#601072
Table of Contents
Alternative titles; symbols
A number sign (#) is used with this entry because autosomal recessive deafness-8 (DFNB8), also known as DFNB10, is caused by homozygous or compound heterozygous mutation in the TMPRSS3 gene (605511) on chromosome 21q22.
Veske et al. (1996) reported a large consanguineous Pakistani kindred segregating nonsyndromic childhood-onset deafness.
Bonne-Tamir et al. (1996) reported a large consanguineous Pakistani family segregating congenital nonsyndromic deafness.
In a large consanguineous kindred in Pakistan, Veske et al. (1996) showed by linkage analysis that nonsyndromic childhood-onset deafness mapped to the distal long arm of chromosome 21, most likely between D21S212 and D21S1225, with the highest lod score of 7.31 at theta = 0.00 for D21S1575 on 21q22.3.
In a large Pakistani family segregating nonsyndromic deafness, Bonne-Tamir et al. (1996) presented evidence for linkage between a locus for the disorder, which they designated DFNB10, and several markers located near the telomere of chromosome 21q. Most of the affected members of this family were the offsrping of consanguineous unions, indicating that they are homozygous for the same genetic defect. Homozygosity of marker alleles was evident for only the most telomeric of 3 linked markers, D21S1259, suggesting that DFNB10 is closest to this locus.
Berry et al. (2000) narrowed the localization of DFNB10 to 21q22.3. By mutation analysis, they eliminated 6 candidate genes in this region.
Scott et al. (2001) determined that both DFNB8 and DFNB10 are caused by mutation in the TMPRSS3 gene (see 605511.0001 and 605511.0002).
Wattenhofer et al. (2002) screened for mutation in the TMPRSS3 gene in 448 unrelated Caucasian patients with severe to profound sensorineural prelingual nonsyndromic deafness who did not have the common 35delG GJB2 mutation (121011.0005). They identified TMPRSS3 mutations in only 2 patients (605511.0006-605511.0007), suggesting that mutation in TMPRSS3 is not a common cause of deafness in this population.
In 2 deaf Turkish brothers born of consanguineous parents, Wattenhofer et al. (2005) identified homozygosity for a missense mutation in the TMPRSS3 gene (605511.0005). The elder brother's deafness, the first case to occur in the family, was discovered at age 1.5 years due to speech delay; deafness in the younger brother was diagnosed at birth. The parents were heterozygous for the mutation, and a hearing sister was homozygous for the normal allele.
Berry, A., Scott, H. S., Kudoh, J., Talior, I., Korostishevsky, M., Wattenhofer, M., Guipponi, M., Barras, C., Rossier, C., Shibuya, K., Wang, J., Kawasaki, K., Asakawa, S., Minoshima, S., Shimizu, N., Antonarakis, S., Bonne-Tamir, B. Refined localization of autosomal recessive nonsyndromic deafness DFNB10 locus using 34 novel microsatellite markers, genomic structure, and exclusion of six known genes in the region. Genomics 68: 22-29, 2000. [PubMed: 10950923, related citations] [Full Text]
Bonne-Tamir, B., DeStefano, A. L., Briggs, C. E., Adair, R., Franklyn, B., Weiss, S., Korostishevsky, M., Frydman, M., Baldwin, C. T., Farrer, L. A. Linkage of congenital recessive deafness (gene DFNB10) to chromosome 21q22.3. Am. J. Hum. Genet. 58: 1254-1259, 1996. [PubMed: 8651303, related citations]
Scott, H. S., Kudoh, J., Wattenhofer, M., Shibuya, K., Berry, A., Chrast, R., Guipponi, M., Wang, J., Kawasaki, K., Asakawa, S., Minoshima, S., Younus, F., and 10 others. Insertion of beta-satellite repeats identifies a transmembrane protease causing both congenital and childhood onset autosomal recessive deafness. Nature Genet. 27: 59-63, 2001. [PubMed: 11137999, related citations] [Full Text]
Veske, A., Oehlmann, R., Younus, F., Mohyuddin, A., Muller-Myhsok, B., Mehdi, S. Q., Gal, A. Autosomal recessive non-syndromic deafness locus (DFNB8) maps on chromosome 21q22 in a large consanguineous kindred from Pakistan. Hum. Molec. Genet. 5: 165-168, 1996. [PubMed: 8789456, related citations] [Full Text]
Wattenhofer, M., Di Iorio, M. V., Rabionet, R., Dougherty, L., Pampanos, A., Schwede, T., Montserrat-Sentis, B., Arbones, M. L., Iliades, T., Pasquadibisceglie, A., D'Amelio, M., Alwan, S., Rossier, C., Dahl, H.-H. M., Petersen, M. B., Estivill, X., Gasparini, P., Scott, H. S., Antonarakis, S. E. Mutations in the TMPRSS3 gene are a rare cause of childhood nonsyndromic deafness in Caucasian patients. J. Molec. Med. 80: 124-131, 2002. [PubMed: 11907649, related citations] [Full Text]
Wattenhofer, M., Sahin-Calapoglu, N., Andreasen, D., Kalay, E., Caylan, R., Braillard, B., Fowler-Jaeger, N., Reymond, A., Rossier, B. C., Karaguzel, A., Antonarakis, S. E. A novel TMPRSS3 missense mutation in a DFNB8/10 family prevents proteolytic activation of the protein. Hum. Genet. 117: 528-535, 2005. [PubMed: 16021470, related citations] [Full Text]
Alternative titles; symbols
ORPHA: 90636; DO: 0110527;
| Location | Phenotype |
Phenotype MIM number |
Inheritance |
Phenotype mapping key |
Gene/Locus |
Gene/Locus MIM number |
|---|---|---|---|---|---|---|
| 21q22.3 | Deafness, autosomal recessive 8/10 | 601072 | Autosomal recessive | 3 | TMPRSS3 | 605511 |
A number sign (#) is used with this entry because autosomal recessive deafness-8 (DFNB8), also known as DFNB10, is caused by homozygous or compound heterozygous mutation in the TMPRSS3 gene (605511) on chromosome 21q22.
