaging, surprisingly showed that mean diffusivity did not have a linear or unidirectional reduction over time, but tended to decrease initially and then reverse and increase towards normalization. Furthermore, there was a strong correlation between worsening of patient clinical function (based on modified Barthel score) and increasing mean diffusivity.

Published

2014

218. The characterization of AD/PART co-pathology in CJD suggests independent pathogenic mechanisms and no cross-seeding between misfolded Aβ and prion proteins

Author

Marcello Rossi, Hideaki Kai, Simone Baiardi, Anna Bartoletti-Stella, Benedetta Carlà, Corrado Zenesini, Sabina Capellari, Tetsuyuki Kitamoto, and Piero Parchi

Subjects

Creutzfeldt-Jakob disease, Prion disease, Prion strain, Aβ-pathology, Tau-pathology, CAA, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Current evidence indicating a role of the human prion protein (PrP) in amyloid-beta (Aβ) formation or a synergistic effect between Aβ and prion pathology remains controversial. Conflicting results also concern the frequency of the association between the two protein misfolding disorders and the issue of whether the apolipoprotein E gene (APOE) and the prion protein gene (PRNP), the major modifiers of Aβ- and PrP-related pathologies, also have a pathogenic role in other proteinopathies, including tau neurofibrillary degeneration. Here, we thoroughly characterized the Alzheimer’s disease/primary age-related tauopathy (AD/PART) spectrum in a series of 450 cases with definite sporadic or genetic Creutzfeldt-Jakob disease (CJD). Moreover, we analyzed: (i) the effect of variables known to affect CJD pathogenesis and the co-occurring Aβ- and tau-related pathologies; (II) the influence of APOE genotype on CJD pathology, and (III) the effect of AD/PART co-pathology on the clinical CJD phenotype. AD/PART characterized 74% of CJD brains, with 53.3% and 8.2% showing low or intermediate-high levels of AD pathology, and 12.4 and 11.8% definite or possible PART. There was no significant correlation between variables affecting CJD (i.e., disease subtype, prion strain, PRNP genotype) and those defining the AD/PART spectrum (i.e., ABC score, Thal phase, prevalence of CAA and Braak stage), and no difference in the distribution of APOE ε4 and ε2 genotypes among CJD subtypes. Moreover, AD/PART co-pathology did not significantly affect the clinical presentation of typical CJD, except for a tendency to increase the frequency of cognitive symptoms. Altogether, the present results seem to exclude an increased prevalence AD/PART co-pathology in sporadic and genetic CJD, and indicate that largely independent pathogenic mechanisms drive AD/PART and CJD pathology even when they coexist in the same brain.

Published

2019

219. The metabolome identity: basis for discovery of biomarkers in neurodegeneration

Author

Julie-Myrtille Bourgognon and Joern R. Steinert

Subjects

metabolome, neurodegeneration, neuroinflammation, nitric oxide, redox stress, biomarker, misfolded protein, prion disease, Neurology. Diseases of the nervous system, RC346-429

Abstract

Neurodegenerative disorders are often associated with cellular dysfunction caused by underlying protein-misfolding signalling. Numerous neuropathologies are diagnosed at late stage symptomatic changes which occur in response to these molecular malfunctions and treatment is often too late or restricted only to the slowing of further cell death. Important new strategies to identify early biomarkers with predictive value to intervene with disease progression at stages where cell dysfunction has not progressed irreversibly is of paramount importance. Thus, the identification of these markers presents an essential opportunity to identify and target disease pathways. This review highlights some important metabolic alterations detected in neurodegeneration caused by misfolded prion protein and discusses common toxicity pathways identified across different neurodegenerative diseases. Thus, having established some commonalities between various degenerative conditions, detectable metabolic changes may be of extreme value as an early diagnostic biomarker in disease.

Published

2019

220. Variable Protease-Sensitive Prionopathy Transmission to Bank Voles

Author

Romolo Nonno, Silvio Notari, Michele Angelo Di Bari, Ignazio Cali, Laura Pirisinu, Claudia d’Agostino, Laura Cracco, Diane Kofskey, Ilaria Vanni, Jody Lavrich, Piero Parchi, Umberto Agrimi, and Pierluigi Gambetti

Subjects

Variable protease-sensitive prionopathy, VPSPr, prion disease, transmissibility, phenotype, bank voles, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

Variably protease-sensitive prionopathy (VPSPr), a recently described human sporadic prion disease, features a protease-resistant, disease-related prion protein (resPrPD) displaying 5 fragments reminiscent of Gerstmann-Sträussler-Scheinker disease. Experimental VPSPr transmission to human PrP–expressing transgenic mice, although replication of the VPSPr resPrPD profile succeeded, has been incomplete because of second passage failure. We bioassayed VPSPr in bank voles, which are susceptible to human prion strains. Transmission was complete; first-passage attack rates were 5%–35%, and second-passage rates reached 100% and survival times were 50% shorter. We observed 3 distinct phenotypes and resPrPD profiles; 2 imitated sporadic Creutzfeldt-Jakob disease resPrPD, and 1 resembled Gerstmann-Sträussler-Scheinker disease resPrPD. The first 2 phenotypes may be related to the presence of minor PrPD components in VPSPr. Full VPSPr transmission confirms permissiveness of bank voles to human prions and suggests that bank vole PrP may efficiently reveal an underrepresented native strain but does not replicate the complex VPSPr PrPD profile.

Published

2019

221. Bilateral hearing loss as an initial presentation of Creutzfeldt-Jakob disease

Author

Janaina Mariana de Araujo Miranda Brito-Marques, Eduardo Sousa de Melo, Fabíola Lys de Medeiros, Cristiano Sobral de Carvalho, and Paulo Roberto de Brito-Marques

Subjects

dementia, prion disease, hypoacusis, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

ABSTRACT. We reported a case of a 61-year-old male patient with anacusis, cerebellar syndrome, myoclonus, and frontal signs. The brain magnetic resonance imaging showed bilateral striated hyperintensity of the fluid-attenuated inversion recovery and restricted diffusion in the diffusion-weighted imaging and hypointense areas corresponding to the apparent diffusion coefficient in the cerebral cortex. The autopsy revealed positive immunohistochemistry for the PrPSc protein. Creutzfeldt–Jakob disease presenting with hearing loss is unusual.

Published

2021

222. Novel Type of Chronic Wasting Disease Detected in Moose (Alces alces), Norway

Author

Laura Pirisinu, Linh Tran, Barbara Chiappini, Ilaria Vanni, Michele A. Di Bari, Gabriele Vaccari, Turid Vikøren, Knut Ivar Madslien, Jørn Våge, Terry Spraker, Gordon Mitchell, Aru Balachandran, Thierry Baron, Cristina Casalone, Christer M. Rolandsen, Knut H. Røed, Umberto Agrimi, Romolo Nonno, and Sylvie L. Benestad

Subjects

prion disease, transmissible spongiform encephalopathies, chronic wasting disease, cervid, moose, zoonoses, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

Chronic wasting disease (CWD) persists in cervid populations of North America and in 2016 was detected for the first time in Europe in a wild reindeer in Norway. We report the detection of CWD in 3 moose (Alces alces) in Norway, identified through a large scale surveillance program. The cases occurred in 13–14-year-old female moose, and we detected an abnormal form of prion protein (PrPSc) in the brain but not in lymphoid tissues. Immunohistochemistry revealed that the moose shared the same neuropathologic phenotype, characterized by mostly intraneuronal deposition of PrPSc. This pattern differed from that observed in reindeer and has not been previously reported in CWD-infected cervids. Moreover, Western blot revealed a PrPSc type distinguishable from previous CWD cases and from known ruminant prion diseases in Europe, with the possible exception of sheep CH1641. These findings suggest that these cases in moose represent a novel type of CWD.

