The N Terminus of Connexin37 Contains an α-Helix That Is Required for Channel Function

Kyle, John W.; Berthoud, Viviana M.; Kurutz, Josh W.; Minogue, Peter J.; Greenspan, Michael D.; Hanck, Dorothy A.; Beyer, Eric C.

doi:10.1074/jbc.m109.016907

Cited by 22 publications

(24 citation statements)

References 54 publications

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“…An N-terminal deletion mutant of ShakBL, an innexin protein found in Drosophila, fails to induce conductance when paired homotypically, and induces much lower conductance when paired heterotypically with functional ShakBL [43]. These are consistent with the works on Cx37 showing that the N-terminal deletion mutants are mostly non-functional [44,45]. It is possible that the conformations of all purified INX-6 Δ N channels are fixed in a closed state by this truncation, which leads to the better crystallinity.…”

Section: Discussionsupporting

confidence: 87%

Hexadecameric structure of an invertebrate gap junction channel

Oshima

Matsuzawa

Murata

et al. 2016

Journal of Molecular Biology

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Innexins are invertebrate-specific gap junction proteins with four transmembrane helices. These proteins oligomerize to constitute intercellular channels that allow for the passage of small signaling molecules associated with neural and muscular electrical activity. In contrast to the large number of structural and functional studies of connexin gap junction channels, few structural studies of recombinant innexin channels are reported. Here we show the three-dimensional structure of two-dimensionally crystallized Caenorhabditis elegans innexin-6 (INX-6) gap junction channels. The N-terminal deleted INX-6 proteins are crystallized in lipid bilayers. The three-dimensional reconstruction determined by cryo-electron crystallography reveals that a single INX-6 gap junction channel comprises 16 subunits, a hexadecamer, in contrast to chordate connexin channels, which comprise 12 subunits. The channel pore diameters at the cytoplasmic entrance and extracellular gap region are larger than those of connexin26. Two bulb densities are observed in each hemichannel, one in the pore and the other at the cytoplasmic side of the hemichannel in the channel pore pathway. These findings imply a structural diversity of gap junction channels among multicellular organisms.

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Section: Discussionsupporting

confidence: 87%

Hexadecameric structure of an invertebrate gap junction channel

Oshima

Matsuzawa

Murata

et al. 2016

Journal of Molecular Biology

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“…10 Bioinformatic secondary structure predictions and NMR studies suggest that the -group connexin NT domain possesses a predominantly -helical pore domain structure between positions W4 and S18. 30 indicate a 15% increase in  j and reduced cation selectivity associated with the Cx40 G2 mutation (Fig. 2), consistent with the interpretation of increased pore volume and less electrostatic charge in the vicinity of the amino terminus.…”

Section: Discussionsupporting

confidence: 82%

Specificity of the connexin W3/4 locus for functional gap junction formation

Lin

Matiukas

et al. 2016

Channels

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The N-terminal (NT) domain of the connexins forms an essential transjunctional voltage (Vj) sensor and pore-forming domain that when truncated, tagged, or mutated often leads to formation of a nonfunctional channel. The NT domain is relatively conserved among the connexins though the α- and δ-group connexins possess a G2 residue not found in the β- and γ-group connexins. Deletion of the connexin40 G2 residue (Cx40G2Δ) affected the Vj gating, increased the single channel conductance (γj), and decreased the relative K(+)/Cl(-) permeability (PK/PCl) ratio of the Cx40 gap junction channel. The conserved α/β-group connexin D2/3 and W3/4 loci are postulated to anchor the NT domain within the pore via hydrophilic and hydrophobic interactions with adjacent connexin T5 and M34 residues. Cx40D3N and D3R mutations produced limited function with progressive reductions in Vj gating and noisy low γj gap junction channels that reduced the γj of wild-type Cx40 channels from 150 pS to < 50 pS when coexpressed. Surprisingly, hydrophobic Cx40 W4F and W4Y substitution mutations were not compatible with function despite their ability to form gap junction plaques. These data are consistent with minor and major contributions of the G2 and D3 residues to the Cx40 channel pore structure, but not with the postulated hydrophobic W4 intermolecular interactions. Our results indicate an absolute requirement for an amphipathic W3/4 residue that is conserved among all α/β/δ/γ-group connexins. We alternatively hypothesize that the connexin D2/3-W3/4 locus interacts with the highly conserved FIFR M1 motif to stabilize the NT domain within the pore.

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“…However, all constructs containing at least 9 amino acids formed gap junction plaques, implying that the absolute length of the NT and the identities of specific amino acids are not requirements for normal biosynthesis of gap junctions. In agreement with these findings, Kyle et al [26] found that expression of a Cx37 mutant containing prolines at positions 10 and 15 (instead of the normal Leu15 and Gln15) also formed plaques. However, all of these mutations disrupted hemichannel and channel function.…”

Section: Role Of Nt In Formation Of Functional Gap Junction Channelsmentioning

confidence: 52%

“…It is interesting that the critical residues implicated in determining these various physiological properties are among the most divergent amino acids within the NT domain (see [26, 32, 35]). Although overall the sequence of this domain is quite conserved, the substitutions confer many of the characteristic properties that differentiate channels formed of different connexins.…”

Section: Roles Of Nt Amino Acids In Channel Gating Unitary Conducmentioning

confidence: 99%

“…The structure of the NT domain was initially investigated by studying synthetic peptides using circular dichroism and nuclear magnetic resonance (NMR) [26,53–55]. Based on the studies of a 15 amino acid peptide, Purnick et al [53] proposed a model for the NT of Cx26 with an α-helix extending from position 1 to 10 and a critical bend at positions 11 and 12 that was suggested to act as a “hinge” allowing the first 10 amino acids to swing into the pore and block the channel.…”

Section: Structure Of the Amino Terminal Domainmentioning

confidence: 99%

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Structural organization of intercellular channels II. Amino terminal domain of the connexins: sequence, functional roles, and structure

Beyer

Lipkind

Kyle

et al. 2012

Biochimica et Biophysica Acta (BBA) - Biomembranes

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The amino terminal domain (NT) of the connexins consists of their first 22–23 amino acids. Site-directed mutagenesis studies have demonstrated that NT amino acids are determinants of gap junction channel properties including unitary conductance, permeability/selectivity, and gating in response to transjunctional voltage. The importance of this region has also been emphasized by the identification of multiple disease-associated connexin mutants affecting amino acid residues in the NT region. The first part of the NT is α-helical. The structure of the Cx26 gap junction channel shows that the NT α-helix localizes within the channel, and lines much of the wall of the pore. Interactions of the amino acid residues in the NT with those in the transmembrane helices may be critical for holding the channel open. The predicted sites of these interactions and the applicability of the Cx26 structure to the NT of other connexins are considered.

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The N Terminus of Connexin37 Contains an α-Helix That Is Required for Channel Function

Cited by 22 publications

References 54 publications

Hexadecameric structure of an invertebrate gap junction channel

Hexadecameric structure of an invertebrate gap junction channel

Specificity of the connexin W3/4 locus for functional gap junction formation

Structural organization of intercellular channels II. Amino terminal domain of the connexins: sequence, functional roles, and structure

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