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1. Identification of FasL as a crucial host factor driving COVID-19 pathology and lethality

Author

Albert, Marie-Christine, Uranga-Murillo, Iratxe, Arias, Maykel, De Miguel, Diego, Peña, Natacha, Montinaro, Antonella, Varanda, Ana Beatriz, Theobald, Sebastian J., Areso, Itziar, Saggau, Julia, Koch, Manuel, Liccardi, Gianmaria, Peltzer, Nieves, Rybniker, Jan, Hurtado-Guerrero, Ramón, Merino, Pedro, Monzón, Marta, Badiola, Juan J., Reindl-Schwaighofer, Roman, Sanz-Pamplona, Rebeca, Cebollada-Solanas, Alberto, Megyesfalvi, Zsolt, Dome, Balazs, Secrier, Maria, Hartmann, Boris, Bergmann, Michael, Pardo, Julián, and Walczak, Henning

Published
2024
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3. Bona fide atypical scrapie faithfully reproduced for the first time in a rodent model

Author

Vidal, Enric, Sánchez-Martín, Manuel A., Eraña, Hasier, Lázaro, Sonia Pérez, Pérez-Castro, Miguel A., Otero, Alicia, Charco, Jorge M., Marín, Belén, López-Moreno, Rafael, Díaz-Domínguez, Carlos M., Geijo, Mariví, Ordóñez, Montserrat, Cantero, Guillermo, di Bari, Michele, Lorenzo, Nuria L., Pirisinu, Laura, d’Agostino, Claudia, Torres, Juan María, Béringue, Vincent, Telling, Glenn, Badiola, Juan J., Pumarola, Martí, Bolea, Rosa, Nonno, Romolo, Requena, Jesús R., and Castilla, Joaquín

Published
2022
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4. In situ assessment of neuroinflammatory cytokines in different stages of ovine natural prion disease.

Author

Guijarro, Isabel M., Garcés, Moisés, Badiola, Juan J., and Monzón, Marta

Subjects
PURKINJE cells, PRION diseases, INFLAMMATORY mediators, INFLAMMATION, DISEASE progression
Abstract

Introduction: According to the neuroinflammatory hypothesis, a cytokine-mediated host innate immune response may be involved in the mechanisms that contribute to the process of neurodegeneration. Specifically, regarding prion diseases, some experimental murine models have evidenced an altered profile of inflammatory intermediaries. However, the local inflammatory response has rarely been assessed, and never in tissues from different natural models throughout the progression of neurodegeneration. Methods: The aim of this study was to use immunohistochemistry (IHC) to in situ assess the temporal protein expression of several cytokines in the cerebellum of sheep suffering from various clinical stages of scrapie. Results and discussion: Clear changes in the expression of most of the assessed markers were observed in the affected sheep compared to the healthy control sheep, and from different stages. In summary, this preliminary IHC study focusing in the Purkinje cell layer changes demonstrate that all cytokines or respective receptors studied (IL-1, IL-1R, IL-2R, IL-6, IL-10R, and TNFαR) except for IFNγR are disease-associated signaling proteins showing an increase or decrease in relation to the progression of clinical disease. In the future, this study will be extended to other inflammatory mediators and brain regions, focusing in particular on the release of these inflammatory mediators by astroglial and microglial populations. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Identification of FasL as a crucial host factor driving COVID-19 pathology and lethality

Author

Albert, Marie Christine, Uranga-Murillo, Iratxe, Arias, Maykel, De Miguel, Diego, Peña, Natacha, Montinaro, Antonella, Varanda, Ana Beatriz, Theobald, Sebastian J., Areso, Itziar, Saggau, Julia, Koch, Manuel, Liccardi, Gianmaria, Peltzer, Nieves, Rybniker, Jan, Hurtado-Guerrero, Ramón, Merino, Pedro, Monzón, Marta, Badiola, Juan J., Reindl-Schwaighofer, Roman, Sanz-Pamplona, Rebeca, Cebollada-Solanas, Alberto, Megyesfalvi, Zsolt, Dome, Balazs, Secrier, Maria, Hartmann, Boris, Bergmann, Michael, Pardo, Julián, Walczak, Henning, Albert, Marie Christine, Uranga-Murillo, Iratxe, Arias, Maykel, De Miguel, Diego, Peña, Natacha, Montinaro, Antonella, Varanda, Ana Beatriz, Theobald, Sebastian J., Areso, Itziar, Saggau, Julia, Koch, Manuel, Liccardi, Gianmaria, Peltzer, Nieves, Rybniker, Jan, Hurtado-Guerrero, Ramón, Merino, Pedro, Monzón, Marta, Badiola, Juan J., Reindl-Schwaighofer, Roman, Sanz-Pamplona, Rebeca, Cebollada-Solanas, Alberto, Megyesfalvi, Zsolt, Dome, Balazs, Secrier, Maria, Hartmann, Boris, Bergmann, Michael, Pardo, Julián, and Walczak, Henning

Abstract

The dysregulated immune response and inflammation resulting in severe COVID-19 are still incompletely understood. Having recently determined that aberrant death-ligand-induced cell death can cause lethal inflammation, we hypothesized that this process might also cause or contribute to inflammatory disease and lung failure following SARS-CoV-2 infection. To test this hypothesis, we developed a novel mouse-adapted SARS-CoV-2 model (MA20) that recapitulates key pathological features of COVID-19. Concomitantly with occurrence of cell death and inflammation, FasL expression was significantly increased on inflammatory monocytic macrophages and NK cells in the lungs of MA20-infected mice. Importantly, therapeutic FasL inhibition markedly increased survival of both, young and old MA20-infected mice coincident with substantially reduced cell death and inflammation in their lungs. Intriguingly, FasL was also increased in the bronchoalveolar lavage fluid of critically-ill COVID-19 patients. Together, these results identify FasL as a crucial host factor driving the immuno-pathology that underlies COVID-19 severity and lethality, and imply that patients with severe COVID-19 may significantly benefit from therapeutic inhibition of FasL., The dysregulated immune response and inflammation resulting in severe COVID-19 are still incompletely understood. Having recently determined that aberrant death-ligand-induced cell death can cause lethal inflammation, we hypothesized that this process might also cause or contribute to inflammatory disease and lung failure following SARS-CoV-2 infection. To test this hypothesis, we developed a novel mouse-adapted SARS-CoV-2 model (MA20) that recapitulates key pathological features of COVID-19. Concomitantly with occurrence of cell death and inflammation, FasL expression was significantly increased on inflammatory monocytic macrophages and NK cells in the lungs of MA20-infected mice. Importantly, therapeutic FasL inhibition markedly increased survival of both, young and old MA20-infected mice coincident with substantially reduced cell death and inflammation in their lungs. Intriguingly, FasL was also increased in the bronchoalveolar lavage fluid of critically-ill COVID-19 patients. Together, these results identify FasL as a crucial host factor driving the immuno-pathology that underlies COVID-19 severity and lethality, and imply that patients with severe COVID-19 may significantly benefit from therapeutic inhibition of FasL.

