Ataxia telangiectasia: Difference between revisions
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{{CMG}} {{AE}}{{Arash.M}} {{ZO}} | |||
'''For patient information, click [[Ataxia telangiectasia (patient information)|here]]''' | '''For patient information, click [[Ataxia telangiectasia (patient information)|here]]''' | ||
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{{Ataxia telangiectasia}} | {{Ataxia telangiectasia}} | ||
{{SK}} Louis-bar syndrome, Boder-sedgwick syndrome. | {{SK}} Louis-bar syndrome, Boder-sedgwick syndrome. | ||
== [[Ataxia telangiectasia overview|Overview]] == | == [[Ataxia telangiectasia overview|Overview]] == | ||
[[Ataxia telangiectasia]] ([[A-T]]) is an [[autosomal recessive disorder]] caused by [[mutations]] in the [[gene]] [[ATM]] ([[ataxia-telangiectasia]] [[mutated]])(11q22.3). This [[gene]] is [[expressed]] commonly and [[encodes]] a [[protein kinase]] ([[ATM]] [[kinase]]) which plays a key role in the control of double-strand-break [[DNA repair]]. | |||
A-T is a [[progressive]], [[multisystem]] [[disease]] that has a large number of complex and diverse manifestations that vary with age. | |||
The clinical picture of this condition can be very variable and the severity of the [[pulmonary]], [[immunological]] and [[neurological]] manifestations varies widely between patients and is related to the severity of the underlying [[mutations]] and any residual [[ATM kinase]] activity. It has been recently suggested that the name [[A-T]] should be replaced by [[ATM]] [[syndrome]]. [[ATM]] [[syndrome]] represents a [[neurodegenerative disorder]] with [[multisystem]] involvement due to the absence or reduced levels of [[ATM]] [[protein]] and [[kinase]] activity. The syndrome is characterised by the presence of movement disorders, such as [[cerebellar ataxia]], [[dystonia]], [[chorea]] and [[myoclonus]], in association with systemic abnormalities such as [[immunodeficiency]], [[malignancies]], [[oculocutaneous]] [[telangiectasias]] and an increase in [[α-fetoprotein]] levels. The disease most commonly presents with [[ataxia]] during the third or fourth year of life. The important first step in the evaluation of young children presenting with [[ataxia]] should be [[α-fetoprotein]] testing. The diagnosis should then be confirmed by [[genetic]] testing to identify the [[mutations]] and measure the product of the [[ATM]] gene, the [[protein]] [[kinase]] [[ATM]]. This [[diagnostic test]] is likely to be available in specialised laboratories only. | |||
Patients with [[A-T]] die prematurely, the leading causes of [[death]] being [[respiratory diseases]] and [[cancer]]. A minimally estimated annual [[mortality]] rate for white patients is 19.5/1000 for ages 15–19 years and reportedly three-fold higher for African-American [[patients]]. | |||
== [[Ataxia telangiectasia historical perspective|Historical Perspective]] == | == [[Ataxia telangiectasia historical perspective|Historical Perspective]] == | ||
The term '''[[Ataxia-Telangiectasia]]''' was initially advanced by Boder and Sedgwick in 1957,in which described eight patients with classical '''[[A-T]]''', while in 1958 Centerwall and Miller entitled it Louis-Bar syndrome which relates to Madame Louis-Bar, a Belgian neurologist who published a case report of a 9 year-old boy with [[cutaneous telangiectasia]] and progressive [[cerebellar ataxia]]. She initially classified this new disease in the group of [[phacomatosis ]] '''[[PPV]]'''. In 1993, a case report was published about a 17 year-old boy with [[cerebellar ataxia]] concomitant [[dystonia]], [[myoclonus]], pyramidal signs, [[pulmonary]] [[infection]], [[persistent]] [[lymphopenia]], [[immunoglobulin]] [[deficiency]] and rising [[alpha-fetoprotein]], termed as '''[[ataxia]] with [[immune deficiency]]'''.<ref name="titleAtaxia-Telangiectasia: Immunodeficiency Disorders: Friedman JH, Weitberg A. [[Ataxia]] without [[telangiectasia]]. Mov Disord">{{cite web |url=https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5161405/#R13}}</ref> | |||
In 1995, the responsible gene for '''[[A-T]]'''('''[[ATM]]''') was identified by Savitsky et al. In 2001, Stewart found a correlation with '''[[ATM]] [[kinase]]''' activity levels in cells and the degree of [[neurological]] [[symptoms]] in '''[[A-T]]''' patients.<ref name="titleAtaxia-Telangiectasia: Immunodeficiency Disorders: Friedman JH, Weitberg A. Ataxia without telangiectasia. Mov Disord">{{cite web |url=https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5161405/#R13}}</ref> | |||
== [[Ataxia telangiectasia classification|Classification]] == | == [[Ataxia telangiectasia classification|Classification]] == | ||
*The [[ataxia]]s can be divided into:<ref name="pmid31048364">{{cite journal| author=de Silva RN, Vallortigara J, Greenfield J, Hunt B, Giunti P, Hadjivassiliou M| title=Diagnosis and management of progressive ataxia in adults. | journal=Pract Neurol | year= 2019 | volume= 19 | issue= 3 | pages= 196-207 | pmid=31048364 | doi=10.1136/practneurol-2018-002096 | pmc=6585307 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=31048364 }} </ref> | |||
**[[Genetic]] (with or without a [[family history]]) and those that are [[acquired]]/[[degenerative]]. | |||
**[[Sporadic]] [[ataxia]] implies there is no [[family history]]. | |||
**[[Acquired]] progressive [[ataxia]]s can be: | |||
***[[Immune]] mediated ([[paraneoplastic]] [[spinocerebellar]] [[degeneration]], [[gluten]] [[ataxia]]) | |||
***[[Degenerative]] ([[cerebellar]] variant of [[multiple systems]] [[atrophy]] (type C)) | |||
***Caused by [[deficiency]] states ([[vitamin B12]], [[vitamin E]]) | |||
***[[Toxicity]] (eg, [[alcohol]]-related [[ataxia]], [[phenytoin]]) | |||
***Associated with [[infection]]s ([[HIV]], [[sporadic]] [[Creutzfeldt-Jakob disease]], [[progressive multifocal leukoencephalopathy]]). | |||
**[[Inherited]] [[ataxia]]s can have [[autosomal dominant]], [[autosomal recessive]], [[X-linked]] or [[mitochondrial]] ([[maternal]]) [[inheritance]]. | |||
**[[Metabolic disorder]]s ([[Niemann-Pick]] type C, [[Tay-Sachs disease]]). | |||
*There is no established system for the classification of [[Ataxia Telangiectasia]]. | |||
== [[Ataxia telangiectasia pathophysiology|Pathophysiology]] == | == [[Ataxia telangiectasia pathophysiology|Pathophysiology]] == | ||