Published

2018

223. Real-Time Quaking-Induced Conversion Detection of PrPSc in Fecal Samples From Chronic Wasting Disease Infected White-Tailed Deer Using Bank Vole Substrate

Author

Soyoun Hwang, Justin J. Greenlee, and Eric M. Nicholson

Subjects

CWD, prion disease, RT-QuIC, transmissible spongiform encephalopathy, TSE, feces, Veterinary medicine, SF600-1100

Abstract

Chronic wasting disease (CWD) is a transmissible spongiform encephalopathy (TSE) that is fatal to free-range and captive cervids. CWD has been reported in the United States, Canada, South Korea, Norway, Finland, and Sweden, and the case numbers in both wild and farmed cervids are increasing rapidly. Studies indicate that lateral transmission of cervids likely occurs through the shedding of infectious prions in saliva, feces, urine, and blood into the environment. Therefore, the detection of CWD early in the incubation time is advantageous for disease management. In this study, we adapt real-time quacking-induced conversion (RT-QuIC) assays to detect the seeding activity of CWD prions in feces samples from clinical and preclinical white-tailed deer. By optimizing reaction conditions for temperature as well as the salt and salt concentration, prion seeding activity from both clinical and preclinical animals were detected by RT-QuIC. More specifically, all fecal samples collected from 6 to 30 months post inoculation showed seeding activity under the conditions of study. The combination of a highly sensitive detection tool paired with a sample type that may be collected non-invasively allows a useful tool to support CWD surveillance in wild and captive cervids.

Published

2021

224. Cerebrospinal Fluid and Blood Neurofilament Light Chain Protein in Prion Disease and Other Rapidly Progressive Dementias: Current State of the Art

Author

Samir Abu-Rumeileh and Piero Parchi

Subjects

Creutzfeldt-Jakob disease, prion disease, neurofilament light chain, Alzheimer’s disease, frontotemporal dementia, encephalitis, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Rapidly progressive dementia (RPD) is an umbrella term referring to several conditions causing a rapid neurological deterioration associated with cognitive decline and short disease duration. They comprise Creutzfeldt–Jakob disease (CJD), the archetypal RPD, rapidly progressive variants of the most common neurodegenerative dementias (NDs), and potentially treatable conditions such as infectious or autoimmune encephalitis and cerebrovascular disease. Given the significant clinical and, sometimes, neuroradiological overlap between these different disorders, biofluid markers also contribute significantly to the differential diagnosis. Among them, the neurofilament light chain protein (NfL) has attracted growing attention in recent years as a biofluid marker of neurodegeneration due to its sensitivity to axonal damage and the reliability of its measurement in both cerebrospinal fluid (CSF) and blood. Here, we summarize current knowledge regarding biological and clinical implications of NfL evaluation in biofluids across RPDs, emphasizing CJD, and other prion diseases. In the latter, NfL demonstrated a good diagnostic and prognostic accuracy and a potential value as a marker of proximity to clinical onset in pre-symptomatic PRNP mutation carriers. Similarly, in Alzheimer’s disease and other NDs, higher NfL concentrations seem to predict a faster disease progression. While increasing evidence indicates a potential clinical value of NfL in monitoring cerebrovascular disease, the association between NfL and prediction of outcome and/or disease activity in autoimmune encephalitis and infectious diseases has only been investigated in few cohorts and deserves confirmatory studies. In the era of precision medicine and evolving therapeutic options, CSF and blood NfL might aid the diagnostic and prognostic assessment of RPDs and the stratification and management of patients according to disease progression in clinical trials.

Published

2021

225. Sporadic Creutzfeldt-Jakob disease in two clinically and virologically controlled Brazilian HIV patients who progressed rapidly to dementia: case reports and literature review

Author

Flávia Esper Dahy, Christina T. G. Novaes, Gabriela A. Bandeira, Laís F. Ramin, Augusto César Penalva de Oliveira, and Jerusa Smid

Subjects

HIV, Dementia, Prion disease, Creutzfeldt-Jakob disease, HAND, Arctic medicine. Tropical medicine, RC955-962, Infectious and parasitic diseases, RC109-216

Abstract

ABSTRACT Human immunodeficiency virus (HIV)-associated neurocognitive disorders are the main cause of cognitive decline and dementia in people living with HIV (PLHIV). However, extensive workup should be done in patients with rapidly progressive dementia (RPD) and HIV, especially when secondary infection in the central nervous system (CNS) is ruled out. Sporadic Creutzfeldt-Jakob disease (sCJD) is the main cause of RPD in non-HIV patients. It is a fatal neurodegenerative condition caused by prions that mainly affects elderly patients. Our objective is to describe two cases of PLHIV presenting with controlled infections and sCJD, and to review the literature. Our patients were younger than expected for sCJD and one of them had a longer disease course. As aging is expected to occur earlier in PLHIV, sCJD must be excluded in younger PLHIV presenting with RPD and without CNS infection.

Published

2021

226. Prion Diseases

Author

Whitechurch, Benjamin C., Welton, Jeremy M., Collins, Steven J., Lawson, Victoria A., Schousboe, Arne, Series editor, Beart, Philip, editor, Robinson, Michael, editor, Rattray, Marcus, editor, and Maragakis, Nicholas J., editor

Published

2017

227. Link Between Metal Homeostasis and Neurodegenerative Diseases: Crosstalk of Metals and Amyloidogenic Proteins at the Synapse

Author

Mizuno, Dai, Kawahara, Masahiro, Ogra, Yasumitsu, editor, and Hirata, Takafumi, editor

Published

2017

228. Prion Disorders

Author

Gore, Ethan, Appleby, Brian S., Tousi, Babak, editor, and Cummings, Jeffrey, editor

Published

2017

229. Early detection of prion protein aggregation with a fluorescent pentameric oligothiophene probe using spectral confocal microscopy.

Author

Stepanchuk, Anastasiia, Tahir, Waqas, Nilsson, K. Peter R., Schatzl, Hermann M., and Stys, Peter K.

