ABSTRACT
Friedreich ataxia (FA) is currently an incurable inherited mitochondrial neurodegenerative disease caused by reduced levels of frataxin. Cardiac failure constitutes the main cause of premature death in FA. While adeno-associated virus-mediated cardiac gene therapy was shown to fully reverse the cardiac and mitochondrial phenotype in mouse models, this was achieved at high dose of vector resulting in the transduction of almost all cardiomyocytes, a dose and biodistribution that is unlikely to be replicated in clinic. The purpose of this study was to define the minimum vector biodistribution corresponding to the therapeutic threshold, at different stages of the disease progression. Correlative analysis of vector cardiac biodistribution, survival, cardiac function and biochemical hallmarks of the disease revealed that full rescue of the cardiac function was achieved when only half of the cardiomyocytes were transduced. In addition, meaningful therapeutic effect was achieved with as little as 30% transduction coverage. This therapeutic effect was mediated through cell-autonomous mechanisms for mitochondria homeostasis, although a significant increase in survival of uncorrected neighboring cells was observed. Overall, this study identifies the biodistribution thresholds and the underlying mechanisms conditioning the success of cardiac gene therapy in Friedreich ataxia and provides guidelines for the development of the clinical administration paradigm.
Subject(s)
Cardiomyopathies/metabolism , Friedreich Ataxia/physiopathology , Myocytes, Cardiac/physiology , Animals , Disease Models, Animal , Dose-Response Relationship, Drug , Female , Friedreich Ataxia/therapy , Genetic Therapy/methods , Humans , Iron-Binding Proteins/physiology , Male , Mice , Mice, Transgenic , Mitochondria/physiology , Myocardium/metabolism , Myocytes, Cardiac/metabolism , Tissue Distribution , FrataxinABSTRACT
The design of antioxidant pharmaceuticals is a major challenge for the treatment of many clinical conditions and in aging. Free radical damage (FRD) is primarily catalysed by iron catalytic centers. Most of the natural and synthetic antioxidants are ineffective in inhibiting FRD because of the achievement of low concentrations at the affected tissues. Despite that many chelators inhibit FRD in vitro and in vivo, only Deferiprone (L1) has been shown to be effective and safe in the reversal of oxidative stress related tissue damage in iron overload and other conditions such as cardiomyopathy, acute kidney disease, Friedreich ataxia etc. Deferiprone, other chelators and their combinations could be used as main, adjuvant and alternative therapies in untreated conditions eg forms of cancer, Alzheimer's and Parkinson's diseases. Therapeutic targeting in each case requires specific chelator selection based on structure/activity correlation and consideration of other parameters eg ADMET. The ability of L1 to reach extracellular and intracellular compartments of almost all tissues including the brain is a major advantage for further development and use in many clinical conditions.
Subject(s)
Antioxidants/therapeutic use , Iron Chelating Agents/therapeutic use , Oxidative Stress/drug effects , Pyridones/therapeutic use , Acute Kidney Injury/physiopathology , Cardiomyopathies/physiopathology , Deferiprone , Free Radicals/antagonists & inhibitors , Friedreich Ataxia/physiopathology , Humans , Iron Overload/physiopathology , Oxidative Stress/physiologyABSTRACT
INTRODUCTION: Friedreich's ataxia (FRDA) is an inherited ataxia with a range of progressive features including axonal degeneration of sensory nerves. The aim of this study was to investigate auditory perception in affected individuals. METHODS: Fourteen subjects with genetically defined FRDA participated. Two control groups, one consisting of healthy, normally hearing individuals and another comprised of subjects with sensorineural hearing loss, were also assessed. Auditory processing was evaluated using structured tasks designed to reveal the listeners' ability to perceive temporal and spectral cues. Findings were then correlated with open-set speech understanding. RESULTS: Nine of 14 individuals with FRDA showed evidence of auditory processing disorder. Gap and amplitude modulation detection levels in these subjects were significantly elevated, indicating impaired encoding of rapid signal changes. Electrophysiologic findings (auditory brainstem response, ABR) also reflected disrupted neural activity. Speech understanding was significantly affected in these listeners and the degree of disruption was related to temporal processing ability. Speech analyses indicated that timing cues (notably consonant voice onset time and vowel duration) were most affected. CONCLUSION: The results suggest that auditory pathway abnormality is a relatively common consequence of FRDA. Regular auditory evaluation should therefore be part of the management regime for all affected individuals. This assessment should include both ABR testing, which can provide insights into the degree to which auditory neural activity is disrupted, and some functional measure of hearing capacity such as speech perception assessment, which can quantify the disorder and provide a basis for intervention.
