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Adenylosuccinate lyase deficiency (ADSLd) is a rare autosomal recessive purine metabolism disorder with several clinical manifestations. While toxic substrate accumulation is a known hallmark, no additional molecular mechanisms have been established. Here, we show that ADSLd is associated with mitochondrial dysfunction, including increased fragmentation, impaired respiration, and reduced ATP production. The severity of mitochondrial impairment correlates with ADSLd pathology, especially in mitochondria-dependent tissues. We also identify defects in mitochondrial dynamics and transport linked to ERK2 and AKT suppression. Notably, overexpressing constitutively active ERK2 or supplementing purine intermediates partially rescues the mitochondrial phenotype. These findings suggest an alternative disease mechanism and highlight mitochondrial metabolism as a potential therapeutic target in ADSLd.

Bordi, M., Testa, B., Compagnucci, C., Colasuonno, F., Cipressa, F., Betterini, E., et al. (2025). ADSL deficiency is a secondary mitochondrial disease affecting organelle homeostasis and ERK2/AKT signaling in a linear genotype-phenotype relation. CELL REPORTS, 44(9) [10.1016/j.celrep.2025.116230].

ADSL deficiency is a secondary mitochondrial disease affecting organelle homeostasis and ERK2/AKT signaling in a linear genotype-phenotype relation

Bordi M
;Colasuonno F;Cipressa F;Panfili FM;Rizza T;Campello S;Frezza C;Cecconi F
2025-01-01

Abstract

Adenylosuccinate lyase deficiency (ADSLd) is a rare autosomal recessive purine metabolism disorder with several clinical manifestations. While toxic substrate accumulation is a known hallmark, no additional molecular mechanisms have been established. Here, we show that ADSLd is associated with mitochondrial dysfunction, including increased fragmentation, impaired respiration, and reduced ATP production. The severity of mitochondrial impairment correlates with ADSLd pathology, especially in mitochondria-dependent tissues. We also identify defects in mitochondrial dynamics and transport linked to ERK2 and AKT suppression. Notably, overexpressing constitutively active ERK2 or supplementing purine intermediates partially rescues the mitochondrial phenotype. These findings suggest an alternative disease mechanism and highlight mitochondrial metabolism as a potential therapeutic target in ADSLd.
2025
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore BIO/10
Settore BIO/06
Settore BIOS-04/A - Anatomia, biologia cellulare e biologia dello sviluppo comparate
Settore BIOS-07/A - Biochimica
English
Con Impact Factor ISI
ADSL
CP: Metabolism
ERK
mitochondria
purine metabolism
rare genetic disease
Bordi, M., Testa, B., Compagnucci, C., Colasuonno, F., Cipressa, F., Betterini, E., et al. (2025). ADSL deficiency is a secondary mitochondrial disease affecting organelle homeostasis and ERK2/AKT signaling in a linear genotype-phenotype relation. CELL REPORTS, 44(9) [10.1016/j.celrep.2025.116230].
Bordi, M; Testa, B; Compagnucci, C; Colasuonno, F; Cipressa, F; Betterini, E; Mancini, A; Carsetti, C; Salvatori, I; Ferraina, C; Yang, M; De Cegli, R...espandi
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/431463
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