Inhibitory modulation by FMRFamide of the voltage‐gated sodium current in identified neurones in Lymnaea stagnalis.

Brussaard, Arjen B.; Lodder, J.C.; Maat, A. Ter; Vlieger, T.A. De; Kits, Karel S.

doi:10.1113/jphysiol.1991.sp018757

Cited by 19 publications

(12 citation statements)

References 28 publications

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“…and occurs at low concentrations (EDs0 = 7 x 10 -9 M) (Brussaard et al, 1988). These three characteristics are strikingly similar to those of the suppression of the sustained calcium current and contrast with the desensitization and slow recovery of the other responses to FMRFa (Brussaard et al, 1988(Brussaard et al, , 1990(Brussaard et al, , 1991aVeerman and Kits, unpublished). Therefore, it is likely that FMRFa suppresses the excitability of the CDCs via the selective inhibition of the sustained calcium current.…”

Section: Divergence Of Fmrfa Responsesmentioning

confidence: 60%

“…FMRFa inhibits CDCs by simultaneous inhibition of the voltage-activated sodium current (Brussaard et al, 1990(Brussaard et al, , 1991a, activation of a potassium current (Brussaard et al, 1988;Veerman and Kits, unpublished) and suppression of the sustained HVA calcium current (this paper). Since it was previously concluded on the basis of structure-activity studies that the multiple responses to FMRFa are mediated by a single receptor type (Brussaard et al, 1989) and that activation of the potassium current by FMRFa proceeds via the arachidonic acid pathway (Veerman and Kits, unpublished), the divergence of the FMRFa responses may occur at the level of the G-protein subtype or the primary effector of the G-protein.…”

Section: Divergence Of Fmrfa Responsesmentioning

confidence: 76%

“…These effects of FMRFa are independent, but mediated through a single FMRFa receptor type (Brussaard et al, 1988(Brussaard et al, , 1989. Voltage-clamp recordings demonstrated that FMRFa activates a potassium current (Veerman and Kits, unpublished) and inhibits the voltage-dependent sodium current (Brussaard et al, 1990(Brussaard et al, , 1991a. In addition, it was suggested that FMRFa inhibits the voltage-dependent calcium current (Brussaard et al, 1990).…”

Section: Introductionmentioning

confidence: 97%

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Inhibition of a slowly inactivating high-voltage-activated calcium current by the neuropeptide FMRFa in molluscan neuroendocrine cells

Dreijer

Verheule

Kits

1995

Invertebrate Neuroscience

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Using the whole-cell voltage-clamp technique, the effects of the neuropeptide Phe-Met-Arg-Phe-NH 2 (FMRFa) on two types of dihydropyridine-sensitive, high-voltage-activated calcium currents were investigated in isolated neuroendocrine caudo-dorsal cells (CDCs), which control egg-laying in the mollusc Lymnaea stagnalis. These currents are: (1) a transient current ('~inact = -10-25 ms) with an activation threshold of-40 mV and maximal amplitude at + 10 mV and (2) a sustained current ('Cinac t = -100-300 ms) with a threshold of -10 mV and a peak at +30 mV.FMRFa caused a partial block of the calcium current that was rapid, reversible and dose-dependent (ED50 = 4.3 nM). The FMRFa-sensitive and insensitive currents differed in voltage-dependence of activation and inactivation, steadystate inactivation characteristics and time course of recovery from inactivation, all indicating that FMRFa selectively suppressed the sustained calcium current.Internal perfusion of CDCs with GTP-?-S or GDP-[3-S depressed the FMRFa response, suggesting the involvement of G-proteins. Experiments aimed at elucidation of the signal transduction pathway between the FMRFa receptor and the calcium channel revealed no involvement of second messengers and protein kinases. The FMRFa-induced inhibition of the sustained calcium current probably results from a direct interaction between a G-protein, activated by the FMRFa receptor, and the calcium channel.The selective inhibition of this calcium current is likely to decrease the influx of calcium during the action potential, which will reduce the release of autoexcitatory CDC-peptides and contribute to a suppression of excitability.

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Section: Divergence Of Fmrfa Responsesmentioning

confidence: 60%

Section: Divergence Of Fmrfa Responsesmentioning

confidence: 76%

Section: Introductionmentioning

confidence: 97%

See 1 more Smart Citation

Inhibition of a slowly inactivating high-voltage-activated calcium current by the neuropeptide FMRFa in molluscan neuroendocrine cells

Dreijer

Verheule

Kits

1995

Invertebrate Neuroscience

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“…Na ϩ currents in Aplysia neurons are modulated by the peptide FMRFamide (Brussaard et al, 1991), but the mechanism of receptor coupling to Na ϩ channel modulation is unknown. Consistent with the present results in hippocampal neurons, activation of dopaminergic receptors modulates whole-cell Na ϩ current in neostriatal neurons via a PKAdependent signaling pathway (Surmeier et al, 1992;Schiffmann et al, 1995).…”