Subjects

*FLUORESCENT proteins, *BOVINE spongiform encephalopathy, *PRIONS, *CONFOCAL microscopy, *CHRONIC wasting disease, *AMYLOID beta-protein, *THIOPHENES

Abstract

Misfolding of the prion protein (PrP) and templating of its pathological conformation onto cognate proteins causes a number of lethal disorders of central nervous system in humans and animals, such as Creutzfeldt–Jacob disease, chronic wasting disease and bovine spongiform encephalopathy. Structural rearrangement of PrPC into PrPSc promotes aggregation of misfolded proteins into β‐sheet‐rich fibrils, which can be visualized by conformationally sensitive fluorescent probes. Early detection of prion misfolding and deposition might provide useful insights into its pathophysiology. Pentameric formyl thiophene acetic acid (pFTAA) is a novel amyloid probe that was shown to sensitively detect various misfolded proteins, including PrP. Here, we compared sensitivity of pFTAA staining and spectral microscopy with conventional methods of prion detection in mouse brains infected with mouse‐adapted 22L prions. pFTAA bound to prion deposits in mouse brain sections exhibited a red‐shifted fluorescence emission spectrum, which quantitatively increased with disease progression. Small prion deposits were detected as early as 50 days post‐inoculation, well before appearance of clinical signs. Moreover, we detected significant spectral shifts in the greater brain parenchyma as early as 25 days post‐inoculation, rivaling the most sensitive conventional method (real‐time quaking‐induced conversion). These results showcase the potential of pFTAA staining combined with spectral imaging for screening of prion‐infected tissue. Not only does this method have comparable sensitivity to established techniques, it is faster and technically simpler. Finally, this readout provides valuable information about the spatial distribution of prion aggregates across tissue in the earliest stages of infection, potentially providing valuable pathophysiological insight into prion transmission. [ABSTRACT FROM AUTHOR]

Published

2021

230. Cerebrospinal Fluid and Blood Neurofilament Light Chain Protein in Prion Disease and Other Rapidly Progressive Dementias: Current State of the Art.

Author

Abu-Rumeileh, Samir and Parchi, Piero

Subjects

PRION diseases, ALZHEIMER'S disease, CEREBROSPINAL fluid, DEMENTIA, CREUTZFELDT-Jakob disease, ANTI-NMDA receptor encephalitis, CEREBROVASCULAR disease

Abstract

Rapidly progressive dementia (RPD) is an umbrella term referring to several conditions causing a rapid neurological deterioration associated with cognitive decline and short disease duration. They comprise Creutzfeldt–Jakob disease (CJD), the archetypal RPD, rapidly progressive variants of the most common neurodegenerative dementias (NDs), and potentially treatable conditions such as infectious or autoimmune encephalitis and cerebrovascular disease. Given the significant clinical and, sometimes, neuroradiological overlap between these different disorders, biofluid markers also contribute significantly to the differential diagnosis. Among them, the neurofilament light chain protein (NfL) has attracted growing attention in recent years as a biofluid marker of neurodegeneration due to its sensitivity to axonal damage and the reliability of its measurement in both cerebrospinal fluid (CSF) and blood. Here, we summarize current knowledge regarding biological and clinical implications of NfL evaluation in biofluids across RPDs, emphasizing CJD, and other prion diseases. In the latter, NfL demonstrated a good diagnostic and prognostic accuracy and a potential value as a marker of proximity to clinical onset in pre-symptomatic PRNP mutation carriers. Similarly, in Alzheimer's disease and other NDs, higher NfL concentrations seem to predict a faster disease progression. While increasing evidence indicates a potential clinical value of NfL in monitoring cerebrovascular disease, the association between NfL and prediction of outcome and/or disease activity in autoimmune encephalitis and infectious diseases has only been investigated in few cohorts and deserves confirmatory studies. In the era of precision medicine and evolving therapeutic options, CSF and blood NfL might aid the diagnostic and prognostic assessment of RPDs and the stratification and management of patients according to disease progression in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2021

231. Cognitive decline heralds onset of symptomatic inherited prion disease.

Author

Mole, Joseph, Mead, Simon, Rudge, Peter, Nihat, Akin, Mok, Tzehow, Collinge, John, and Caine, Diana

Subjects

*PRION diseases, *GENETIC disorders, *TRAIL Making Test, *STROOP effect, *SYMPTOMS

Abstract

The clinical effectiveness of any disease-modifying treatment for prion disease, as for other neurodegenerative disorders, will depend on early treatment before damage to neural tissue is irrevocable. Thus, there is a need to identify markers that predict disease onset in healthy at-risk individuals. Whilst imaging and neurophysiological biomarkers have shown limited use in this regard, we recently reported progressive neurophysiological changes in individuals with the inherited prion disease mutation P102L. We have also previously demonstrated a signature pattern of fronto-parietal dysfunction in mild prion disease. Here we address whether these cognitive features anticipate the onset of symptoms in a unique sample of patients with inherited prion disease. In the cross-sectional analysis, we analysed the performance of patients at three time points in the course of disease onset: prior to symptoms (n = 27), onset of subjective symptoms without positive clinical findings (n = 8) and symptomatic with positive clinical findings (n = 24). In the longitudinal analysis, we analysed data from 24 patients who were presymptomatic at the time of recruitment and were followed up over a period of up to 17 years, of whom 16 remained healthy and eight converted to become symptomatic. In the cross-sectional analysis, the key finding was that, relative to a group of 25 healthy non-gene carrier controls, patients with subjective symptoms but without positive clinical findings were impaired on a smaller but similar set of tests (Trail Making Test part A, Stroop test, Performance IQ, gesture repetition, figure recall) to those previously found to be impaired in mild prion disease. In the longitudinal analysis, Trail Making Test parts A and B, Stroop test and Performance IQ scores significantly discriminated between patients who remained presymptomatic and those who converted, even before the converters reached criteria for formal diagnosis. Notably, performance on the Stroop test significantly discriminated between presymptomatic patients and converters before the onset of clinical symptoms [area under the curve = 0.83 (95% confidence interval, 0.62-1.00), P = 0.009]. Thus, we report here, for the first time, neuropsychological abnormalities in healthy patients prior to either symptom onset or clinical diagnosis of inherited prion disease. This constitutes an important component of an evolving profile of clinical and biomarker abnormalities in this crucial group for preventive medicine. [ABSTRACT FROM AUTHOR]

Published

2021

232. Evaluation of proteinase K-resistant prion protein (PrPres) in Korean native black goats carrying a potential scrapie-susceptible haplotype of the prion protein gene (PRNP).