Veske et al. (1996) reported a large consanguineous Pakistani kindred segregating nonsyndromic childhood-onset deafness.
Bonne-Tamir et al. (1996) reported a large consanguineous Pakistani family segregating congenital nonsyndromic deafness.
In a large consanguineous kindred in Pakistan, Veske et al. (1996) showed by linkage analysis that nonsyndromic childhood-onset deafness mapped to the distal long arm of chromosome 21, most likely between D21S212 and D21S1225, with the highest lod score of 7.31 at theta = 0.00 for D21S1575 on 21q22.3.
In a large Pakistani family segregating nonsyndromic deafness, Bonne-Tamir et al. (1996) presented evidence for linkage between a locus for the disorder, which they designated DFNB10, and several markers located near the telomere of chromosome 21q. Most of the affected members of this family were the offsrping of consanguineous unions, indicating that they are homozygous for the same genetic defect. Homozygosity of marker alleles was evident for only the most telomeric of 3 linked markers, D21S1259, suggesting that DFNB10 is closest to this locus.
Berry et al. (2000) narrowed the localization of DFNB10 to 21q22.3. By mutation analysis, they eliminated 6 candidate genes in this region.
Scott et al. (2001) determined that both DFNB8 and DFNB10 are caused by mutation in the TMPRSS3 gene (see 605511.0001 and 605511.0002).
Wattenhofer et al. (2002) screened for mutation in the TMPRSS3 gene in 448 unrelated Caucasian patients with severe to profound sensorineural prelingual nonsyndromic deafness who did not have the common 35delG GJB2 mutation (121011.0005). They identified TMPRSS3 mutations in only 2 patients (605511.0006-605511.0007), suggesting that mutation in TMPRSS3 is not a common cause of deafness in this population.
In 2 deaf Turkish brothers born of consanguineous parents, Wattenhofer et al. (2005) identified homozygosity for a missense mutation in the TMPRSS3 gene (605511.0005). The elder brother's deafness, the first case to occur in the family, was discovered at age 1.5 years due to speech delay; deafness in the younger brother was diagnosed at birth. The parents were heterozygous for the mutation, and a hearing sister was homozygous for the normal allele.
Berry, A., Scott, H. S., Kudoh, J., Talior, I., Korostishevsky, M., Wattenhofer, M., Guipponi, M., Barras, C., Rossier, C., Shibuya, K., Wang, J., Kawasaki, K., Asakawa, S., Minoshima, S., Shimizu, N., Antonarakis, S., Bonne-Tamir, B. Refined localization of autosomal recessive nonsyndromic deafness DFNB10 locus using 34 novel microsatellite markers, genomic structure, and exclusion of six known genes in the region. Genomics 68: 22-29, 2000. [PubMed: 10950923] [Full Text: https://doi.org/10.1006/geno.2000.6253]
Bonne-Tamir, B., DeStefano, A. L., Briggs, C. E., Adair, R., Franklyn, B., Weiss, S., Korostishevsky, M., Frydman, M., Baldwin, C. T., Farrer, L. A. Linkage of congenital recessive deafness (gene DFNB10) to chromosome 21q22.3. Am. J. Hum. Genet. 58: 1254-1259, 1996. [PubMed: 8651303]
Scott, H. S., Kudoh, J., Wattenhofer, M., Shibuya, K., Berry, A., Chrast, R., Guipponi, M., Wang, J., Kawasaki, K., Asakawa, S., Minoshima, S., Younus, F., and 10 others. Insertion of beta-satellite repeats identifies a transmembrane protease causing both congenital and childhood onset autosomal recessive deafness. Nature Genet. 27: 59-63, 2001. [PubMed: 11137999] [Full Text: https://doi.org/10.1038/83768]
Veske, A., Oehlmann, R., Younus, F., Mohyuddin, A., Muller-Myhsok, B., Mehdi, S. Q., Gal, A. Autosomal recessive non-syndromic deafness locus (DFNB8) maps on chromosome 21q22 in a large consanguineous kindred from Pakistan. Hum. Molec. Genet. 5: 165-168, 1996. [PubMed: 8789456] [Full Text: https://doi.org/10.1093/hmg/5.1.165]
Wattenhofer, M., Di Iorio, M. V., Rabionet, R., Dougherty, L., Pampanos, A., Schwede, T., Montserrat-Sentis, B., Arbones, M. L., Iliades, T., Pasquadibisceglie, A., D'Amelio, M., Alwan, S., Rossier, C., Dahl, H.-H. M., Petersen, M. B., Estivill, X., Gasparini, P., Scott, H. S., Antonarakis, S. E. Mutations in the TMPRSS3 gene are a rare cause of childhood nonsyndromic deafness in Caucasian patients. J. Molec. Med. 80: 124-131, 2002. [PubMed: 11907649] [Full Text: https://doi.org/10.1007/s00109-001-0310-6]
Wattenhofer, M., Sahin-Calapoglu, N., Andreasen, D., Kalay, E., Caylan, R., Braillard, B., Fowler-Jaeger, N., Reymond, A., Rossier, B. C., Karaguzel, A., Antonarakis, S. E. A novel TMPRSS3 missense mutation in a DFNB8/10 family prevents proteolytic activation of the protein. Hum. Genet. 117: 528-535, 2005. [PubMed: 16021470] [Full Text: https://doi.org/10.1007/s00439-005-1332-x]
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