A heterozygous mutation in <i>GJB2</i> (Cx26F142L) associated with deafness and recurrent skin rashes results in connexin assembly deficiencies

Albuloushi, Ahmad; Lovgren, Marie‐Louise; Steel, Ainsley; Yeoh, Yeelon; Waters, Alexandra; Zamiri, M.; Martin, Patricia

doi:10.1111/exd.14187

Cited by 6 publications

(13 citation statements)

References 54 publications

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“…Dye uptake assays showed that cells expressing the N54K mutant demonstrated a highly variable incidence of PI uptake, and cells expressing the S183F mutant displayed no increase in PI uptake, indicating nonfunctional hemichannels [ 24 ]. Marziano et al [ 52 ] and Albuloushi et al [ 87 ] obtained similar results for the hemichannel activity of the D66H and F142L mutants. Both variants resulted in syndromic HL and had reduced hemichannel activity.…”

Section: Association Between Gjb2 Missense Variant...mentioning

confidence: 53%

Molecular Mechanisms and Clinical Phenotypes of GJB2 Missense Variants

Mao

Wang²,

et al. 2023

Biology

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The GJB2 gene is the most common gene responsible for hearing loss (HL) worldwide, and missense variants are the most abundant type. GJB2 pathogenic missense variants cause nonsyndromic HL (autosomal recessive and dominant) and syndromic HL combined with skin diseases. However, the mechanism by which these different missense variants cause the different phenotypes is unknown. Over 2/3 of the GJB2 missense variants have yet to be functionally studied and are currently classified as variants of uncertain significance (VUS). Based on these functionally determined missense variants, we reviewed the clinical phenotypes and investigated the molecular mechanisms that affected hemichannel and gap junction functions, including connexin biosynthesis, trafficking, oligomerization into connexons, permeability, and interactions between other coexpressed connexins. We predict that all possible GJB2 missense variants will be described in the future by deep mutational scanning technology and optimizing computational models. Therefore, the mechanisms by which different missense variants cause different phenotypes will be fully elucidated.

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Section: Association Between Gjb2 Missense Variant...mentioning

confidence: 53%

Molecular Mechanisms and Clinical Phenotypes of GJB2 Missense Variants

Mao

Wang²,

et al. 2023

Biology

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“…Several mutations induce lethal phenotypes and are associated with loss of cell viability [ 83 , 84 , 85 ]. Recently, we proposed a further Class 4 mutation group associated with hyperkeratosis, mucositis and deafness, where cell model studies revealed cell death and a collapse of the microtubule network, but limited connexin channel function (e.g., F142L, CX31G45E) [ 86 , 87 ].…”

Section: Connexins and The Skinmentioning

confidence: 99%

“…As such, CX26 and CX43, critical connexins in epithelial tissue are unable to form heterotypic structures [ 88 , 89 ]. Recent studies report changes in CX26 mutation oligomerization compatibility, allowing aberrant interactions with CX43 with exacerbated hemichannel activity but non-functional gap junction channels [ 78 , 86 , 90 ], with each mutation uniquely altering the 3D structure in terms of charge, pore size, hydrophobicity, etc. It is also conceivable that altered CX43:CX26 heteromeric channels influence unique metabolic exchange and influence asymmetric cell division required for the stratification of the epidermis, thereby contributing to the hyperproliferative status of the skin [ 91 ].…”

Section: Connexins and The Skinmentioning

confidence: 99%

“…Mutations in CX26 affect hemichannel permeability. As discussed, CX26 KID syndrome mutations provoke ‘leaky’ hemichannels and allow the aberrant formation of CX43-CX26 hetero-hemichannels presenting abnormal permeability [ 66 , 78 , 86 , 145 , 146 , 147 ]. Some of these mutations also alter CX26 PCO 2 gating sensitivity, which may contribute to CO 2 -dependent regulation of breathing in mammals [ 148 , 149 , 150 , 151 ].…”

Section: Connexins and Inflammationmentioning

confidence: 99%

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Connexins and the Epithelial Tissue Barrier: A Focus on Connexin 26

Garcia-Vega

O'Shaughnessy

Albuloushi

et al. 2021

Biology

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Epithelial tissue responds rapidly to environmental triggers and is constantly renewed. This tissue is also highly accessible for therapeutic targeting. This review highlights the role of connexin mediated communication in avascular epithelial tissue. These proteins form communication conduits with the extracellular space (hemichannels) and between neighboring cells (gap junctions). Regulated exchange of small metabolites less than 1kDa aide the co-ordination of cellular activities and in spatial communication compartments segregating tissue networks. Dysregulation of connexin expression and function has profound impact on physiological processes in epithelial tissue including wound healing. Connexin 26, one of the smallest connexins, is expressed in diverse epithelial tissue and mutations in this protein are associated with hearing loss, skin and eye conditions of differing severity. The functional consequences of dysregulated connexin activity is discussed and the development of connexin targeted therapeutic strategies highlighted.

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“…This disease is usually accompanied by many other medical disorders, for example sensorineural deafness, ichthyosis, vitiligo and mental retardation, severely affecting the patients' physical and mental health 2 . However, the effective therapeutic treatment of VS is still lacking in the clinical settings 3 …”

Section: Introductionmentioning

confidence: 99%

4‐octyl itaconate improves the viability of D66H cells by regulating the KEAP1‐NRF2‐GCLC/HO‐1 pathway

Chen

Wang

Song

et al. 2023

J Cellular Molecular Medi

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As a rare and refractory hereditary skin disease belonging to the familial and autosomal dominant dermatosis, the Vohwinkel syndrome (VS) is characterized by diffuse hyperkeratosis in the palms of hands and soles of feet, which would develop to auto-amputation if not treated adequately. 1,2 This disease is usually accompanied by many other medical disorders, for example sensorineural deafness, ichthyosis, vitiligo and mental retardation, severely affecting the patients' physical and mental health. 2 However, the effective therapeutic treatment of VS is still lacking in the clinical settings. 3 Recent studies have shown that there are two types of palmoplantar keratoderma mutilating. One is an ichthyosis-related variant caused by the insertional mutations in the loricrin gene. [4][5][6] The other

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A heterozygous mutation in GJB2 (Cx26F142L) associated with deafness and recurrent skin rashes results in connexin assembly deficiencies

Cited by 6 publications

References 54 publications

Molecular Mechanisms and Clinical Phenotypes of GJB2 Missense Variants

Molecular Mechanisms and Clinical Phenotypes of GJB2 Missense Variants

Connexins and the Epithelial Tissue Barrier: A Focus on Connexin 26

4‐octyl itaconate improves the viability of D66H cells by regulating the KEAP1‐NRF2‐GCLC/HO‐1 pathway

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