Effects of persistent sodium current blockade in respiratory circuits depend on the pharmacological mechanism of action and network dynamics

Segal, Michael M. and Andrea F. Douglas. Late sodium channel openings underlying epileptiform activity are preferentially diminished by the anticonvulsant phenytoin. J. Neurophysiol. 77: 3021–3034, 1997. Late openings of sodium channels were observed in outside-out patch recordings from hippocampal neurons in culture. In previous studies of such neurons, a persistent sodium current appeared to underlie the ictal epileptiform activity. All the channel currents were blocked by tetrodotoxin. In addition to the transient openings of sodium channels making up the peak sodium current, there were two types of late channel openings: brief late and burst openings. These late channel openings occurred throughout voltage pulses that lasted 750 ms, producing a persistent sodium current. At −30 mV, this current was 0.4% of the peak current. The late channel openings occurred throughout the physiological range of trans-membrane voltages. The anticonvulsant phenytoin reduced the late channel openings more than the peak currents. The effect on the persistent current was greatest at more depolarized voltages, whereas the effect on peak currents was not substantially voltage dependent. In the presence of 60 μM phenytoin, peak sodium currents at −30 mV were 40–41% of control, as calculated using different methods of analysis. Late currents were 22–24% of control. Phenytoin primarily decreased the number of channel openings, with less effect on the duration of channel openings and no effect on open channel current. This set of findings is consistent with models in which phenytoin binds to the inactivated state of the channel. The preferential effect of phenytoin on the persistent sodium current suggests that an important pharmacological mechanism for a sodium channel anticonvulsant is to reduce late openings of sodium channels, rather than reducing all sodium channel openings. We hypothesize that pharmacological interventions that are most selective in reducing late openings of sodium channels, while leaving early channel openings relatively intact, will be those that produce an anticonvulsant effect while interfering minimally with normal function.

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Muscarinic Enhancement of Persistent Sodium Current Synchronizes Striatal Medium Spiny Neurons

Journal of Neurophysiology ◽

10.1152/jn.00134.2009 ◽

2009 ◽

Vol 102 (2) ◽

pp. 682-690 ◽

Cited By ~ 20

Author(s):

Luis Carrillo-Reid ◽

Fatuel Tecuapetla ◽

Nicolas Vautrelle ◽

Adán Hernández ◽

Ramiro Vergara ◽

...

Keyword(s):

Sodium Current ◽

Network Dynamics ◽

Receptor Activation ◽

Procedural Memory ◽

Negative Slope ◽

Medium Spiny Neurons ◽

Persistent Sodium Current ◽

Intrinsic Properties ◽

Bistable Behavior ◽

Spiny Neurons

Network dynamics denoted by synchronous firing of neuronal pools rely on synaptic interactions and intrinsic properties. In striatal medium spiny neurons, N-methyl-d-aspartate (NMDA) receptor activation endows neurons with nonlinear capabilities by inducing a negative-slope conductance region (NSCR) in the current–voltage relationship. Nonlinearities underlie associative learning, procedural memory, and the sequential organization of behavior in basal ganglia nuclei. The cholinergic system modulates the function of medium spiny projection neurons through the activation of muscarinic receptors, increasing the NMDA-induced NSCR. This enhancement is reflected as a change in the NMDA-induced network dynamics, making it more synchronous. Nevertheless, little is known about the contribution of intrinsic properties that promote this activity. To investigate the mechanisms underlying the cholinergic modulation of bistable behavior in the striatum, we used whole cell and calcium-imaging techniques. A persistent sodium current modulated by muscarinic receptor activation participated in the enhancement of the NSCR and the increased network synchrony. These experiments provide evidence that persistent sodium current generates bistable behavior in striatal neurons and contributes to the regulation of synchronous network activity. The neuromodulation of bistable properties could represent a cellular and network mechanism for cholinergic actions in the striatum.

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Faculty Opinions recommendation of Molecular determinants for modulation of persistent sodium current by G-protein betagamma subunits.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.1025012.294762 ◽

2005 ◽

Author(s):

Patrick Delmas

Keyword(s):

G Protein ◽

Sodium Current ◽

Persistent Sodium Current ◽

Molecular Determinants ◽

Betagamma Subunits

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Sodium Currents in Neurons From the Rostroventrolateral Medulla of the Rat

Journal of Neurophysiology ◽

10.1152/jn.00150.2003 ◽

2003 ◽

Vol 90 (3) ◽

pp. 1635-1642 ◽

Cited By ~ 40

Author(s):

Ilya A. Rybak ◽

Krzysztof Ptak ◽

Natalia A. Shevtsova ◽

Donald R. McCrimmon

Keyword(s):

Sodium Channels ◽

Sodium Current ◽

Cell Voltage ◽

Kinetic Properties ◽

Persistent Sodium Current ◽

Sodium Currents ◽

Bötzinger Complex ◽

Window Current ◽

Bursting Activity

Rapidly inactivating and persistent sodium currents have been characterized in acutely dissociated neurons from the area of rostroventrolateral medulla that included the pre-Bötzinger Complex. As demonstrated in many studies in vitro, this area can generate endogenous rhythmic bursting activity. Experiments were performed on neonate and young rats (P1-15). Neurons were investigated using the whole cell voltage-clamp technique. Standard activation and inactivation protocols were used to characterize the steady-state and kinetic properties of the rapidly inactivating sodium current. Slow depolarizing ramp protocols were used to characterize the noninactivating sodium current. The “window” component of the rapidly inactivating sodium current was calculated using mathematical modeling. The persistent sodium current was revealed by subtraction of the window current from the total noninactivating sodium current. Our results provide evidence of the presence of persistent sodium currents in neurons of the rat rostroventrolateral medulla and determine voltage-gated characteristics of activation and inactivation of rapidly inactivating and persistent sodium channels in these neurons.

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