The responsible [[gene]] in [[AT]], [[ataxia telangiectasia mutated|ataxia-telangiectasia mutated]] ([[ATM]]), was discovered in 1995 by Savitsky et al.,<ref name="Savitsky">{{cite journal |author=Savitsky K, Bar-Shira A, Gilad S, ''et al'' |title=A single ataxia telangiectasia gene with a product similar to PI-3 kinase |journal=Science |volume=268 |issue=5218 |pages=1749-53 |year=1995 |pmid=7792600 |doi=10.1126/science.7792600}}</ref> a team led by Yosef Shiloh of Tel Aviv University in Israel. Researchers linked the [[hyper-sensitivity]] of [[AT]] patients to [[ionizing radiation]] ([[IR]]) and [[predisposition]] to [[cancer]], to "[[chromosomal]] [[instability,]] abnormalities in [[genetic recombination]], and [[defective signaling]] to [[programmed cell death]] and several [[cell cycle]] checkpoints activated by [[DNA]] damage".<ref>{{cite journal |author=Canman CE, Lim DS |title=The role of [[ATM]] in [[DNA damage]] responses and [[cancer]] |journal=Oncogene |volume=17 |issue=25 |pages=3301-8 |year=1998 |pmid=9916992 |doi=10.1038/sj.onc.1202577}}</ref> Earlier observations predicted that the gene altered in AT played a role in DNA damage recognition. These predictions were confirmed when a single gene on chromosome 11 (11q 22-23) was discovered.<ref name="Savitsky"> </ref><ref>{{cite journal |author=Gatti RA, Bick M, Tam CF, ''et al'' |title=Ataxia-Telangiectasia: a multiparameter analysis of eight families |journal=Clin. Immunol. Immunopathol. |volume=23 |issue=2 |pages=501-16 |year=1982 |pmid=6213343 |doi=10.1016/0090-1229(82)90134-9}}</ref> Since its discovery, the [[protein]] product of the [[ATM]] gene has been shown to be a part of [[eukaryotic]] [[cell cycle]] control, [[DNA repair]], and [[DNA]] [[recombination]] (Lavin, 2004). Specifically, the [[AT]] [[gene]] serves as a [[tumor suppressor gene]] by contributing to a network of genes that link double stranded breaks in DNA to cell cycle arrest and [[apoptosis]] ([[programmed cell death]]). Patients with [[ATM]] have a defective [[AT]] [[gene]], which leaves them susceptible to contracting cancer. For example, female [[ATM]] patients have a two-fold higher chance of ever having [[breast cancer]], which often occur before the age of 50. [[ATM]] patients must try avoiding [[x-rays]] at all costs since the [[radiation]] induces double-stranded breaks. | |||
=== Genetics === | |||
*[[AT]] is an [[autosomal recessive]] disorder caused by [[mutations]] in the [[ATM]] gene located on [[chromosome]] 11q22-23. <ref>{{OMIM|209800}}</ref> | |||
*It was characterised in June of 1995 and is made up of 66 exons spread across 150kb of genomic [[DNA]]. | |||
*It [[encode]]s a 13kb mature [[transcript]] with an open reading frame of 9168 nucleotides. | |||
*The [[ATM]] protein is about 370kDa and is ubiquitously expressed and is localised to the cell [[nucleus]]. | |||
*The [[ATM]] [[protein]] is a large [[serine-threonine kinase]] thought to play a role in regulating cell cycle checkpoints, repair of double stranded [[DNA]] and [[meiosis]] (similar to the [[BRCA]] genes). | |||
*[[ATM]] is also known to play a role in regulating [[p53]], [[BRCA1]] and [[CHEK2]]. | |||
*Part of [[ATM]]’s role in [[DNA]] repair is known to be that of [[telomere]] repair as [[telomere]]s degrade more rapidly in people affected with [[AT]]. | |||
*[[Mutation]]s in the [[ATM]] gene are thought to come in two types: | |||
**Null [[mutation]]s are those which cause complete loss of function of the [[protein]] and are therefore [[inherited]] in a [[recessive]] manner and cause [[AT]]. | |||
**‘[[Missense]] [[mutation]]s which produce stable, full sized [[protein]] with reduced function e.g. substitutions, short in-frame insertions and deletions etc. | |||
*These mutations act by [[dominantly]] interfering with the normal copy of the protein. | |||
*The majority of [[AT]] sufferers, 65-70%, have [[truncating]] [[mutations]], with exon skipping [[mutation]]s being particularly common. | |||
*This results in very low or undetectable levels of [[ATM]] [[protein]]. | |||
*Missense [[mutations]] are the most common type of [[mutation]] found in carriers with [[breast cancer]]. | |||
*Individuals with two [[missense]] mutations are believed to have a milder form of AT, which may account for cases of attenuated AT. | |||
*Therefore it is thought that "subtle constitutional alterations of ATM may impart an increased risk of developing breast cancer and therefore act as a low penetrance, high prevalence gene in the general population" (Maillet et al 2002). | |||
*[[Oculo]]-[[cutaneous]] [[telangiectasia]] combined with [[ataxia]] are the defining features of the condition. | |||
*Some patients with [[AT]], even those with two null [[mutation]]s who produce no [[ATM]] [[protein]] at all, may never present with [[oculo]]-[[cutaneous]] [[telangiectasia]]. | |||
== [[Ataxia telangiectasia causes|Causes]] == | == [[Ataxia telangiectasia causes|Causes]] == | ||
* [[Ataxia-telangiectasia]] is [[inherited]], which means it is passed down through families. It is an [[autosomal recessive trait]]. This means that both parents must provide a defective gene for the child to have symptoms of the disorder. | |||
* The [[disease]] results from defects in the '''[[ataxia telangiectasia mutated]] ([[ATM]]) [[gene]]'''. The '''[[ATM]]''' [[gene]] is involved in making protein that control [[cell division]] and DNA repair. The '''ATM''' protein helps cells to identify damaged and broken [[DNA]] and activates enzymes which fix the broken parts.<ref name="titleAtaxia-Telangiectasia: Immunodeficiency Disorder: Genetic Home Reference">{{cite web |url=http://www.ghr.nlm.nih.gov/condition/ataxia-telangiectasia#inheritance}}</ref>. Defects in this gene can lead to abnormal cell death in various places of the body, including the part of the brain that helps coordinate movement. | |||
* Boys and girls are equally affected. | |||
==[[Ataxia telangiectasia differential diagnosis|Differentiating Ataxia telangiectasia from other Diseases]]== | ==[[Ataxia telangiectasia differential diagnosis|Differentiating Ataxia telangiectasia from other Diseases]]== | ||
[[Ataxia telangiectasia like disorder]] ([[ATLD]]) is an extremely rare condition which could be considered as a differential diagnosis to [[AT]]. [[ATLD]] patients are very similar to [[AT]] patients in showing a [[progressive]] [[cerebellar ataxia]], [[hypersensitivity]] to [[ionising]] [[radiation]] and [[genomic]] [[instability]]. However, [[ATLD]] can be [[distinguished]] from [[AT]] by the absence of [[telangiectasia]]s, normal [[immunoglobulin]] levels, a later onset of the condition and a slower progression of the disease. It is not known whether [[ATLD]] individuals are also predisposed to [[tumors]]. The [[gene]] [[mutated]] in ATLD is [[hMre11]] and is located on [[chromosome]] 11q21. | |||
[[Nijmegen breakage syndrome]] ([[NBS]]), also known as [[ataxia telangiectasia]] variant 1, is a very rare syndrome which could be considered as a differential diagnosis to [[AT]]. People with [[Nijmegen breakage syndrome]] show the same [[immunodeficiency]], [[radiosensitivity]] and risk of [[cancer]] as AT but do not have any [[ataxia]] or [[oculo]]-[[cutaneous]] [[telangiectasia]]. [[Nijmegen breakage syndrome]] sufferers also show [[microcephaly]]. The gene associated with [[Nijmegen breakage syndrome]] ([[NBS]]) is known to be located on 8q21. | |||
