Abstract

Usher Syndrome is a hereditary disorder that causes hearing loss (HL) and retinitis pigmentosa (RP). The three major clinical types, Usher syndrome types I, II and II, are distinguished by severity of hearing loss and by presence or absence of vestibular dysfunction. Type I patients have severe hearing loss, RP, and vestibular dysfunction. Type I patients have severe hearing loss, RP, and vestibular dysfunction. Type III is distinguishable from types I and II by a progressive HL and variable vestibular deficit. At least ten distinct genetic loci are now believed to be associated with the three clinical types of Usher syndrome. We have collected the world's largest series of Usher families, a unique resource suitable for the studies proposed in this project. We propose to work towards a clarification of the problem of heterogeneity by testing hypotheses relating to the existence of all Usher loci and by estimating the relative contribution of each to the overall frequency of Usher syndrome. In addition, we propose to determine the distribution of mutations in MYO7A and USH2A, to identify and characterize the genes causing Usher types IIb, Ia, Id/f, Ie, and III, and to localize the gene for Usher type II c and any other new Usher genes uncovered by this research. Since Usher Syndrome results in the loss of the two most vital human senses, the burden to patients with this disorder is tremendous. It acts to isolate them from the rest of society and reduces their ability to act independently. Close to 1 in 15,000 individuals are affected with Usher Syndrome. The capability of Usher subtype diagnosis disorder will be enhanced leading to more accurate genetic counseling. A better understanding of the underlying etiology of Usher Syndrome is a critical first step towards the development of effective therapy. Usher syndrome offers a way of studying how the two major senses are related and answers to questions regarding the etiology of Usher Syndrome will reveal important and novel information about the developmental, metabolic and/or regulatory pathways common to normal retinal and auditory function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Research Program Projects (P01)
Project #
5P01DC001813-08
Application #
6448944
Study Section
Special Emphasis Panel (ZDC1)
Project Start
2001-05-01
Project End
2002-04-30
Budget Start
Budget End
Support Year
8
Fiscal Year
2001
Total Cost
$163,278
Indirect Cost

  Institution

Name
Father Flanagan's Boys' Home
Department
Type
DUNS #
City
Boys Town
State
NE
Country
United States
Zip Code
68010

  Publications

Jaijo, Teresa; Oshima, Aki; Aller, Elena et al. (2012) Mutation screening of the PCDH15 gene in Spanish patients with Usher syndrome type I. Mol Vis 18:1719-26
Malm, Eva; Ponjavic, Vesna; Möller, Claes et al. (2011) Alteration of rod and cone function in children with Usher syndrome. Eur J Ophthalmol 21:30-8
Hmani-Aifa, Mounira; Benzina, Zeineb; Zulfiqar, Fareeha et al. (2009) Identification of two new mutations in the GPR98 and the PDE6B genes segregating in a Tunisian family. Eur J Hum Genet 17:474-82
Tamayo, M L; Lopez, G; Gelvez, N et al. (2008) Genetic counseling in Usher syndrome: linkage and mutational analysis of 10 Colombian families. Genet Couns 19:15-27
Oshima, A; Jaijo, T; Aller, E et al. (2008) Mutation profile of the CDH23 gene in 56 probands with Usher syndrome type I. Hum Mutat 29:E37-46
Gopalarao, Deepika; Kimberling, William J; Jesteadt, Walt et al. (2008) Is hearing loss due to mutations in the Connexin 26 gene progressive? Int J Audiol 47:11-20
Cremers, Frans P M; Kimberling, William J; Kulm, Maigi et al. (2007) Development of a genotyping microarray for Usher syndrome. J Med Genet 44:153-60
Yang, Yan-Jun; Wang, Yan-Bo; Lei, Shu-Feng et al. (2007) AHSG gene polymorphisms are associated with bone mineral density in Caucasian nuclear families. Eur J Epidemiol 22:527-32
Chen, Xiang-Ding; Shen, Hui; Lei, Shu-Feng et al. (2006) Exclusion mapping of chromosomes 1, 4, 6 and 14 with bone mineral density in 79 Caucasian pedigrees. Bone 38:450-5
Huang, Qing-Yang; Shen, Hui; Deng, Hong-Yi et al. (2006) CA repeat polymorphism of the TNFR2 gene is not associated with bone mineral density in two independent Caucasian populations. J Bone Miner Metab 24:132-7

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