Your search keyword '"gene PRNP"' showing total 5 results

1. Homozygous R136S mutation in PRNP gene causes inherited early onset prion disease.

Author

Ximelis T, Marín-Moreno A, Espinosa JC, Eraña H, Charco JM, Hernández I, Riveira C, Alcolea D, González-Roca E, Aldecoa I, Molina-Porcel L, Parchi P, Rossi M, Castilla J, Ruiz-García R, Gelpi E, Torres JM, and Sánchez-Valle R

Subjects

Animals, Brain diagnostic imaging, Brain metabolism, Female, Humans, Mice, Mutation genetics, Prion Proteins genetics, Recombinant Proteins, Gerstmann-Straussler-Scheinker Disease genetics, Prion Diseases genetics, Prions metabolism

Abstract

Background: More than 40 pathogenic heterozygous PRNP mutations causing inherited prion diseases have been identified to date. Recessive inherited prion disease has not been described to date., Methods: We describe the clinical and neuropathological data of inherited early-onset prion disease caused by the rare PRNP homozygous mutation R136S. In vitro PrP Sc propagation studies were performed using recombinant-adapted protein misfolding cyclic amplification technique. Brain material from two R136S homozygous patients was intracranially inoculated in TgMet129 and TgVal129 transgenic mice to assess the transmissibility of this rare inherited form of prion disease., Results: The index case presented symptoms of early-onset dementia beginning at the age of 49 and died at the age of 53. Neuropathological evaluation of the proband revealed abundant multicentric PrP plaques and Western blotting revealed a ~ 8 kDa protease-resistant, unglycosylated PrP Sc fragment, consistent with a Gerstmann-Sträussler-Scheinker phenotype. Her youngest sibling suffered from progressive cognitive decline, motor impairment, and myoclonus with onset in her late 30s and died at the age of 48. Genetic analysis revealed the presence of the R136S mutation in homozygosis in the two affected subjects linked to homozygous methionine at codon 129. One sibling carrying the heterozygous R136S mutation, linked to homozygous methionine at codon 129, is still asymptomatic at the age of 74. The inoculation of human brain homogenates from our index case and an independent case from a Portuguese family with the same mutation in transgenic mice expressing human PrP and in vitro propagation of PrP Sc studies failed to show disease transmissibility., Conclusion: In conclusion, biallelic R136S substitution is a rare variant that produces inherited early-onset human prion disease with a Gerstmann-Sträussler-Scheinker neuropathological and molecular signature. Even if the R136S variant is predicted to be "probably damaging", heterozygous carriers are protected, at least from an early onset providing evidence for a potentially recessive pattern of inheritance in human prion diseases., (© 2021. The Author(s).)

Published

2021

2. Neuropathology of Animal Prion Diseases.

Author

Orge L, Lima C, Machado C, Tavares P, Mendonça P, Carvalho P, Silva J, Pinto ML, Bastos E, Pereira JC, Gonçalves-Anjo N, Gama A, Esteves A, Alves A, Matos AC, Seixas F, Silva F, Pires I, Figueira L, Vieira-Pinto M, Sargo R, and Pires MDA

Subjects

Animals, Cattle, Humans, Prion Proteins metabolism, Scrapie metabolism, Scrapie pathology, Encephalopathy, Bovine Spongiform metabolism, Encephalopathy, Bovine Spongiform pathology, Prion Diseases metabolism, Prion Diseases pathology, Prions metabolism

Abstract

Transmissible Spongiform Encephalopathies (TSEs) or prion diseases are a fatal group of infectious, inherited and spontaneous neurodegenerative diseases affecting human and animals. They are caused by the conversion of cellular prion protein (PrP C ) into a misfolded pathological isoform (PrP Sc or prion- proteinaceous infectious particle) that self-propagates by conformational conversion of PrP C . Yet by an unknown mechanism, PrP C can fold into different PrP Sc conformers that may result in different prion strains that display specific disease phenotype (incubation time, clinical signs and lesion profile). Although the pathways for neurodegeneration as well as the involvement of brain inflammation in these diseases are not well understood, the spongiform changes, neuronal loss, gliosis and accumulation of PrP Sc are the characteristic neuropathological lesions. Scrapie affecting small ruminants was the first identified TSE and has been considered the archetype of prion diseases, though atypical and new animal prion diseases continue to emerge highlighting the importance to investigate the lesion profile in naturally affected animals. In this report, we review the neuropathology and the neuroinflammation of animal prion diseases in natural hosts from scrapie, going through the zoonotic bovine spongiform encephalopathy (BSE), the chronic wasting disease (CWD) to the newly identified camel prion disease (CPD).