Published
2024

7. Diagnosis in Scrapie: Conventional Methods and New Biomarkers

Author

Sola, Diego, primary, Betancor, Marina, additional, Marco Lorente, Paula A., additional, Pérez Lázaro, Sonia, additional, Barrio, Tomás, additional, Sevilla, Eloisa, additional, Marín, Belén, additional, Moreno, Bernardino, additional, Monzón, Marta, additional, Acín, Cristina, additional, Bolea, Rosa, additional, Badiola, Juan J., additional, and Otero, Alicia, additional

Published
2023
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8. Bona fide atypical scrapie faithfully reproduced for the first time in a rodent model

Author

Ministerio de Economía y Competitividad (España), European Commission, Fundació La Marató de TV3, Generalitat de Catalunya, Vidal, Enric [0000-0002-4965-3286], Sánchez-Martín, Manuel A.[0000-0001-8370-1336], Eraña, Hasier [0000-0001-8776-4211], Lázaro, Sonia Pérez [0000-0002-2079-0711], Pérez-Castro, Miguel A.[0000-0003-2850-3470], Otero, Alicia [0000-0001-9075-2764], Charco, Jorge M. [0000-0003-3476-1855], Marín, Belén [0000-0002-1590-3347], López-Moreno, Rafael [0000-0002-2155-8965], Díaz-Domínguez, Carlos M. [0000-0002-0410-1963], Geijo, Mariví [0000-0002-3120-1038], Ordóñez, Montserrat [0000-0002-2389-7733], Cantero, Guillermo [0000-0003-4200-503X], di Bari, Michele [0000-0003-0943-6823], Lorenzo, Nuria L.[0000-0002-6444-6269], Pirisinu, Laura [0000-0002-6548-8225], Torres, Juan María [0000-0003-0443-9232], Béringue, V. [0000-0001-6706-5712], Telling, Glenn [0000-0002-6294-1805], Badiola, Juan J. [0000-0002-7173-7216], Pumarola, Martí [0000-0002-0935-7941], Bolea, Rosa [0000-0002-2746-3932], Nonno, Romolo [0000-0001-7556-1564], Requena, J. R. [0000-0003-1954-4975], Castilla, Joaquín [0000-0002-2216-1361], Vidal, Enric, Sánchez-Martín, Manuel Adolfo, Eraña, Hasier, Lázaro, Sonia Pérez, Pérez-Castro, Miguel A., Otero, Alicia, Charco, Jorge M., Marín, Belén, López-Moreno, Rafael, Díaz-Domínguez, Carlos M., Geijo, Mariví, Ordóñez, Montserrat, Cantero, Guillermo, di Bari, Michele, Lorenzo, Nuria L., Pirisinu, Laura, D'Agostino, Claudia, Torres, Juan María, Béringue, V., Telling, Glenn, Badiola, Juan J., Pumarola, Martí, Bolea, Rosa, Nonno, Romolo, Requena, Jesús R., Castilla, Joaquín, Ministerio de Economía y Competitividad (España), European Commission, Fundació La Marató de TV3, Generalitat de Catalunya, Vidal, Enric [0000-0002-4965-3286], Sánchez-Martín, Manuel A.[0000-0001-8370-1336], Eraña, Hasier [0000-0001-8776-4211], Lázaro, Sonia Pérez [0000-0002-2079-0711], Pérez-Castro, Miguel A.[0000-0003-2850-3470], Otero, Alicia [0000-0001-9075-2764], Charco, Jorge M. [0000-0003-3476-1855], Marín, Belén [0000-0002-1590-3347], López-Moreno, Rafael [0000-0002-2155-8965], Díaz-Domínguez, Carlos M. [0000-0002-0410-1963], Geijo, Mariví [0000-0002-3120-1038], Ordóñez, Montserrat [0000-0002-2389-7733], Cantero, Guillermo [0000-0003-4200-503X], di Bari, Michele [0000-0003-0943-6823], Lorenzo, Nuria L.[0000-0002-6444-6269], Pirisinu, Laura [0000-0002-6548-8225], Torres, Juan María [0000-0003-0443-9232], Béringue, V. [0000-0001-6706-5712], Telling, Glenn [0000-0002-6294-1805], Badiola, Juan J. [0000-0002-7173-7216], Pumarola, Martí [0000-0002-0935-7941], Bolea, Rosa [0000-0002-2746-3932], Nonno, Romolo [0000-0001-7556-1564], Requena, J. R. [0000-0003-1954-4975], Castilla, Joaquín [0000-0002-2216-1361], Vidal, Enric, Sánchez-Martín, Manuel Adolfo, Eraña, Hasier, Lázaro, Sonia Pérez, Pérez-Castro, Miguel A., Otero, Alicia, Charco, Jorge M., Marín, Belén, López-Moreno, Rafael, Díaz-Domínguez, Carlos M., Geijo, Mariví, Ordóñez, Montserrat, Cantero, Guillermo, di Bari, Michele, Lorenzo, Nuria L., Pirisinu, Laura, D'Agostino, Claudia, Torres, Juan María, Béringue, V., Telling, Glenn, Badiola, Juan J., Pumarola, Martí, Bolea, Rosa, Nonno, Romolo, Requena, Jesús R., and Castilla, Joaquín

Abstract

Atypical Scrapie, which is not linked to epidemics, is assumed to be an idiopathic spontaneous prion disease in small ruminants. Therefore, its occurrence is unlikely to be controlled through selective breeding or other strategies as it is done for classical scrapie outbreaks. Its spontaneous nature and its sporadic incidence worldwide is reminiscent of the incidence of idiopathic spontaneous prion diseases in humans, which account for more than 85% of the cases in humans. Hence, developing animal models that consistently reproduce this phenomenon of spontaneous PrP misfolding, is of importance to study the pathobiology of idiopathic spontaneous prion disorders. Transgenic mice overexpressing sheep PrPC with I112 polymorphism (TgShI112, 1-2 × PrP levels compared to sheep brain) manifest clinical signs of a spongiform encephalopathy spontaneously as early as 380 days of age. The brains of these animals show the neuropathological hallmarks of prion disease and biochemical analyses of the misfolded prion protein show a ladder-like PrPres pattern with a predominant 7-10 kDa band. Brain homogenates from spontaneously diseased transgenic mice were inoculated in several models to assess their transmissibility and characterize the prion strain generated: TgShI112 (ovine I112 ARQ PrPC), Tg338 (ovine VRQ PrPC), Tg501 (ovine ARQ PrPC), Tg340 (human M129 PrPC), Tg361 (human V129 PrPC), TgVole (bank vole I109 PrPC), bank vole (I109I PrPC), and sheep (AHQ/ARR and AHQ/AHQ churra-tensina breeds). Our analysis of the results of these bioassays concludes that the strain generated in this model is indistinguishable to that causing atypical scrapie (Nor98). Thus, we present the first faithful model for a bona fide, transmissible, ovine, atypical scrapie prion disease.

