Fragile X-associated tremor/ataxia syndrome (FXTAS) is a late-onset

neurodegenerative disorder A neurodegenerative disease is caused by the progressive loss of neurons, in the process known as neurodegeneration. Neuronal damage may also ultimately result in their death. Neurodegenerative diseases include amyotrophic lateral sclerosis, mul ...

most frequently seen in male premutation carriers of

Fragile X syndrome Fragile X syndrome (FXS) is a genetic neurodevelopmental disorder. The average IQ in males with FXS is under 55, while affected females tend to be in the borderline to normal range, typically around 70–85. Physical features may include a lo ...

(FXS) over the age of 50. The main clinical features of FXTAS include problems of movement with cerebellar gait ataxia and action

tremor A tremor is an involuntary, somewhat rhythmic muscle contraction and relaxation involving neural oscillations, oscillations or twitching movements of one or more body parts. It is the most common of all involuntary movements and can affect the h ...

. Associated features include

parkinsonism Parkinsonism is a clinical syndrome characterized by tremor, bradykinesia (slowed movements), Rigidity (neurology), rigidity, and balance disorder, postural instability. Both hypokinetic features (bradykinesia and akinesia) and hyperkinetic f ...

, cognitive decline, and dysfunction of the

autonomic nervous system The autonomic nervous system (ANS), sometimes called the visceral nervous system and formerly the vegetative nervous system, is a division of the nervous system that operates viscera, internal organs, smooth muscle and glands. The autonomic nervo ...

. FXTAS is found in Fragile X "premutation" carriers, which is defined as a

trinucleotide repeat expansion A trinucleotide repeat expansion, also known as a triplet repeat expansion, is the DNA mutation responsible for causing any type of disorder categorized as a trinucleotide repeat disorder. These are labelled in dynamical genetics as dynamic muta ...

of 55-200 CGG repeats in the Fragile X mental retardation-1 (''

FMR1 ''FMR1'' (Fragile X Messenger Ribonucleoprotein 1) is a human gene that codes for a protein called ''fragile X messenger ribonucleoprotein'', or FMRP. This protein, most commonly found in the brain, is essential for normal cognitive developmen ...

'') gene. 4-40 CGG repeats in this gene is considered normal, while individual with >200 repeats have full Fragile X Syndrome. In contrast to FXS full mutation, which is diagnosed early in childhood, symptoms of FXTAS manifest in individuals over the age of 50. Like FXS, FXTAS is most common and most severe in males due to the mutation's X-linked inheritance pattern. FXTAS has an incidence of 30-40% (male) and 8-15% (female) among FXS premutation carriers over the age of 50. ''FMR1''

mRNA In molecular biology, messenger ribonucleic acid (mRNA) is a single-stranded molecule of RNA that corresponds to the genetic sequence of a gene, and is read by a ribosome in the process of Protein biosynthesis, synthesizing a protein. mRNA is ...

is found to be elevated in patients with FXTAS in contrast to FXS, where the ''FMR1'' gene is transcriptionally silenced via

DNA methylation DNA methylation is a biological process by which methyl groups are added to the DNA molecule. Methylation can change the activity of a DNA segment without changing the sequence. When located in a gene promoter (genetics), promoter, DNA methylati ...

. In both diseases the ''FMR1'' gene product, Fragile X mental retardation protein (FMRP) is diminished, but in FXTAS this is believed to be mediated by RNA toxicity, while in FXS, FMRP is absent due to transcriptional silencing. There is no cure for FXTAS, but several of the symptoms can be managed with medication.

Symptoms and signs

The physical symptoms of FXTAS include an intention tremor, cerebellar ataxia, and

. This includes small, shuffling steps, muscle rigidity and slowed speech, as well as neuropathic symptoms. As the disease progresses to the more advanced stages, an individual with FXTAS is also at risk of autonomic dysfunction: hypertension, bowel and bladder dysfunction, and impotence. An individual with FXTAS may also exhibit the following symptoms: a decrease in cognition, which includes diminishing short-term memory and executive function skills, declining math and spelling abilities and decision-making abilities. FXTAS may also result in changes in personality, due to alterations of the limbic area in the brain. This includes increased irritability, angry outbursts, and impulsive behaviour

