Interaction of batrachotoxin with the local anesthetic receptor site in transmembrane segment IVS6 of the voltage-gated sodium channel

Linford, Nancy J.; Cantrell, Angela R.; Qu, Yusheng; Scheuer, Todd; Catterall, William A.

doi:10.1073/pnas.95.23.13947

Cited by 116 publications

(133 citation statements)

References 38 publications

(44 reference statements)

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“…The close functional association, as well as the close positional association, has further been demonstrated by the findings that point mutations in D4-S6, which inhibit the action of LAs on conductance of Na ϩ channels, also block the binding of BTX to the Na ϩ channel (21,22). Likewise, mutations in D1-S6, which block the binding of BTX, also block the inhibiting action of local anesthetics on the Na ϩ channel (23).…”

Section: Discussionmentioning

confidence: 89%

Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na ⁺ channels

Xiao

Ke²,

Wang³

et al. 2001

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

112

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Suppression of cardiac voltage-gated Na ؉ currents is probably one of the important factors for the cardioprotective effects of the n-3 polyunsaturated fatty acids (PUFAs) against lethal arrhythmias. The ␣ subunit of the human cardiac Na ؉ channel (hH1␣) and its mutants were expressed in human embryonic kidney (HEK293t) cells. The effects of single amino acid point mutations on fatty acid-induced inhibition of the hH1 ␣ Na ؉ current (INa) were assessed. Eicosapentaenoic acid (EPA, C20:5n-3) significantly reduced I Na in HEK293t cells expressing the wild type, Y1767K, and F1760K of hH1␣ Na ؉ channels. The inhibition was voltage and concentration-dependent with a significant hyperpolarizing shift of the steady state of INa. In contrast, the mutant N406K was significantly less sensitive to the inhibitory effect of EPA. The values of the shift at 1, 5, and 10 M EPA were significantly smaller for N406K than for the wild type. Coexpression of the ␤1 subunit and N406K further decreased the inhibitory effects of EPA on I Na in HEK293t cells. In addition, EPA produced a smaller hyperpolarizing shift of the V1/2 of the steady-state inactivation in HEK293t cells coexpressing the ␤1 subunit and N406K. These results demonstrate that substitution of asparagine with lysine at the site of 406 in the domain-1-segment-6 region (D1-S6) significantly decreased the inhibitory effect of PUFAs on I Na, and coexpression with ␤1 decreased this effect even more. Therefore, asparagine at the 406 site in hH1␣ may be important for the inhibition by the PUFAs of cardiac voltage-gated Na ؉ currents, which play a significant role in the antiarrhythmic actions of PUFAs.human cardiac Na ϩ channel ͉ ␤1 subunit ͉ polyunsaturated fatty acids

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Section: Discussionmentioning

confidence: 89%

Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na ⁺ channels

Xiao

Ke²,

Wang³

et al. 2001

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

112

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“…The highaffinity-pyrethroid-binding site is located likely at the interface between domains I and II where the amino acid residues V409 and L993 reside, which is also suggested in the house fly sodium channel (Lee and Soderlund, 2001). Such domain interface models have been proposed for several classes of lipophilic neurotoxins acting on calcium and sodium channels (Hockerman et al, 1997;Linford et al, 1998). For example, sodium channel site 2 neurotoxin BTX activates sodium channels by binding to a site formed by unique amino acid determinants in IS6 and IVS6 (Linford et al, 1998).…”

Section: Discussionmentioning

confidence: 90%

“…Such domain interface models have been proposed for several classes of lipophilic neurotoxins acting on calcium and sodium channels (Hockerman et al, 1997;Linford et al, 1998). For example, sodium channel site 2 neurotoxin BTX activates sodium channels by binding to a site formed by unique amino acid determinants in IS6 and IVS6 (Linford et al, 1998).…”

Section: Discussionmentioning

confidence: 99%

Synergistic interaction between two cockroach sodium channel mutations and a tobacco budworm sodium channel mutation in reducing channel sensitivity to a pyrethroid insecticide