Published
2022

11. Glycans are not necessary to maintain the pathobiological features of bovine spongiform encephalopathy

Author

Otero, Alicia, Barrio, Tomás, Eraña, Hasier, Charco, Jorge M., Betancor, Marina, Díaz-Domínguez, Carlos M., Marín, Belén, Andréoletti, Olivier, Torres, Juan M., Kong, Qingzhong, Badiola, Juan J., Bolea, Rosa, and Castilla, Joaquín

Subjects
Sheep, Swine, Prions, Immunology, Brain, Mice, Transgenic, Microbiology, Creutzfeldt-Jakob Syndrome, Encephalopathy, Bovine Spongiform, Mice, Polysaccharides, Virology, Genetics, Animals, Humans, Cattle, Parasitology, Molecular Biology, Sheep, Domestic
Abstract

The role of the glycosylation status of PrPC in the conversion to its pathological counterpart and on cross-species transmission of prion strains has been widely discussed. Here, we assessed the effect on strain characteristics of bovine spongiform encephalopathy (BSE) isolates with different transmission histories upon propagation on a model expressing a non-glycosylated human PrPC. Bovine, ovine and porcine-passaged BSE, and variant Creutzfeldt-Jakob disease (vCJD) isolates were used as seeds/inocula in both in vitro and in vivo propagation assays using the non-glycosylated human PrPC-expressing mouse model (TgNN6h). After protein misfolding cyclic amplification (PMCA), all isolates maintained the biochemical characteristics of BSE. On bioassay, all PMCA-propagated BSE prions were readily transmitted to TgNN6h mice, in agreement with our previous in vitro results. TgNN6h mice reproduced the characteristic neuropathological and biochemical hallmarks of BSE, suggesting that the absence of glycans did not alter the pathobiological features of BSE prions. Moreover, back-passage of TgNN6h-adapted BSE prions to BoTg110 mice recovered the full BSE phenotype, confirming that the glycosylation of human PrPC is not essential for the preservation of the human transmission barrier for BSE prions or for the maintenance of BSE strain properties.

Published
2022

12. Peripheral neuropathy caused by fenugreek (Trigonella foenum-graecum) straw intoxication in cattle and experimental reproduction in sheep and goats

Author

Moreno, Bernardino, primary, Marín, Belén, additional, Otero, Alicia, additional, García, Mirta, additional, Raksa, Helen, additional, Guijarro, María I., additional, Climent, María, additional, Morales, Mariano, additional, Zabala, Javier, additional, Loste, Juan M., additional, Acín, Cristina, additional, and Badiola, Juan J., additional

Published
2022
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13. Glycans are not necessary to maintain the pathobiological features of bovine spongiform encephalopathy

Author

Otero, Alicia, primary, Barrio, Tomás, additional, Eraña, Hasier, additional, Charco, Jorge M., additional, Betancor, Marina, additional, Díaz-Domínguez, Carlos M., additional, Marín, Belén, additional, Andréoletti, Olivier, additional, Torres, Juan M., additional, Kong, Qingzhong, additional, Badiola, Juan J., additional, Bolea, Rosa, additional, and Castilla, Joaquín, additional

Published
2022
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14. Classical BSE prions emerge from asymptomatic pigs challenged with atypical/Nor98 scrapie

Author

European Commission, Ministerio de Ciencia e Innovación (España), Marín, Belén [0000-0002-1590-3347], Otero, Alicia [0000-0001-9075-2764], Espinosa Martín, Juan Carlos [0000-0002-6719-9902], Marín-Moreno, Alba [0000-0002-4023-6398], Vidal, Enric [0000-0002-4965-3286], Hedman, Carlos [0000-0002-0827-110X], Pumarola, Martí[0000-0002-0935-7941], Badiola, Juan J [0000-0002-7173-7216], Torres, Juan María [0000-0003-0443-9232], Andréoletti, Olivier [0000-0002-7369-6016], Bolea, Rosa [0000-0002-2746-3932], Marín, Belén, Otero, Alicia, Lugan, Séverine, Espinosa Martín, Juan Carlos, Marín-Moreno, Alba, Vidal, Enric, Hedman, Carlos, Romero, Antonio, Pumarola, Martí, Badiola, Juan J., Torres, Juan María, Andréoletti, Olivier, Bolea, Rosa, European Commission, Ministerio de Ciencia e Innovación (España), Marín, Belén [0000-0002-1590-3347], Otero, Alicia [0000-0001-9075-2764], Espinosa Martín, Juan Carlos [0000-0002-6719-9902], Marín-Moreno, Alba [0000-0002-4023-6398], Vidal, Enric [0000-0002-4965-3286], Hedman, Carlos [0000-0002-0827-110X], Pumarola, Martí[0000-0002-0935-7941], Badiola, Juan J [0000-0002-7173-7216], Torres, Juan María [0000-0003-0443-9232], Andréoletti, Olivier [0000-0002-7369-6016], Bolea, Rosa [0000-0002-2746-3932], Marín, Belén, Otero, Alicia, Lugan, Séverine, Espinosa Martín, Juan Carlos, Marín-Moreno, Alba, Vidal, Enric, Hedman, Carlos, Romero, Antonio, Pumarola, Martí, Badiola, Juan J., Torres, Juan María, Andréoletti, Olivier, and Bolea, Rosa

Abstract

Pigs are susceptible to infection with the classical bovine spongiform encephalopathy (C-BSE) agent following experimental inoculation, and PrPSc accumulation was detected in porcine tissues after the inoculation of certain scrapie and chronic wasting disease isolates. However, a robust transmission barrier has been described in this species and, although they were exposed to C-BSE agent in many European countries, no cases of natural transmissible spongiform encephalopathies (TSE) infections have been reported in pigs. Transmission of atypical scrapie to bovinized mice resulted in the emergence of C-BSE prions. Here, we conducted a study to determine if pigs are susceptible to atypical scrapie. To this end, 12, 8-9-month-old minipigs were intracerebrally inoculated with two atypical scrapie sources. Animals were euthanized between 22- and 72-months post inoculation without clinical signs of TSE. All pigs tested negative for PrPSc accumulation by enzyme immunoassay, immunohistochemistry, western blotting and bioassay in porcine PrP mice. Surprisingly, in vitro protein misfolding cyclic amplification demonstrated the presence of C-BSE prions in different brain areas from seven pigs inoculated with both atypical scrapie isolates. Our results suggest that pigs exposed to atypical scrapie prions could become a reservoir for C-BSE and corroborate that C-BSE prions emerge during interspecies passage of atypical scrapie.