Interestingly, the [[protein]]s expressed by the hMre11 and Nbs1 genes exist in the cell as a complex, along with a third [[protein]] expressed by the hRad50 gene. This complex, known as the [[MRN complex]], plays an important role in [[DNA]] damage repair and signaling and is required to recruit [[ATM]] to the sites of [[DNA double strand]] breaks. Mre11 and Nbs1 are also targets for [[phosphorylation]] by the [[ATM]] [[kinase]]. Thus, the similarity of the three diseases can be explained in part by the fact that the protein products of the three genes mutated in these disorders interact in common pathways in the cell. | |||
In the early [[ataxic]] stages children may be diagnosed with [[cerebral palsy]]. | |||
Other differential diagnoses are: | |||
* [[Ataxia oculomotor apraxia type 1]] | |||
* [[Ataxia oculomotor apraxia type 2]] | |||
* [[Gaucher disease]] | |||
* [[Hartnup disease]] | |||
* [[Niemann-Pick disease]] | |||
* [[Refsum disease]] | |||
[[Ataxia telangiectasia]] must be differentiated from other diseases that cause [[neurological]] manifestations in infants. | |||
{| | |||
|- style="background: #4479BA; color: #FFFFFF; text-align: center;" | |||
! rowspan="2" |Diseases | |||
! colspan="4" |Type of motor abnormality | |||
! rowspan="2" |Clinical findings | |||
! rowspan="2" |Laboratory findings and diagnostic tests | |||
! rowspan="2" |Radiographic findings | |||
|- style="background: #4479BA; color: #FFFFFF; text-align: center;" | |||
!Spasticity | |||
!Hypotonia | |||
!Ataxia | |||
!Dystonia | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Leigh syndrome]] | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>+</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Progressive [[psychomotor]] regression | |||
* [[Seizures]] | |||
* External [[ophthalmoplegia]] | |||
* [[Lactic acidosis]] | |||
* [[Vomiting]] | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Increased [[lactate]] levels in [[blood]] and [[CSF]] | |||
* Genetic testing | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* MRI: abnormal [[white matter]] signal in the [[putamen]], [[basal ganglia]], and [[brainstem]] on T2 images | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Niemann-Pick]] disease type C | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Progressive [[neurodegeneration]] | |||
* [[Hepatosplenomegaly]] | |||
* Systemic involvement of [[liver]], [[spleen]], or [[lung]] preceedes [[neurologic]] symptoms | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Abnormal [[liver]] function tests | |||
* [[Fibroblast]] cell culture with filipin staining | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* MRI: | |||
**[[Cerebral]] and [[cerebellar]] [[atrophy]] | |||
**Thinning of the [[corpus callosum]] | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Infantile Refsum disease]] | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Abnormalities of the [[optic nerve]] and disc | |||
* [[Retinitis pigmentosa]] | |||
* [[Sensorineural]] hearing loss | |||
* [[Hepatomegaly]] and [[cirrhosis]] | |||
* [[Neurologic]] deterioration is slower than in [[Zellweger syndrome]] or [[ALD]] | |||
| style="background: #F5F5F5; padding: 5px;" |Elevated plasma VLCFA levels | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Adrenoleukodystrophy]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Cognitive]] and behavioral abnormalities | |||
* [[Adrenal insufficiency]] | |||
* [[Hyperpigmented]] skin | |||
* [[Gonadal dysfunction]] | |||
* [[Neurologic]] deterioration progresses at a variable rate | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Elevated plasma VLCFA levels | |||
* Molecular [[genetic testing]] for mutations in the ABCD1 gene | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Zellweger syndrome]] | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Craniofacial]] dysmorphism | |||
* [[Hepatomegaly]] | |||
* Neonatal [[seizures]] | |||
* Profound developmental delay | |||
* [[MRI]] findings include [[cortical]] and [[white matter]] abnormalities | |||
* [[Neurologic deterioration]] is rapid and infants rarely survive beyond six months of age | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Elevated plasma VLCFA levels | |||
* Elevated levels of [[phytanic acid]], [[pristanic acid]], and [[pipecolic acid]] in plasma and [[fibroblasts]] | |||
* Reduced plasmalogen in [[erythrocytes]] | |||
* Molecular [[genetic]] testing for [[mutations]] in the PEX1 or PEX6 genes | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Pyruvate dehydrogenase deficiency]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Lactic acidosis]] | |||
* [[Seizures]] | |||
* [[Intellectual disability]] | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Elevated [[lactate]] and pyruvate levels in [[blood]] and CSF | |||
* Abnormal PDH enzymatic activity in cultured fibroblasts | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Arginase deficiency]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Hyperammonemia]] | |||
* [[Encephalopathy]] | |||
* [[Respiratory alkalosis]] | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Elevated [[ammonia]] level | |||
* Elevated [[arginine]] level | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |Holocarboxylase synthetase deficiency | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Ketoacidosis]] | |||
* [[Dermatitis]] | |||
* [[Alopecia]] | |||
* [[Seizures]] | |||
* [[Developmental delay]] | |||
| style="background: #F5F5F5; padding: 5px;" |Elevated levels of: | |||
* Beta-hydroxyisovalerate | |||
* Beta-methylcrotonylglycine | |||
* Beta-hydroxypropionate | |||
* Methylcitrate | |||
* Tiglylglycine | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |Glutaric aciduria type 1 | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>-</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>-</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>-</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>+</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Episodes of [[metabolic decompensation]] and [[encephalopathy]] often precipitated by [[infection]] and [[fever]] | |||
* Rarely presents in the newborn period | |||
* Microencephalic [[macrocephaly]] | |||
* [[Seizures]] (approximately 20 percent) | |||
* [[Cognitive function]] is preserved | |||
| style="background: #F5F5F5; padding: 5px;" |Elevated levels of: | |||
* [[glutaric acid]] | |||
* 3-hydroxyglutaric acid | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* MRI: | |||
**[[Frontal]] and [[temporal]] [[atrophy]] | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Ataxia telangiectasia]] | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>-</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>-</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>+</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" |<nowiki>-</nowiki> | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Progressive [[cerebellar]] [[ataxia]] | |||
* Abnormal eye movements | |||
* [[Oculocutaneous]] [[telangiectasias]] | |||
* Immune deficiency | |||
* Increased risk of [[malignancy]] | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Elevated serum alpha-fetoprotein level | |||