Published

2021

3. Homozygous R136S mutation in PRNP gene causes inherited early onset prion disease

Author

Ximelis, Teresa, Marín-Moreno, Alba, Espinosa, J. C., Eraña, H., Charco, J. M., Hernández, I., Riveira, C., Alcolea, Daniel, González-Roca, E., Aldecoa, Iban, Molina-Porcel, L., Parchi, P., Rossi, M., Castilla, Joaquín, Ruiz-García, R., Gelpi, E., Torres, J. M., Sánchez-Valle, Raquel, Universitat Autònoma de Barcelona, Instituto de Salud Carlos III, Ministerio de Ciencia e Innovación (España), Fundació La Marató de TV3, CSIC - Instituto Nacional de Investigación y Tecnología Agraria y Alimentaria (INIA), Ximelis, Teresa, Marín-Moreno, Alba, Espinosa, Juan Carlos, Eraña, Hasier, Charco, Jorge M, Alcolea, Daniel, González-Roca, Eva, Aldecoa, Iban, Molina-Porcel, Laura, Parchi, Piero, Rossi, Marcello, Castilla, Joaquín, Ruiz-García, Raquel, Gelpi, Ellen, Torres, Juan María, Sánchez-Valle, Raquel, Ximelis, Teresa [0000-0002-9634-1496], Marín-Moreno, Alba [0000-0002-4023-6398], Espinosa, Juan Carlos [0000-0002-6719-9902], Eraña, Hasier [0000-0001-8776-4211], Charco, Jorge M [0000-0003-3476-1855], Alcolea, Daniel [0000-0002-3819-3245], González-Roca, Eva [0000-0002-1126-0321], Aldecoa, Iban [0000-0001-5774-7453], Molina-Porcel, Laura [0000-0003-4068-8578], Parchi, Piero [0000-0002-9444-9524], Rossi, Marcello [0000-0002-8125-6571], Castilla, Joaquín [0000-0002-2216-1361], Ruiz-García, Raquel [0000-0002-8403-3613], Gelpi, Ellen [0000-0003-2948-4187], Torres, Juan María [0000-0003-0443-9232], Sánchez-Valle, Raquel [0000-0001-7750-896X], Ximelis T., Marin-Moreno A., Espinosa J.C., Erana H., Charco J.M., Hernandez I., Riveira C., Alcolea D., Gonzalez-Roca E., Aldecoa I., Molina-Porcel L., Parchi P., Rossi M., Castilla J., Ruiz-Garcia R., Gelpi E., Torres J.M., and Sanchez-Valle R.

Subjects

Proband, Prions, Cognitive Neuroscience, animal diseases, Neurosciences. Biological psychiatry. Neuropsychiatry, Neuropathology, Biology, medicine.disease_cause, Prion Protein, Genetic analysis, Prion Proteins, Prion Diseases, PRNP, Mice, Gene PRNP, medicine, Animals, Humans, Gerstmann-Straussler-Scheinker Disease, GSS, Homozygous, RC346-429, Index case, Genetics, Mutation, Animal, Research, Brain, Homozygou, Recombinant Protein, Recombinant Proteins, Prion Disease, nervous system diseases, Neurology, Prion, Protein Misfolding Cyclic Amplification, Female, Neurology (clinical), Neurology. Diseases of the nervous system, medicine.symptom, Myoclonus, Human, RC321-571

Abstract

13 Pág. Centro de Investigación en Sanidad Animal (CISA), More than 40 pathogenic heterozygous PRNP mutations causing inherited prion diseases have been identified to date. Recessive inherited prion disease has not been described to date., This work was funded by the Instituto de Salud Carlos III (grant no. PI20/00448 to RSV), Spanish Ministerio de Ciencia e Innovación (grant no. PDI2019-105837RB-I00 to J.M.T. and J.C.E., and RTI2018-098515-B-I00 to J.C.), Fundació La Marató de TV3 (grant no. 201821-31 to J.C.E.), Instituto Nacional de Investigación y Tecnología Agraria y Agroalimentaria (fellowship INIA-FPI-SGIT-2015-02 to A.M.M.) and Dr Baselga funds for CJD research. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Published