Published
2021

15. MicroRNA Alterations in a Tg501 Mouse Model of Prion Disease

Author

Ministerio de Economía y Competitividad (España), Ministerio de Ciencia e Innovación (España), Agencia Estatal de Investigación (España), Instituto de Salud Carlos III, European Commission, CSIC - Instituto Nacional de Investigación y Tecnología Agraria y Alimentaria (INIA), Gobierno de Aragón, Centro Investigación Biomédica en Red Enfermedades Neurodegenerativas (España), Toivonen, Janne Markus [0000-0002-7243-1737], Sánz-Rubio, David [0000-0002-5228-248X], López-Pérez, Óscar [0000-0003-2454-2114], Marín-Moreno, Alba [0000-0002-4023-6398], Bolea, Rosa [0000-0002-2746-3932], Osta, Rosario [0000-0001-5687-6704], Badiola, Juan J. [0000-0002-7173-7216], Espinosa Martín, Juan Carlos [0000-0002-6719-9902], Torres, Juan María [0000-0003-0443-9232], Martín-Burriel, Inmaculada [0000-0001-6016-4726], Toivonen, Janne Markus, Sánz-Rubio, David, López-Pérez, Óscar, Marín-Moreno, Alba, Bolea, Rosa, Osta, Rosario, Badiola, Juan J., Zaragoza, P., Espinosa Martín, Juan Carlos, Torres, Juan María, Martín-Burriel, Inmaculada, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia e Innovación (España), Agencia Estatal de Investigación (España), Instituto de Salud Carlos III, European Commission, CSIC - Instituto Nacional de Investigación y Tecnología Agraria y Alimentaria (INIA), Gobierno de Aragón, Centro Investigación Biomédica en Red Enfermedades Neurodegenerativas (España), Toivonen, Janne Markus [0000-0002-7243-1737], Sánz-Rubio, David [0000-0002-5228-248X], López-Pérez, Óscar [0000-0003-2454-2114], Marín-Moreno, Alba [0000-0002-4023-6398], Bolea, Rosa [0000-0002-2746-3932], Osta, Rosario [0000-0001-5687-6704], Badiola, Juan J. [0000-0002-7173-7216], Espinosa Martín, Juan Carlos [0000-0002-6719-9902], Torres, Juan María [0000-0003-0443-9232], Martín-Burriel, Inmaculada [0000-0001-6016-4726], Toivonen, Janne Markus, Sánz-Rubio, David, López-Pérez, Óscar, Marín-Moreno, Alba, Bolea, Rosa, Osta, Rosario, Badiola, Juan J., Zaragoza, P., Espinosa Martín, Juan Carlos, Torres, Juan María, and Martín-Burriel, Inmaculada

Abstract

MicroRNAs (miRNAs) may contribute to the development and pathology of many neurodegenerative diseases, including prion diseases. They are also promising biomarker candidates due to their stability in body fluids. We investigated miRNA alterations in a Tg501 mouse model of prion diseases that expresses a transgene encoding the goat prion protein (PRNP). Tg501 mice intracranially inoculated with mouse-adapted goat scrapie were compared with age-matched, mock inoculated controls in preclinical and clinical stages. Small RNA sequencing from the cervical spinal cord indicated that miR-223-3p, miR-151-3p, and miR-144-5p were dysregulated in scrapie-inoculated animals before the onset of symptoms. In clinical-stage animals, 23 significant miRNA alterations were found. These miRNAs were predicted to modify the Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways including prion disease, extracellular matrix interactions, glutaminergic synapse, axon guidance, and transforming growth factor-beta signaling. MicroRNAs miR-146a-5p (up in cervical spinal cord) and miR-342-3p (down in cervical spinal cord, cerebellum and plasma), both indicated in neurodegenerative diseases earlier, were verified by quantitative real-time polymerase chain reaction (qRT-PCR). Minimal changes observed before the disease onset suggests that most miRNA alterations observed here are driven by advanced prion-associated pathology, possibly limiting their use as diagnostic markers. However, the results encourage further mechanistic studies on miRNA-regulated pathways involved in these neurodegenerative conditions.

Published
2020

16. Mixtures of prion substrains in natural scrapie cases revealed by ovinised murine models

Author

Ministerio de Educación, Cultura y Deporte (España), Ministerio de Economía y Competitividad (España), European Commission, Barrio, Tomás [0000-0002-7037-6316], Filali, Hicham [0000-0003-3352-740X], Otero, Alicia [0000-0001-9075-2764], Sheleby-Elías, Jessica [0000-0001-7370-5763], Marín, Belén [0000-0002-1590-3347], Vidal, Enric [0000-0002-4965-3286], Béringue, V. [0000-0001-6706-5712], Torres, Juan María [0000-0003-0443-9232], Groschup, M. H. [0000-0003-0215-185X], Andréoletti, Olivier [0000-0002-7369-6016], Badiola, Juan J. [0000-0002-7173-7216], Bolea, Rosa [0000-0002-2746-3932], Barrio, Tomás, Filali, Hicham, Otero, Alicia, Sheleby-Elías, Jessica, Marín, Belén, Vidal, Enric, Béringue, V., Torres, Juan María, Groschup, M. H., Andréoletti, Olivier, Badiola, Juan J., Bolea, Rosa, Ministerio de Educación, Cultura y Deporte (España), Ministerio de Economía y Competitividad (España), European Commission, Barrio, Tomás [0000-0002-7037-6316], Filali, Hicham [0000-0003-3352-740X], Otero, Alicia [0000-0001-9075-2764], Sheleby-Elías, Jessica [0000-0001-7370-5763], Marín, Belén [0000-0002-1590-3347], Vidal, Enric [0000-0002-4965-3286], Béringue, V. [0000-0001-6706-5712], Torres, Juan María [0000-0003-0443-9232], Groschup, M. H. [0000-0003-0215-185X], Andréoletti, Olivier [0000-0002-7369-6016], Badiola, Juan J. [0000-0002-7173-7216], Bolea, Rosa [0000-0002-2746-3932], Barrio, Tomás, Filali, Hicham, Otero, Alicia, Sheleby-Elías, Jessica, Marín, Belén, Vidal, Enric, Béringue, V., Torres, Juan María, Groschup, M. H., Andréoletti, Olivier, Badiola, Juan J., and Bolea, Rosa

Abstract

Phenotypic variability in prion diseases, such as scrapie, is associated to the existence of prion strains, which are different pathogenic prion protein (PrPSc) conformations with distinct pathobiological properties. To faithfully study scrapie strain variability in natural sheep isolates, transgenic mice expressing sheep cellular prion protein (PrPC) are used. In this study, we used two of such models to bioassay 20 scrapie isolates from the Spain-France-Andorra transboundary territory. Animals were intracerebrally inoculated and survival periods, proteinase K-resistant PrP (PrPres) banding patterns, lesion profiles and PrPSc distribution were studied. Inocula showed a remarkable homogeneity on banding patterns, all of them but one showing 19-kDa PrPres. However, a number of isolates caused accumulation of 21-kDa PrPres in TgShp XI. A different subgroup of isolates caused long survival periods and presence of 21-kDa PrPres in Tg338 mice. It seemed that one major 19-kDa prion isoform and two distinct 21-kDa variants coexisted in source inocula, and that they could be separated by bioassay in each transgenic model. The reason why each model favours a specific component of the mixture is unknown, although PrPC expression level may play a role. Our results indicate that coinfection with more than one substrain is more frequent than infection with a single component.