Subject(s)
Auditory Perceptual Disorders/diagnosis , Friedreich Ataxia/diagnosis , Acoustic Stimulation , Adolescent , Adult , Auditory Pathways/physiopathology , Auditory Perceptual Disorders/genetics , Auditory Perceptual Disorders/physiopathology , Brain Stem/physiopathology , Cohort Studies , Cues , Evoked Potentials, Auditory, Brain Stem/genetics , Evoked Potentials, Auditory, Brain Stem/physiology , Female , Friedreich Ataxia/genetics , Friedreich Ataxia/physiopathology , Hearing Loss, Sensorineural/diagnosis , Hearing Loss, Sensorineural/genetics , Hearing Loss, Sensorineural/physiopathology , Humans , Male , Middle Aged , Phonetics , Pitch Perception , Reference Values , Sound Spectrography , Speech Acoustics , Speech Perception/genetics , Speech Perception/physiology , Time Perception , Young AdultABSTRACT
BACKGROUND AND PURPOSE: A pilot study of high dose coenzyme Q(10) (CoQ(10))/vitamin E therapy in Friedreich's ataxia (FRDA) patients resulted in significant clinical improvements in most patients. This study investigated the potential for this treatment to modify clinical progression in FRDA in a randomized double blind trial. METHODS: Fifty FRDA patients were randomly divided into high or low dose CoQ(10)/ vitamin E groups. The change in International Co-operative Ataxia Ratings Scale (ICARS) was assessed over 2 years as the primary end-point. A post hoc analysis was made using cross-sectional data. RESULTS: At baseline serum CoQ(10) and vitamin E levels were significantly decreased in the FRDA patients (P < 0.001). During the trial CoQ(10) and vitamin E levels significantly increased in both groups (P < 0.01). The primary and secondary end-points were not significantly different between the therapy groups. When compared to cross-sectional data 49% of all patients demonstrated improved ICARS scores. This responder group had significantly lower baseline serum CoQ(10) levels. CONCLUSIONS: A high proportion of FRDA patients have a decreased serum CoQ(10) level which was the best predictor of a positive clinical response to CoQ(10)/vitamin E therapy. Low and high dose CoQ(10)/vitamin E therapies were equally effective in improving ICARS scores.
Subject(s)
Friedreich Ataxia/drug therapy , Ubiquinone/analogs & derivatives , Vitamin E Deficiency/drug therapy , Vitamin E/administration & dosage , Adolescent , Adult , Antioxidants/administration & dosage , Dose-Response Relationship, Drug , Electron Transport Chain Complex Proteins/genetics , Electron Transport Chain Complex Proteins/metabolism , Endpoint Determination , Energy Metabolism/drug effects , Energy Metabolism/physiology , Female , Friedreich Ataxia/metabolism , Friedreich Ataxia/physiopathology , Humans , Male , Mitochondria/genetics , Mitochondria/metabolism , Muscle, Striated/metabolism , Muscle, Striated/physiopathology , Oxidative Stress/drug effects , Oxidative Stress/physiology , Predictive Value of Tests , Treatment Outcome , Ubiquinone/administration & dosage , Ubiquinone/blood , Ubiquinone/deficiency , Up-Regulation/drug effects , Up-Regulation/physiology , Vitamin E Deficiency/blood , Vitamin E Deficiency/physiopathology , Young AdultABSTRACT
BACKGROUND: Friedreich's ataxia is an autosomal recessive neurodegenerative disease where impaired mitochondrial function and excessive production of free radicals play a central pathogenetic role. Idebenone, a synthetic analogue of coenzyme Q, is a powerful antioxidant that was first administrated to Friedreich's ataxia patients less than 10 years ago. OBJECTIVE: The aim of this study was to evaluate the efficacy of idebenone administration and define the optimal dosage. METHODS: A critical evaluation of all open and double-blinded idebenone trials in Friedreich's ataxia patients was undertaken. RESULTS/CONCLUSIONS: Idebenone is well tolerated in paediatric and adult patients. Most trials demonstrated a positive effect on cardiac hypertrophy. The neurological function is in general not modified in adult patients, but a dose-dependent effect was demonstrated in young Friedreich's ataxia patients. Further double-blinded high-dose trials should evaluate idebenone in Friedreich's ataxia early in the disease course.
