Prolongation of prion disease-associated symptomatic phase relates to CD3(+) T cell recruitment into the CNS in murine scrapie-infected mice - INRAE - Institut national de recherche pour l’agriculture, l’alimentation et l’environnement
Article Dans Une Revue Brain, Behavior, and Immunity Année : 2012

Prolongation of prion disease-associated symptomatic phase relates to CD3(+) T cell recruitment into the CNS in murine scrapie-infected mice

Résumé

Prion diseases are caused by the transconformation of the host cellular prion protein PrPc into an infectious neurotoxic isoform called PrPSc. While vaccine-induced PrP-specific CD4(+)T cells and antibodies partially protect scrapie-infected mice from disease, the potential autoreactivity of CD8(+) cytotoxic T lymphocytes (CTLs) received little attention. Beneficial or pathogenic influence of PrPc-specific CTL was evaluated by stimulating a CD8(+) T-cell-only response against PrP in scrapie-infected C57BL/6 mice. To circumvent immune tolerance to PrP, five PrP-derived nonamer peptides identified using prediction algorithms were anchored-optimized to improve binding affinity for H-2D(b) and immunogenicity (NP-peptides). All of the NP-peptide; elicited a significant number of IFN gamma secreting CD8(+) T cells that better recognized the NP-peptides than the natives; three of them induced T cells that were lytic in vivo for NP-peptide-loaded target cells. Peptides 168 and 192 were naturally processed and presented by the 1C11 neuronal cell line. Mini:genes encoding immunogenic NP-peptides inserted into adenovirus (rAds) vectors enhanced the specific CD8(+)T-cell responses. Immunization with rAd encoding 168NP before scrapie inoculation significantly prolonged the survival of infected mice. This effect was attributable to a significant lengthening of the symptomatic phase and was associated with enhanced CD3(+) T cell recruitment to the CNS. However, immunization with Ad168NP in scrapie-incubating mice induced IFN gamma-secreting CD8(+) T cells that were not cytolytic in vivo and did not influence disease progression nor infiltrated the brain. In conclusion, the data suggest that vaccine-induced PrP-specific CD8(+) T cells interact with prions into the CNS during the clinical phase of the disease. (C) 2012 Elsevier Inc. All rights reserved.

Dates et versions

hal-02650045 , version 1 (29-05-2020)

Identifiants

Citer

Antoine Sacquin, Thomas Chaigneau, Valerie Defaweux, Micheline Adam, Benoît Schneider, et al.. Prolongation of prion disease-associated symptomatic phase relates to CD3(+) T cell recruitment into the CNS in murine scrapie-infected mice. Brain, Behavior, and Immunity, 2012, 26 (6), pp.919 - 930. ⟨10.1016/j.bbi.2012.04.002⟩. ⟨hal-02650045⟩
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