Published
2020

17. Glycans are not necessary to maintain the pathobiological features of bovine spongiform encephalopathy

Author

Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), European Commission, Torres, Juan María [0000-0003-0443-9232], Castilla, Joaquín [0000-0002-2216-1361], Otero, Alicia, Barrio, Tomás, Eraña, Hasier, Charco, Jorge M., Betancor, Marina, Díaz-Domínguez, Carlos M., Marín, Belén, Andréoletti, Olivier, Torres, Juan María, Kong, Qingzhong, Badiola, Juan J., Bolea, Rosa, Castilla, Joaquín, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), European Commission, Torres, Juan María [0000-0003-0443-9232], Castilla, Joaquín [0000-0002-2216-1361], Otero, Alicia, Barrio, Tomás, Eraña, Hasier, Charco, Jorge M., Betancor, Marina, Díaz-Domínguez, Carlos M., Marín, Belén, Andréoletti, Olivier, Torres, Juan María, Kong, Qingzhong, Badiola, Juan J., Bolea, Rosa, and Castilla, Joaquín

Abstract

The role of the glycosylation status of PrPC in the conversion to its pathological counterpart and on cross-species transmission of prion strains has been widely discussed. Here, we assessed the effect on strain characteristics of bovine spongiform encephalopathy (BSE) isolates with different transmission histories upon propagation on a model expressing a non-glycosylated human PrPC. Bovine, ovine and porcine-passaged BSE, and variant Creutzfeldt-Jakob disease (vCJD) isolates were used as seeds/inocula in both in vitro and in vivo propagation assays using the non-glycosylated human PrPC-expressing mouse model (TgNN6h). After protein misfolding cyclic amplification (PMCA), all isolates maintained the biochemical characteristics of BSE. On bioassay, all PMCA-propagated BSE prions were readily transmitted to TgNN6h mice, in agreement with our previous in vitro results. TgNN6h mice reproduced the characteristic neuropathological and biochemical hallmarks of BSE, suggesting that the absence of glycans did not alter the pathobiological features of BSE prions. Moreover, back-passage of TgNN6h-adapted BSE prions to BoTg110 mice recovered the full BSE phenotype, confirming that the glycosylation of human PrPC is not essential for the preservation of the human transmission barrier for BSE prions or for the maintenance of BSE strain properties.

Published
2022

19. sj-pdf-1-vet-10.1177_03009858221137020 – Supplemental material for Peripheral neuropathy caused by fenugreek (Trigonella foenum-graecum) straw intoxication in cattle and experimental reproduction in sheep and goats

Author

Moreno, Bernardino, Marín, Belén, Otero, Alicia, García, Mirta, Raksa, Helen, Guijarro, María I., Climent, María, Morales, Mariano, Zabala, Javier, Loste, Juan M., Acín, Cristina, and Badiola, Juan J.

Subjects
70706 Veterinary Medicine, FOS: Clinical medicine, FOS: Veterinary sciences, 111599 Pharmacology and Pharmaceutical Sciences not elsewhere classified
Abstract

Supplemental material, sj-pdf-1-vet-10.1177_03009858221137020 for Peripheral neuropathy caused by fenugreek (Trigonella foenum-graecum) straw intoxication in cattle and experimental reproduction in sheep and goats by Bernardino Moreno, Belén Marín, Alicia Otero, Mirta García, Helen Raksa, María I. Guijarro, María Climent, Mariano Morales, Javier Zabala, Juan M. Loste, Cristina Acín and Juan J. Badiola in Veterinary Pathology

Published
2022
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20. Genome-Wide Methylation Profiling in the Thalamus of Scrapie Sheep

Author

Hernaiz, Adelaida, primary, Sanz, Arianne, additional, Sentre, Sara, additional, Ranera, Beatriz, additional, Lopez-Pérez, Oscar, additional, Zaragoza, Pilar, additional, Badiola, Juan J., additional, Filali, Hicham, additional, Bolea, Rosa, additional, Toivonen, Janne M., additional, and Martín-Burriel, Inmaculada, additional

Published
2022
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22. Peripheral neuropathy caused by fenugreek (Trigonella foenum-graecum) straw intoxication in cattle and experimental reproduction in sheep and goats.

Author

Moreno, Bernardino, Marín, Belén, Otero, Alicia, García, Mirta, Raksa, Helen, Guijarro, María I., Climent, María, Morales, Mariano, Zabala, Javier, Loste, Juan M., Acín, Cristina, and Badiola, Juan J.

Subjects
CATTLE reproduction, FENUGREEK, PERIPHERAL neuropathy, SHEEP, GOATS, CATTLE feeding & feeds
Abstract

Trigonella foenum-graecum (fenugreek) is a legume widely used as a food supplement in humans and less frequently in ruminants. Toxicity has been described sporadically in ruminants grazing mature fenugreek plants or stubble; however, the pathological features are unclear. This report describes a natural outbreak of intoxication in cattle fed fenugreek straw and the experimental reproduction using 8 sheep and 8 goats. Affected cattle presented clinical signs approximately 1 month after consuming the straw and 100 of 400 cattle (25%) were affected, of which 60 of 100 (60%) died or were euthanized. Clinical signs were characterized by proprioceptive positioning defects with abnormal postures and weakness of hindlimbs. Forelimbs were also affected in severely affected animals, and cattle became recumbent. Locomotion was characterized by trembling, and some cattle showed high-stepping movements of their forelimbs and knuckled over in their fetlocks. Experimental intoxication induced clinical signs only in sheep and were similar to cattle, although with signs starting in the forelegs. Gross and microscopic lesions were similar in spontaneous and experimental intoxications. Macroscopic changes corresponded with muscular hemorrhages and edema, mainly surrounding the peripheral nerves. Microscopic examination only demonstrated lesions in the distal peripheral nerves, which included edema, hemorrhages, and Wallerian degeneration. Neurofilament immunohistochemistry revealed altered axon labeling and S100 showed a decrease in myelin intensity and loss of its typical compact arrangement around axons. Biochemical and hematological abnormalities included elevated levels of muscle and liver enzymes and thrombocytopenia. These findings indicate that fenugreek straw induces peripheral neuropathy in cattle and sheep, but not in goats. [ABSTRACT FROM AUTHOR]

Published
2023
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23. Reflections on cerebellar neuropathology in classical scrapie

Author

Toledano-Díaz, A., Álvarez, M. Isabel, Rodríguez, J. J., Badiola, Juan J., Monzón, M., Toledano Gasca, Adolfo, Toledano-Díaz, A., Álvarez, M. Isabel, Rodríguez, J. J., Badiola, Juan J., Monzón, M., and Toledano Gasca, Adolfo

Abstract

In this review, the most important neuropathological changes found in the cerebella of sheep affected by classical natural scrapie are discussed. This disease is the oldest known of a group of unconventional “infections” caused by toxic prions of different origins. Scrapie is currently considered a “transmissible spongiform encephalopathy” (due to its neuropathological characteristics and its transmission), which is the paradigm of prion pathologies as well as many encephalopathies (prion-like) that present aberrant deposits of insoluble protein with neurotoxic effects due to errors in their catabolization (“misfolding protein diseases”). The study of this disease is, therefore, of great relevance. Our work data from the authors’ previous publications as well as other research in the field. The four most important types of neuropathological changes are neuron abnormalities and loss, neurogliosis, tissue vacuolization (spongiosis) and pathological or abnormal prion protein (PrP) deposits/deposition. These findings were analyzed and compared to other neuropathologies. Various aspects related to the presentation and progression of the disease, the involution of different neuronal types, the neuroglial responses and the appearance of abnormal PrP deposits are discussed. The most important points of controversy in scrapie neuropathology are presented.

