Friedreich's ataxia
Friedreich's ataxia is an autosomal recessive genetic disease that causes difficulty walking, a loss of sensation in the arms and legs and impaired speech that worsens over time. Symptoms generally start between 5 and 20 years of age. Many develop hypertrophic cardiomyopathy and will require a mobility aid such as a cane, walker or wheelchair in their teens. As the disease progresses, people lose their sight and hearing. Other complications include scoliosis and diabetes mellitus.
The condition is caused by mutations in the FXN gene on chromosome 9. The FXN gene makes a protein called frataxin. In FRDA, the patient produces less frataxin. Degeneration of nerve tissue in the spinal cord causes the ataxia; particularly affected are the sensory neurons essential for directing muscle movement of the arms and legs through connections with the cerebellum. The spinal cord becomes thinner and nerve cells lose some myelin sheath.
No effective treatment exists, but there are several therapies in trials. FRDA shortens life expectancy due to heart disease and some people can live into their sixties or older.
FRDA affects 1 in 50,000 people in the United States and is the most common inherited ataxia. Rates are highest in people of Western European descent. The condition is named after the German physician Nikolaus Friedreich, who first described it in the 1860s.
Signs and symptoms
Symptoms typically start between the ages of 5 and 15, but in Late Onset FRDA they may occur after age 25 years. The progressive loss of coordination and muscle strength leads to loss of ambulation and the full-time use of a wheelchair. Most young people diagnosed with FRDA require mobility aids such as a cane, walker, or wheelchair by their childhood or early 20s.The disease is progressive with increasing staggering or stumbling gait and frequent falling. Lower extremities are more severely involved. On average, after 10–15 years, people lose the ability to stand or walk without assistance. However, disease progression is variable, and people may be able to walk decades after onset, while others require a wheelchair within a few years.
Symptoms may include the following:
- 91% of people develop heart problems such as cardiomegaly, symmetrical hypertrophy, heart murmurs, atrial fibrillation, tachycardia, hypertrophic cardiomyopathy and conduction defects
- Cerebellar: nystagmus, fast saccadic eye movements, dysmetria, loss of coordination
- Vision impairment
- Hearing impairment
- Slurred speech
- Abnormal curvature of the spine
- Dorsal column: Loss of vibratory sensation and proprioceptive sensation occurs
- About 20% of people have trouble metabolizing carbohydrates and 10% develop diabetes mellitus
- Lower motor neuron lesion: absent deep tendon reflexes
- Pyramidal: extensor plantar responses, and distal weakness
- Muscle weakness in the arms and legs
- High plantar arches
Genetics
In 96% of cases the mutant FXN gene has 90–1,300 GAA trinucleotide repeat expansions in intron 1 of both alleles. This expansion causes epigenetic changes and formation of heterochromatin near the repeat. The length of the shorter GAA repeat is correlated with the age of onset and disease severity. The formation of heterochromatin results in reduced transcription of the gene and low levels of frataxin. People with FDRA might have 5-35% of the frataxin protein compared to healthy individuals. Heterozygous carriers of the mutant FXN gene have 50% lower frataxin levels but this decrease is not enough to cause symptoms.
In about 4% of cases the disease is caused by a point mutation, where the patient has an expansion in one allele and a point mutation in the other. A missense point mutation can have milder symptoms.
Depending on the point mutation a patient may end up with no frataxin, nonfunctional frataxin or frataxin that is not properly localized to the mitochondria.
Pathophysiology
FRDA affects the nervous system, heart and pancreas and other systems. Degeneration of nerve tissue in the spinal cord causes ataxia. The sensory neurons essential for directing muscle movement of the arms and legs through connections with the cerebellum are particularly affected. The disease primarily affects the spinal cord and peripheral nerves. The spinal cord becomes thinner and nerve cells lose some myelin sheath. The diameter of the spinal cord is smaller than that of unaffected individuals mainly due to smaller dorsal root ganglia. The motor neurons of the spinal cord are affected to a lesser extent than sensory neurons. In peripheral nerves there is a loss of large myelinated sensory fibers.Structures in the brain are also affected by FRDA, notably the dentate nucleus of the cerebellum. In the heart, FRDA patients often develop some fibrosis, and over time many patients develop left ventricle hypertrophy and dilatation of the left ventricle.
Frataxin
The exact role of frataxin remains unclear. Frataxin assists iron-sulfur protein synthesis in the electron transport chain to generate adenosine triphosphate, the energy molecule necessary to carry out metabolic functions in cells. Frataxin also regulates iron transfer in the mitochondria by providing a proper amount of reactive oxygen species to maintain normal processes. One result of frataxin deficiency is mitochondrial iron overload, which damages many proteins due to effects on cellular metabolism.Without frataxin, the energy in the mitochondria falls, and excess iron creates extra ROS, leading to further cell damage. Low frataxin levels lead to insufficient biosynthesis of iron–sulfur clusters that are required for mitochondrial electron transport and assembly of functional aconitase and iron dysmetabolism of the entire cell.