Author

Won, Sae-Young, Kim, Yong-Chan, and Jeong, Byung-Hoon

Subjects

CHRONIC wasting disease, PRIONS, GOATS, PRION diseases, PROTEINASES, PROTEINS

Abstract

Prion disease is a fatal neurodegenerative disease with a broad host range in humans and animals. It is caused by proteinase K-resistant prion protein (PrPres). In previous studies, a heterogeneous infection in Cervidae and Caprinae was reported. Chronic wasting disease (CWD) has been frequently reported as the only prion disease in Korea that occurs in livestock. Thus, there is a possibility of transmission of CWD to Korean native black goats. However, PrPres has not been investigated thus far in Korean native black goats. We found strong linkage disequilibrium between c.126G>A and c.414T>C (r2 = 1) and between c.718C>T and c.126G>A (r2 = 0.638). In addition, the haplotype GTGTAAAC (representing codons 42, 102, 127, 138, 143, 146, 218 and 240) showed the highest frequency with 45.1%. Among 41 Korean native black goats, 20 animals (48.78%) were homozygous for the susceptible haplotypes (histidine at codon 143, asparagine at codon 146 and arginine at codon 154). Interestingly, we did not detect PrPres bands in any of the tested animals, including the 20 animals carrying potential scrapie susceptible haplotypes. [ABSTRACT FROM AUTHOR]

Published

2021

233. Role of Biomarkers for the Diagnosis of Prion Diseases: A Narrative Review

Author

Miren Altuna, Iñigo Ruiz, María Victoria Zelaya, and Maite Mendioroz

Subjects

prion disease, biomarkers, diagnosis, dementia, neurodegeneration, Medicine (General), R5-920

Abstract

Prion diseases are progressive and irreversible neurodegenerative disorders with a low incidence (1.5–2 cases per million per year). Genetic (10–15%), acquired (anecdotal) and sporadic (85%) forms of the disease have been described. The clinical spectrum of prion diseases is very varied, although the most common symptoms are rapidly progressive dementia, cerebellar ataxia and myoclonus. Mean life expectancy from the onset of symptoms is 6 months. There are currently diagnostic criteria based on clinical phenotype, as well as neuroimaging biomarkers (magnetic resonance imaging), neurophysiological tests (electroencephalogram and polysomnogram), and cerebrospinal fluid biomarkers (14-3-3 protein and real-time quaking-induced conversion (RT-QuIC)). The sensitivity and specificity of some of these tests (electroencephalogram and 14-3-3 protein) is under debate and the applicability of other tests, such as RT-QuIC, is not universal. However, the usefulness of these biomarkers beyond the most frequent prion disease, sporadic Creutzfeldt–Jakob disease, remains unclear. Therefore, research is being carried out on new, more efficient cerebrospinal fluid biomarkers (total tau, ratio total tau/phosphorylated tau and neurofilament light chain) and potential blood biomarkers (neurofilament light chain, among others) to try to universalize access to early diagnosis in the case of prion diseases.

Published

2022

234. Gene-Edited Cell Models to Study Chronic Wasting Disease

Author

Simrika Thapa, Cristobal Marrero Winkens, Waqas Tahir, Maria I. Arifin, Sabine Gilch, and Hermann M. Schatzl

Subjects

prion, prion disease, chronic wasting disease, CWD, gene-editing, gene-edited cells, Microbiology, QR1-502

Abstract

Prion diseases are fatal infectious neurodegenerative disorders affecting both humans and animals. They are caused by the misfolded isoform of the cellular prion protein (PrPC), PrPSc, and currently no options exist to prevent or cure prion diseases. Chronic wasting disease (CWD) in deer, elk and other cervids is considered the most contagious prion disease, with extensive shedding of infectivity into the environment. Cell culture models provide a versatile platform for convenient quantification of prions, for studying the molecular and cellular biology of prions, and for performing high-throughput screening of potential therapeutic compounds. Unfortunately, only a very limited number of cell lines are available that facilitate robust and persistent propagation of CWD prions. Gene-editing using programmable nucleases (e.g., CRISPR-Cas9 (CC9)) has proven to be a valuable tool for high precision site-specific gene modification, including gene deletion, insertion, and replacement. CC9-based gene editing was used recently for replacing the PrP gene in mouse and cell culture models, as efficient prion propagation usually requires matching sequence homology between infecting prions and prion protein in the recipient host. As expected, such gene-editing proved to be useful for developing CWD models. Several transgenic mouse models were available that propagate CWD prions effectively, however, mostly fail to reproduce CWD pathogenesis as found in the cervid host, including CWD prion shedding. This is different for the few currently available knock-in mouse models that seem to do so. In this review, we discuss the available in vitro and in vivo models of CWD, and the impact of gene-editing strategies.

Published

2022

235. Ethics in prion disease

Author

Bechtel, Kendra and Geschwind, Michael D

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Neurosciences, Psychology, Transmissible Spongiform Encephalopathy (TSE), Genetics, Infectious Diseases, Neurodegenerative, Emerging Infectious Diseases, Rare Diseases, Human Genome, Generic health relevance, Neurological, Good Health and Well Being, Animals, Biomedical Research, Humans, Neurology, Prion Diseases, Creutzfeldt-Jakob Disease CJD, Prion disease, Ethics, Neurodegenerative disorders, Prion, BSE, Bovine Spongiform Encephalopathy, CDC, CJD, CSF, CWD, Centers for Disease Control, Chronic Wasting Disease, Creutzfeldt-Jakob Disease, DWI, Diffusion Weighted imaging, FDA, FFI, FLAIR, Familial CJD, Fatal Familial Insomnia, Fluid Attenduated Inversion Recovery, Food and Drug Administration, GINA, GSS, Genetic Information Nondiscrimination Act, Genetic Prion Disease, Gerstmann–Sträussler–Scheinker, HD, Huntington's Disease, Iatrogenic CJD, NGT, NSE, Nasogastric Tube, Neuron Specific Enolase, OPRI, Octopeptide Repeat Insertion, PGD, PPS, Pentosan Polysulphate, Preimplantation Genetic Diagnosis, RPD, Rapidly Progressive Dementia, Sporadic CJD, TSE, Transmissible Spongiform Encephalopathy, University of California, San Francisco, Variant CJD, WHO, World Health Organization, fCJD, gPrD, iCJD, sCJD, vCJD, Cognitive Sciences, Neurology & Neurosurgery, Biological psychology

Abstract

This paper is intended to discuss some of the scientific and ethical issues that are created by increased research efforts towards earlier diagnosis, as well as to treatment of, human prion diseases (and related dementias), including the resulting consequences for individuals, their families, and society. Most patients with prion disease currently are diagnosed when they are about 2/3 of the way through their disease course (Geschwind et al., 2010a; Paterson et al., 2012b), when the disease has progressed so far that even treatments that stop the disease process would probably have little benefit. Although there are currently no treatments available for prion diseases, we and others have realized that we must diagnose patients earlier and with greater accuracy so that future treatments have hope of success. As approximately 15% of prion diseases have a autosomal dominant genetic etiology, this further adds to the complexity of ethical issues, particularly regarding when to conduct genetic testing, release of genetic results, and when or if to implement experimental therapies. Human prion diseases are both infectious and transmissible; great care is required to balance the needs of the family and individual with both public health needs and strained hospital budgets. It is essential to proactively examine and address the ethical issues involved, as well as to define and in turn provide best standards of care.

