Your search keyword '"Espinosa Martín, Juan Carlos"' showing total 6 results

1. Protective effect of Val129-PrP against bovine spongiform encephalopathy but not variant Creutzfeldt-Jakob disease

Author

Kitamoto, Tetsuyuki [0000-0002-6298-2439], Marín-Moreno, Alba [0000-0002-4023-6398], Fernández-Borges, N., Espinosa Martín, Juan Carlos, Marín-Moreno, Alba, Aguilar-Calvo, Patricia, Asante, E. A., Kitamoto, Tetsuyuki, Mohri, S., Andréoletti, Olivier, Torres, J. M., Kitamoto, Tetsuyuki [0000-0002-6298-2439], Marín-Moreno, Alba [0000-0002-4023-6398], Fernández-Borges, N., Espinosa Martín, Juan Carlos, Marín-Moreno, Alba, Aguilar-Calvo, Patricia, Asante, E. A., Kitamoto, Tetsuyuki, Mohri, S., Andréoletti, Olivier, and Torres, J. M.

Abstract

Bovine spongiform encephalopathy (BSE) is the only known zoonotic prion that causes variant Creutzfeldt-Jakob disease (vCJD) in humans. The major risk determinant for this disease is the polymorphic codon 129 of the human prion protein (Hu-PrP), where either methionine (Met129) or valine (Val129) can be encoded. To date, all clinical and neuropathologically confirmed vCJD cases have been Met129 homozygous, with the exception of 1 recently reported Met/Val heterozygous case. Here, we found that transgenic mice homozygous for Val129 Hu-PrP show severely restricted propagation of the BSE prion strain, but this constraint can be partially overcome by adaptation of the BSE agent to the Met129 Hu-PrP. In addition, the transmission of vCJD to transgenic mice homozygous for Val129 Hu-PrP resulted in a prion with distinct strain features. These observations may indicate increased risk for vCJD secondary transmission in Val129 Hu-PrP–positive humans with the emergence of new strain features.

Published

2017

2. Transmission characteristics of variably protease-sensitive prionopathy

Author

Notari, S., Xiao, X., Espinosa Martín, Juan Carlos, Cohen, Y., Qing, L., Aguilar-Calvo, Patricia, Kofskey, D., Cali, Ignazio, Cracco, L., Kong, Qingzhong, Torres, J. M., Zou, Wenquan, Gambetti, Pierluigi, Notari, S., Xiao, X., Espinosa Martín, Juan Carlos, Cohen, Y., Qing, L., Aguilar-Calvo, Patricia, Kofskey, D., Cali, Ignazio, Cracco, L., Kong, Qingzhong, Torres, J. M., Zou, Wenquan, and Gambetti, Pierluigi

Abstract

Variably protease-sensitive prionopathy (VPSPr), a recently identified and seemingly sporadic human prion disease, is distinct from Creutzfeldt-Jakob disease (CJD) but shares features of Gerstmann-Sträussler-Scheinker disease (GSS). However, contrary to exclusively inherited GSS, no prion protein (PrP) gene variations have been detected in VPSPr, suggesting that VPSPr might be the long-sought sporadic form of GSS. The VPSPr atypical features raised the issue of transmissibility, a prototypical property of prion diseases. We inoculated VPSPr brain homogenate into transgenic mice expressing various levels of human PrP (PrPC). On first passage, 54% of challenged mice showed histopathologic lesions, and 34% harbored abnormal PrP similar to that of VPSPr. Surprisingly, no prion disease was detected on second passage. We concluded that VPSPr is transmissible; thus, it is an authentic prion disease. However, we speculate that normal human PrPC is not an efficient conversion substrate (or mouse brain not a favorable environment) and therefore cannot sustain replication beyond the first passage. © 2014, Centers for Disease Control and Prevention (CDC). All rights reserved.

Published

2014

3. Spontaneous generation of infectious prion disease in transgenic mice

Author

Castilla, Joaquín [0000-0002-2216-1361], Arroba, Ana I. [0000-0002-5136-1725], Torres, J. M., Castilla, Joaquín, Pintado, B., Gutiérrez-Adán, Alfonso, Andréoletti, Olivier, Aguilar-Calvo, Patricia, Arroba, Ana I., Parra-Arrondo, B., Ferrer, Isidro, Manzanares, Jorge, Espinosa Martín, Juan Carlos, Castilla, Joaquín [0000-0002-2216-1361], Arroba, Ana I. [0000-0002-5136-1725], Torres, J. M., Castilla, Joaquín, Pintado, B., Gutiérrez-Adán, Alfonso, Andréoletti, Olivier, Aguilar-Calvo, Patricia, Arroba, Ana I., Parra-Arrondo, B., Ferrer, Isidro, Manzanares, Jorge, and Espinosa Martín, Juan Carlos

Abstract

We generated transgenic mice expressing bovine cellular prion protein (PrPC) with a leucine substitution at codon 113 (113L). This protein is homologous to human protein with mutation 102L, and its genetic link with Gerstmann- Sträussler-Scheinker syndrome has been established. This mutation in bovine PrPC causes a fully penetrant, lethal, spongiform encephalopathy. This genetic disease was transmitted by intracerebral inoculation of brain homogenate from ill mice expressing mutant bovine PrP to mice expressing wild-type bovine PrP, which indicated de novo generation of infectious prions. Our findings demonstrate that a single amino acid change in the PrPC sequence can induce spontaneous generation of an infectious prion disease that differs from all others identified in hosts expressing the same PrPC sequence. These observations support the view that a variety of infectious prion strains might spontaneously emerge in hosts displaying random genetic PrPC mutations.

