Ataxia with Telangiectasia

Synonyms: Louis-Bar syndrome

Ataxia Telangiectasia (A-T) is a rare autosomal recessive disorder characterised by:

• Cerebellar ataxia
• Oculocutaneous telangiectasia
• Immune defects
• Predisposition to malignancy
• Hypersensitivity to ionizing radiation
• Chromosomal breakage (t(7;14) translocations typically)

A-T is a rare disease:

• It is present throughout the world with clusters in Turkey, Norway, Costa Rica, Iran, Saudi Arabia and among North African Jews and South African Scots.¹
• It is sometimes associated with high rates of consanguinity.²
• A study in West Midlands found prevalence of A-T in those less than 50 years to be 1 in 514,000 and birth frequency to be about 1 in 300,000.³
• This study and others have found a lower rate of A-T in siblings than would be expected on the basis of strict autosomal recessive inheritance (1 in 7, rather than 1 in 4), suggesting that in some instances A-T may develop as a new dominant mutation.

Carriers (heterozygotes) of A-T locus mutations however form about 1.4-2% of the US population and have a significantly reduced life-expectancy compared to non-carriers (on average, dying 7-8 years earlier) with increased risk of death from cancer and ischaemic heart disease.⁴ Female heterozygotes have a particular risk of breast cancer.^5,6

The molecular pathology of A-T has been well described in recent times:

• The classical form of A-T results from the presence of two A-T mutated (ATM) genes on chromosome 11 leading to total loss of the ATM protein (a protein kinase). ATM protein normally recognises DNA damage, activates the DNA repair machinery and the cell cycle check points to repair and minimise the risk of genetic damage.
• Understanding ATM's function through the effect of its loss in A-T has provided broader insights into cancer predisposition and some aspects of neurodegeneration.⁷
• Milder forms of A-T with later-onset or slower progressing neurological degeneration seems to reflect some retained ATM protein kinase activity due to the impact of different mutations.⁸

• A-T usually presents by the age of 2 years with a progressive cerebellar ataxia.
• Other symptoms which may be present include:
  • Lack of facial expression
  • Tendency to drool
  • Slow slurred speech
  • Recurrent infections particularly sinuses and respiratory (due to decreased IgA)
• Telangiectasia develop from about 3 years old and may not be present until the age of 10, but will be present in all cases. The telangiectasia may be present anywhere on the body - most usually involving the conjunctivae, pinnae, face, sternum and flexures.
• Other signs include:
  • Truncal ataxia
  • Occulomotor apraxia
  • Decreased tendon reflexes
  • Pulmonary infections
  • Sinus infections
  • Bulbar dysfunction
  • Recurrent aspiration
  • Gonadal atrophy
  • Dystonia
  • Chorea
  • Sensory neuropathy
  • Growth retardation

There is a need to differentiate from other autosomal recessive ataxias:⁹ Friedreich's ataxia (most common in European countries) and much rarer conditions such as ataxia with vitamin E deficiency, abetalipoproteinaemia, Refsum's syndrome, spastic ataxia, infantile onset spinocerebellar ataxia and ataxia with oculomotor apraxia.
A-T is usually distinguished by an earlier age of onset, the presence of telangiectasia and the later development of dystonia and chorea and by specific investigations.

• Serum alpha fetoprotein level ( raised in 90%)
• Genetic testing for ATM genes and absence of ATM protein in nuclear extracts
• In vitro radiosensitivity testing (colony survival assay)

Increased cancer risk

• The life-time frequency of cancer in ataxia telangiectasia patients is approximately 38% with 1 in 20 developing more than one malignancy.
• Lymphoreticular malignancies (lymphomas and ALL) dominate in the first two decades followed by solid tumours thereafter.
• Patients with A-T and cancer are particularly sensitive to therapeutic levels of ionising radiation.

Immunodeficiency¹¹

• A-T is associated with a high prevalence of laboratory immunological abnormalities - most commonly Ig A, G and E deficiencies and lymphopenia with reduced B-lymphocytes, CD4 and CD8 T-cells.
• Recurrent upper and lower respiratory tract infections are common. Severe systemic bacterial or viral and opportunistic infections are uncommon in A-T. The immune defect does not appear progressive.

Currently there is no cure and no treatment for slowing the progression of the ataxia. A-T is a multisystem disorder requiring multiple therapeutic interventions to halt the progressive neurodegeneration, to prevent or treat the tumours and to correct the associated immunodeficiency. Despite an increased molecular understanding of the disease, we have no effective answer to these challenges. In the future, embryonic stem cell transfer, use of antioxidants and targeted gene therapy may offer some hope.¹²

Pragmatic treatment of the condition consists of:

• Treatment of neurologic symptoms is generally disappointing. Basal ganglia dysfunction can be attempted with L-DOPA derivatives, dopamine antagonists and anticholinergics. Loss of balance, speech and coordination problems may be improved by the use of amantadine, fluoxetine and buspirone. Tremors can be treated with gabapentin, clonazepam and propranolol.¹²
• Prompt supportive treatment of infections and, in some cases, use of prophylactic antibiotics. Regular injection of immunoglobulins has been used in some centres.. Fetal thymus implants have not been shown to be beneficial.
• Screening for swallow-related problems and aspiration. Consider the use of thickeners and enteral feeding.¹²
• Some advocate regular screening for malignancies with FBC and serum tumour markers.
• Multidisciplinary team involvement - input of physio, speech and occupational therapists is particularly important.
• High-dose vitamin regimes, folic acid and alpha lipoic acid have all been advocated due to their claimed anti-cancer properties. Multivitamins do not correct the ataxia of A-T however.¹²
• Avoid X-rays wherever possible, unless treatment is dependent on them and an alternative (such as MRI or ultrasound) is not possible.

• A-T is an incurable and unremitting disease.
• Most A-T children are wheelchair dependent by their teens.
• Communication becomes progressively difficult as handwriting, speech and eye movement control deteriorates.
• Median survival 19-25 years (wide range) with death due to cancer and respiratory failure.¹³

Pre-natal testing is available for families considered at risk, but is not carried out routinely.