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Metabolic consequences of mitochondrial coenzyme A deficiency in patients with PANK2 mutations

Authors :
Emilio Ciusani
Amy Deik
Laura Strittmatter
Barbara Garavaglia
Sabrina Dusi
Giovanna Zorzi
Claudio Caccia
Valeria Tiranti
Marco Rimoldi
Vamsi K. Mootha
Enrico Bertini
Amanda Souza
Clary B. Clish
Paola Venco
Federica Zibordi
Nardo Nardocci
Valerio Leoni
Leoni, V
Strittmatter, L
Zorzi, G
Zibordi, F
Dusi, S
Garavaglia, B
Venco, P
Caccia, C
Souza, A
Deik, A
Clish, C
Rimoldi, M
Ciusani, E
Bertini, E
Nardocci N
Mootha, V
Tiranti, V
Leoni, Valerio
Strittmatter, Laura
Zorzi, Giovanna
Zibordi, Federica
Dusi, Sabrina
Garavaglia, Barbara
Venco, Paola
Caccia, Claudio
Souza, Amanda L.
Deik, Amy
Clish, Clary B.
Rimoldi, Marco
Ciusani, Emilio
Bertini, Enrico
Nardocci, Nardo
Mootha, Vamsi K.
Tiranti, Valeria
Publication Year :
2012

Abstract

Pantothenate kinase-associated neurodegeneration (PKAN) is a rare, inborn error of metabolism characterized by iron accumulation in the basal ganglia and by the presence of dystonia, dysarthria, and retinal degeneration. Mutations in pantothenate kinase 2 (PANK2), the rate-limiting enzyme in mitochondrial coenzyme A biosynthesis, represent the most common genetic cause of this disorder. How mutations in this core metabolic enzyme give rise to such a broad clinical spectrum of pathology remains a mystery. To systematically explore its pathogenesis, we performed global metabolic profiling on plasma from a cohort of 14 genetically defined patients and 18 controls. Notably, lactate is elevated in PKAN patients, suggesting dysfunctional mitochondrial metabolism. As predicted, but never previously reported, pantothenate levels are higher in patients with premature stop mutations in PANK2. Global metabolic profiling and follow-up studies in patient-derived fibroblasts also reveal defects in bile acid conjugation and lipid metabolism, pathways that require coenzyme A. These findings raise a novel therapeutic hypothesis, namely, that dietary fats and bile acid supplements may hold potential as disease-modifying interventions. Our study illustrates the value of metabolic profiling as a tool for systematically exploring the biochemical basis of inherited metabolic diseases. © 2011 Elsevier Inc.

Subjects

Subjects :
Male
Sphingomyelin
Lipid Metabolism Disorder
Endocrinology, Diabetes and Metabolism
Lipid Metabolism Disorders
Mitochondrion
Biochemistry
Pantothenic Acid
Cohort Studies
chemistry.chemical_compound
Endocrinology
Iron Metabolism Disorder
Neuroaxonal Dystrophie
Child
Genetics
Bile Acids and Salt
Sphingomyelins
Mitochondria
Phosphotransferases (Alcohol Group Acceptor)
Cholesterol
Codon, Nonsense
Child, Preschool
Metabolome
Female
Human
Adult
medicine.medical_specialty
Adolescent
Coenzyme A
PKAN
Neuroaxonal Dystrophies
Metabolomic
Biology
Pantothenate kinase-associated neurodegeneration
Article
Bile Acids and Salts
Young Adult
Genetic
Internal medicine
Bile acid conjugation
medicine
Humans
Lactic Acid
Molecular Biology
Pantothenate Kinase-Associated Neurodegeneration
Lipid metabolism
PANK2
medicine.disease
Lipid Metabolism
Iron Metabolism Disorders
chemistry
Inborn error of metabolism
metabolomics, mass spectrometry, oxysterols, cholesterol, organic acid
Cohort Studie

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....895851d2c5d70cb2e13ab97783bdd4d3

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