Subscribe to RSS
DOI: 10.1055/s-2001-19576
Connexin26 und -30 im Innenohr und ihre klinische Bedeutung
Connexin26 and -30 in the Cochlea and their Clinical RelevancePublication History
Publication Date:
16 January 2002 (online)
Zusammenfassung
Hintergrund: Gap-junction-Kanäle (Nexus) bestehen aus unterschiedlichen Connexin-Proteinen und spielen im Innenohr eine wichtige Rolle für die Physiologie des Hörens. Connexin26 und Connexin30 wurden in der Cochlea durch Immunhistochemie und Northern-Blot-Analyse nachgewiesen. Mutationen in den Genen von Connexin26 und Connexin30 wurden als Ursache nicht-syndromaler erblicher Innenohrschwerhörigkeit beschrieben. Methode: Die Häufigkeit von Mutationen im Connexin26- und Connexin30-Gen wurde durch SSCP-Analyse und Sequenzierung bei hochgradig schwerhörigen bis tauben Patienten untersucht. Ergebnisse: Bei 134 hochgradig schwerhörigen bis tauben Patienten konnten 30 Connexin26-Mutationen (22 %) nachgewiesen werden. In 25 Fällen (19 %) wurde die häufigste Connexin26-Mutation 30delG identifiziert, in 5 Fällen seltenere Connexin26-Mutationen. Eine Connexin30-Mutation konnte bei keinem Patienten nachgewiesen werden. Schlussfolgerung: Somit haben Connexin26-Mutationen auch in Deutschland eine große Bedeutung bei nicht-syndromaler Innenohrschwerhörigkeit und sollten bei Patienten mit Verdacht auf hereditäre Schwerhörigkeit ausgeschlossen werden.
Connexin26 and -30 in the Cochlea and their Clinical Relevance
Introduction: Gap junction channels consist of different connexin proteins and play an important role in the physiology of hearing. Connexin26 and connexin30 have been demonstrated in the inner ear by immunohistochemistry and Northern Blot analysis. Mutations in the genes for connexin26 and connexin30 have been described to be responsible for non-syndromic hearing loss. Methods: We investigated the prevalence of connexin26 and connexin30 mutations in patients with profound hearing loss or deafness by SSCP-analysis and sequencing. Results: 30 connexin26 mutations (22 %) were detected among 134 patients with profound hearing loss or deafness. The most frequent connexin26 mutation 30delG was found in 25 patients. In 5 patients other connexin26 mutations were identified. No connexin30 mutation was found. Conclusion: Therefore connexin26 mutations also play an important role for non-syndromic hearing loss in Germany. We propose that every patient with suspected hereditary hearing loss should be screened for a connexin26 mutation.
Schlüsselwörter:
Connexine - Gap-junctions - Hörverlust
Key words:
Connexins - Gap junctions - Hearing loss
Literatur
- 1 Dermietzel R, Hwang T K, Spray D S. The gap junction family: structure, function, chemistry. Anat Embryol. 1990; 182 517-528
- 2 Kumar N M, Gilula N B. The gap junction communication channel. Cell. 1996; 884 381-388
- 3 Jahnke K. The fine structure of freeze-fractured intercellular junctions in the guinea pig inner ear. Acta Otolaryngol (Stockh). 1975; 336 1-40
- 4 Jahnke K. Die Feinstruktur gefriergeätzter Zellmembran-Haftstellen der Stria vascularis. Anat Embryol. 1975; 147 189-201
- 5 Iurato S, Franke K, Luciano L, Wermbter G, Pannese E, Reale E. Intercellular junctions in the organ of Corti as revealed by freeze fracturing. Acta Otolaryngol (Stockh). 1976; 82 57-69
- 6 Kikuchi T, Kimura R S, Paul D L, Adams J C. Gap junctions in the rat cochlea: immunohistochemical and ultrastructural analysis. Anat Embryol. 1995; 191 101-118
- 7 Spicer S S, Schulte B A. Evidence for a medial K+ recycling pathway from inner hair cells. Hear Res. 1998; 118 1-12
- 8 Kikuchi T, Kimura R S, Paul D L, Takasaka T, Adams J C. Gap junction systems in the mammalian cochlea. Brain Research Reviews. 2000; 32 163-166
- 9 Xia J, Liu C, Tang B, Pan Q, Huang L, Dai H, Zhang B, Xie W, Hu D, Zheng D, Shi X, Wang D, Xia K, Yu K, Liao X, Feng Y, Yang Y, Xiao J, Xie D, Huang J. Mutations in the gene encoding gap junction protein β-3 associated with autosomal dominant hearing impairment. Nature Genet. 1998; 20 370-373
