Mitochondrial Iron and Energetic Dysfunction Distinguish Fibroblasts and Induced Neurons from Pantothenate Kinase-associated Neurodegeneration Patients

Overview

Journal Neurobiol Dis

Specialty Neurology

Date 2015 Apr 4

PMID 25836419

Citations 45

Authors

Paolo Santambrogio

Sabrina Dusi

Michela Guaraldo

Luisa Ida Rotundo

Vania Broccoli

Barbara Garavaglia

Valeria Tiranti

Sonia Levi

Affiliations

Soon will be listed here.

Abstract

Pantothenate kinase-associated neurodegeneration is an early onset autosomal recessive movement disorder caused by mutation of the pantothenate kinase-2 gene, which encodes a mitochondrial enzyme involved in coenzyme A synthesis. The disorder is characterised by high iron levels in the brain, although the pathological mechanism leading to this accumulation is unknown. To address this question, we tested primary skin fibroblasts from three patients and three healthy subjects, as well as neurons induced by direct fibroblast reprogramming, for oxidative status, mitochondrial functionality and iron parameters. The patients' fibroblasts showed altered oxidative status, reduced antioxidant defence, and impaired cytosolic and mitochondrial aconitase activities compared to control cells. Mitochondrial iron homeostasis and functionality analysis of patient fibroblasts indicated increased labile iron pool content and reactive oxygen species development, altered mitochondrial shape, decreased membrane potential and reduced ATP levels. Furthermore, analysis of induced neurons, performed at a single cell level, confirmed some of the results obtained in fibroblasts, indicating an altered oxidative status and signs of mitochondrial dysfunction, possibly due to iron mishandling. Thus, for the first time, altered biological processes have been identified in vitro in live diseased neurons. Moreover, the obtained induced neurons can be considered a suitable human neuronal model for the identification of candidate therapeutic compounds for this disease.

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