Published

2013

4. Classical bovine spongiform encephalopathy by transmission of H-type prion in homologous prion protein context

Author

Torres, J. M., Andréoletti, Olivier, Lacroux, C., Prieto, Irene, Lorenzo, Patricia, Larska, M., Baron, T., Espinosa Martín, Juan Carlos, Torres, J. M., Andréoletti, Olivier, Lacroux, C., Prieto, Irene, Lorenzo, Patricia, Larska, M., Baron, T., and Espinosa Martín, Juan Carlos

Abstract

Bovine spongiform encephalopathy (BSE) and BSErelated disorders have been associated with a single major prion strain. Recently, 2 atypical, presumably sporadic forms of BSE have been associated with 2 distinct prion strains that are characterized mainly by distinct Western blot profi les of abnormal protease-resistant prion protein (PrPres), named high-type (BSE-H) and low-type (BSE-L), that also differed from classical BSE. We characterized 5 atypical BSE-H isolates by analyzing their molecular and neuropathologic properties during transmission in transgenic mice expressing homologous bovine prion protein. Unexpectedly, in several inoculated animals, strain features emerged that were highly similar to those of classical BSE agent. These fi ndings demonstrate the capability of an atypical bovine prion to acquire classical BSE-like properties during propagation in a homologous bovine prion protein context and support the view that the epidemic BSE agent could have originated from such a cattle prion.

Published

2011

5. Transgenic mice expressing porcine prion protein resistant to classical scrapie but susceptible to sheep bovine spongiform encephalopathy and atypical scrapie

Author

Cassard, Hervé [0000-0001-8651-6179], Castilla, Joaquín [0000-0002-2216-1361], Lantier, Isabelle [0000-0003-1250-767X], Espinosa Martín, Juan Carlos, Herva, M. E., Andréoletti, Olivier, Padilla, D., Lacroux, C., Cassard, Hervé, Lantier, Isabelle, Castilla, Joaquín, Torres, J. M., Cassard, Hervé [0000-0001-8651-6179], Castilla, Joaquín [0000-0002-2216-1361], Lantier, Isabelle [0000-0003-1250-767X], Espinosa Martín, Juan Carlos, Herva, M. E., Andréoletti, Olivier, Padilla, D., Lacroux, C., Cassard, Hervé, Lantier, Isabelle, Castilla, Joaquín, and Torres, J. M.

Abstract

How susceptible pigs are to infection with sheep prions is unknown. We show, through transmission experiments in transgenic mice expressing porcine prion protein (PrP), that the susceptibility of this mouse model to bovine spongiform encephalopathy (BSE) can be enhanced after its passage in ARQ sheep, indicating that the pathogenicity of the BSE agent is modified after passage in sheep. Transgenic mice expressing porcine PrP were, nevertheless, completely resistant to infection with a broad panel of classical scrapie isolates from different sheep PrP genotypes and with different biochemical characteristics. The atypical (Nor98 like) isolate (SC-PS152) was the only scrapie isolate capable of transmission in these mice, although with a marked transmission barrier. Unexpectedly, the atypical scrapie agent appeared to undergo a strain phenotype shift upon transmission to porcine-PrP transgenic mice and acquired new strain properties, suggesting that atypical scrapie agent may exhibit different phenotypes depending on the host cellular PrP or other genetic factors.

Published

2009

6. Classic scrapie in sheep with the ARR/ARR prion genotype in Germany and France

Author

Groschup, M. H., Lacroux, C., Buschmann, A., Lühken, G., Mathey, J., Eiden, M., Lugan, Séverine, Hoffmann, C., Espinosa Martín, Juan Carlos, Baron, T., Torres, J. M., Erhardt, G., Andréoletti, Olivier, Groschup, M. H., Lacroux, C., Buschmann, A., Lühken, G., Mathey, J., Eiden, M., Lugan, Séverine, Hoffmann, C., Espinosa Martín, Juan Carlos, Baron, T., Torres, J. M., Erhardt, G., and Andréoletti, Olivier

Abstract

In the past, natural scrapie and bovine spongiform encephalopathy (BSE) infections have essentially not been diagnosed in sheep homozygous for the A136R154R171 haplotype of the prion protein. This genotype was therefore assumed to confer resistance to BSE and classic scrapie under natural exposure conditions. Hence, to exclude prions from the human food chain, massive breeding efforts have been undertaken in the European Union to amplify this gene. We report the identification of 2 natural scrapie cases in ARR/ARR sheep that have biochemical and transmission characteristics similar to cases of classic scrapie, although the abnormally folded prion protein (PrPSc) was associated with a lower proteinase-K resistance. PrPSc was clearly distinct from BSE prions passaged in sheep and from atypical scrapie prions. These findings strongly support the idea that scrapie prions are a mosaic of agents, which harbor different biologic properties, rather than a unique entity.

Published

2007