Subject(s)
Antioxidants/therapeutic use , Friedreich Ataxia/drug therapy , Ubiquinone/analogs & derivatives , Antioxidants/pharmacology , Clinical Trials as Topic , Dose-Response Relationship, Drug , Friedreich Ataxia/diagnosis , Friedreich Ataxia/physiopathology , Humans , Magnetic Resonance Angiography , Ubiquinone/pharmacology , Ubiquinone/therapeutic useABSTRACT
BACKGROUND: Friedreich's ataxia (FA) is a progressive, multisystem, degenerative disorder caused by a reduction in frataxin. Loss of frataxin results in mitochondrial dysfunction and oxidative damage in patients and model systems. Previous studies have indicated that the antioxidant idebenone (5 mg/kg daily) reduces cardiac hypertrophy, but definite improvement in neurological function has not been shown. METHODS: 48 genetically confirmed FA patients, aged 9-17 years, were enrolled in a 6-month, randomised, double-blind, placebo-controlled study. The patients received placebo or one of three doses of idebenone (approximately 5 mg/kg, 15 mg/kg, and 45 mg/kg), stratified by body weight. The primary endpoint was change from baseline in urinary 8-hydroxy-2'-deoxyguanosine (8OH2'dG), a marker of oxidative DNA damage. Secondary endpoints included changes in the international cooperative ataxia rating scale (ICARS), the FA rating scale (FARS), and a survey of activities of daily living (ADL). This study is registered with ClinicalTrials.gov, number NCT00229632. FINDINGS: Idebenone was generally well tolerated with similar numbers of adverse events in each group. One child receiving high-dose idebenone developed neutropenia after 6 months, which resolved after discontinuation of treatment. 8OH2'dG concentrations were not increased, and did not significantly change with idebenone treatment. Whereas an overall analysis did not show a significant difference in ICARS, FARS, or ADL total scores, there were indications of a dose-dependent response in the ICARS score. A second, pre-specified analysis, excluding patients who required wheelchair assistance, showed a significant improvement in ICARS (Bonferroni p=0.03) and suggested a dose-related response in ICARS, FARS, and ADL scores. INTERPRETATION: Treatment with higher doses of idebenone was generally well tolerated and associated with improvement in neurological function and ADL in patients with FA. The degree of improvement correlated with the dose of idebenone, suggesting that higher doses may be necessary to have a beneficial effect on neurological function.
Subject(s)
Antioxidants/therapeutic use , Benzoquinones/therapeutic use , Friedreich Ataxia/drug therapy , Friedreich Ataxia/physiopathology , Nervous System/drug effects , Nervous System/physiopathology , 8-Hydroxy-2'-Deoxyguanosine , Activities of Daily Living , Adolescent , Antioxidants/administration & dosage , Antioxidants/adverse effects , Benzoquinones/administration & dosage , Benzoquinones/adverse effects , Child , DNA Damage , Deoxyguanosine/analogs & derivatives , Deoxyguanosine/urine , Dose-Response Relationship, Drug , Female , Friedreich Ataxia/genetics , Friedreich Ataxia/urine , Humans , Male , Neutropenia/chemically induced , Severity of Illness Index , Ubiquinone/analogs & derivativesABSTRACT
There is currently no effective treatment for Friedreich's ataxia (FA), the most common of the hereditary ataxias. The disease is caused by mutations in FRDA that drastically reduce expression levels of the mitochondrial protein frataxin. In FA animal models, a key difficulty is obtaining the precise levels of frataxin expression in the appropriate tissues to provoke pathology without early lethality. To develop strategies to circumvent these problems, conditional frataxin transgenic mice have been generated. We now show that frataxin expression can be eliminated in neurons from these loxP[frda] mice by infection with CRE-expressing herpes simplex virus type 1 (HSV-1) amplicon vectors. We have also achieved in vivo delivery by stereotaxic injection of these CRE-expressing vectors into the brainstem of loxP[frda] mice to generate a localized gene knockout model. These mice develop a behavioral deficit in the rotarod assay detectable after 4 weeks, and when re-injected with HSV-1 amplicon vectors expressing human frataxin complementary DNA (cDNA) exhibit behavioral recovery as early as 4 weeks after the second injection. To the best of our knowledge, this is the first proof of principle of recovery of neurological function by a therapeutic agent aimed at correcting frataxin deficiency.