* Low [[IgA]] and [[IgG]] levels | |||
* [[Lymphopenia]] | |||
* Genetic testing for [[mutation]] in the ATM gene | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Pontocerebellar]] [[hypoplasias]] | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Progressive muscle [[atrophy]] | |||
* [[Microcephaly]] | |||
* [[Developmental delay]] | |||
| style="background: #F5F5F5; padding: 5px;" |[[Genetic]] testing for PCH gene mutations | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* MRI : | |||
**Small [[cerebellum]] and [[brainstem]] including the [[pons]] | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Metachromatic leukodystrophy]] | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Regression of motor skills | |||
* [[Seizures]] | |||
* [[Optic atrophy]] | |||
* Reduced or absent [[deep tendon reflexes]] | |||
* [[Intellectual disability]] | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Deficient arylsulfatase A enzyme activity in [[leukocytes]] or cultured skin [[fibroblasts]] | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Pelizaeus-Merzbacher]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Nystagmus]] | |||
* [[Cognitive impairment]] | |||
* Onset in infancy | |||
* Slowly progressive | |||
* Language development may be normal | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Genetic]] testing for [[mutations]] in PLP1 gene | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
*MRI: | |||
**[[White matter]] abnormalities | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Angelman syndrome]] | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Profound [[intellectual disability]] | |||
* Postnatal [[microcephaly]] | |||
* Typical abnormal behaviors (paroxysmal laughter, easily excitable) | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Methylation studies and [[chromosome]] microarray to detect chromosome 15 anomalies and UBE3A mutations | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Rett syndrome]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Occurs almost exclusively in females | |||
* Normal development during first six months followed by regression and loss of milestones | |||
* Loss of speech capability | |||
* Stereotypic hand movements | |||
* [[Seizures]] | |||
* [[Autistic]] features | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Clinical diagnosis | |||
* [[Genetic]] testing for MECP2 mutations | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Lesch-Nyhan syndrome]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Self-mutilating]] behavior | |||
* [[Urinary]] stones due to [[hyperuricemia]] | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Elevated [[uric acid]] level | |||
* Abnormal enzymatic activity of HPRT in cultured [[fibroblasts]] | |||
* [[Genetic]] testing for [[HPRT gene]] [[mutations]] | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |[[Miller-Dieker lissencephaly]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* [[Lissencephaly]] | |||
* [[Microcephaly]] | |||
* [[Dysmorphic]] features | |||
* [[Seizures]] | |||
* Failure to thrive | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Cytogenetic testing for 17p13.3 microdeletion | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|- | |||
| style="background: #DCDCDC; padding: 5px; text-align: center;" |Dopa-responsive [[dystonia]] | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | - | |||
| style="background: #F5F5F5; padding: 5px;" | + | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Onset in early childhood | |||
* Symptoms worsen with [[fatigue]] and exercise | |||
| style="background: #F5F5F5; padding: 5px;" | | |||
* Positive response to a trial of [[levodopa]] | |||
| style="background: #F5F5F5; padding: 5px; text-align: center;" |-- | |||
|} | |||
Comparison of the clinical features, biomarkers and brain imaging between [[ataxia telangiectasia]] ([[AT]]), [[ataxiatelangiectasia-like disorder type 1]] ([[ATLD1]]) and [[ataxia telangiectasia-like disorder type 2]] ([[ATLD2]]) | |||
{| style="border: 2px solid #4479BA; align="left" | |||
! style="width: 200px; background: #4479BA;" | {{fontcolor|#FFF|Clinical Features}} | |||
! style="width: 300px; background: #4479BA;" | {{fontcolor|#FFF|AT (ATM)}} | |||
! style="width: 400px; background: #4479BA;" | {{fontcolor|#FFF|ATLD1 (MRE11A)}} | |||
! style="width: 500px; background: #4479BA;" | {{fontcolor|#FFF|ATLD2 (PCNA)}} | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Ataxia]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Dysarthria]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Telangiectasia]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Eye movement]] [[disorders]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Photophobia]] and [[photosensitivity]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Movement disorders]] ([[choreoathetosis]], [[dystonia]], [[myoclonus]], [[tremor]]) | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Cognitive dysfunction]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Sensorineural hearing loss]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Skin]] abnormalities | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Microcephaly]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Short stature]], developmental delay | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Lymphoid]] [[tumors]] predisposition | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | Unknown | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | Recurrent [[infections]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | Increased levels of [[alpha-fetoprotein]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | Unknown | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | Reduced levels of [[Immunoglobulin]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | - | |||
|- | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | [[Cerebellar]] [[atrophy]] | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
| style="padding: 0 5px; background: #F5F5F5; text-align: left;" | + | |||
|- | |||
|} | |||
[[AT]], [[ataxia telangiectasia]]; [[ATLD1]], ataxia telangiectasia-like disorder type 1; [[ATLD2]], ataxia telangiectasia-like disorder type 2. | |||
== [[Ataxia telangiectasia epidemiology and demographics|Epidemiology and Demographics]] == | == [[Ataxia telangiectasia epidemiology and demographics|Epidemiology and Demographics]] == | ||
'''Epidemiology''': | |||
[[Ataxia-Telangiectasia]] [[prevalence]] is estimated between 1 in 40,000 and 1 in 100,000.<ref name="pmid27884168">{{cite journal| author=Rothblum-Oviatt C, Wright J, Lefton-Greif MA, McGrath-Morrow SA, Crawford TO, Lederman HM| title=Ataxia telangiectasia: a review. | journal=Orphanet J Rare Dis | year= 2016 | volume= 11 | issue= 1 | pages= 159 | pmid=27884168 | doi=10.1186/s13023-016-0543-7 | pmc=5123280 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=27884168 }} </ref> | |||