Published

2013

236. Single-chain fragment variable passive immunotherapies for neurodegenerative diseases.

Author

Huang, Liang, Su, Xiaomin, and Federoff, Howard J

Subjects

Humans, Neurodegenerative Diseases, Nerve Tissue Proteins, Prions, Immunization, Passive, alpha-Synuclein, Single-Chain Antibodies, Amyloid beta-Peptides, Huntingtin Protein, scFv, immunotherapy, Prion disease, Alzheimer's disease, Parkinson's disease, Huntington's disease, PrP, A beta, SNCA, Htt, Chemical Physics, Other Chemical Sciences, Genetics, Other Biological Sciences

Abstract

Accumulation of misfolded proteins has been implicated in a variety of neurodegenerative diseases including prion diseases, Alzheimer's disease (AD), Parkinson's disease (PD), and Huntington's disease (HD). In the past decade, single-chain fragment variable (scFv) -based immunotherapies have been developed to target abnormal proteins or various forms of protein aggregates including Aβ, SNCA, Htt, and PrP proteins. The scFvs are produced by fusing the variable regions of the antibody heavy and light chains, creating a much smaller protein with unaltered specificity. Because of its small size and relative ease of production, scFvs are promising diagnostic and therapeutic reagents for protein misfolded diseases. Studies have demonstrated the efficacy and safety of scFvs in preventing amyloid protein aggregation in preclinical models. Herein, we discuss recent developments of these immunotherapeutics. We review efforts of our group and others using scFv in neurodegenerative disease models. We illustrate the advantages of scFvs, including engineering to enhance misfolded conformer specificity and subcellular targeting to optimize therapeutic action.

Published

2013

237. Towards Optimization of Arylamides As Novel, Potent, and Brain-Penetrant Antiprion Lead Compounds

Author

Li, Zhe, Rao, Satish, Gever, Joel R, Widjaja, Kartika, Prusiner, Stanley B, and Silber, B Michael

Subjects

Rare Diseases, Infectious Diseases, Neurosciences, Transmissible Spongiform Encephalopathy (TSE), Neurological, Neurodegenerative diseases, prion disease, Creutzfeldt-Jakob-disease, amide, arylamide, SAR, Creutzfeldt-Jakob disease, Medicinal and Biomolecular Chemistry, Organic Chemistry, Pharmacology and Pharmaceutical Sciences

Abstract

The prion diseases caused by PrPSc, an alternatively folded form of the cellular prion protein (PrPC), are rapidly progressive, fatal, and untreatable neurodegenerative syndromes. We employed HTS ELISA assays to identify compounds that lower the level of PrPSc in prion-infected mouse neuroblastoma (ScN2a-cl3) cells and identified a series of arylamides. SAR studies indicated that small amides with one aromatic, or heteroaromatic ring, on each side of the amide bond are of modest potency. Of note, benzamide (7), with an EC50 of 2200 nM, was one of only a few arylamide hits with a piperazine group on its aniline moiety. The basic piperazine nitrogen can be protonated at physiologic pH, improving solubility, and therefore we wanted to exploit this feature in our search for a drug candidate. An SAR campaign resulted in several key analogs, including a set with biaryl groups introduced on the carbonyl side for improved potency. Several of these biaryl analogs have submicromolar potency, with the most potent analog 17 having an EC50 = 22 nM. More importantly, 17 and several biarylamides (20, 24, 26, 27) were able to traverse the BBB and displayed excellent drug levels in the brains of mice following oral dosing. These biarylamides may represent good starting points for further lead optimization for the identification of potential drug candidates for the treatment of prion diseases.

Published

2013

238. Optimization of Arylamides as Novel, Potent and Brain-penetrant Antiprion Lead Compounds.

Author

Li, Zhe, Rao, Satish, Gever, Joel R, Widjaja, Kartika, Prusiner, Stanley B, and Silber, B Michael

Subjects

Creutzfeldt-Jakob disease, Neurodegenerative diseases, SAR, amide, arylamide, prion disease, Creutzfeldt-Jakob-disease, Medicinal and Biomolecular Chemistry, Pharmacology and Pharmaceutical Sciences, Organic Chemistry

Abstract

The prion diseases caused by PrPSc, an alternatively folded form of the cellular prion protein (PrPC), are rapidly progressive, fatal, and untreatable neurodegenerative syndromes. We employed HTS ELISA assays to identify compounds that lower the level of PrPSc in prion-infected mouse neuroblastoma (ScN2a-cl3) cells and identified a series of arylamides. SAR studies indicated that small amides with one aromatic, or heteroaromatic ring, on each side of the amide bond are of modest potency. Of note, benzamide (7), with an EC50 of 2200 nM, was one of only a few arylamide hits with a piperazine group on its aniline moiety. The basic piperazine nitrogen can be protonated at physiologic pH, improving solubility, and therefore we wanted to exploit this feature in our search for a drug candidate. An SAR campaign resulted in several key analogs, including a set with biaryl groups introduced on the carbonyl side for improved potency. Several of these biaryl analogs have submicromolar potency, with the most potent analog 17 having an EC50 = 22 nM. More importantly, 17 and several biarylamides (20, 24, 26, 27) were able to traverse the BBB and displayed excellent drug levels in the brains of mice following oral dosing. These biarylamides may represent good starting points for further lead optimization for the identification of potential drug candidates for the treatment of prion diseases.

Published

2013

239. 2-Aminothiazoles with improved pharmacotherapeutic properties for treatment of prion disease.

Author

Li, Zhe, Silber, B Michael, Rao, Satish, Gever, Joel R, Bryant, Clifford, Gallardo-Godoy, Alejandra, Dolghih, Elena, Widjaja, Kartika, Elepano, Manuel, Jacobson, Matthew P, Prusiner, Stanley B, and Renslo, Adam R

Subjects

Cell Line, Animals, Humans, Mice, Prion Diseases, Thiazoles, Pregnancy Proteins, Administration, Oral, Cell Survival, Molecular Structure, Structure-Activity Relationship, Dose-Response Relationship, Drug, Quantum Theory, Models, Molecular, 2-aminothiazoles, neurological agents, pharmacokinetic optimization, prion disease, structureactivity relationships, Administration, Oral, Dose-Response Relationship, Drug, Models, Molecular, Orphan Drug, Neurodegenerative, Brain Disorders, Neurosciences, Rare Diseases, Neurological, Medicinal & Biomolecular Chemistry, Medicinal and Biomolecular Chemistry, Organic Chemistry, Pharmacology and Pharmaceutical Sciences

Abstract

Recently, we described the aminothiazole lead (4-biphenyl-4-ylthiazol-2-yl)-(6-methylpyridin-2-yl)-amine (1), which exhibits many desirable properties, including excellent stability in liver microsomes, oral bioavailability of ∼40 %, and high exposure in the brains of mice. Despite its good pharmacokinetic properties, compound 1 exhibited only modest potency in mouse neuroblastoma cells overexpressing the disease-causing prion protein PrP(Sc) . Accordingly, we sought to identify analogues of 1 with improved antiprion potency in ScN2a-cl3 cells while retaining similar or superior properties. Herein we report the discovery of improved lead compounds such as (6-methylpyridin-2-yl)-[4-(4-pyridin-3-yl-phenyl)thiazol-2-yl]amine and cyclopropanecarboxylic acid (4-biphenylthiazol-2-yl)amide, which exhibit brain exposure/EC50 ratios at least tenfold greater than that of compound 1.