Diagnosis
Balance difficulty, loss of proprioception, an absence of reflexes, and signs of other neurological problems are common signs from a physical examination.Diagnostic tests to support a physical examination include
- Electromyogram, which measures the electrical activity of muscle cells
- Nerve conduction studies, which measure the speed with which nerves transmit impulses
- Electrocardiogram, which gives a graphic presentation of the electrical activity or beat pattern of the heart
- Echocardiogram, which records the position and motion of the heart muscle
- Blood tests for elevated glucose levels and vitamin E levels
- X-ray radiograph for scoliosis
- MRI and CT scans of brain and spinal cord to rule out other neurological conditions
- Genetic testing
Management
As there is no cure, physical therapy is ‘a way of life’ for the patient. Physical therapists have a critical role to play in educating patients and caregivers as to correct posture, muscle use and the identification and avoidance of features which aggravate spasticity such as tight clothing, poorly adjusted wheelchairs, pain and infection.Because there is no cure, it is important that all FA patients engage with key community resources to contribute to the research process:
- : a database of all FA patients which can be used for accelerating research
- : an ongoing study charting FA over time which can be used for understanding the condition better.
- : an ongoing study charting FA over time which can be used for understanding the condition better.
- : the global patient alliance for FA; coordinates and funds research, is a center of news and information regarding FA
Rehabilitation
Physical therapy should consist of intensive motor coordination, balance, and stabilization training to preserve gains.To address the ataxic gait pattern and loss of proprioception, physical therapists can use visual cueing during gait training to help facilitate a more efficient gait pattern. Frenkel exercises and Proprioceptive Neuromuscular Facilitation stretching might help improve proprioception. Low intensity strengthening exercises should be incorporated to maintain functional use of the upper and lower extremities. Stabilization exercises of the trunk and lower back can help with postural control and the management of scoliosis, especially if the patient requires a wheelchair. Stretching and muscle relaxation exercises can be prescribed to help manage spasticity and prevent deformities. Other goals can be set according to the needs and wishes of the patient, including increased transfer and locomotion independence; muscle strengthening; increased physical resilience; “safe fall” strategy; learning to use mobility aids; learning how to reduce the body's energy expenditure; and developing specific breathing patterns.
Speech therapy is recommended.
Devices
Well-fitted orthoses can promote correct posture, support normal joint alignment, stabilize joints during walking, improve range of motion and gait, reduce spasticity and prevent foot deformities and scoliosis.Functional electrical stimulation or transcutaneous nerve stimulation devices may alleviate symptoms.
As progression of ataxia continues, assistive devices such as a cane, walker, or wheelchair may be required for mobility and independence. A standing frame can help reduce the secondary complications of prolonged use of a wheelchair.
Medication and surgery
Cardiac abnormalities can be controlled with ACE inhibitors such as enalapril, ramipril, lisinopril or trandolapril, sometimes used in conjunction with beta blockers. Patients with symptomatic heart failure might be prescribed eplerenone or digoxin to keep cardiac abnormalities under control.Surgery may correct deformities caused by abnormal muscle tone. Titanium screws and rods inserted in the spine help prevent or slow the progression of scoliosis. Surgery to lengthen the Achilles tendon can improve independence and mobility in patients suffering from equinus deformity. Patients experiencing severe heart failure can have an automated implantable cardioverter-defibrillator implanted or a cardiac transplant.
Prognosis
Every patient has a particular form of evolution of the disease. In general, patients who were younger at diagnosis, and those with longer GAA triplet expansions, tend to have more severe symptoms.Congestive heart failure and cardiac arrhythmia are the leading cause of death. However, patients with less severe symptoms can live into their sixties or older.
Epidemiology
FRDA affects Indo-European populations. It is rare in East Asians, Sub-Saharan Africans, and Native Americans.FRDA is the most prevalent inherited ataxia, affecting about 1 in 50,000 people in the United States. Males and females are affected equally. The estimated carrier prevalence is 1:100.
A 1990-1996 study of Europeans calculated the incidence rate was 2.8:100,000. A later study estimated prevalence of 3-4 cases per 100,000 individuals.
FRDA follows the same pattern as haplogroup R1b. Haplogroup R1b is the most frequently occurring paternal lineage in western Europe. FRDA and Haplogroup R1b are more common in northern Spain, Ireland and France, rare in Russia and Scandinavia, and follow a gradient through central and eastern Europe. A population carrying the disease went through a population bottleneck in the Franco-Cantabrian region during the last ice age.
A study of Japanese patients with spinocerebellar degeneration found a rate of 2.4% making the prevalence rate of FRDA much rarer at 1:1,000,000.
History
The condition is named after the 1860s German pathologist and neurologist, Nikolaus Friedreich. Friedreich reported five patients in three papers in 1863 at the University of Heidelberg. Further observations appeared in a paper in 1876.Frantz Fanon wrote his medical thesis on FRDA, in 1951.
A 1984 Canadian study traced 40 cases to one common ancestral couple arriving in New France in 1634.
FRDA was first linked to a GAA repeat expansion on chromosome 9 in 1996.