Some studies have shown that the [[prevalence]] of [[A-T]] among adults younger than age 50 is approximately 1 in 500,000. Some mutations are more common than others is certain geographical regions for example, the 7636del9 mutation is a common mutation in European populations which has been shown to increase the risk of [[breast cancer]] in carriers. | |||
'''Etiology''': | |||
[[Ataxia-Telangiectasia]] is caused by [[mutations]] in the [[ATM]] ([[Ataxia Telangiectasia]], [[Mutated]]) gene which encodes a [[protein]] of the same name. The primary role of the [[ATM]] [[protein]] is coordination of cellular signaling pathways in response to [[DNA]] [[double strand breaks]], [[oxidative stress]] and other [[genotoxic stress]]. | |||
== [[Ataxia telangiectasia risk factors|Risk Factors]] == | == [[Ataxia telangiectasia risk factors|Risk Factors]] == | ||
*There are no established risk factors for Ataxia Telangiectasia. | |||
*Ataxia Telangiectasia patients are at 40% risk of developing cancer, especially leukemia and lymphoma (85%). | |||
*They are also have increasing risk of developing breast cancer, ovarian, stomach, skin, bone and soft tissue cancers. Lifestyle changes to reduce the risk of cancer are important to A-T patients. | |||
*A carrier of the ATM gene has been linked to a high rate of breast cancer in some families as per the American Cancer Society. | |||
*A 2021 review study identified a specific mutation or ATM variant associated with increased breast cancer risk called the V2424G mutation. | |||
*General risk factors for cancer include: | |||
**Older age | |||
**Family history of cancer | |||
**Tobacco | |||
**Obesity | |||
**Alcohol | |||
**Viral infections, such as human papillomavirus (HPV) | |||
**Specific chemicals | |||
**Exposure to radiation, such as ultraviolet radiation (UV) | |||
== [[Ataxia telangiectasia screening|Screening]] == | == [[Ataxia telangiectasia screening|Screening]] == | ||
One of the defective screening test for newborn is [[severe combined immunodeficiency]] ('''[[SCID]]'''), which detect '''[[T cells]]''' and '''[[B cells]]''' deficiency or absence from [[infant]] dried [[blood]] spots. Although there is no modifying therapy or cure for '''A-T''' recently, '''SCID''' screening test allows for early family education and genetic counseling. | |||
<br> [[Pre-implantation genetic diagnosis]] ('''[[PGD]]''') can avoid the birth of an affected child. By this screening test, parents who have an affected child (or children) with '''[[A-T''' take its advantages. | |||
<br> Antenatal diagnosis can also be performed using haplotype analysis if a diagnosis has been made for the affected child. In this case, [[DNA polymorphisms]] within and around the [[ATM]] gene can be utilized even if the [[pathogenic]] [[mutations]] are not known. <ref>{{https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5123280}}</ref> | |||
== [[Ataxia telangiectasia natural history, complications and prognosis|Natural History, Complications and Prognosis]] == | == [[Ataxia telangiectasia natural history, complications and prognosis|Natural History, Complications and Prognosis]] == | ||
===Natural History=== | |||
The outlook for [[AT]] patients is not good, mainly due to the compromised [[immune system]] which results in recurrent [[respiratory infections]]. [[Neurological]] features are progressive as is deterioration and aging of the [[skin]] and [[hair]] with [[ataxia]] usually seen in the first year of life. Patients are usually wheelchair bound by the age of 10 or 11. [[Telangiectasia]]s are not seen in the early stages of the disease and begin to appear after a few years i.e. between 3-6 years of age, in the corners of the [[eyes]], [[ears]] and [[cheeks]]. Individuals are also at a 10% risk of developing [[cancer]], usually [[lymphomas]] and often [[breast cancer]]. However due to patients [[hyper-sensitivity]] to [[ionizing radiation]], [[radiotherapy]] and [[chemotherapy]] must be used with extreme caution. [[Oculo]]-[[cutaneous]] [[telangiectasia]] is often not obvious in the early stages of the disease. Other features of the disease may include mild [[diabetes mellitus]], [[premature]] graying of the hair, [[dysphagia]], and delayed physical and sexual development. People with the disease usually have normal intelligence. Mental retardation is uncommon in people with A-T.<ref>{{eMedicine|ped|2862}}</ref> | |||
===Complications=== | |||
Carriers of any type of ATM mutation have a 5-8 fold increased risk of cancer and on average die 7-8 years earlier than the normal population, often from heart disease. Individuals with a single ATM mutation are also at a higher risk from lung, gastric and lymphoid tumours, as well as breast cancer. S707P is known to be particularly common in breast cancer patients and F1463S is known to be associated with Hodgkin’s lymphoma. A recent study suggests that the majority of AT sufferers die from pulmonary infections (46%), with 21% dying from malignancies and 28% from malignancies and pulmonary infection. If pulmonary infections could be completely eradicated AT is consistent with survival into the 5th or 6th decade. | |||
===Prognosis=== | |||
The prognosis for [[AT]] sufferers is not good. Those with the disease usually die in their teens or early 20s although some individuals have been know to live to over 40. [[Carriers]] of [[ATM]] [[missense mutations]] are believed to have a 60% penetrance by age 70 and a risk of [[breast cancer]] 16x that of the normal population. Some papers state a lifetime risk for people with both null and [[missense mutations]] of 10-38%, which is still a hundred fold increase from population risk. | |||
== Diagnosis == | == Diagnosis == | ||
Line 47: | Line 553: | ||
== Treatment == | == Treatment == | ||
[[Ataxia telangiectasia medical therapy|Medical Therapy | [[Ataxia telangiectasia medical therapy|Medical Therapy]] | [[Ataxia telangiectasia cost-effectiveness of therapy|Cost Effectiveness of Therapy]] | [[Ataxia telangiectasia future or investigational therapies|Future or Investigational Therapies]] | ||
== Case Studies == | == Case Studies == | ||
[[Ataxia telangiectasia case study one|Case #1]] | :[[Ataxia telangiectasia case study one|Case #1]] | ||
{{Phakomatoses and other congenital malformations not elsewhere classified}} | {{Phakomatoses and other congenital malformations not elsewhere classified}} |
Latest revision as of 17:36, 8 January 2022
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Seyed Arash Javadmoosavi, MD[2] Zaida Obeidat, M.D. For patient information, click here
Ataxia telangiectasia | |
ICD-10 | G11.3 |
---|---|
ICD-9 | 334.8 |
OMIM | 208900 |
DiseasesDB | 1025 |
MedlinePlus | 001394 |
MeSH | D001260 |
Ataxia telangiectasia Microchapters |
Diagnosis |
---|
Treatment |
Case Studies |
Ataxia telangiectasia On the Web |
American Roentgen Ray Society Images of Ataxia telangiectasia |
Synonyms and keywords: Louis-bar syndrome, Boder-sedgwick syndrome.