Published
2021

25. Effect of Scrapie Prion Infection in Ovine Bone Marrow-Derived Mesenchymal Stem Cells and Ovine Mesenchymal Stem Cell-Derived Neurons

Author

García-Mendívil, Laura, primary, Mediano, Diego R., additional, Hernaiz, Adelaida, additional, Sanz-Rubio, David, additional, Vázquez, Francisco J., additional, Marín, Belén, additional, López-Pérez, Óscar, additional, Otero, Alicia, additional, Badiola, Juan J., additional, Zaragoza, Pilar, additional, Ordovás, Laura, additional, Bolea, Rosa, additional, and Martín-Burriel, Inmaculada, additional

Published
2021
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30. MicroRNA Alterations in a Tg501 Mouse Model of Prion Disease

Author

Toivonen, Janne M., primary, Sanz-Rubio, David, additional, López-Pérez, Óscar, additional, Marín-Moreno, Alba, additional, Bolea, Rosa, additional, Osta, Rosario, additional, Badiola, Juan J., additional, Zaragoza, Pilar, additional, Espinosa, Juan-Carlos, additional, Torres, Juan-Maria, additional, and Martín-Burriel, Inmaculada, additional

Published
2020
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32. Antimicrobial resistance among canine enteric Escherichia coli isolates and prevalence of attaching–effacing and extraintestinal pathogenic virulence factors in Spain

Author

Sevilla, Eloisa, primary, Mainar-Jaime, Raúl C., additional, Moreno, Bernardino, additional, Martín-Burriel, Inmaculada, additional, Morales, Mariano, additional, Andrés-Lasheras, Sara, additional, Chirino-Trejo, Manuel, additional, Badiola, Juan J., additional, and Bolea, Rosa, additional

Published
2020
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34. Medulla oblongata transcriptome changes during presymptomatic natural scrapie and their association with prion-related lesions

Author

Filali Hicham, Martin-Burriel Inmaculada, Harders Frank, Varona Luis, Serrano Carmen, Acín Cristina, Badiola Juan J, Bossers Alex, and Bolea Rosa

Subjects
Natural scrapie, Preclinical sheep, Microarray, Genetic expression, Real time PCR, Prion, Biotechnology, TP248.13-248.65, Genetics, QH426-470
Abstract

Abstract Background The pathogenesis of natural scrapie and other prion diseases is still poorly understood. Determining the variations in the transcriptome in the early phases of the disease might clarify some of the molecular mechanisms of the prion-induced pathology and allow for the development of new biomarkers for diagnosis and therapy. This study is the first to focus on the identification of genes regulated during the preclinical phases of natural scrapie in the ovine medulla oblongata (MO) and the association of these genes with prion deposition, astrocytosis and spongiosis. Results A custom microarray platform revealed that 86 significant probes had expression changes greater than 2-fold. From these probes, we identified 32 genes with known function; the highest number of regulated genes was included in the phosphoprotein-encoding group. Genes encoding extracellular marker proteins and those involved in the immune response and apoptosis were also differentially expressed. In addition, we investigated the relationship between the gene expression profiles and the appearance of the main scrapie-associated brain lesions. Quantitative Real-time PCR was used to validate the expression of some of the regulated genes, thus showing the reliability of the microarray hybridization technology. Conclusions Genes involved in protein and metal binding and oxidoreductase activity were associated with prion deposition. The expression of glial fibrillary acidic protein (GFAP) was associated with changes in the expression of genes encoding proteins with oxidoreductase and phosphatase activity, and the expression of spongiosis was related to genes encoding extracellular matrix components or transmembrane transporters. This is the first genome-wide expression study performed in naturally infected sheep with preclinical scrapie. As in previous studies, our findings confirm the close relationship between scrapie and other neurodegenerative diseases.

Published
2012
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36. Changes in HSP gene and protein expression in natural scrapie with brain damage

Author

Serrano Carmen, Bolea Rosa, Lyahyai Jaber, Filali Hicham, Varona Luis, Marcos-Carcavilla Ane, Acín Cristina, Calvo Jorge H, Serrano Magdalena, Badiola Juan J, Zaragoza Pilar, and Martín-Burriel Inmaculada

Subjects
Veterinary medicine, SF600-1100
Abstract

Abstract Heat shock proteins (Hsp) perform cytoprotective functions such as apoptosis regulation and inflammatory response control. These proteins can also be secreted to the extracellular medium, acting as inflammatory mediators, and their chaperone activity permits correct folding of proteins and avoids the aggregation of anomalous isoforms. Several studies have proposed the implication of Hsp in prion diseases. We analysed the gene expression and protein distribution of different members of the Hsp27, Hsp70, and Hsp90 families in the central nervous system of sheep naturally infected with scrapie. Different expression profiles were observed in the areas analysed. Whereas changes in transcript levels were not observed in the cerebellum or medulla oblongata, a significant decrease in HSP27 and HSP90 was detected in the prefrontal cortex. In contrast, HSP73 was over-expressed in diencephalons of scrapie animals. Western blotting did not reveal significant differences in Hsp90 and Hsp70 protein expression between scrapie and control animals. Expression rates identified by real-time RT-PCR and western blotting were compared with the extent of classical scrapie lesions using stepwise regression. Changes in Hsp gene and protein expression were associated with prion protein deposition, gliosis and spongiosis rather than with apoptosis. Finally, immunohistochemistry revealed intense Hsp70 and Hsp90 immunolabelling in Purkinje cells of scrapie sheep. In contrast, controls displayed little or no staining in these cells. The observed differences in gene expression and protein distribution suggest that the heat shock proteins analysed play a role in the natural form of the disease.

Published
2011
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40. Morphological Changes of Glia in Prion and a Prion-Like Disord

Author

Universidad de Zaragoza, Garcés, M., Toledano Gasca, Adolfo, Badiola, Juan J., Monzón, M., Universidad de Zaragoza, Garcés, M., Toledano Gasca, Adolfo, Badiola, Juan J., and Monzón, M.

