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Article Abstract

We investigate the interaction of hemin with four fragments of prion protein (PrP) containing from one to four histidines (PrP, PrP, PrP, PrP) for its potential relevance to prion diseases and possibly traumatic brain injury. The binding properties of hemin-PrP complexes have been evaluated by UV-visible spectrophotometric titration. PrP peptides form a 1:1 adduct with hemin with affinity that increases with the number of histidines and length of the peptide; the following log K binding constants have been calculated: 6.48 for PrP, 6.1 for PrP, 4.80 for PrP, whereas for PrP, the interaction is too weak to allow a reliable binding constant calculation. These constants are similar to that of amyloid-β (Aβ) for hemin, and similarly to hemin-Aβ, PrP peptides tend to form a six-coordinated low-spin complex. However, the concomitant aggregation of PrP induced by hemin prevents calculation of the K binding constant. The turbidimetry analysis of [hemin-PrP] shows that, once aggregated, this complex is scarcely soluble and undergoes precipitation. Finally, a detailed study of the peroxidase-like activity of [hemin-(PrP)] shows a moderate increase of the reactivity with respect to free hemin, but considering the activity over long time, as for neurodegenerative pathologies, it might contribute to neuronal oxidative stress.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7589926PMC
http://dx.doi.org/10.3390/ijms21207553DOI Listing

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