Overview
Ataxia telangiectasia (A-T) is an autosomal recessive disorder caused by mutations in the gene ATM (ataxia-telangiectasia mutated)(11q22.3). This gene is expressed commonly and encodes a protein kinase (ATM kinase) which plays a key role in the control of double-strand-break DNA repair. A-T is a progressive, multisystem disease that has a large number of complex and diverse manifestations that vary with age. The clinical picture of this condition can be very variable and the severity of the pulmonary, immunological and neurological manifestations varies widely between patients and is related to the severity of the underlying mutations and any residual ATM kinase activity. It has been recently suggested that the name A-T should be replaced by ATM syndrome. ATM syndrome represents a neurodegenerative disorder with multisystem involvement due to the absence or reduced levels of ATM protein and kinase activity. The syndrome is characterised by the presence of movement disorders, such as cerebellar ataxia, dystonia, chorea and myoclonus, in association with systemic abnormalities such as immunodeficiency, malignancies, oculocutaneous telangiectasias and an increase in α-fetoprotein levels. The disease most commonly presents with ataxia during the third or fourth year of life. The important first step in the evaluation of young children presenting with ataxia should be α-fetoprotein testing. The diagnosis should then be confirmed by genetic testing to identify the mutations and measure the product of the ATM gene, the protein kinase ATM. This diagnostic test is likely to be available in specialised laboratories only. Patients with A-T die prematurely, the leading causes of death being respiratory diseases and cancer. A minimally estimated annual mortality rate for white patients is 19.5/1000 for ages 15–19 years and reportedly three-fold higher for African-American patients.
Historical Perspective
The term Ataxia-Telangiectasia was initially advanced by Boder and Sedgwick in 1957,in which described eight patients with classical A-T, while in 1958 Centerwall and Miller entitled it Louis-Bar syndrome which relates to Madame Louis-Bar, a Belgian neurologist who published a case report of a 9 year-old boy with cutaneous telangiectasia and progressive cerebellar ataxia. She initially classified this new disease in the group of phacomatosis PPV. In 1993, a case report was published about a 17 year-old boy with cerebellar ataxia concomitant dystonia, myoclonus, pyramidal signs, pulmonary infection, persistent lymphopenia, immunoglobulin deficiency and rising alpha-fetoprotein, termed as ataxia with immune deficiency.[1] In 1995, the responsible gene for A-T(ATM) was identified by Savitsky et al. In 2001, Stewart found a correlation with ATM kinase activity levels in cells and the degree of neurological symptoms in A-T patients.[2]
Classification
- The ataxias can be divided into:[3]
- Genetic (with or without a family history) and those that are acquired/degenerative.
- Sporadic ataxia implies there is no family history.
- Acquired progressive ataxias can be:
- Immune mediated (paraneoplastic spinocerebellar degeneration, gluten ataxia)
- Degenerative (cerebellar variant of multiple systems atrophy (type C))
- Caused by deficiency states (vitamin B12, vitamin E)
- Toxicity (eg, alcohol-related ataxia, phenytoin)
- Associated with infections (HIV, sporadic Creutzfeldt-Jakob disease, progressive multifocal leukoencephalopathy).
- Inherited ataxias can have autosomal dominant, autosomal recessive, X-linked or mitochondrial (maternal) inheritance.
- Metabolic disorders (Niemann-Pick type C, Tay-Sachs disease).
- There is no established system for the classification of Ataxia Telangiectasia.
Pathophysiology
The responsible gene in AT, ataxia-telangiectasia mutated (ATM), was discovered in 1995 by Savitsky et al.,[4] a team led by Yosef Shiloh of Tel Aviv University in Israel. Researchers linked the hyper-sensitivity of AT patients to ionizing radiation (IR) and predisposition to cancer, to "chromosomal instability, abnormalities in genetic recombination, and defective signaling to programmed cell death and several cell cycle checkpoints activated by DNA damage".[5] Earlier observations predicted that the gene altered in AT played a role in DNA damage recognition. These predictions were confirmed when a single gene on chromosome 11 (11q 22-23) was discovered.[4][6] Since its discovery, the protein product of the ATM gene has been shown to be a part of eukaryotic cell cycle control, DNA repair, and DNA recombination (Lavin, 2004). Specifically, the AT gene serves as a tumor suppressor gene by contributing to a network of genes that link double stranded breaks in DNA to cell cycle arrest and apoptosis (programmed cell death). Patients with ATM have a defective AT gene, which leaves them susceptible to contracting cancer. For example, female ATM patients have a two-fold higher chance of ever having breast cancer, which often occur before the age of 50. ATM patients must try avoiding x-rays at all costs since the radiation induces double-stranded breaks.
Genetics
- AT is an autosomal recessive disorder caused by mutations in the ATM gene located on chromosome 11q22-23. [7]
- It was characterised in June of 1995 and is made up of 66 exons spread across 150kb of genomic DNA.
- It encodes a 13kb mature transcript with an open reading frame of 9168 nucleotides.
- The ATM protein is about 370kDa and is ubiquitously expressed and is localised to the cell nucleus.
- The ATM protein is a large serine-threonine kinase thought to play a role in regulating cell cycle checkpoints, repair of double stranded DNA and meiosis (similar to the BRCA genes).
- ATM is also known to play a role in regulating p53, BRCA1 and CHEK2.