Subject(s)
Friedreich Ataxia/therapy , Herpesvirus 1, Human/genetics , Iron-Binding Proteins/genetics , Animals , Blotting, Western , Brain Stem/metabolism , Cells, Cultured , Disease Models, Animal , Female , Friedreich Ataxia/genetics , Friedreich Ataxia/physiopathology , Gene Amplification , Gene Library , Genetic Vectors/administration & dosage , Genetic Vectors/genetics , Humans , Iron-Binding Proteins/metabolism , Iron-Binding Proteins/physiology , Mice , Mice, Knockout , Mice, Transgenic , Mutation , Neurons/metabolism , Rotarod Performance Test , FrataxinABSTRACT
Peripheral nervous system (PNS) sensory neurons are directly involved in the pathophysiology of a number of debilitating inherited and acquired neurological conditions. The lack of effective treatments for many such conditions provides a strong rationale for exploring novel therapeutic approaches, including gene therapy. Friedreich ataxia (FRDA), a sensory neuropathy, is a progressive neurodegenerative disease associated with a loss of large sensory neurons from the dorsal root ganglia. Because a mouse model for this well-characterized disease has been generated, we elected to use FRDA as a model disease. In previous studies we achieved efficient and sustained delivery of a reporter gene to PNS sensory neurons, using recombinant adeno-associated viral (AAV) and lentiviral (LV) vectors. In the current study, AAV and LV vectors encoding the human frataxin cDNA were constructed and assessed for frataxin expression and function in primary FRDA patient fibroblast cell lines. FRDA fibroblasts have been shown to exhibit subtle biochemical changes, including increased mitochondrial iron and sensitivity to oxidant stress. Despite the inherent difficulty in working with primary cells, transduction of patient fibroblasts with either vector resulted in the expression of appropriately localized frataxin and partial reversal of phenotype.
Subject(s)
Friedreich Ataxia/genetics , Friedreich Ataxia/therapy , Gene Transfer Techniques , Genetic Therapy/methods , Iron-Binding Proteins/genetics , Oxidative Stress , Adenoviridae/genetics , DNA, Complementary/genetics , Epithelial Cells/physiology , Fibroblasts , Friedreich Ataxia/physiopathology , Genetic Vectors , HeLa Cells , Humans , In Vitro Techniques , Iron/analysis , Lentivirus/genetics , Mitochondria/chemistry , Phenotype , Treatment Outcome , FrataxinABSTRACT
Friedreich's ataxia is caused by a pronounced lack of frataxin, a mitochondrial protein of not fully understood function. Lack of frataxin homologues in yeast and mice leads to increased sensitivity to oxidative stress, depletion of proteins with iron-sulfur clusters like respiratory chain complexes I-III and aconitase, and to iron accumulation in mitochondria. Similar effects have been demonstrated in human disease with increased markers of oxidative DNA damage in urine and impaired oxidative phosphorylation in in vivo exercise studies using 31 Phosphorus magnetic resonance spectroscopy (31P-MRS). Therapeutical trials mainly focus on antioxidative treatment with coenzyme Q10 or its short-chain variant idebenone. Promising effects on cardiac hypertrophy in uncontrolled preliminary studies contrast with minor effects in controlled trials and no effect of antioxidants on neurological deficits has been established. Preliminary encouraging 31P-MRS data exist for the treatment with L-carnitine but not with creatine. However, all these interventions may take effect too late in the pathogenic process. Alternative strategies aiming at an enhancement of frataxin by stem cell transplantation, gene transfer or frataxin supplementation are desirable. Additionally, more efficient biomarkers are needed to monitor treatment effects.
Subject(s)
Friedreich Ataxia/therapy , Animals , Friedreich Ataxia/genetics , Friedreich Ataxia/physiopathology , HumansABSTRACT
Friedreich's ataxia (FRDA) is a neuro-degenerative disease causing limb and gait ataxia and hypertrophic cardiomyopathy. It results from a triplet expansion in the first intron of the frataxin gene encoding a mitochondrial protein of yet unknown function. Cells with low frataxin content display generalized deficiency of mitochondrial iron-sulfur cluster-containing proteins, which presumably denotes overproduction of superoxide radicals in these organelles. Idebenone, a short-chain quinone, may act as a potent free radical scavenger protecting mitochondria against oxidative stress. We therefore carried out an open trial of idebenone (oral supplementation; 5mg/kg/day) in a large series of FRDA patients and followed their left ventricular mass and function. Consistent and definitive worsening being observed in the natural course of the disease and cardiac hypertrophy having no chance of spontaneous reversal and to be subject to a placebo effect, the patient's heart status before and after the treatment was used to unambiguously establish the effect of the drug. After six months, heart ultrasound revealed more than 20% reduction of left ventricular mass in about half of the patients (p < 0.001) and no significant change in the other half. Since any measurable reversion of this pathogenic trait is highly significant, this demonstrates the efficiency of idebenone in controlling heart hypertrophy in FRDA. Owing to the absence of side effects of the drug, idebenone (up to 15mg/kg/day) should be prescribed for FRDA patients continuously as early as possible.