Novel mutations in GJB2 encoding connexin-26 in Japanese patients with keratitis-ichthyosis-deafness syndrome

Yotsumoto, Shinichi; Hashiguchi, Tsutomu; Chen, X.; Ohtake, Naoto; Tomitaka, Akiko; Akamatsu, Hirohiko; Matsunaga, Kayoko; Shiraishi, Satoshi; Miura, Hideharu; Adachi, Jun; Kanzaki, Tamotsu

doi:10.1046/j.1365-2133.2003.05245.x

Cited by 80 publications

(60 citation statements)

References 28 publications

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“…Mutações no gene GJB2 que codifica a conexina 26 -componente das "gap junctions" das células epiteliais -recentemente têm sido descritas em pacientes com síndrome KID. Embora a distribuição da conexina 26 na córnea ainda não esteja bem definida, disfunções nas "gap junctions" do epitélio corneano podem ser responsáveis por alterações da superfície ocular (10)(11)(12) . O tratamento ocular na síndrome KID é sintomático, não havendo ainda descrição de drogas ou tratamento cirúrgico que possam modificar o curso e prognóstico dessa doença.…”

Section: Discussionunclassified

Uso do bevacizumab (Avastin®) na síndrome KID: relato de caso

Caye¹,

Scheid²,

Pizzol³

et al. 2010

Arq. Bras. Oftalmol.

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Section: Discussionunclassified

Uso do bevacizumab (Avastin®) na síndrome KID: relato de caso

Caye¹,

Scheid²,

Pizzol³

et al. 2010

Arq. Bras. Oftalmol.

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“…The CB1-CG1 bond rotation affects the angle (105.45 o for wild-type to 111.17 o for mutant) and the decrease in the force field energy of the protein from 6946.490 kJ/mol to 6811.053 kJ/mol ( Table 2). The substitution of the conserved residue aspartic acid 50 by asparagine (Asp50Asn) in the first extracellular domain of connexin 26 causes Keratitis-Ichthyosis-Deafness Syndrome (Yotsumoto et al, 2003). This mutation is likely to be the factor that disturbs the communication of ions, metabolites, and signaling molecules in neighboring cells and affects homeostasis by disturbing the bonding and energies (Saez et al, 2000).…”

Section: Discussionmentioning

confidence: 99%

“…About 20 mutations of gap junction β-2 have been described as being related to diseases (Abe et al, 2000) and various syndromes, such as Bart-Pumphrey Syndrome, KeratitisIchthyosis-Deafness Syndrome, and Vohwinkel Syndrome. (Richard et al, 2004;Snoeckx et al, 2005;Yotsumoto et al, 2003). The mutations alter the amino acid sequence of connexin 26 and result in impaired functioning of the protein associated with ion channels, especially.…”

Section: Introductionmentioning

confidence: 99%

In Silico Study of Human Gap Junction Beta-2 Protein by Homology Modeling

Shehzadi¹,

Masood²

2010

Genomics & Informatics

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Asp66his, Asp54Lys, and Asp50Asn are mutations in connexin 26 that are observed in the clinic and give rise to autosomal dominant syndromes. They are the result of point mutations in the human gap junction β-2 gene. In order to investigate the structural mechanism of Bart-Pumphrey Syndrome, Keratitis-Ichthyosis-Deafness Syndrome, and Vohwinkel Syndrome, homology modeling was carried out. Asp66 has direct contact with Asn62 by two hydrogen bonds in the wild-type protein, and in Asp66His, the biggest change observed is a tremendous energy increase caused by hydrogen bond breakage to Asn62. Shifts in the side chain and new hydrogen bond formation are observed for Lys54 compared to the wild-type protein (Asn54) and result in closer contact to Val84. Asp50Asn causes a significant decrease in bond energy, and residual charge reversal repels the ion and metabolites and, hence, inhibits their transportation. Such perturbations are likely to be a factor contributing to abnormal functioning of ion channels, resulting cell death and disease.

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“…Heterozygous missense mutations in GJB2 were found in several conditions associating deafness and hyperkeratosis: D66H in mutilating keratoderma with sensorineural deafness (Vohwinkel's syndrome, OMIM 124500) [Maestrini et al, 2002], G59A and R75Q in palmoplantar hyperkeratosis with deafness (PPKD, OMIM 148350) [Heathcote et al, 2000;Uyguner et al, 2002], as well as D50Y and D50N in keratitisichthyosis-deafness syndrome (KID, OMIM 148210), and in hystrix like-ichthyosis-deafness syndrome (HID, OMIM 602540) [Richard et al, 2002;van Geel et al, 2002;Yotsumoto et al, 2003]. Richard et al [2002] also described two sporadic cases of KID syndrome with G12R and S17F missense mutations, each patient showing a different mutation.…”

Section: To the Editormentioning

confidence: 99%