Prions are deadly infectious agents made of PrPSc, a misfolded variant of the cellular prion protein (PrPC) which self-propagates by inducing misfolding of native PrPC. PrPSc can adopt different pathogenic conformations (prion strains), which can be resistant to potential drugs, or acquire drug resistance, hampering the development of effective therapies. We identified Zn(II)-BnPyP, a tetracationic porphyrin that binds to distinct domains of native PrPC, eliciting a dual anti-prion effect. Zn(II)-BnPyP binding to a C-terminal pocket destabilizes the native PrPC fold, hindering conversion to PrPSc; Zn(II)-BnPyP binding to the flexible N-terminal tail disrupts N-to C-terminal interactions, triggering PrPC endocytosis and lysosomal degradation, thus reducing the substrate for PrPSc generation. Zn(II)-BnPyP inhibits propagation of different prion strains in vitro, in neuronal cells and organotypic brain cultures. These results identify a PrPC-targeting compound with an unprecedented dual mechanism of action which might be exploited to achieve anti-prion effects without engendering drug resistance.

Masone, A., Zucchelli, C., Caruso, E., Lavigna, G., Eraña, H., Giachin, G., et al. (2023). A tetracationic porphyrin with dual anti-prion activity. ISCIENCE, 26(9) [10.1016/j.isci.2023.107480].

A tetracationic porphyrin with dual anti-prion activity

Taiarol L.;Banfi S.;
2023

Abstract

Prions are deadly infectious agents made of PrPSc, a misfolded variant of the cellular prion protein (PrPC) which self-propagates by inducing misfolding of native PrPC. PrPSc can adopt different pathogenic conformations (prion strains), which can be resistant to potential drugs, or acquire drug resistance, hampering the development of effective therapies. We identified Zn(II)-BnPyP, a tetracationic porphyrin that binds to distinct domains of native PrPC, eliciting a dual anti-prion effect. Zn(II)-BnPyP binding to a C-terminal pocket destabilizes the native PrPC fold, hindering conversion to PrPSc; Zn(II)-BnPyP binding to the flexible N-terminal tail disrupts N-to C-terminal interactions, triggering PrPC endocytosis and lysosomal degradation, thus reducing the substrate for PrPSc generation. Zn(II)-BnPyP inhibits propagation of different prion strains in vitro, in neuronal cells and organotypic brain cultures. These results identify a PrPC-targeting compound with an unprecedented dual mechanism of action which might be exploited to achieve anti-prion effects without engendering drug resistance.
Articolo in rivista - Articolo scientifico
Cell biology; Molecular neuroscience; Pharmacology;
English
27-lug-2023
2023
26
9
107480
open
Masone, A., Zucchelli, C., Caruso, E., Lavigna, G., Eraña, H., Giachin, G., et al. (2023). A tetracationic porphyrin with dual anti-prion activity. ISCIENCE, 26(9) [10.1016/j.isci.2023.107480].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/525488
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