Liu

Tan

Valles

et al. 2002

Insect Biochemistry and Molecular Biology

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Pyrethroid insecticide resistance due to reduced nerve sensitivity, known as knockdown resistance (kdr or kdr-type), is linked to multiple point mutations in the para-homologous sodium channel genes. Previously we demonstrated that two mutations (E434K and C764R) in the German cockroach sodium channel greatly enhanced the ability of the L993F mutation (a known kdr -type mutation) to reduce sodium channel sensitivity to deltamethrin, a pyrethroid insecticide. Neither E434K nor C764R alone, however, altered sodium channel sensitivity. To examine whether E434K and C764R also enhance the effect of pyrethroid resistance-associated sodium channel mutations identified in other insects, we introduced a V to M mutation (V409M) into the cockroach sodium channel protein at the position that corresponds to the V421M mutation in the Heliothis virescens sodium channel protein. We found that the V409M mutation alone modified the gating properties of the sodium channel and reduced channel sensitivity to deltamethrin by 10-fold. Combining the V409M mutation with either the E434K or C764K alone did not reduce the V409M channel sensitivity to deltamethrin further. However, the triple mutation combination (V409M, E434K and C764R) dramatically reduced channel sensitivity by 100-fold compared with the wild-type channel. These results suggest that the E434K and C764R mutations are important modifiers of sodium channel sensitivity to pyrethroid insecticides.

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“…Plasmids pCDM8-rIIA (containing the cDNA fragment of the full-length rat Na v 1.2a ␣ subunit; Linford et al, 1998) and pCDM8-rH1 (containing the cDNA of the full-length rat heart Na v 1.5 sodium channel ␣ subunit; Qu et al, 1994) have been described. The rSKM1 cDNA encoding the Na v 1.4 ␣ subunit (Featherstone et al, 1998) was a kind gift from Dr. Peter Ruben (Utah State University) and was subcloned into pCDM8 to produce pCDM8-rSKM1.…”

Section: Methodsmentioning

confidence: 99%

Sodium Channel β4, a New Disulfide-Linked Auxiliary Subunit with Similarity to β2

et al. 2003

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The principal ␣ subunit of voltage-gated sodium channels is associated with auxiliary ␤ subunits that modify channel function and mediate protein-protein interactions. We have identified a new ␤ subunit termed ␤4. Like the ␤1-␤3 subunits, ␤4 contains a cleaved signal sequence, an extracellular Ig-like fold, a transmembrane segment, and a short intracellular C-terminal tail. Using TaqMan reverse transcription-PCR analysis, in situ hybridization, and immunocytochemistry, we show that ␤4 is widely distributed in neurons in the brain, spinal cord, and some sensory neurons. ␤4 is most similar to the ␤2 subunit (35% identity), and, like the ␤2 subunit, the Ig-like fold of ␤4 contains an unpaired cysteine that may interact with the ␣ subunit. Under nonreducing conditions, ␤4 has a molecular mass exceeding 250 kDa because of its covalent linkage to Na v 1.2a, whereas on reduction, it migrates with a molecular mass of 38 kDa, similar to the mature glycosylated forms of the other ␤ subunits. Coexpression of ␤4 with brain Na v 1.2a and skeletal muscle Na v 1.4 ␣ subunits in tsA-201 cells resulted in a negative shift in the voltage dependence of channel activation, which overrode the opposite effects of ␤1 and ␤3 subunits when they were present. This novel, disulfide-linked ␤ subunit is likely to affect both protein-protein interactions and physiological function of multiple sodium channel ␣ subunits.

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Interaction of batrachotoxin with the local anesthetic receptor site in transmembrane segment IVS6 of the voltage-gated sodium channel

Cited by 116 publications

References 38 publications

Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na ⁺ channels

Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na ⁺ channels

Synergistic interaction between two cockroach sodium channel mutations and a tobacco budworm sodium channel mutation in reducing channel sensitivity to a pyrethroid insecticide

Sodium Channel β4, a New Disulfide-Linked Auxiliary Subunit with Similarity to β2

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Interaction of batrachotoxin with the local anesthetic receptor site in transmembrane segment IVS6 of the voltage-gated sodium channel

Cited by 116 publications

References 38 publications

Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na + channels

Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na + channels

Synergistic interaction between two cockroach sodium channel mutations and a tobacco budworm sodium channel mutation in reducing channel sensitivity to a pyrethroid insecticide

Sodium Channel β4, a New Disulfide-Linked Auxiliary Subunit with Similarity to β2

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Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na ⁺ channels

Single point mutations affect fatty acid block of human myocardial sodium channel α subunit Na ⁺ channels