Abstract
In prion diseases, PrPc, a widely expressed protein, is transformed into a pathogenic form called PrPSc, which is in itself infectious. Antibodies directed against PrPc have been shown to inhibit PrPc to PrPSc conversion in vitro and protect in vivo from disease. Other effectors with potential to eliminate PrPSc-producing cells are cytotoxic T cells directed against PrP-derived peptides but their ability to protect or to induce deleterious autoimmune reactions is not known. The natural tolerance to PrPc makes difficult to raise efficient adaptive responses. To break tolerance, adenovirus (Ad) encoding human PrP (hPrP) or control Ad were administered to wild-type mice by direct injection or by transfer of Ad-transduced dendritic cells (DCs). Control Ad-transduced DCs from Tg650 mice overexpressing hPrP were also used for immunization. DC-mediated but not direct administration of AdhPrP elicited antibodies that bound to murine native PrPc. Frequencies of PrP-specific IFNγ-secreting T cells were low and in vivo lytic activity only targeted cells strongly expressing hPrP. Immunohistochemical analysis revealed that CD3+ T cell infiltration was similar in the brain of vaccinated and unvaccinated 139A-infected mice suggesting the absence of autoimmune reactions. Early splenic PrPSc replication was strongly inhibited ten weeks post infection and mean survival time prolonged from 209 days in untreated 139A-infected mice to 246 days in mice vaccinated with DCs expressing the hPrP. The efficacy appeared to be associated with antibody but not with cytotoxic cell-mediated PrP-specific responses.
Highlights
In prion diseases, cellular prion protein (PrPc), a normal host protein present in the majority of tissues and highly expressed in the nervous system [1], is converted into a protease resistant form (PrPres), called scrapie PrP (PrPSc), which is in itself infectious [2]
Immunization of wt mice with AdhPrP induces weak immune responses against murine PrP and little increase in survival time after scrapie challenge We demonstrated in a previous study that cells transduced with
After immunization with AdhPrP but not with Ad not expressing hPrP transgene (AdTA), Prnp2/2 mice developed an humoral response to native murine PrP (mPrP) validating Ad vectors as efficient immunogens
Summary
Cellular prion protein (PrPc), a normal host protein present in the majority of tissues and highly expressed in the nervous system [1], is converted into a protease resistant form (PrPres), called scrapie PrP (PrPSc), which is in itself infectious [2]. PrPc is a protease sensitive glycoprotein which is attached to the cell membrane by a glycophosphatidylinositol anchor. PrPSc has a high b-sheet content and prone to aggregation. In the most widely accepted model, PrPSc interacts with PrPc and converts it into PrPSc [3]. Prion diseases are characterized by long asymptomatic periods of incubation. It has been reported that when PrPSc accumulation is stopped, PrPSc can be cleared, injury is reduced by compensatory neuronal mechanisms and synaptic function is restored [4], paving the way to therapeutics aimed at blocking PrPSc accumulation
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
