Pubblicazioni

Molecular and cellular studies reveal folding defects of human ornithine aminotransferase variants associated with gyrate atrophy of the choroid and retina  (2021)

Autori:
Montioli, Riccardo; Sgaravizzi, Giada; Desbats, Maria Andrea; Grottelli, Silvia; Voltattorni, Carla Borri; Salviati, Leonardo; Cellini, Barbara
Titolo:
Molecular and cellular studies reveal folding defects of human ornithine aminotransferase variants associated with gyrate atrophy of the choroid and retina
Anno:
2021
Tipologia prodotto:
Articolo in Rivista
Tipologia ANVUR:
Articolo su rivista
Lingua:
Inglese
Formato:
Elettronico
Referee:
Nome rivista:
FRONTIERS IN MOLECULAR BIOSCIENCES
ISSN Rivista:
2296-889X
N° Volume:
8
Numero o Fascicolo:
695205
Intervallo pagine:
1-13
Parole chiave:
gyrate atrophy; ornithine aminotransferase; pathogenic variant; pyridoxal phosphate; vitamin B6
Breve descrizione dei contenuti:
The deficit of human ornithine aminotransferase (hOAT) is responsible for gyrate atrophy (GA), a rare recessive inherited disorder. Although more than 60 disease-associated mutations have been identified to date, the molecular mechanisms explaining how each mutation leads to the deficit of OAT are mostly unknown. To fill this gap, we considered six representative missense mutations present in homozygous patients concerning residues spread over the hOAT structure. E. coli expression, spectroscopic, kinetic and bioinformatic analyses, reveal that the R154L and G237D mutations induce a catalytic more than a folding defect, the Q90E and R271K mutations mainly impact folding efficiency, while the E318K and C394Y mutations give rise to both folding and catalytic defects. In a human cellular model of disease folding-defective variants, although at a different extent, display reduced protein levels and/or specific activity, due to increased aggregation and/or degradation propensity. The supplementation with Vitamin B6, to mimic a treatment strategy available for GA patients, does not significantly improve the expression/activity of folding-defective variants, in contrast with the clinical responsiveness of patients bearing the E318K mutation. Thus, we speculate that the action of vitamin B6 could be also independent of hOAT. Overall, these data represent a further effort toward a comprehensive analysis of GA pathogenesis at molecular and cellular level, with important relapses for the improvement of genotype/phenotype correlations and the development of novel treatments.
Pagina Web:
https://doi.org/10.3389/fmolb.2021.695205
Id prodotto:
122099
Handle IRIS:
11562/1047384
ultima modifica:
8 novembre 2022
Citazione bibliografica:
Montioli, Riccardo; Sgaravizzi, Giada; Desbats, Maria Andrea; Grottelli, Silvia; Voltattorni, Carla Borri; Salviati, Leonardo; Cellini, Barbara, Molecular and cellular studies reveal folding defects of human ornithine aminotransferase variants associated with gyrate atrophy of the choroid and retina «FRONTIERS IN MOLECULAR BIOSCIENCES» , vol. 8 , n. 6952052021pp. 1-13

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