Published

2013

240. Discovery and Preliminary Structure–Activity Relationship of Arylpiperazines as Novel, Brain-Penetrant Antiprion Compounds

Author

Li, Zhe, Gever, Joel R, Rao, Satish, Widjaja, Kartika, Prusiner, Stanley B, and Silber, B Michael

Subjects

Transmissible Spongiform Encephalopathy (TSE), Emerging Infectious Diseases, Orphan Drug, Neurodegenerative, Neurosciences, Infectious Diseases, Rare Diseases, Neurological, Neurodegenerative diseases, prion disease, Creutzfeldt-Jakob disease, piperazine, arylpiperazine, structure-activity relationship, SAR, Medicinal and Biomolecular Chemistry, Organic Chemistry, Pharmacology and Pharmaceutical Sciences

Abstract

Prion diseases are a group of fatal neurodegenerative disorders that include Creutzfeldt-Jakob disease (CJD) and kuru in humans, BSE in cattle, and scrapie in sheep. Such illnesses are caused by the conversion and accumulation of a misfolded pathogenic isoform (termed PrPSc) of a normally benign, host cellular protein, denoted PrPC. We employed high-throughput screening (HTS) ELISAs to evaluate compounds for their ability to reduce the level of PrPSc in Rocky Mountain Laboratory (RML) prion-infected mouse neuroblastoma cells (ScN2a-cl3). Arylpiperazines were among the active compounds identified but the initial hits suffered from low potency and poor drug-likeness. The best of those hits, such as 1, 7, 13, and 19, displayed moderate antiprion activity with EC50 values in the micromolar range. Key analogs were designed and synthesized based on the SAR, with analogs 41, 44, 46, and 47 found to have sub-micromolar potency. Analogs 41 and 44 were able to penetrate the blood-brain barrier (BBB) and achieved excellent drug concentrations in the brains of mice after oral dosing. These compounds represent good starting points for further lead optimization in our pursuit of potential drug candidates for the treatment of prion diseases.

Published

2013

241. Discovery and Preliminary SAR of Arylpiperazines as Novel, Brainpenetrant Antiprion Compounds.

Author

Li, Zhe, Gever, Joel, Rao, Satish, Widjaja, Kartika, Prusiner, Stanley B, and Silber, B Michael

Subjects

Creutzfeldt-Jakob disease, Neurodegenerative diseases, SAR, arylpiperazine, piperazine, prion disease, structure-activity relationship, Medicinal and Biomolecular Chemistry, Pharmacology and Pharmaceutical Sciences, Organic Chemistry

Abstract

Prion diseases are a group of fatal neurodegenerative disorders that include Creutzfeldt-Jakob disease (CJD) and kuru in humans, BSE in cattle, and scrapie in sheep. Such illnesses are caused by the conversion and accumulation of a misfolded pathogenic isoform (termed PrPSc) of a normally benign, host cellular protein, denoted PrPC. We employed high-throughput screening (HTS) ELISAs to evaluate compounds for their ability to reduce the level of PrPSc in Rocky Mountain Laboratory (RML) prion-infected mouse neuroblastoma cells (ScN2a-cl3). Arylpiperazines were among the active compounds identified but the initial hits suffered from low potency and poor drug-likeness. The best of those hits, such as 1, 7, 13, and 19, displayed moderate antiprion activity with EC50 values in the micromolar range. Key analogs were designed and synthesized based on the SAR, with analogs 41, 44, 46, and 47 found to have sub-micromolar potency. Analogs 41 and 44 were able to penetrate the blood-brain barrier (BBB) and achieved excellent drug concentrations in the brains of mice after oral dosing. These compounds represent good starting points for further lead optimization in our pursuit of potential drug candidates for the treatment of prion diseases.

Published

2013

242. Pharmacokinetics and Metabolism of 2-Aminothiazoles with Antiprion Activity in Mice

Author

Silber, B Michael, Rao, Satish, Fife, Kimberly L, Gallardo-Godoy, Alejandra, Renslo, Adam R, Dalvie, Deepak K, Giles, Kurt, Freyman, Yevgeniy, Elepano, Manuel, Gever, Joel R, Li, Zhe, Jacobson, Matthew P, Huang, Yong, Benet, Leslie Z, and Prusiner, Stanley B

Subjects

Transmissible Spongiform Encephalopathy (TSE), Rare Diseases, Infectious Diseases, Neurosciences, Brain Disorders, Emerging Infectious Diseases, Neurological, ATP Binding Cassette Transporter, Subfamily B, Member 1, Animals, Area Under Curve, Biological Availability, Brain, Cell Line, Cytochrome P-450 Enzyme System, Humans, Mice, Microsomes, Liver, PrPSc Proteins, Prion Diseases, Protein Isoforms, Solubility, Thiazoles, antiprion drugs, drug discovery, IND24, IND81, prion disease, Pharmacology and Pharmaceutical Sciences, Pharmacology & Pharmacy

Abstract

PurposeTo discover drugs lowering PrP(Sc) in prion-infected cultured neuronal cells that achieve high concentrations in brain to test in mouse models of prion disease and then treat people with these fatal diseases.MethodsWe tested 2-AMT analogs for EC50 and PK after a 40 mg/kg single dose and 40-210 mg/kg/day doses for 3 days. We calculated plasma and brain AUC, ratio of AUC/EC50 after dosing. We reasoned that compounds with high AUC/EC50 ratios should be good candidates going forward.ResultsWe evaluated 27 2-AMTs in single-dose and 10 in 3-day PK studies, of which IND24 and IND81 were selected for testing in mouse models of prion disease. They had high concentrations in brain after oral dosing. Absolute bioavailability ranged from 27-40%. AUC/EC50 ratios after 3 days were >100 (total) and 48-113 (unbound). Stability in liver microsomes ranged from 30->60 min. Ring hydroxylated metabolites were observed in microsomes. Neither was a substrate for the MDR1 transporter.ConclusionsIND24 and IND81 are active in vitro and show high AUC/EC50 ratios (total and unbound) in plasma and brain. These will be evaluated in mouse models of prion disease.

Published

2013

243. Remodeling Alzheimer-amyloidosis models by seeding.

Author

Ulm, Brittany S., Borchelt, David R., and Moore, Brenda D.

