Gap-Junction Channels Dysfunction in Deafness and Hearing Loss

Martı́nez, Agustı́n D.; Acuña, Rodrigo; Figueroa, Vania; Maripillán, Jaime; Nicholson, Bruce J.

doi:10.1089/ars.2008.2138

Cited by 132 publications

(114 citation statements)

References 117 publications

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“…The major causative alleles, c.35delG and c.235delC, have been well characterized in many studies, and the carrier frequencies of these mutations vary in different ethnic populations (Park et al, 2000;Green et al, 1999;Han et al, 2008;Zelante et al, 1997). In addition, a number of novel GJB2 variants that contain amino acid substitutions have been identified in numerous genetic studies (Martinez et al, 2009, Connexin-Deafness Homepage: World Wide Web URL: http://davinci.crg.es/deafness/). These variants were predicted to be pathogenic since the mutations were only found in patients and the residues were highly conserved among different species.…”

Section: Discussionmentioning

confidence: 99%

“…Therefore, the dominant-negative effect of the p.D46E mutation may be due to defective docking of the two opposing connexin hemichannels. In many cases, mutations in extracellular domains are associated with dominant inheritance and syndromic phenotype, such as skin disorders and other ectodermal abnormalities (Deng et al, 2006;Martinez et al, 2009;Marziano et al, 2003;Matos et al, 2008;Melchionda et al, 2005;Sun et al, 2005). Two different mutations in the EC1 (p.W44C and p.W44S) have been reported to be associated with dominantly inherited nonsyndromic hearing loss and to exert a dominant-negative effect on gap junction permeability (Martin et al, 1999;Marziano et al, 2003).…”

Section: Discussionmentioning

confidence: 99%

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Different functional consequences of two missense mutations in theGJB2gene associated with non-syndromic hearing loss

Choi

Park²,

Lee

et al. 2009

Hum. Mutat.

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Mutations in the GJB2 gene, which encodes the gap junction (GJ) protein connexin26 (Cx26), are the most common cause of inherited non-syndromic hearing loss (NSHL). We identified two missense mutations, p.D46E (c.138T>G) and p.T86R (c.257C>G), of GJB2 in Korean HL families. The novel p.D46E mutation exhibited autosomal dominant inheritance, while the p.T86R mutation, which is exclusively found in Asians, segregated with an autosomal recessive pattern. Thus, we sought to elucidate the pathogenic nature of such different inherited patterns of HL. We studied protein localization and gap junction functions in cells transfected with wild-type or mutant Cx26 tagged with fluorescent proteins, which allowed visual confirmation of homozygous or heterozygous mutant GJs. The Cx26-D46E mutant was targeted to the plasma membrane, but this mutant protein failed to transfer Ca 2+ or propidium iodide intercellularly, suggesting disruption of both ionic and biochemical coupling. Heterozygous GJs also showed dysfunctional intercellular couplings and hemichannel opening, confirming the dominant-negative nature of the p.D46E mutation. The Cx26-T86R mutant protein did not form GJs, since the mutated protein was confined in the cytoplasm and not transported to the cell membrane. When Cx26-T86R was co-expressed with Cx26-WT, ionic and biochemical coupling was normal, consistent with the recessive nature of the mutation. These studies revealed distinct pathogenic mechanisms of two GJB2 mutations identified in Korean families.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Different functional consequences of two missense mutations in theGJB2gene associated with non-syndromic hearing loss

Choi

Park²,

Lee

et al. 2009

Hum. Mutat.

View full text Add to dashboard Cite

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“…Electrical synapses also have essential roles in the developing brain, where they regulate the formation of chemical synapses (3)(4)(5). In humans, mutations that affect electrical synapses are associated with neurological conditions such as epilepsy, deafness, and peripheral neuropathies (6)(7)(8). However, it is difficult to study electrical synapses in detail because there are few simple functional assays or pharmacological tools that selectively target their activity.…”

mentioning

confidence: 99%

Dissection of neuronal gap junction circuits that regulate social behavior in Caenorhabditis elegans

Jang

Levy

Flavell

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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A hub-and-spoke circuit of neurons connected by gap junctions controls aggregation behavior and related behavioral responses to oxygen, pheromones, and food in Caenorhabditis elegans. The molecular composition of the gap junctions connecting RMG hub neurons with sensory spoke neurons is unknown. We show here that the innexin gene unc-9 is required in RMG hub neurons to drive aggregation and related behaviors, indicating that UNC-9-containing gap junctions mediate RMG signaling. To dissect the circuit in detail, we developed methods to inhibit unc-9-based gap junctions with dominant-negative unc-1 transgenes. unc-1(dn) alters a stomatin-like protein that regulates unc-9 electrical signaling; its disruptive effects can be rescued by a constitutively active UNC-9::GFP protein, demonstrating specificity. Expression of unc-1(dn) in RMG hub neurons, ADL or ASK pheromone-sensing neurons, or URX oxygen-sensing neurons disrupts specific elements of aggregation-related behaviors. In ADL, unc-1(dn) has effects opposite to those of tetanus toxin light chain, separating the roles of ADL electrical and chemical synapses. These results reveal roles of gap junctions in a complex behavior at cellular resolution and provide a tool for similar exploration of other gap junction circuits.innexin | neural circuits | electrical synapses | stomatin | sensory behavior

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“…It is widely accepted that hyperactive connexin hemichannels play pathological roles. For instance, several human connexin mutations that cause human pathologies produce exacerbated hemichannel activity at the plasma membrane, which has deleterious consequences (3)(4)(5). Similarly, in nongenetic pathologies, including ischemia and muscular dystrophy, there is strong evidence that opening of hemichannels enhances tissue damage (6)(7)(8).…”

mentioning

confidence: 99%

Mechanism of gating by calcium in connexin hemichannels

Lopez

Ramachandran

Alsamarah

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Aberrant opening of nonjunctional connexin hemichannels at the plasma membrane is associated with many diseases, including ischemia and muscular dystrophy. Proper control of hemichannel opening is essential to maintain cell viability and is achieved by physiological levels of extracellular Ca 2+ , which drastically reduce hemichannel activity. Here we examined the role of conserved charged residues that form electrostatic networks near the extracellular entrance of the connexin pore, a region thought to be involved in gating rearrangements of hemichannels. Molecular dynamics simulations indicate discrete sites for Ca 2+ interaction and consequent disruption of salt bridges in the open hemichannels. Experimentally, we found that disruption of these salt bridges by mutations facilitates hemichannel closing. Two negatively charged residues in these networks are putative Ca 2+ binding sites, forming a Ca 2+ -gating ring near the extracellular entrance of the pore. Accessibility studies showed that this Ca 2+ -bound gating ring does not prevent access of ions or small molecules to positions deeper into the pore, indicating that the physical gate is below the Ca 2+ -gating ring. We conclude that intra-and intersubunit electrostatic networks at the extracellular entrance of the hemichannel pore play critical roles in hemichannel gating reactions and are tightly controlled by extracellular Ca 2+ . Our findings provide a general mechanism for Ca 2+ gating among different connexin hemichannel isoforms.connexin | hemichannels | gating

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Gap-Junction Channels Dysfunction in Deafness and Hearing Loss

Cited by 132 publications

References 117 publications

Different functional consequences of two missense mutations in theGJB2gene associated with non-syndromic hearing loss

Different functional consequences of two missense mutations in theGJB2gene associated with non-syndromic hearing loss

Dissection of neuronal gap junction circuits that regulate social behavior in Caenorhabditis elegans

Mechanism of gating by calcium in connexin hemichannels

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