Abstract

Several neurodegenerative diseases such as Alzheimer’s, Parkinson’s and Huntington’s are considered to be prion-like disorders in that they are all proteinopathies where in aberrant proteins spread throughout the brain during disease progression, and thus they may share molecular basis and mechanisms of propagation. Therefore, studies elucidating mechanisms of prion propagation may be relevant to other neurodegenerative diseases. While substantial progress has been made, the pathogenesis of these neurodegenerative diseases is still largely unknown, and as consequence, to date no truly effective treatments that prevent onset or delay progression of these diseases have been identified. In addition to propagation of misfolded proteins, these diseases all induce a host response that includes activation of astrocytes and microglial cells. However, in our opinion, the glial response in each of these diseases has not been well-defined. Since a role for glial response in prion disease has been clearly demonstrated in a previous study concerning Scrapie in sheep, a similar approach to analysis of astrocytic gliosis has been taken here for Creutzfeldt-Jakob (CJD) and Alzheimer’s Diseases (AD). Here, morphological analysis of glial cells in cerebella from CJD and AD patients (as the most common prion and prion-like disorders, respectively) was performed. The results presented in this study support the involvement of glial cells not only in the pathogenesis of CJD, but also of AD. A relationship between intensity and morphology is observed in astroglia from the molecular layer in both pathologies. By contrast, the involvement of microgliosis in AD-affected samples showed a lower relevance from that observed in CJD, since reactive microglia were much more abundant in prion disease. Further analysis of the role of gliosis in CJD and AD, as well as other neurodegenerative diseases, may well advance knowledge of the mechanisms underlying these diseases and may also provide new targ

Published
2016

41. Ultrastructural changes in the progress of natural Scrapie regardless fixation protocol

Author

Sarasa, R., Junquera C., Toledano Gasca, Adolfo, Badiola, Juan J., Monzón, M., Sarasa, R., Junquera C., Toledano Gasca, Adolfo, Badiola, Juan J., and Monzón, M.

Abstract

© 2015, Springer-Verlag Berlin Heidelberg. Because few studies regarding ultrastructural pathological changes associated with natural prion diseases have been performed, the present study primarily intended to determine consistent lesions at the subcellular level and to demonstrate whether these changes are evident regardless of the fixation protocol. Thus far, no assessment method has been developed for classifying the possible variations according to the disease stage, although such an assessment would contribute to clarifying the pathogenesis of this neurodegenerative disease. Therefore, animals at different disease stages were included here. This study presents the first description of lesions associated with natural Scrapie in the cerebellum. Vacuolation, which preferentially occurs around Purkinje cells and which displays a close relation with glial cells, is one of the most novel observations provided in this study. The disruption of hypolemmal cisterns in this neuronal type and the presence of a primary cilium in the granular layer both represent the first findings concerning prion diseases. The possibility of including samples regardless of their fixation protocol is confirmed in this work. Therefore, a high proportion of tissue bank samples that are currently being wasted can be included in ultrastructural studies, which constitute a valuable source for information regarding physiological and pathological samples.

Published
2015

42. Characterization of mesenchymal stem cells in sheep naturally infected with scrapie

Author

Mediano, Diego R., primary, Sanz-Rubio, David, additional, Bolea, Rosa, additional, Marín, Belén, additional, Vázquez, Francisco J., additional, Remacha, Ana R., additional, López-Pérez, Óscar, additional, Fernández-Borges, Natalia, additional, Castilla, Joaquín, additional, Zaragoza, Pilar, additional, Badiola, Juan J., additional, Rodellar, Clementina, additional, and Martín-Burriel, Inmaculada, additional

Published
2015
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44. Changes induced by natural scrapie in the calretinin-immunopositive cells and fibres of the sheep cerebellar cortex

Author

Toledano-Díaz, A., Álvarez, M. Isabel, Monleón, E., Badiola, Juan J., Monzón, M., Toledano-Díaz, A., Álvarez, M. Isabel, Monleón, E., Badiola, Juan J., and Monzón, M.

Abstract

Calretinin (CR)-immunopositive cells and fibres in the cerebellar cortex (vermal archicerebellum and neocerebellum) of scrapie-affected, ARQ/ARQ, Rasa Aragonesa breed sheep were studied in comparison with healthy, young and aged, ARQ/ARQ, Rasa Aragonesa animals and with Manchega breed sheep. The scrapie-affected sheep showed signs of both cellular involution and hypertrophic/ hyperimmunoreactive responses in all neuronal subtypes; the distribution of the neuronal subtypes in the archi- and neocerebellum, however, did not change compared with controls. The results suggest that the different CR expression and/or CR content of cerebellar cortical neurons in scrapie-affected sheep are more related to their specific functions than any neuroprotective response. The reduction in the cell density of some CR-immunopositive neuronal subsets (i.e. unipolar brush cells) is contradictory to the supposed neuroprotective role of the calcium binding protein CR. However, the hyperimmunoreactivity of many CR-immunopositive neuronal subsets (e.g. the Purkinje cells) suggests the involvement of an over-expression of CR (transitory or restricted to selected neurons) as an adaptative mechanism to fight against the neurodegeneration caused by this prion disease. The changes in the number of immunopositive cells and the hypertrophic/ hyperimmunoreactive response seen in scrapie-affected and aged sheep suggests that some different and some similar mechanisms are at work in this disease and aging. ©Springer Science+Business Media, LLC 2011.

Published
2012

45. Attenuated Mycobacterium tuberculosis SO2 vaccine candidate is unable to induce cell death

Author

Ministerio de Economía y Competitividad (España), Ministerio de Ciencia e Innovación (España), European Commission, ARAID Foundation, Aporta, Adriana, Arbues, Ainhoa, Aguilo, Juan I., Monzón, Marta, Badiola, Juan J., Martino, Alba de, Ferrer, Nadia, Marinova, Dessislava, Anel, Alberto, Martin, Carlos, Pardo, Julián, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia e Innovación (España), European Commission, ARAID Foundation, Aporta, Adriana, Arbues, Ainhoa, Aguilo, Juan I., Monzón, Marta, Badiola, Juan J., Martino, Alba de, Ferrer, Nadia, Marinova, Dessislava, Anel, Alberto, Martin, Carlos, and Pardo, Julián

Abstract

It has been proposed that Mycobacterium tuberculosis virulent strains inhibit apoptosis and trigger cell death by necrosis of host macrophages to evade innate immunity, while non-virulent strains induce typical apoptosis activating a protective host response. As part of the characterization of a novel tuberculosis vaccine candidate, the M. tuberculosis phoP mutant SO2, we sought to evaluate its potential to induce host cell death. The parental M. tuberculosis MT103 strain and the current vaccine against tuberculosis Bacillus Calmette-Guérin (BCG) were used as comparators in mouse models in vitro and in vivo. Our data reveal that attenuated SO2 was unable to induce apoptotic events neither in mouse macrophages in vitro nor during lung infection in vivo. In contrast, virulent MT103 triggers typical apoptotic events with phosphatidylserine exposure, caspase-3 activation and nuclear condensation and fragmentation. BCG strain behaved like SO2 and did not induce apoptosis. A clonogenic survival assay confirmed that viability of BCG- or SO2-infected macrophages was unaffected. Our results discard apoptosis as the protective mechanism induced by SO2 vaccine and provide evidence for positive correlation between classical apoptosis induction and virulent strains, suggesting apoptosis as a possible virulence determinant during M. tuberculosis infection.