Subjects

*TAU proteins, *AMYLOID beta-protein precursor, *ALZHEIMER'S disease, *PRESENILINS, *BRAIN diseases, *SEEDS

Abstract

Alzheimer's disease (AD) is among the most prevalent neurodegenerative diseases, with brain pathology defined by extracellular amyloid beta deposits and intracellular tau aggregates. To aid in research efforts to improve understanding of this disease, transgenic murine models have been developed that replicate aspects of AD pathology. Familial AD is associated with mutations in the amyloid precursor protein and in the presenilins (associated with amyloidosis); transgenic amyloid models feature one or more of these mutant genes. Recent advances in seeding methods provide a means to alter the morphology of resultant amyloid deposits and the age that pathology develops. In this review, we discuss the variety of factors that influence the seeding of amyloid beta pathology, including the source of seed, the time interval after seeding, the nature of the transgenic host, and the preparation of the seeding inoculum. [ABSTRACT FROM AUTHOR]

Published

2021

244. Sporadic Creutzfeldt-Jakob Disease: Diagnosing Typical and Atypical Presentations under Limited Circumstances.

Author

Khan, Shazma and Khan, Sara

Subjects

*CREUTZFELDT-Jakob disease diagnosis, *ELECTROENCEPHALOGRAPHY, *BIOPSY, *CREUTZFELDT-Jakob disease, *TERTIARY care, *MAGNETIC resonance imaging, *CEREBROSPINAL fluid, *DIAGNOSTIC errors, *SYMPTOMS, DEVELOPING countries

Abstract

Introduction: Sporadic Creutzfeldt-Jakob disease (sCJD) is a transmissible disorder of the central nervous system caused by the transformation of normal prion protein into an abnormal misfolded form. The process begins spontaneously and runs a vicious cycle to cause spongiform encephalopathy, rapidly resulting in death. Amply described in the western literature, CJD is scarcely reported in Asia due to certain limitations including missed diagnosis, under-reporting, and rarity of the disease. Brain MRI, electroencephalogram, cerebrospinal fluid testing, and biopsy of the infected brain tissue support the diagnosis in cases of clinical suspicion. However, the diagnosis can still be made with limited available resources in developing countries. Method: A review of CJD cases evaluated in the neurology department of a tertiary care hospital in Pakistan was done from 2002 to 2018. Results: Eleven cases labeled as sCJD are identified based on the European MRI-CJD consortium criteria. This is the first study on CJD from Pakistan, which includes both the typical and atypical presentations. Conclusion: Even with limited testing available, the diagnosis of CJD can be made with confidence in the developing countries, provided the suspicion is kept high in cases of rapid onset dementia and acute behavioral changes. [ABSTRACT FROM AUTHOR]

Published

2021

245. Sporadic Creutzfeldt-Jakob disease in two clinically and virologically controlled Brazilian HIV patients who progressed rapidly to dementia: case reports and literature review.

Author

Esper Dahy, Flávia, Novaes, Christina T. G., Bandeira, Gabriela A., Ramin, Laís F., Penalva de Oliveira, Augusto César, and Smid, Jerusa

Subjects

CREUTZFELDT-Jakob disease, CENTRAL nervous system infections, HIV-positive persons, DEMENTIA, NEUROBEHAVIORAL disorders

Abstract

Human immunodeficiency virus (HIV)-associated neurocognitive disorders are the main cause of cognitive decline and dementia in people living with HIV (PLHIV). However, extensive workup should be done in patients with rapidly progressive dementia (RPD) and HIV, especially when secondary infection in the central nervous system (CNS) is ruled out. Sporadic Creutzfeldt-Jakob disease (sCJD) is the main cause of RPD in non-HIV patients. It is a fatal neurodegenerative condition caused by prions that mainly affects elderly patients. Our objective is to describe two cases of PLHIV presenting with controlled infections and sCJD, and to review the literature. Our patients were younger than expected for sCJD and one of them had a longer disease course. As aging is expected to occur earlier in PLHIV, sCJD must be excluded in younger PLHIV presenting with RPD and without CNS infection. [ABSTRACT FROM AUTHOR]

Published

2021

246. Characterization of Anchorless Human PrP With Q227X Stop Mutation Linked to Gerstmann-Sträussler-Scheinker Syndrome In Vivo and In Vitro.

Author

Shen, Pingping, Dang, Johnny, Wang, Zerui, Zhang, Weiguanliu, Yuan, Jue, Lang, Yue, Ding, Mingxuan, Mitchell, Marcus, Kong, Qingzhong, Feng, Jiachun, Rozemuller, Annemiek J. M., Cui, Li, Petersen, Robert B., and Zou, Wen-Quan

Abstract

Alteration in cellular prion protein (PrPC) localization on the cell surface through mediation of the glycosylphosphatidylinositol (GPI) anchor has been reported to dramatically affect the formation and infectivity of its pathological isoform (PrPSc). A patient with Gerstmann-Sträussler-Scheinker (GSS) syndrome was previously found to have a nonsense heterozygous PrP-Q227X mutation resulting in an anchorless PrP. However, the allelic origin of this anchorless PrPSc and cellular trafficking of PrPQ227X remain to be determined. Here, we show that PrPSc in the brain of this GSS patient is mainly composed of the mutant but not wild-type PrP (PrPWt), suggesting pathological PrPQ227X is incapable of recruiting PrPWt in vivo. This mutant anchorless protein, however, is able to recruit PrPWt from humanized transgenic mouse brain but not from autopsied human brain homogenates to produce a protease-resistant PrPSc-like form in vitro by protein misfolding cyclic amplification (PMCA). To further investigate the characteristics of this mutation, constructs expressing human PrPQ227X or PrPWt were transfected into neuroblastoma cells (M17). Fractionation of the M17 cells demonstrated that most PrPWt is recovered in the cell lysate fraction, while most of the mutant PrPQ227X is recovered in the medium fraction, consistent with the results obtained by immunofluorescence microscopy. Two-dimensional gel-electrophoresis and Western blotting showed that cellular PrPQ227X spots clustered at molecular weights of 22–25 kDa with an isoelectric point (pI) of 3.5–5.5, whereas protein spots from the medium are at 18–26 kDa with a pI of 7–10. Our findings suggest that the role of GPI anchor in prion propagation between the anchorless mutant PrP and wild-type PrP relies on the cellular distribution of the protein. [ABSTRACT FROM AUTHOR]

Published

2021

247. Quaternary Structure Changes for PrPSc Predate PrPC Downregulation and Neuronal Death During Progression of Experimental Scrapie Disease.

Author

Eskandari-Sedighi, Ghazaleh, Cortez, Leonardo M., Yang, Jing, Daude, Nathalie, Shmeit, Klinton, Sim, Valerie, and Westaway, David

Abstract

Prion diseases are fatal neurodegenerative diseases in mammals with the unique characteristics of misfolding and aggregation of the cellular prion protein (PrPC) to the scrapie prion (PrPSc). Although neuroinflammation and neuronal loss feature within the disease process, the details of PrPC/PrPSc molecular transition to generate different aggregated species, and the correlation between each species and sequence of cellular events in disease pathogenesis are not fully understood. In this study, using mice inoculated with the RML isolate of mouse-adapted scrapie as a model, we applied asymmetric flow field-flow fractionation to monitor PrPC and PrPSc particle sizes and we also measured seeding activity and resistance to proteases. For cellular analysis in brain tissue, we measured inflammatory markers and synaptic damage, and used the isotropic fractionator to measure neuronal loss; these techniques were applied at different timepoints in a cross-sectional study of disease progression. Our analyses align with previous reports defining significant decreases in PrPC levels at pre-clinical stages of the disease and demonstrate that these decreases become significant before neuronal loss. We also identified the earliest PrPSc assemblies at a timepoint equivalent to 40% elapsed time for the disease incubation period; we propose that these assemblies, mostly composed of proteinase K (PK)–sensitive species, play an important role in triggering disease pathogenesis. Lastly, we show that the PK-resistant assemblies of PrPSc that appear at timepoints close to the terminal stage have similar biophysical characteristics, and hence that preparative use of PK-digestion selects for this specific subpopulation. In sum, our data argue that qualitative, as well as quantitative, changes in PrP conformers occur at the midpoint of subclinical phase; these changes affect quaternary structure and may occur at the threshold where adaptive responses become inadequate to deal with pathogenic processes. [ABSTRACT FROM AUTHOR]

