2005
DOI: 10.1002/ajmg.a.30929
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Connexin 26 variants and auditory neuropathy/dys‐synchrony among children in schools for the deaf

Abstract: Genetic and auditory studies of 731 children with severe-to-profound hearing loss in US schools for the deaf and 46 additional children receiving clinical services for hearing loss ranging from moderate to profound demonstrated that mutations in the connexin 26 (GJB2) and connexin 30 (GJB6) genes explain at least 12% of those with nonsyndromic sensorineural deafness. Otoacoustic emissions (OAEs) testing to detect functional outer hair cells indicated that 76 of the children had emissions and therefore may have… Show more

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Cited by 51 publications
(48 citation statements)
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“…Audiological examination of patients carrying GJB2 mutations exhibit reduced or missing distortion product oto-acoustic emissions (DPOAEs; Engel-Yeger et al 2002;Engel-Yeger et al 2003;Medica et al 2005;Morell et al 1998) although not in every case (Cheng et al 2005;Santarelli et al 2008). As reduction of the DPOAE is a sign of non-functional OHCs, such finding suggests that the underlying pathology in this case might be reduced OHC electromotility, essential for the active amplification of sound as shown by animal experiments where the 'motor' protein has been deleted (Liberman et al 2002) or reduced (Cheatham et al 2009).…”
Section: Introductionmentioning
confidence: 99%
“…Audiological examination of patients carrying GJB2 mutations exhibit reduced or missing distortion product oto-acoustic emissions (DPOAEs; Engel-Yeger et al 2002;Engel-Yeger et al 2003;Medica et al 2005;Morell et al 1998) although not in every case (Cheng et al 2005;Santarelli et al 2008). As reduction of the DPOAE is a sign of non-functional OHCs, such finding suggests that the underlying pathology in this case might be reduced OHC electromotility, essential for the active amplification of sound as shown by animal experiments where the 'motor' protein has been deleted (Liberman et al 2002) or reduced (Cheatham et al 2009).…”
Section: Introductionmentioning
confidence: 99%
“…However, there is no scientific evidence to support the real relationship between AN and mutations in the connexin 26 gene. Two studies detected mutations in this gene among patients with AN [43][44][45] .…”
Section: Discussionmentioning
confidence: 99%
“…Em recém--nascidos, diversos fatores como prematuridade, hiperbilirrubinemia, hipercolesterolemia, hipóxia, imaturidade do sistema nervoso central, baixo peso ao nascer, condições idiopáticas, fatores genéticos e ainda outros foram propostos como contribuintes, isoladamente ou em combinação, para o desenvolvimento de NA. [3][4][5][6] Estão propostas diversas teorias no que diz respeito aos locais de lesão auditiva que cursam com NA, tais como a membrana tectorial, as células ciliadas internas (CCI), as células ciliadas externas (CCE), alterações da liberação de neurotransmissores nas sinapses entre as células ciliadas internas e as fibras dos neurónios do gânglio espiral, alterações na transmissão elétrica das fibras do nervo coclear, problemas axonais diversos ou mesmo relacionados à mielinização do nervo coclear. 7 A prevalência descrita da NA em doentes pediátricos com hipoacúsia severa ou profunda é de cerca de 13,4%.…”
Section: Introductionunclassified
“…8 De entre os fatores genéticos, muito estudados, estão estabelecidas algumas mutações em genes classicamente descritos e relacionados com a NA, como o OTOF e o PJVAK. 4 Acredita-se que tais genes possam ser responsáveis por disfunções relacionadas com as CCI. 9 Estão já mapeados quatro loci considerados na literatura médica como responsáveis pela NA em doentes não--sindrómicos, de entre os quais: DFNB9 (OTOF) e DFNB59 (PJVK) para casos autossómicos recessivos; AUNA1 (DIA-PH3) em casos autossómicos dominantes; 1 AUNX1 em casos ligados ao X.…”
Section: Introductionunclassified
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