Variant-dependent pharmacological rescue of phenylalanine hydroxylase supports a precision therapeutic strategy for phenylketonuria
Conde-Giménez, María ; Salillas, Sandra ; Galiana-Cameo, María ; Martínez-Oliván, Juan E. ; Mahía, Alejandro ; Ledesma, Manuel ; Galano-Frutos, Juan José ; Maity, Ritwik ; Velázquez-Campoy, Adrián (Universidad de Zaragoza) ; Díaz-de-Villegas, María D. ; Hurtado-Guerrero, Ramón ; Sancho, Javier
Resumen: Phenylketonuria (PKU) is an inherited metabolic disorder caused by pathogenic variants in phenylalanine hydroxylase (PAH), leading to toxic phenylalanine accumulation and severe neurological complications if untreated. Current pharmacological treatment relies on tetrahydrobiopterin (BH4), which benefits only a subset of patients, highlighting a major unmet need for alternative therapies. Here, we combined high-throughput screening, computational modelling, and drug repurposing to identify pharmacological chaperones capable of rescuing PAH function. We evaluated 26 structurally diverse small molecules in HEK293T cells expressing wild-type PAH or one of eight PKU-associated variants spanning phenotypes from mild to classical disease. Chaperoning efficacy was strongly variant-dependent, and for every variant tested at least one compound produced a greater activity increase than BH4 under identical assay conditions. Notably, belinostat, a clinically approved histone deacetylase inhibitor, emerged as the most effective compound for several clinically severe variants. Mechanistically, functional rescue consistently correlated with an increased population of tetrameric, catalytically competent PAH, as quantified by mass photometry. The crystal structure of the PAH–belinostat complex (PDB ID: 9T1O), together with structural models for all compounds, provide a framework for rational optimization. These results establish a preclinical proof-of-concept for genotype-guided pharmacological chaperone therapy in PKU and support the feasibility of personalized, variant-specific treatment strategies.
Idioma: Inglés
DOI: 10.1016/j.biopha.2026.119371
Año: 2026
Publicado en: BIOMEDICINE & PHARMACOTHERAPY 199 (2026), 119371 [15 pp.]
ISSN: 0753-3322
Financiación: info:eu-repo/grantAgreement/ES/DGA/E45-20R
Financiación: info:eu-repo/grantAgreement/ES/DGA/E45-23R
Financiación: info:eu-repo/grantAgreement/EC/H2020/101004806/EU/MOlecular-Scale Biophysics Research Infrastructure/MOSBRI
Financiación: info:eu-repo/grantAgreement/ES/MICINN/PID2019-107293GB-I00
Financiación: info:eu-repo/grantAgreement/ES/MICINN/PID2022-141068NB-I00
Tipo y forma: Article (Published version)
Área (Departamento): Área Bioquímica y Biolog.Mole. (Dpto. Bioq.Biolog.Mol. Celular)
Exportado de SIDERAL (2026-04-22-08:33:14)
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Idioma: Inglés
DOI: 10.1016/j.biopha.2026.119371
Año: 2026
Publicado en: BIOMEDICINE & PHARMACOTHERAPY 199 (2026), 119371 [15 pp.]
ISSN: 0753-3322
Financiación: info:eu-repo/grantAgreement/ES/DGA/E45-20R
Financiación: info:eu-repo/grantAgreement/ES/DGA/E45-23R
Financiación: info:eu-repo/grantAgreement/EC/H2020/101004806/EU/MOlecular-Scale Biophysics Research Infrastructure/MOSBRI
Financiación: info:eu-repo/grantAgreement/ES/MICINN/PID2019-107293GB-I00
Financiación: info:eu-repo/grantAgreement/ES/MICINN/PID2022-141068NB-I00
Tipo y forma: Article (Published version)
Área (Departamento): Área Bioquímica y Biolog.Mole. (Dpto. Bioq.Biolog.Mol. Celular)
Exportado de SIDERAL (2026-04-22-08:33:14)
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articulos > articulos-por-area > bioquimica_y_biologia_molecular
Notice créée le 2026-04-22, modifiée le 2026-04-22