Section: Activation Of D1-like Dopamine Receptors In Hippocampal Pyramentioning

confidence: 99%

Dopaminergic Modulation of Sodium Current in Hippocampal Neurons via cAMP-Dependent Phosphorylation of Specific Sites in the Sodium Channel α Subunit

et al. 1997

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Phosphorylation of brain Na ϩ channel ␣ subunits by cAMPdependent protein kinase (PKA) decreases peak Na ϩ current in cultured brain neurons and in mammalian cells and Xenopus oocytes expressing cloned brain Na ϩ channels. We have studied PKA regulation of Na ϩ channel function by activation of D1-like dopamine receptors in acutely isolated hippocampal neurons using whole-cell voltage-clamp recording techniques. The D1 agonist SKF 81297 reversibly reduced peak Na ϩ current in a concentration-dependent manner. No changes in the voltage dependence or kinetics of activation or inactivation were observed. This effect was mediated by PKA, as it was mimicked by application of the PKA activator Sp-5,6-dichloro-1-␤-D-ribofuranosylbenzimidazole-3Ј,5Ј-monophosphorothioate (cBIMPS) and was inhibited by the specific PKA inhibitor peptide PKAI [5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20][21][22][23][24] . cBIMPS had similar effects on type IIA brain Na ϩ channel ␣ subunits expressed in tsA-201 cells, but no effect was observed on a mutant Na ϩ channel ␣ subunit in which serine residues in five PKA phosphorylation sites in the intracellular loop connecting domains I and II (L I-II ) had been replaced by alanine. A single mutation, S573A, similarly eliminated cBIMPS modulation. Thus, activation of D1-like dopamine receptors results in PKA-dependent phosphorylation of specific sites in L I-II of the Na ϩ channel ␣ subunit, causing a reduction in Na ϩ current. Such modulation is expected to exert a profound influence on overall neuronal excitability. Dopaminergic input to the hippocampus from the mesocorticolimbic system may exert this influence in vivo.

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“…Because voltage-gated sodium channels are responsible for the initiation and propagation of the action potential (Eccles, 1964), modulation of their activity is expected to affect dramatically neuronal excitability. In different cellular preparations, activation of the ,-adrenergic (Schubert, Vandongen, Kirsch & Brown, 1989), thyrotropin-releasing hormone (Lopez-Barneo, Castellano & Toledo-Aral, 1990), dopamine (Surmeier et al 1992) and FMRFamide receptors (Brussaard, Lodder, Ter Maat, de Vlieger & Kits, 1991) have been reported to modulate a voltage-gated sodium current. However, the transduction mechanisms involved in all of these neurotransmitter effects remains largely unknown.…”

mentioning

confidence: 99%

Dopamine D1 receptor modulates the voltage‐gated sodium current in rat striatal neurones through a protein kinase A.

Schiffmann

Lledo

Vincent

1995

The Journal of Physiology

139

108

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1. Whole-cell recordings were made from striatal neurones obtained from neonatal rats and maintained in primary cultures. The effects of dopamine D1 receptor activation were studied on the voltage-gated sodium current. 2. Bath application of a specific D1 agonist, SKF38393 (1 /uM), reduced the neuronal excitability recorded in current-clamp by increasing the threshold for generation of action potentials. 3. In voltage-clamp recordings, SKF38393 (1 /uM) reversibly reduced the peak amplitude of the sodium current by 37.8 + 4'95%. This effect was reversed by the D1 antagonist SCH23390 and was blocked by the intracellular loading of GDP-fl-S (2 mM) suggesting GTP-binding protein involvement. 4. The D1 agonist reduced the peak amplitude of the sodium current without significantly affecting (i) the voltage dependence of the current-voltage relationship, (ii) the voltage dependence of the steady-state activation and inactivation, (iii) the kinetics of the timedependent inactivation, and (iv) the kinetics of recovery from inactivation. 5. The peak amplitude of the sodium current was progressively reduced by intracellular loading of cyclic AMP-dependent protein kinase (100 U ml-1). 6. Diffusion of a specific peptide inhibitor of the cyclic AMP-dependent protein kinase (PKI; 10 /LM) into the cytosol of neurones blocked the effect of the D1 agonist on the sodium current amplitude. 7. These results demonstrate that dopamine acting at the D1 receptor reduces the amplitude of the sodium current without modifying its voltage-and time-dependent properties. This effect involves activation of the cyclic AMP-dependent protein kinase and results in a depression of the striatal neuronal excitability by increasing the threshold for generation of action potentials.

show abstract

Inhibitory modulation by FMRFamide of the voltage‐gated sodium current in identified neurones in Lymnaea stagnalis.

Cited by 19 publications

References 28 publications

Inhibition of a slowly inactivating high-voltage-activated calcium current by the neuropeptide FMRFa in molluscan neuroendocrine cells

Inhibition of a slowly inactivating high-voltage-activated calcium current by the neuropeptide FMRFa in molluscan neuroendocrine cells

Dopaminergic Modulation of Sodium Current in Hippocampal Neurons via cAMP-Dependent Phosphorylation of Specific Sites in the Sodium Channel α Subunit

Dopamine D1 receptor modulates the voltage‐gated sodium current in rat striatal neurones through a protein kinase A.

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