- 10 Lautermann J, ten Cate W JF, Altenhoff P, Grümmer R, Traub O, Frank H G, Jahnke K, Winterhager E. Expression of the gap-junction connexins 26 and 30 in the rat cochlea. Cell Tissue Res. 1998; 294 415-420
- 11 Kelsell D P, Dunlop J, Stevens H P, Lench N J, Liang J N, Parry G, Mueller R F, Leigh I M. Connexin 26 mutations in hereditary non-syndromic sensorineural deafness. Nature. 1997; 387 80-83
- 12 Lautermann J, Frank H G, Jahnke K, Traub O, Winterhager E. Developmental expression patterns of connexin26 and -30 in the rat cochlea. Developmental Genetics. 1999; 25 306-311
- 13 Zhao H B, Santos-Sacchi J. Voltage gating of gap junctions in cochlear supporting cells: evidence for nonhomotypic channels. J Membrane Biol. 2000; 175 17-24
- 14 Henley C M, Rybak L P. Ototoxicity in developing mammals. Brain Res. 1995; 20 68-90
- 15 Lavigne-Rebillard M, Bagger-Sjöback D. Development of the human stria vascularis. Hear Res. 1992; 64 39-51
- 16 Pujol R, Lavigne-Rebillard M, Uziel A. Development of the human cochlea. Acta Otolaryngol (Stockh). 1991; 482 7-12
- 17 Cohn E S, Kelley P M. Clinical phenotype and mutations in connexin26 (DFNB1/GJB2) the most common cause of childhood hearing loss. Am J Med Genet. 1999; 24 130-136
- 18 Denoyelle F, Weil D, Maw M A, Wilcox S A, Lench N J, Allen-Powell D R, Osborn A H, Dahl H H, Middleton A, Houseman M J, Dode C, Marlin S, Boulila-ElGaied A, Grati M, Ayadi H, BenArab S, Bitoun P, Lina-Granada G, Godet J, Mustapha M, Loiselet J, El-Zir E, Aubois A, Joannard A, Petit C . et al . Prelingual deafness: high prevalence of a 30delG mutation in the connexin26 gene. Hum Mol Genet. 1997; 6 2173-2177
- 19 Kelley P M, Harris D J, Comer B C, Askew J W, Fowler T, Smith S D, Kimberling W J. Novel mutations in the connexin26 gene (GJB2) that cause autosomal recessive (DFNB1) hearing loss. Am J Hum Genet. 1998; 62 792-799
- 20 Denoyelle F, Marlin S, Weil D, Moatti L, Chauvin P, Garabedian E N, Petit C. Clinical features of the prevalent form of childhood deafness, DFNB1, due to a connexin-26 gene defect: implications for genetic counselling. Lancet. 1999; 17 1298-1303
- 21 Abe S, Usami S, Shinkawa H, Kelley P M, Kimberling W J. Prevalent connexin26 gene (GJB2) mutations in Japanese. J Med Genet. 2000; 37 41-43
- 22 Estvill X, Fortina P, Surrey S, Rabionet R, Melchionda S, D’Agruma L, Mansfield F, Rappaport E, Govea N, Milà M, Zelante L, Gasparini P. Connexin-26 mutations in sporadic and inherited sensorineural deafness. Lancet. 1998; 351 394-398
- 23 Gasparini P, Rabionet R, Barbujani G, Melchionda S, Petersen M, Brondum-Nielsen K, Metspalu A, Oitmaa E, Pisano M, Fortina P, Zelante L, Estivill X. High carrier frequency of the 35delG deafness mutation in European populations. Genetic analysis consortium of GJB2 35delG. Eur J Hum Genet. 2000; 8 19-23
- 24 Kupka S, Mirghomizadeh F, Haug T, Braun S, Leistenschneider P, Schmitz-Salue C, Arold R, Blin N, Zenner H P, Pfister M. Mutationsanalyse des Connexin26-Gens bei sporadischen Fällen mittel- bis hochgradiger Schwerhörigkeit. HNO. 2000; 48 671-674
- 25 Kelley P M, Abe S, Askew J W, Smith S D, Usami S, Kimberling W J. Human connexin30 (GJB6), a candidate gene for nonsyndromic hearing loss: molecular cloning, tissue-specific expression and assignment to chromosome 13q12. Genomics. 1999; 1 172-176
- 26 Grifa A, Wagner C A, D’Ambrosio L, Melchionda S, Bernardi F, Lopez-Bigas N, Rabionet R, Arbones M, Monica M D, Estivill X, Zelante L, Lang F, Gasparini P. Mutations in GJB6 cause nonsyndromic autosomal dominant deafness at DFNA3 locus. Nat Genet. 1999; 23 16-18
- 27 Cohn E S, Kelley P M, Fowler T W, Gorga M P, Lefkowitz D M, Kuehn H J, Schaefer G B, Gobar L S, Hahn F J, Harris D J, Kimberling W J. Clinical studies of families with hearing loss attributable to mutations in the connexin26 gene. Pediatrics. 1999; 103 546-550
- 28 Jun A I, McGuirt W T, Hinojosa R, Green G F, Fischel-Ghodsian N, Smith R JH. Temporal bone histopathology in Connexin26-related hearing loss. Laryngoscope. 2000; 110 269-275
Priv.-Doz. Dr. J. Lautermann
Universitäts-Hals-, Nasen-, Ohrenklinik Essen
Hufelandstraße 55
45122 Essen