Published

2021

248. Expression of Toll-like receptors in the cerebellum during pathogenesis of prion disease.

Author

Liao X, Zhu W, Liao X, Liu W, Hou Y, and Wan J

Abstract

Prion diseases, such as scrapie, entail the accumulation of disease-specific prion protein ( PrP Sc ) within the brain. Toll-like receptors (TLRs) are crucial components of the pattern recognition system. They recognize pathogen-associated molecular patterns (PAMPs) and play a central role in orchestrating host innate immune responses. The expression levels of Toll-like receptors (TLRs) in the central nervous system (CNS) were not well-defined. To establish a model of prion diseases in BALB/C mice, the 22L strain was employed. The features of the 22L strain were analyzed, and the cerebellum exhibited severe pathological changes. TLR1-13 levels in the cerebellum were measured using quantitative polymerase chain reaction (qPCR) at time points of 60, 90, 120, and the final end point (145 days post-infection). During the pathogenesis, the expression levels of Toll-like receptors (TLRs) 1, 2, 7, 8, and 9 increased in a time-dependent manner. This trend mirrored the expression patterns of PrP Sc (the pathological isoform of the prion protein) and glial fibrillary acidic protein. Notably, at the end point, TLR1-13 levels were significantly elevated. Protein level of TLR7 and TLR9 showed increasing at the end point of the 22L-infected mice. A deeper understanding of the increased Toll-like receptors (TLRs) in prion diseases could shed light on their role in initiating immune responses at various stages during pathogenesis. This insight is particularly relevant when considering TLRs as potential therapeutic targets for prion diseases., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Liao, Zhu, Liao, Liu, Hou and Wan.)

Published

2024

249. Targeting Neuroinflammation by Pharmacologic Downregulation of Inflammatory Pathways Is Neuroprotective in Protein Misfolding Disorders.

Author

Risen SJ, Boland SW, Sharma S, Weisman GM, Shirley PM, Latham AS, Hay AJD, Gilberto VS, Hines AD, Brindley S, Brown JM, McGrath S, Chatterjee A, Nagpal P, and Moreno JA

Subjects

Humans, Mice, Animals, NLR Family, Pyrin Domain-Containing 3 Protein metabolism, NF-kappa B metabolism, Neuroinflammatory Diseases, Down-Regulation, Neurons metabolism, Inflammation metabolism, Neurodegenerative Diseases metabolism, Alzheimer Disease metabolism, Parkinson Disease metabolism, Prion Diseases drug therapy, Prion Diseases metabolism, Prions metabolism, Proteostasis Deficiencies drug therapy, Proteostasis Deficiencies metabolism

Abstract

Neuroinflammation plays a crucial role in the development of neurodegenerative protein misfolding disorders. This category of progressive diseases includes, but is not limited to, Alzheimer's disease, Parkinson's disease, and prion diseases. Shared pathogenesis involves the accumulation of misfolded proteins, chronic neuroinflammation, and synaptic dysfunction, ultimately leading to irreversible neuronal loss, measurable cognitive deficits, and death. Presently, there are few to no effective treatments to halt the advancement of neurodegenerative diseases. We hypothesized that directly targeting neuroinflammation by downregulating the transcription factor, NF-κB, and the inflammasome protein, NLRP3, would be neuroprotective. To achieve this, we used a cocktail of RNA targeting therapeutics (SB&#95;NI&#95;112) shown to be brain-penetrant, nontoxic, and effective inhibitors of both NF-κB and NLRP3. We utilized a mouse-adapted prion strain as a model for neurodegenerative diseases to assess the aggregation of misfolded proteins, glial inflammation, neuronal loss, cognitive deficits, and lifespan. Prion-diseased mice were treated either intraperitoneally or intranasally with SB&#95;NI&#95;112. Behavioral and cognitive deficits were significantly protected by this combination of NF-κB and NLRP3 downregulators. Treatment reduced glial inflammation, protected against neuronal loss, prevented spongiotic change, rescued cognitive deficits, and significantly lengthened the lifespan of prion-diseased mice. We have identified a nontoxic, systemic pharmacologic that downregulates NF-κB and NLRP3, prevents neuronal death, and slows the progression of neurodegenerative diseases. Though mouse models do not always predict human patient success and the study was limited due to sample size and number of dosing methods utilized, these findings serve as a proof of principle for continued translation of the therapeutic SB&#95;NI&#95;112 for prion disease and other neurodegenerative diseases. Based on the success in a murine prion model, we will continue testing SB&#95;NI&#95;112 in a variety of neurodegenerative disease models, including Alzheimer's disease and Parkinson's disease.

Published

2024

250. Gerstmann-Sträussler-Scheinker Disease Presenting as Late-Onset Slowly Progressive Spinocerebellar Ataxia, and Comparative Case Series with Neuropathology.

Author

Stephen CD, de Gusmao CM, Srinivasan SR, Olsen A, Freua F, Kok F, Montes Garcia Barbosa R, Chen JYH, Appleby BS, Prior T, Frosch MP, and Schmahmann JD

Subjects

Humans, Aged, Prion Proteins genetics, Gerstmann-Straussler-Scheinker Disease diagnosis, Prions genetics, Cerebellar Ataxia complications, Spinocerebellar Ataxias diagnosis

Abstract

Background: Genetic prion diseases, including Gerstmann-Sträussler-Scheinker disease (GSS), are extremely rare, fatal neurodegenerative disorders, often associated with progressive ataxia and cognitive/neuropsychiatric symptoms. GSS typically presents as a rapidly progressive cerebellar ataxia, associated with cognitive decline. Late-onset cases are rare., Objective: To compare a novel GSS phenotype with six other cases and present pathological findings from a single case., Methods: Case series of seven GSS patients, one proceeding to autopsy., Results: Case 1 developed slowly progressive gait difficulties at age 71, mimicking a spinocerebellar ataxia, with a family history of balance problems in old age. Genome sequencing revealed a heterozygous c.392G > A (p.G131E) pathogenic variant and a c.395A > G resulting in p.129 M/V polymorphism in the PRNP gene. Probability analyses considering family history, phenotype, and a similar previously reported point mutation (p.G131V) suggest p.G131E as a new pathogenic variant. Clinical features and imaging of this case are compared with those six additional cases harboring p.P102L mutations. Autopsy findings of a case are described and were consistent with the prion pathology of GSS., Conclusions: We describe a patient with GSS with a novel p.G131E mutation in the PRNP gene, presenting with a late-onset, slowly progressive phenotype, mimicking a spinocerebellar ataxia, and six additional cases with the typical P102L mutation., (© 2024 International Parkinson and Movement Disorder Society.)

Published

2024