Diagnosis

FXTAS can be diagnosed using a combination of molecular, clinical, and radiological findings. In order for individuals to develop FXTAS, they must first be premutation carriers, having between 55 and 200 CGG

of the ''

'' gene. A definite, probable, or possible diagnosis of FXTAS can be assigned based on combined clinical or radiological findings in conjunction with the molecular premutation. Clinical findings are divided into major and minor symptoms. Major symptoms include

intention tremor Intention tremor is a dyskinesia, dyskinetic disorder characterized by a broad, coarse, and low-frequency (below 5 Hz) tremor evident during deliberate and visually-guided movement (hence the name intention tremor). An intention tremor is usua ...

and gait

ataxia Ataxia (from Greek α- negative prefix+ -τάξις rder= "lack of order") is a neurological sign consisting of lack of voluntary coordination of muscle movements that can include gait abnormality, speech changes, and abnormalities in e ...

. Minor symptoms such as

, short-term memory deficit, and executive function decline can further contribute to a diagnosis of FXTAS. Radiological findings are similarly divided into major and minor categories. As patients with FXTAS can have distinct brain scans from other movement disorders, a scan showing white matter lesions of the middle cerebellar peduncle is a major finding that can be attributed to FXTAS. Overall or generalized brain tissue atrophy and cerebral white matter lesions can also be minor indicators for a diagnosis. For a definite diagnosis to be made, a major radiological finding and one major clinical finding must be present. Probable diagnosis is based on the presence of either a major radiological finding and a minor clinical finding, or two major clinical findings alone. The possible category for diagnosis can be made with a minor radiological finding and a major clinical finding.

Management

The medical management of FXTAS aims to reduce the level of disability and minimize symptoms. Currently, there are many gaps in the research on the management of FXTAS. The disorder was first described in the literature in 2001. There is no treatment modality aimed at reversing the pathology of FXTAS. However, there are a variety of drug therapies that are being utilized in the management of FXTAS symptoms. There is a lack of randomized control trials assessing the efficacy these therapies, and support is limited to anecdotal evidence. Therefore, many of the treatments are based on what has been helpful in disorders with similar clinical presentations. There is no cure for FXTAS. Current treatment includes medications for alleviating symptoms of tremor, ataxia, mood changes, anxiety, cognitive decline, dementia, neuropathic pain, or fibromyalgia. Neurological rehabilitation has not been studied for patients with FXTAS but should also be considered as a possible form of therapy. Additionally, occupational and physical therapy may help to improve function. .

Prognosis

The progression of symptoms varies widely between each case of FXTAS; the onset of symptoms may be gradual, with progression of the disease spanning multiple years or decades. Alternatively, symptoms may progress rapidly. FXTAS has shown strong age-dependent penetrance, affecting older premutation carriers with greater prevalence. Male carriers, age 50 and above have a 30% chance of developing FXTAS, while male carriers, age 75 and above, have a 75% chance of developing the disorder. While initially described as affecting male carriers, female carriers of the

gene mutation have also been found to develop FXTAS. However, due to X-inactivation, female carriers are much less likely to develop dementia or classic ataxia and tremor, instead demonstrating symptoms such as

fibromyalgia Fibromyalgia (FM) is a functional somatic syndrome with symptoms of widespread chronic pain, accompanied by fatigue, sleep disturbance including awakening unrefreshed, and Cognitive deficit, cognitive symptoms. Other symptoms can include he ...

, thyroid disease,

hypertension Hypertension, also known as high blood pressure, is a Chronic condition, long-term Disease, medical condition in which the blood pressure in the artery, arteries is persistently elevated. High blood pressure usually does not cause symptoms i ...

, and

seizures A seizure is a sudden, brief disruption of brain activity caused by abnormal, excessive, or synchronous neuronal firing. Depending on the regions of the brain involved, seizures can lead to changes in movement, sensation, behavior, awareness, o ...

References

# Jump up^ Amiri et al. Fragile X–Associated Tremor/Ataxia Syndrome. Archives of Neurology. VOL 65 (NO. 1), Jan 2008 # ^ Jump up to:^''a'' ^''b'' # ^ Jump up to:^''a'' ^''b'' ^''c'' # Jump up^ {{DEFAULTSORT:Fragile X-associated tremor ataxia syndrome Neurodegenerative disorders Syndromes affecting the nervous system

Symptoms and signs

Diagnosis

Management

Prognosis

See also

References