Research
Modulation of transcriptional factor Nrf2
- Reata Pharmaceuticals developed a drug RTA 408 to target activation of a transcriptional factor, Nrf2 and tested it in rodents. Nrf2 is decreased in FRDA cells. Omaveloxolone increased the number and efficiency of mitochondria in rats. In October 2019, Reata announced the results of the second part of a Phase 2/3 clinical trial. The MOXIe trial met the goal of the Friedreich's Ataxia Rating Scale after 48 weeks of treatment. This randomized, placebo-controlled, double-blind study evaluated the safety and efficacy of 150 mg omaveloxone.
Protection of mitochondrial membranes with a deuterated fatty acid
- Retrotope is advancing its first drug RT001 after releasing positive Phase 1b/2a results in 2018. RT001 is a deuterated synthetic homologue of ethyl linoleate, a polyunsaturated fatty acid or PUFAs. PUFAs are the major component of lipid membranes, particularly in mitochondria. Their high susceptibility to oxidation by reactive oxygen species might be reduced by the replacement of hydrogen atoms with the isotope deuterium. Primary endpoints were safety, tolerability, and pharmacokinetics. Secondary endpoints included the , a timed foot-walk test and cardiopulmonary exercise testing. The study met its primary safety and tolerability endpoints. An improvement in peak workload and VO2 max in the RT001 group compared to placebo, as well as a positive trend in the neurological scales in the drug group were detected.
Increasing synthesis of glutathione
- EPI-743 is a related compound to A0001 being developed by BioElectron which used to be known as Edison Pharmaceuticals. Open label studies were completed in 2012. EPI-743 is a para-benzoquinone and targets the NADH dehydrogenase enzyme to increase the biosynthesis of glutathione. Glutathione controls oxidative stress. It is being used in a number of related mitochondrial diseases clinical trials such as Leigh syndrome and is planned for a clinical trial for FRDA in 2019.
Flavonoids (food additives)
- Epicatechin is a natural flavonoid being developed by Cardero Therapeutics. In 2018 Cardero completed and open study in FRDA patients. Treatment with epicatechin was safe and tolerable over 24 weeks and resulted in neurological improvement of total Friedreich's Ataxia Rating Scale score, 8-m timed walk, nine-hole peg test, and a reduction in the left ventricular myocardial mass index in a subset of patients.
Frataxin replacements or stabilizers
- EPO mimetics are orally available peptide imitations of erythropoietin. They are small molecules erythropoietin receptor agonists designed to activate the tissue-protective erythropoietin receptor. STATegics plans to start a preclinical PK-PD study with a lead compound.
- Ubiquitin competitors. Since carriers of FRDA are asymptomatic but have a reduced level of frataxin it might be enough to just prevent existing frataxin degradation and increase levels of frataxin. Fratagene Therapeutics is developing a small molecule called RNF126 to inhibit an enzyme which degrades frataxin.
FXN gene expression
- BNM 290 is a second generation HDAC inhibitor which came from an acquisition by Biogen of Repligen's RG2833. HDAC inhibitors interfere with the histone deacetylase which functions to keep the DNA of a gene tightly coiled and silence protein expression. BioMarin planned to file an Investigational New Drug application in 2018.
- Jupiter Orphan Therapeutics is using resveratrol to improve mitochondrial function. In 2016, IND enabling studies were started in Australia for a modified compound normally found in the skins of red grapes.
- RNA-based approach to try to unsilence FXN gene and increase the expression of frataxin. This could be an effect of epigenetics and identifying novel non-coding RNA responsible for directing the localized epigenetic silencing of the FXN gene.
- Nicotinamide was found effective in preclinical FRDA models and well tolerated by patients. An open-label, dose-escalation study demonstrated that higher doses boosted frataxin expression but failed to establish any clinical benefit in a 12-month study.
- Etravirine, an antiviral drug used to treat HIV, was found in a drug repositioning screening to increase frataxin levels in peripheral cells derived from Friedreich's ataxia patients.
- Dimethyl fumarate has been shown to increase frataxin levels in FA patient-derived cells, mouse models, and humans. Multiple sclerosis patients treated with DMF showed an 85% increase in frataxin expression over 3 months.
Gene therapy
- An adeno-associated virus vector was used to reduce mitochondrial cardiomyopathy in a mice model in 2014.
- Lentivirus-mediated delivery of the FXN gene has been shown to increase frataxin expression and prevent DNA damage in human and mouse fibroblasts.
- CRISPR Therapeutics received a grant from the Friedreich's Ataxia Research Alliance to investigate gene editing as a potential treatment for the disease in 2017.
Society and culture
The Ataxian is a documentary that tells the story of Kyle Bryant, an athlete with FRDA who completes a long-distance bike race in an adaptive "trike" to raise money for research.
Dynah Haubert is a lawyer with FRDA who works for Disability Rights Pennsylvania. She spoke at the 2016 Democratic National Convention about her support for Hillary Clinton and her work supporting Americans with disabilities.
Geraint Williams in an athlete affected by FRDA who is known for scaling Mount Kilimanjaro in an adaptive wheelchair.
Shobhika Kalra is an activist with FRDA who helped build over 1000 wheelchair ramps across the UAE, with the goal to make Dubai fully wheelchair-friendly by 2020.