- Part of ATM’s role in DNA repair is known to be that of telomere repair as telomeres degrade more rapidly in people affected with AT.
- Mutations in the ATM gene are thought to come in two types:
- These mutations act by dominantly interfering with the normal copy of the protein.
- The majority of AT sufferers, 65-70%, have truncating mutations, with exon skipping mutations being particularly common.
- This results in very low or undetectable levels of ATM protein.
- Missense mutations are the most common type of mutation found in carriers with breast cancer.
- Individuals with two missense mutations are believed to have a milder form of AT, which may account for cases of attenuated AT.
- Therefore it is thought that "subtle constitutional alterations of ATM may impart an increased risk of developing breast cancer and therefore act as a low penetrance, high prevalence gene in the general population" (Maillet et al 2002).
- Oculo-cutaneous telangiectasia combined with ataxia are the defining features of the condition.
- Some patients with AT, even those with two null mutations who produce no ATM protein at all, may never present with oculo-cutaneous telangiectasia.
Causes
- Ataxia-telangiectasia is inherited, which means it is passed down through families. It is an autosomal recessive trait. This means that both parents must provide a defective gene for the child to have symptoms of the disorder.
- The disease results from defects in the ataxia telangiectasia mutated (ATM) gene. The ATM gene is involved in making protein that control cell division and DNA repair. The ATM protein helps cells to identify damaged and broken DNA and activates enzymes which fix the broken parts.[8]. Defects in this gene can lead to abnormal cell death in various places of the body, including the part of the brain that helps coordinate movement.
- Boys and girls are equally affected.
Differentiating Ataxia telangiectasia from other Diseases
Ataxia telangiectasia like disorder (ATLD) is an extremely rare condition which could be considered as a differential diagnosis to AT. ATLD patients are very similar to AT patients in showing a progressive cerebellar ataxia, hypersensitivity to ionising radiation and genomic instability. However, ATLD can be distinguished from AT by the absence of telangiectasias, normal immunoglobulin levels, a later onset of the condition and a slower progression of the disease. It is not known whether ATLD individuals are also predisposed to tumors. The gene mutated in ATLD is hMre11 and is located on chromosome 11q21.
Nijmegen breakage syndrome (NBS), also known as ataxia telangiectasia variant 1, is a very rare syndrome which could be considered as a differential diagnosis to AT. People with Nijmegen breakage syndrome show the same immunodeficiency, radiosensitivity and risk of cancer as AT but do not have any ataxia or oculo-cutaneous telangiectasia. Nijmegen breakage syndrome sufferers also show microcephaly. The gene associated with Nijmegen breakage syndrome (NBS) is known to be located on 8q21.
Interestingly, the proteins expressed by the hMre11 and Nbs1 genes exist in the cell as a complex, along with a third protein expressed by the hRad50 gene. This complex, known as the MRN complex, plays an important role in DNA damage repair and signaling and is required to recruit ATM to the sites of DNA double strand breaks. Mre11 and Nbs1 are also targets for phosphorylation by the ATM kinase. Thus, the similarity of the three diseases can be explained in part by the fact that the protein products of the three genes mutated in these disorders interact in common pathways in the cell.
In the early ataxic stages children may be diagnosed with cerebral palsy.
Other differential diagnoses are:
- Ataxia oculomotor apraxia type 1
- Ataxia oculomotor apraxia type 2
- Gaucher disease
- Hartnup disease
- Niemann-Pick disease
- Refsum disease
Ataxia telangiectasia must be differentiated from other diseases that cause neurological manifestations in infants.
Diseases | Type of motor abnormality | Clinical findings | Laboratory findings and diagnostic tests | Radiographic findings | |||
---|---|---|---|---|---|---|---|
Spasticity | Hypotonia | Ataxia | Dystonia | ||||
Leigh syndrome | - | - | + | + |
|
| |
Niemann-Pick disease type C | - | - | + | + |
|
|
|
Infantile Refsum disease | - | + | + | - |
|
Elevated plasma VLCFA levels | -- |
Adrenoleukodystrophy | + | - | - | - |
|
|
-- |
Zellweger syndrome | - | + | - | - |
|
|
-- |
Pyruvate dehydrogenase deficiency | + | + | + | - | -- | ||
Arginase deficiency | + | - | - | - | -- | ||
Holocarboxylase synthetase deficiency | - | + | - | - | Elevated levels of:
|
-- | |
Glutaric aciduria type 1 | - | - | - | + |
|
Elevated levels of:
|
|
Ataxia telangiectasia | - | - | + | - |
|
|
-- |
Pontocerebellar hypoplasias | - | + | - | - |
|
Genetic testing for PCH gene mutations |
|
Metachromatic leukodystrophy | - | + | + | - |
|
|
-- |
Pelizaeus-Merzbacher | + | - | + | - |
|
| |
Angelman syndrome | - | - | + | - |
|
|
-- |
Rett syndrome | + | - | - | + |
|
-- | |
Lesch-Nyhan syndrome | + | - | - | + |
|
|
-- |
Miller-Dieker lissencephaly | + | + | - | - |
|
|
-- |
Dopa-responsive dystonia | + | - | - | + |
|
|
-- |
Comparison of the clinical features, biomarkers and brain imaging between ataxia telangiectasia (AT), ataxiatelangiectasia-like disorder type 1 (ATLD1) and ataxia telangiectasia-like disorder type 2 (ATLD2)
Clinical Features | AT (ATM) | ATLD1 (MRE11A) | ATLD2 (PCNA) |
---|---|---|---|
Ataxia | + | + | + |
Dysarthria | + | + | + |
Telangiectasia | + | - | + |
Eye movement disorders | + | + | - |
Photophobia and photosensitivity | - | - | + |
Movement disorders (choreoathetosis, dystonia, myoclonus, tremor) | + | + | - |
Cognitive dysfunction | + | + | + |
Sensorineural hearing loss | - | - | + |
Skin abnormalities | + | - | + |
Microcephaly | - | - | + |
Short stature, developmental delay | + | + | + |
Lymphoid tumors predisposition | + | - | Unknown |
Recurrent infections | + | - | - |
Increased levels of alpha-fetoprotein | + | - | Unknown |
Reduced levels of Immunoglobulin | + | - | - |
Cerebellar atrophy | + | + | + |
AT, ataxia telangiectasia; ATLD1, ataxia telangiectasia-like disorder type 1; ATLD2, ataxia telangiectasia-like disorder type 2.