Published
2012

46. Changes in HSP gene and protein expression in natural scrapie with brain damage

Author

Acin, Cristina [0000-0001-5105-6133], Martín-Burriel, Inmaculada [0000-0001-6016-4726], Serrano, Carmen, Bolea, Rosa, Lyahyai, J., Filali, Hicham, Varona, Luis, Marcos-Carcavilla, A., Acin, Cristina, Calvo, Jorge Hugo, Serrano Noreña, Magdalena, Badiola, Juan J., Zaragoza, P., Martín-Burriel, Inmaculada, Acin, Cristina [0000-0001-5105-6133], Martín-Burriel, Inmaculada [0000-0001-6016-4726], Serrano, Carmen, Bolea, Rosa, Lyahyai, J., Filali, Hicham, Varona, Luis, Marcos-Carcavilla, A., Acin, Cristina, Calvo, Jorge Hugo, Serrano Noreña, Magdalena, Badiola, Juan J., Zaragoza, P., and Martín-Burriel, Inmaculada

Abstract

Heat shock proteins (Hsp) perform cytoprotective functions such as apoptosis regulation and inflammatory response control. These proteins can also be secreted to the extracellular medium, acting as inflammatory mediators, and their chaperone activity permits correct folding of proteins and avoids the aggregation of anomalous isoforms. Several studies have proposed the implication of Hsp in prion diseases. We analysed the gene expression and protein distribution of different members of the Hsp27, Hsp70, and Hsp90 families in the central nervous system of sheep naturally infected with scrapie. Different expression profiles were observed in the areas analysed. Whereas changes in transcript levels were not observed in the cerebellum or medulla oblongata, a significant decrease in HSP27 and HSP90 was detected in the prefrontal cortex. In contrast, HSP73 was over-expressed in diencephalons of scrapie animals. Western blotting did not reveal significant differences in Hsp90 and Hsp70 protein expression between scrapie and control animals. Expression rates identified by real-time RT-PCR and western blotting were compared with the extent of classical scrapie lesions using stepwise regression. Changes in Hsp gene and protein expression were associated with prion protein deposition, gliosis and spongiosis rather than with apoptosis. Finally, immunohistochemistry revealed intense Hsp70 and Hsp90 immunolabelling in Purkinje cells of scrapie sheep. In contrast, controls displayed little or no staining in these cells. The observed differences in gene expression and protein distribution suggest that the heat shock proteins analysed play a role in the natural form of the disease. © 2011 Serrano et al; licensee BioMed Central Ltd.

Published
2011

47. Calretinin-immunopositive cells and fibers in the cerebellar cortex of normal sheep

Author

Álvarez, M. Isabel, Lacruz, C., Toledano-Díaz, A., Monleón, E., Monzón, M., Badiola, Juan J., Álvarez, M. Isabel, Lacruz, C., Toledano-Díaz, A., Monleón, E., Monzón, M., and Badiola, Juan J.

Abstract

Calretinin (CR)-immunopositive cells and fibers in the cerebellar cortex (vermal archicerebellum-lobules X and IX-and neocerebellum-lobules VIIb and VIII) of two and 4-year-old Manchega and Rasa Aragonesa sheep were studied. CR-immunoreactivity was seen in subsets of all neurons and afferent fibers described in the cerebellar cortex. Generally, immunopositive cells were seen in very high densities in lobules X and IX, and in low density in lobule VIIb. Apparently, all unipolar brush cells were CR-immunopositive and showed a greater variety of shape than had been reported in other species. CR-immunoreactivity of Purkinje cells was either absent or varied from low to medium intensity. Few granule cell perikarya were immunostained (<5%) but a large number of their axons were CR-immunopositive. Subsets of stellate and basket cells were CR-immunoreactive-quite different to what is seen in most of mammalian species. Strongly CR-immunopositive mossy and climbing fibers, isolated or grouped, were observed in all lobules. Although we found neither a difference in CR-immunoreactivity between the two breds of sheep, nor between the two ages examined, we observed important differences in CR-immunoreactivity between sheep and other mammalian species. Our observation of neuronal clusters and groups of fibers with very high CR-immunopositivity supports the idea of a heterogeneous species-specific functional organization for the cerebellar cortex within an apparent homogeneous histological structure maintained throughout mammalian evolution. The results also suggest that the varied levels of CR expression may be related to the specific functions of these immunopositive neurons and fibers rather than to a general neuroprotective role played by calretinin in the cerebellar cortex. © 2008 Springer Science+Business Media, LLC.

Published
2008

48. Calretinin-immunopositive cells and fibers in the cerebellar cortex of normal sheep

Author

Álvarez-Vicente, María Isabel, Lacruz, César, Toledano-Díaz, A., Monleón, E., Monzón, Marta, Badiola, Juan J., Toledano Gasca, Adolfo, Álvarez-Vicente, María Isabel, Lacruz, César, Toledano-Díaz, A., Monleón, E., Monzón, Marta, Badiola, Juan J., and Toledano Gasca, Adolfo

Abstract

Calretinin (CR)-immunopositive cells and fibers in the cerebellar cortex (vermal archicerebellum-lobules X and IX-and neocerebellum-lobules VIIb and VIII) of two and 4-year-old Manchega and Rasa Aragonesa sheep were studied. CR-immunoreactivity was seen in subsets of all neurons and afferent fibers described in the cerebellar cortex. Generally, immunopositive cells were seen in very high densities in lobules X and IX, and in low density in lobule VIIb. Apparently, all unipolar brush cells were CR-immunopositive and showed a greater variety of shape than had been reported in other species. CR-immunoreactivity of Purkinje cells was either absent or varied from low to medium intensity. Few granule cell perikarya were immunostained (<5%) but a large number of their axons were CR-immunopositive. Subsets of stellate and basket cells were CR-immunoreactive-quite different to what is seen in most of mammalian species. Strongly CR-immunopositive mossy and climbing fibers, isolated or grouped, were observed in all lobules. Although we found neither a difference in CR-immunoreactivity between the two breds of sheep, nor between the two ages examined, we observed important differences in CR-immunoreactivity between sheep and other mammalian species. Our observation of neuronal clusters and groups of fibers with very high CR-immunopositivity supports the idea of a heterogeneous species-specific functional organization for the cerebellar cortex within an apparent homogeneous histological structure maintained throughout mammalian evolution. The results also suggest that the varied levels of CR expression may be related to the specific functions of these immunopositive neurons and fibers rather than to a general neuroprotective role played by calretinin in the cerebellar cortex. © 2008 Springer Science+Business Media, LLC.

Published
2008

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