2021

4. Neuropathology of Animal Prion Diseases

Author

Paulo Carvalho, Isabel Pires, Leonor Orge, Ana Cristina Matos, Alexandra Esteves, Jorge C. Pereira, Maria de Lurdes Pinto, Maria dos Anjos Pires, Nuno Gonçalves-Anjo, Paula Tavares, Carla Machado, Roberto Sargo, Filipe Silva, Fernanda Seixas, Paula Mendonça, Madalena Vieira-Pinto, Estela Bastos, Anabela Alves, Adelina Gama, João Silva, Carla Lima, and L. Figueira

Subjects

Prion diseases, 040301 veterinary sciences, gene PRNP, Prions, Bovine spongiform encephalopathy, animal diseases, lcsh:QR1-502, Scrapie, Disease, Neuropathology, Review, Biology, Biochemistry, lcsh:Microbiology, Prion Proteins, neuroinflammation, Prion Diseases, 0403 veterinary science, prion, 03 medical and health sciences, Transmissible Spongiform Encephalopathies, Proteinaceous infectious particle, spongiform degeneration, medicine, Animals, Humans, education, Molecular Biology, 030304 developmental biology, 0303 health sciences, education.field_of_study, neuropathology, Neurodegeneration, 04 agricultural and veterinary sciences, animal TSE, Chronic wasting disease, medicine.disease, Virology, nervous system diseases, Encephalopathy, Bovine Spongiform, Gliosis, Cattle, medicine.symptom, PrPSc

Abstract

Transmissible Spongiform Encephalopathies (TSEs) or prion diseases are a fatal group of infectious, inherited and spontaneous neurodegenerative diseases affecting human and animals. They are caused by the conversion of cellular prion protein (PrPC) into a misfolded pathological isoform (PrPSc or prion- proteinaceous infectious particle) that self-propagates by conformational conversion of PrPC. Yet by an unknown mechanism, PrPC can fold into different PrPSc conformers that may result in different prion strains that display specific disease phenotype (incubation time, clinical signs and lesion profile). Although the pathways for neurodegeneration as well as the involvement of brain inflammation in these diseases are not well understood, the spongiform changes, neuronal loss, gliosis and accumulation of PrPSc are the characteristic neuropathological lesions. Scrapie affecting small ruminants was the first identified TSE and has been considered the archetype of prion diseases, though atypical and new animal prion diseases continue to emerge highlighting the importance to investigate the lesion profile in naturally affected animals. In this report, we review the neuropathology and the neuroinflammation of animal prion diseases in natural hosts from scrapie, going through the zoonotic bovine spongiform encephalopathy (BSE), the chronic wasting disease (CWD) to the newly identified camel prion disease (CPD).

Published

2021

5. Genotypic profile of Pantanal creole sheep regarding susceptibility or resistance to scrapie

Author

GONÇALVES, A. N. D., SOARES, C. O., SANCHES, S. C., REIS, F. A., ROSINHA, G. M. S., ALINE NAJARA DOMINGOS GONÇALVES, Universidade Federal de Mato Grosso do sul, CLEBER OLIVEIRA SOARES, CNPGC, SIMONE CAMARGO SANCHES, Universidade Federal de Mato Grosso do Sul, FERNANDO ALVARENGA REIS, CNPC, and GRACIA MARIA SOARES ROSINHA, CNPGC.

Subjects

Encefalopatia espongiforme transmissivel, Gene PRNP, genotyping, prion diseases, Single nucleotide polymorphisms, Transmissible spongiform encephalopathies, Genotipagem, Polimorfismo de nucleotídeo único

Abstract

The objective of this work was to determine the genotypic profile specific to scrapie in codons 136, 154, and 171 of the PRNP gene of the Pantanal creole sheep. Genomic DNA was extracted from blood samples collected from 66 sheep, and the regions of interest on the DNA strand were amplified by PCR. Five haplotypes were identified: ARR, alanine, arginine, arginine; ARQ, alanine, arginine, glutamine; AHQ, alanine, histidine, glutamine; ARH, alanine, arginine, histidine; and VRQ, valine, arginine, glutamine. The most common genotypes were ARQ/ARQ (27%) and ARR/ARQ (24%). The genotypic profile of the Pantanal creole sheep shows low to moderate susceptibility. Notas científicas.

Published

2016