Epidemiology and Demographics
Epidemiology:
Ataxia-Telangiectasia prevalence is estimated between 1 in 40,000 and 1 in 100,000.[9] Some studies have shown that the prevalence of A-T among adults younger than age 50 is approximately 1 in 500,000. Some mutations are more common than others is certain geographical regions for example, the 7636del9 mutation is a common mutation in European populations which has been shown to increase the risk of breast cancer in carriers.
Etiology:
Ataxia-Telangiectasia is caused by mutations in the ATM (Ataxia Telangiectasia, Mutated) gene which encodes a protein of the same name. The primary role of the ATM protein is coordination of cellular signaling pathways in response to DNA double strand breaks, oxidative stress and other genotoxic stress.
Risk Factors
- There are no established risk factors for Ataxia Telangiectasia.
- Ataxia Telangiectasia patients are at 40% risk of developing cancer, especially leukemia and lymphoma (85%).
- They are also have increasing risk of developing breast cancer, ovarian, stomach, skin, bone and soft tissue cancers. Lifestyle changes to reduce the risk of cancer are important to A-T patients.
- A carrier of the ATM gene has been linked to a high rate of breast cancer in some families as per the American Cancer Society.
- A 2021 review study identified a specific mutation or ATM variant associated with increased breast cancer risk called the V2424G mutation.
- General risk factors for cancer include:
- Older age
- Family history of cancer
- Tobacco
- Obesity
- Alcohol
- Viral infections, such as human papillomavirus (HPV)
- Specific chemicals
- Exposure to radiation, such as ultraviolet radiation (UV)
Screening
One of the defective screening test for newborn is severe combined immunodeficiency (SCID), which detect T cells and B cells deficiency or absence from infant dried blood spots. Although there is no modifying therapy or cure for A-T recently, SCID screening test allows for early family education and genetic counseling.
Pre-implantation genetic diagnosis (PGD) can avoid the birth of an affected child. By this screening test, parents who have an affected child (or children) with [[A-T take its advantages.
Antenatal diagnosis can also be performed using haplotype analysis if a diagnosis has been made for the affected child. In this case, DNA polymorphisms within and around the ATM gene can be utilized even if the pathogenic mutations are not known. [10]
Natural History, Complications and Prognosis
Natural History
The outlook for AT patients is not good, mainly due to the compromised immune system which results in recurrent respiratory infections. Neurological features are progressive as is deterioration and aging of the skin and hair with ataxia usually seen in the first year of life. Patients are usually wheelchair bound by the age of 10 or 11. Telangiectasias are not seen in the early stages of the disease and begin to appear after a few years i.e. between 3-6 years of age, in the corners of the eyes, ears and cheeks. Individuals are also at a 10% risk of developing cancer, usually lymphomas and often breast cancer. However due to patients hyper-sensitivity to ionizing radiation, radiotherapy and chemotherapy must be used with extreme caution. Oculo-cutaneous telangiectasia is often not obvious in the early stages of the disease. Other features of the disease may include mild diabetes mellitus, premature graying of the hair, dysphagia, and delayed physical and sexual development. People with the disease usually have normal intelligence. Mental retardation is uncommon in people with A-T.[11]
Complications
Carriers of any type of ATM mutation have a 5-8 fold increased risk of cancer and on average die 7-8 years earlier than the normal population, often from heart disease. Individuals with a single ATM mutation are also at a higher risk from lung, gastric and lymphoid tumours, as well as breast cancer. S707P is known to be particularly common in breast cancer patients and F1463S is known to be associated with Hodgkin’s lymphoma. A recent study suggests that the majority of AT sufferers die from pulmonary infections (46%), with 21% dying from malignancies and 28% from malignancies and pulmonary infection. If pulmonary infections could be completely eradicated AT is consistent with survival into the 5th or 6th decade.
Prognosis
The prognosis for AT sufferers is not good. Those with the disease usually die in their teens or early 20s although some individuals have been know to live to over 40. Carriers of ATM missense mutations are believed to have a 60% penetrance by age 70 and a risk of breast cancer 16x that of the normal population. Some papers state a lifetime risk for people with both null and missense mutations of 10-38%, which is still a hundred fold increase from population risk.
Diagnosis
History and Symptoms | Physical Examination | Laboratory Findings | CT | MRI | Other Diagnostic Studies
Treatment
Medical Therapy | Cost Effectiveness of Therapy | Future or Investigational Therapies
Case Studies
Template:Phakomatoses and other congenital malformations not elsewhere classified
Template:Diseases of the nervous system
de:Louis-Bar-Syndrom it:Atassia teleangectasica he:תסמונת אטקסיה טלנגיאקטזיה sr:Атаксија-телеангиектатика
- ↑ https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5161405/#R13. Missing or empty
|title=
(help) - ↑ https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5161405/#R13. Missing or empty
|title=
(help) - ↑ de Silva RN, Vallortigara J, Greenfield J, Hunt B, Giunti P, Hadjivassiliou M (2019). "Diagnosis and management of progressive ataxia in adults". Pract Neurol. 19 (3): 196–207. doi:10.1136/practneurol-2018-002096. PMC 6585307 Check
|pmc=
value (help). PMID 31048364. - ↑ 4.0 4.1 Savitsky K, Bar-Shira A, Gilad S; et al. (1995). "A single ataxia telangiectasia gene with a product similar to PI-3 kinase". Science. 268 (5218): 1749–53. doi:10.1126/science.7792600. PMID 7792600.
- ↑ Canman CE, Lim DS (1998). "The role of ATM in DNA damage responses and cancer". Oncogene. 17 (25): 3301–8. doi:10.1038/sj.onc.1202577. PMID 9916992.
- ↑ Gatti RA, Bick M, Tam CF; et al. (1982). "Ataxia-Telangiectasia: a multiparameter analysis of eight families". Clin. Immunol. Immunopathol. 23 (2): 501–16. doi:10.1016/0090-1229(82)90134-9. PMID 6213343.
- ↑ Online Mendelian Inheritance in Man (OMIM) 209800
- ↑ http://www.ghr.nlm.nih.gov/condition/ataxia-telangiectasia#inheritance. Missing or empty
|title=
(help) - ↑ Rothblum-Oviatt C, Wright J, Lefton-Greif MA, McGrath-Morrow SA, Crawford TO, Lederman HM (2016). "Ataxia telangiectasia: a review". Orphanet J Rare Dis. 11 (1): 159. doi:10.1186/s13023-016-0543-7. PMC 5123280. PMID 27884168.
- ↑ Template:Https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5123280
- ↑ ped/2862 at eMedicine