vestibular dysfunction

Usher Syndrome Type III

Clinical Characteristics

Ocular Features:

Retinitis pigmentosa is a cardinal feature with onset of severe symptoms of nightblindness and tunnel vision by the second decade of life. The ERG shows depressed responses. Central vision may also be lost in young adults. Hypermetropic astigmatism has been reported as the most typical refractive error for type III in the presence of nightblindness and hearing loss, at least in Finnish patients.

Systemic Features:

Hearing loss is progressive but later in onset than in type I and type II. Infants are usually born with normal hearing and often experience some loss of hearing by the end of the first decade of life. Speech can develop normally because of the late onset of the hearing deficit. Hearing loss is progressive early with older patients having a profound and eventually more stable hearing deficit. The amount of vestibular dysfunction is variable but usually is severe enough to cause significant unsteadiness. The mental changes associated with type I are absent.

Genetics

Usher syndrome is a clinically and genetically heterogeneous condition. Type IIIA is caused by a mutation in the CLRN1 gene (3q21-q25). It is inherited in an autosomal recessive pattern. Type IIIB (614505) is the result of homozygous mutations in HARS (5q31.3).

There is also a disorder resembling Usher that results from homozygous mutations in ABHD12 (20p11.21) that also causes PHARC (612674) (polyneuropathy, hearing loss, ataxia, retinitis pigmentosa, and early onset cataract).

This is the least common type of Usher syndrome. Three additional types of Usher syndrome are recognized: type I (276900) results from mutations in at least 7 different genes, type II (276901) from mutations in 4 genes, and Type IV resulting from mutations in the ARSG gene.

Pedigree:

Autosomal recessive

Treatment

Treatment Options:

Hearing aids might be helpful early but cochlear implants may be needed in older patients with severe deafness. Low vision aids are often helpful.

References

Article Title:

Targeted next-generation sequencing identifies a homozygous nonsense mutation in ABHD12, the gene underlying PHARC, in a family clinically diagnosed with Usher syndrome type 3

Eisenberger T, Slim R, Mansour A, Nauck M, N?ornberg G, N?ornberg P, Decker C, Dafinger C, Ebermann I, Bergmann C, Bolz HJ. Targeted next-generation sequencing identifies a homozygous nonsense mutation in ABHD12, the gene underlying PHARC, in a family clinically diagnosed with Usher syndrome type 3. Orphanet J Rare Dis. 2012 Sep 2;7(1):59. [Epub ahead of print]

PubMed ID:

22938382

Usher syndrome IIIA gene clarin-1 is essential for hair cell function and associated neural activation

Geng R, Geller SF, Hayashi T, Ray CA, Reh TA, Bermingham-McDonogh O, Jones SM, Wright CG, Melki S, Imanishi Y, Palczewski K, Alagramam KN, Flannery JG. Usher syndrome IIIA gene clarin-1 is essential for hair cell function and associated neural activation. Hum Mol Genet. 2009 Aug 1;18(15):2748-60. Epub 2009 May 3.

PubMed ID:

19414487

Mutation screening of USH3 gene (clarin-1) in Spanish patients with Usher syndrome: low prevalence and phenotypic variability

Aller E, Jaijo T, Oltra S, Ali?? J, Gal?degn F, N?degjera C, Beneyto M, Mill?degn JM. Mutation screening of USH3 gene (clarin-1) in Spanish patients with Usher syndrome: low prevalence and phenotypic variability. Clin Genet. 2004 Dec;66(6):525-9.

PubMed ID:

15521980

The ophthalmological course of Usher syndrome type III

Pakarinen L, Tuppurainen K, Laippala P, M?SSntyj?SSrvi M, Puhakka H. The ophthalmological course of Usher syndrome type III. Int Ophthalmol. 1995-1996;19(5):307-11.

PubMed ID:

8864816

Usher Syndrome Type I

Clinical Characteristics

Ocular Features:

The fundus dystrophy of retinitis pigmentosa in Usher syndrome is indistinguishable from isolated retinitis pigmentosa. Night blindness begins by about 10 years of age and the ERG by that time is often markedly diminished or absent. Patches of hyperfluorescence are seen in younger individuals and these enlarge and coalesce with age. Tunnel vision occurs early as the peripheral visual field is constricted to 5-10 degrees by midlife. The retinal disease is progressive and blindness may be the final result.

Systemic Features:

Type I Usher syndrome is characterized by profound hearing impairment beginning at birth, vestibular dysfunction, and unintelligible speech in addition to retinitis pigmentosa. Vestibular areflexia is virtually complete and constitutes a defining feature. Ataxic gait disturbances are common secondary to labyrinthine dysfunction and many children do not walk until 18-24 months of age. Sitting alone may also be delayed. Sperm motility is abnormal which is likely the basis for reduced fertility in male patients. An abnormal exoneme morphology from ciliated progenitors is likely the common basis for these clinical findings. MRI imaging has found a significant decrease in intracranial volume and brain size. About 1 in 4 children have behavioral problems or psychosocial difficulties.

