Abstract

Genetic impairment of hearing affects about one in every 2,000 children. Identification of genes leading to hearing impairment is essential for understanding factors necessary for normal auditory function and for development of therapeutic strategies. The genetic analysis of mouse deafness mutations has proven instrumental in the identification of several human deafness genes. A new mutation causing hearing and balance defects spontaneously arose in a colony of BALB/cByJ inbred mice at The Jackson Laboratory. The recessive mutation was named 'hypoplasia of the membranous labyrinth' (symbol hml) because it mainly affects inner ear morphology and development. The human homolog of the gene responsible for the hml phenotype in mice may play a role in the etiology and pathogenesis of some cases of human inherited deafness. Currently the pathogenetic mechanism and the identity of hml are not known. A small panel of intercross mice was used to map the hml locus to the middle region of mouse chromosome (Chr) 10. The genetic map position of the mouse hml gene suggests that the homologous human gene may be located on Chr 9pl3, where a particular form of genetic deafness in humans (DFNB15) has been previously mapped. In order to characterize the genetic and developmental dysfunction responsible for this morphogenetic inner ear mutation in mice, and ultimately extend that new found knowledge to improve our understanding of DFNB15 or other deafness traits in humans, the identification and characterization of the hml gene needs to be carried out.
Aim 1. Generate a high-resolution genetic map of the region surrounding hml and screen candidate genes for the mutation.
Aim 2. Construct a physical contig of YACS and BACS clones across the minimal genetic region.
Aim 3. Fully characterize the development and pathology of inner ears from hml/hml mice compared with hml/+ and +/+ controls.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Small Research Grants (R03)
Project #
1R03DC004376-01A1
Application #
6209955
Study Section
Special Emphasis Panel (ZDC1-SRB-O (23))
Program Officer
Johnson, Thomas E
Project Start
2000-08-01
Project End
2003-07-31
Budget Start
2000-08-01
Budget End
2001-07-31
Support Year
1
Fiscal Year
2000
Total Cost
$82,500
Indirect Cost

  Institution

Name
Jackson Laboratory
Department
Type
DUNS #
042140483
City
Bar Harbor
State
ME
Country
United States
Zip Code
04609

  Publications

Tian, Cong; Liu, Xue Z; Han, Fengchan et al. (2010) Ush1c gene expression levels in the ear and eye suggest different roles for Ush1c in neurosensory organs in a new Ush1c knockout mouse. Brain Res 1328:57-70
Han, Fengchan; Yu, Heping; Zhang, Jiangping et al. (2009) Otitis media in a mouse model for Down syndrome. Int J Exp Pathol 90:480-8
Mao, Mao; Thedens, Daniel R; Chang, Bo et al. (2009) The podosomal-adaptor protein SH3PXD2B is essential for normal postnatal development. Mamm Genome 20:462-75
Zhang, Jiangping; Kaga, Kimitaka; Zheng, Qing Yin (2007) Small papillary tumor in the saccule. Int J Pediatr Otorhinolaryngol Extra 2:107-110
Zheng, Qing Yin; Tong, Yi-Cai Isaac; Alagramam, Kumar N et al. (2007) Tympanometry assessment of 61 inbred strains of mice. Hear Res 231:23-31
Hertzano, Ronna; Montcouquiol, Mireille; Rashi-Elkeles, Sharon et al. (2004) Transcription profiling of inner ears from Pou4f3(ddl/ddl) identifies Gfi1 as a target of the Pou4f3 deafness gene. Hum Mol Genet 13:2143-53
Johnson, Kenneth R; Gagnon, Leona H; Webb, Lisa S et al. (2003) Mouse models of USH1C and DFNB18: phenotypic and molecular analyses of two new spontaneous mutations of the Ush1c gene. Hum Mol Genet 12:3075-86