1. Neurotrophin p75 Receptor Is Involved in Neuronal Damage by Prion Peptide-(106–126)
- Author
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Ilaria Dal-Pra, Ubaldo Armato, Valeria Politi, Filippo Rossi, Giuliano Della Valle, Vittorina Della-Bianca, Giovanni Perini, and Claudio Costantini
- Subjects
Programmed cell death ,Time Factors ,Prions ,Blotting, Western ,prion peptide(106-126) ,Receptors, Nerve Growth Factor ,Plasma protein binding ,Caspase 8 ,Receptor, Nerve Growth Factor ,Biochemistry ,Neuroblastoma ,Tumor Cells, Cultured ,Extracellular ,Humans ,Low-affinity nerve growth factor receptor ,p75 neurotrophin receptor ,Enzyme Inhibitors ,Binding site ,Receptor ,Molecular Biology ,Neurons ,Binding Sites ,Dose-Response Relationship, Drug ,biology ,human neuroblastoma cells ,Cell Biology ,Blotting, Northern ,Staurosporine ,Molecular biology ,Caspase 9 ,Peptide Fragments ,Cell biology ,Enzyme Activation ,Oxygen ,Microscopy, Fluorescence ,nervous system ,Caspases ,cytotoxicity ,biology.protein ,Protein Binding ,Neurotrophin - Abstract
In this work we have investigated the molecular basis of the neuronal damage induced by the prion peptide by searching for a surface receptor whose activation could be the first step of a cascade of events responsible for cell death. By using a human neuroblastoma cell line lacking all the neurotrophin receptors and derived clones expressing the full-length or truncated forms of the low affinity neurotrophin receptor (p75(NTR)), we have been able to demonstrate that the neuronal death induced by the prion protein fragment PrP-(106-126) is an active process mediated by a) the binding of the peptide to the extracellular region of p75(NTR), b) the signaling function of the intracytoplasmic region of the receptor, and c) the activation of caspase-8 and the production of oxidant species.
- Published
- 2001
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