Genetics

Type I Usher syndrome is an autosomal recessive genetically heterogeneous disorder as mutations in at least 8 genes produce a similar disease. These are: MYO7A (276900) at 11q13.5 causing USH1B (USH1A is now considered to be the same), USH1C at 11p15.1 causing USH1C (276904), CDH23 at 10q21-q22, causing USH1D (601067), PCDH15 at 10q21.1 causing USH1F (602083), and USH1G at 17q24-25 causing USH1G (606943). Mutations in as yet unnamed genes in loci at 21q21 (USH1E; 602097), 10p11.21-q21.1 (USH1K), and 15q22-q23 (USH1H; 612632) may also cause this type I phenotype. They are discussed here as a single entity designated type I since the clinical features of each are indistinguishable.'

A varant of USH1C resulting from homozygous deletions in 11p15-p14, known as homozygous 11p15-p14 deletion syndrome, has the additional feature of severe hyperinsulinemia due to the involvement of ABCC8 and KCNJ11 genes (606528).

Clinical differences have led to the categorization of three types of Usher syndrome: type I described here, type II (276901) caused by mutations in at least 4 genes, and type III (276902) caused by mutations in CLRN1.

Pedigree:

Autosomal recessive

Treatment

Treatment Options:

At-risk infants should have hearing evaluations as soon as possible after birth. Assistive hearing devices are of little benefit. Unless cochlear implants are placed in young children, speech may not develop. Extra precautions during physical activities such as swimming, bicycling, and night-time driving are highly recommended. Speech therapy and low vision aids can be beneficial.

References

Article Title:

Targeted exon sequencing in Usher syndrome type I

Bujakowska KM, Consugar MB, Place E, Harper S, Lena J, Taub DG, White J, Navarro-Gomez D, Weigel-DiFranco C, Farkas MH, Gai X, Berson EL, Pierce EA. Targeted exon sequencing in Usher syndrome type I. Invest Ophthalmol Vis Sci. 2014 Dec 2. [Epub ahead of print].

PubMed ID:

25468891

Clinical Aspects of Usher Syndrome and the USH2A Gene in a Cohort of 433 Patients

Blanco-Kelly F, Jaijo T, Aller E, Avila-Fernandez A, Lopez-Molina MI, Gimenez A, Garcia-Sandoval B, Millan JM, Ayuso C. Clinical Aspects of Usher Syndrome and the USH2A Gene in a Cohort of 433 Patients. JAMA Ophthalmol. 2014 Nov 6. [Epub ahead of print].

PubMed ID:

25375654

Heterogeneity in Phenotype of Usher-Congenital Hyperinsulinism Syndrome: Hearing Loss, Retinitis Pigmentosa, and Hyperinsulinemic Hypoglycemia Ranging from Severe to Mild with Conversion to Diabetes

Al Mutair AN, Brusgaard K, Bin-Abbas B, Hussain K, Felimban N, Al Shaikh A, Christesen HT. Heterogeneity in Phenotype of Usher-Congenital Hyperinsulinism Syndrome: Hearing Loss, Retinitis Pigmentosa, and Hyperinsulinemic Hypoglycemia Ranging from Severe to Mild with Conversion to Diabetes. Diabetes Care. 2012 Nov 12. [Epub ahead of print].

PubMed ID:

23150283

USH1K, a novel locus for type I Usher syndrome, maps to chromosome 10p11.21-q21

Jaworek TJ, Bhatti R, Latief N, Khan SN, Riazuddin S, Ahmed ZM. USH1K, a novel locus for type I Usher syndrome, maps to chromosome 10p11.21-q21.1. J Hum Genet. 2012 Jun 21. doi: 10.1038/jhg.2012.79. [Epub ahead of print].

PubMed ID:

22718019

The molecular genetics of Usher syndrome

Ahmed ZM, Riazuddin S, Riazuddin S, Wilcox ER. The molecular genetics of Usher syndrome. Clin Genet. 2003 Jun;63(6):431-44. Review.

PubMed ID:

12786748

Clinical diagnosis of the Usher syndromes. Usher Syndrome Consortium

Smith RJ, Berlin CI, Hejtmancik JF, Keats BJ, Kimberling WJ, Lewis RA, Moller CG, Pelias MZ, Tranebjaerg L. Clinical diagnosis of the Usher syndromes. Usher Syndrome Consortium. Am J Med Genet. 1994 Mar 1;50(1):32-8.

PubMed ID:

8160750

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