Post-translational modifications in prion diseases - Département de biologie
Article Dans Une Revue (Article De Synthèse) Frontiers in Molecular Neuroscience Année : 2024

Post-translational modifications in prion diseases

Résumé

More than 650 reversible and irreversible post-translational modifications (PTMs) of proteins have been listed so far. Canonical PTMs of proteins consist of the covalent addition of functional or chemical groups on target backbone amino-acids or the cleavage of the protein itself, giving rise to modified proteins with specific properties in terms of stability, solubility, cell distribution, activity, or interactions with other biomolecules. PTMs of protein contribute to cell homeostatic processes, enabling basal cell functions, allowing the cell to respond and adapt to variations of its environment, and globally maintaining the constancy of the milieu interieur (the body’s inner environment) to sustain human health. Abnormal protein PTMs are, however, associated with several disease states, such as cancers, metabolic disorders, or neurodegenerative diseases. Abnormal PTMs alter the functional properties of the protein or even cause a loss of protein function. One example of dramatic PTMs concerns the cellular prion protein (PrP C ), a GPI-anchored signaling molecule at the plasma membrane, whose irreversible post-translational conformational conversion (PTCC) into pathogenic prions (PrP Sc ) provokes neurodegeneration. PrP C PTCC into PrP Sc is an additional type of PTM that affects the tridimensional structure and physiological function of PrP C and generates a protein conformer with neurotoxic properties. PrP C PTCC into PrP Sc in neurons is the first step of a deleterious sequence of events at the root of a group of neurodegenerative disorders affecting both humans (Creutzfeldt–Jakob diseases for the most representative diseases) and animals (scrapie in sheep, bovine spongiform encephalopathy in cow, and chronic wasting disease in elk and deer). There are currently no therapies to block PrP C PTCC into PrP Sc and stop neurodegeneration in prion diseases. Here, we review known PrP C PTMs that influence PrP C conversion into PrP Sc . We summarized how PrP C PTCC into PrP Sc impacts the PrP C interactome at the plasma membrane and the downstream intracellular controlled protein effectors, whose abnormal activation or trafficking caused by altered PTMs promotes neurodegeneration. We discussed these effectors as candidate drug targets for prion diseases and possibly other neurodegenerative diseases.
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Dates et versions

hal-04788270 , version 1 (18-11-2024)

Identifiants

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Chloé Bizingre, Clara Bianchi, Anne Baudry, Aurélie Alleaume-Butaux, Benoit Schneider, et al.. Post-translational modifications in prion diseases. Frontiers in Molecular Neuroscience, 2024, 17, pp.1405415. ⟨10.3389/fnmol.2024.1405415⟩. ⟨hal-04788270⟩
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