Effects of Ethanol and Temperature on a Crab Motor Axon Action Potential: A Possible Mechanism for Peripheral Spike Generation

1. In autotomized walking limbs of Pachygrapsus crassipes, microelectrode recordings of evoked action potentials were made in the meropodite from the E2 excitor axon to the bender muscle. 2. The action potential spike was followed by a depolarizing after-potential. Increases in temperature resulted in a decline in the amplitude and time course of the spike, and an increase in the amplitude of the after-potential. Low levels of ethanol or increased levels of calcium increased the size of the after-potential and decreased the temperature threshold for peripheral spike generation. 3. At high temperatures a single orthodromic E2 axon spike provoked the generation of additional impulses at the periphery, with an inter-spike interval of 2–3.5 ms. 4. The after-potential lasted longer than the refractory period following the spike. The axon membrane, therefore, was depolarized after the refractory period and this resulted in a period of low threshold for spike generation. Increases in temperature shortened the refractory period. 5. We suggest that additional spikes are generated at the periphery where the E2 axon diameter is decreased. The increased membrane resistance at these sites increases the size of the depolarizing after-potential. Therefore, if the depolarization following the refractory period is at or above threshold for firing, additional action potentials will be generated at the periphery.

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Calcium Dynamics and Compartmentalization in Leech Neurons

Journal of Neurophysiology ◽

10.1152/jn.00695.2005 ◽

2005 ◽

Vol 94 (6) ◽

pp. 4430-4440 ◽

Cited By ~ 2

Author(s):

Sofija Andjelic ◽

Vincent Torre

Keyword(s):

Information Processing ◽

Action Potential ◽

Action Potentials ◽

Time Course ◽

Ccd Camera ◽

Calcium Dynamics ◽

Single Action ◽

Single Action Potential ◽

Calcium Indicator ◽

Mechanosensory Neurons

Calcium dynamics in leech neurons were studied using a fast CCD camera. Fluorescence changes (Δ F/ F) of the membrane impermeable calcium indicator Oregon Green were measured. The dye was pressure injected into the soma of neurons under investigation. Δ F/ F caused by a single action potential (AP) in mechanosensory neurons had approximately the same amplitude and time course in the soma and in distal processes. By contrast, in other neurons such as the Anterior Pagoda neuron, the Annulus Erector motoneuron, the L motoneuron, and other motoneurons, APs evoked by passing depolarizing current in the soma produced much larger fluorescence changes in distal processes than in the soma. When APs were evoked by stimulating one distal axon through the root, Δ F/ F was large in all distal processes but very small in the soma. Our results show a clear compartmentalization of calcium dynamics in most leech neurons in which the soma does not give propagating action potentials. In such cells, the soma, while not excitable, can affect information processing by modulating the sites of origin and conduction of AP propagation in distal excitable processes.

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Time course of postnatal changes in rat heart action potential and in transient outward current is different

AJP Heart and Circulatory Physiology ◽

10.1152/ajpheart.1994.267.3.h1157 ◽

1994 ◽

Vol 267 (3) ◽

pp. H1157-H1166 ◽

Cited By ~ 5

Author(s):

G. M. Wahler ◽

S. J. Dollinger ◽

J. M. Smith ◽

K. L. Flemal

Keyword(s):

Action Potential ◽

Rat Heart ◽

Action Potentials ◽

Time Course ◽

Outward Current ◽

Transient Outward Current ◽

Papillary Muscles ◽

Isolated Cells ◽

Time Courses ◽

Action Potential Shortening

The rat ventricular action potential shortens after birth. The contribution of increases in the transient outward current (Ito) to postnatal action potential shortening was assessed by measuring Ito in isolated cells and by determining the effect of 2 mM 4-aminopyridine (4-AP) on the action potentials of papillary muscles. 4-AP had no effect on 1-day action potential duration at 25% repolarization (APD25), and 1-day cells had little Ito. In 8- to 10-day muscles, 4-AP caused a small, but significant, increase in APD25. Ito increased slightly between day 1 and days 8-10, but this increase was not significant. Most of the increase in Ito (79%) and in the response to 4-AP (64%) occurred between days 8-10 and adult; however, approximately 75% of the APD25 shortening took place by days 8-10. Thus, while Ito may contribute to repolarization in late neonatal and adult cells, the different time courses of action potential shortening and increases in Ito suggest that changes in Ito are unlikely to be responsible for most of the postnatal action potential shortening.

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CHARACTERIZATION OF SIGNAL CONDUCTION ALONG DEMYELINATED AXONS BY ACTION-POTENTIAL-ENCODED SECOND HARMONIC GENERATION

Journal of Innovative Optical Health Sciences ◽

10.1142/s1793545813300036 ◽

2014 ◽

Vol 07 (01) ◽

pp. 1330003 ◽

Cited By ~ 2

Author(s):

ZHI-HUI LUO ◽

JIANG-XU CHEN ◽

YI-MEI HUANG ◽

HONG-QIN YANG ◽

JU-QIANG LIN ◽

...

Keyword(s):

Action Potential ◽

Second Harmonic Generation ◽

Harmonic Generation ◽

Refractory Period ◽

Action Potentials ◽

Demyelinating Disease ◽

Second Harmonic ◽

Temporal Distribution ◽

Demyelinating Diseases

Action-potential-encoded optical second harmonic generation (SHG) has been recently proposed for use in detecting the axonal damage in patients with demyelinating diseases. In this study, the characterization of signal conduction along axons of two different levels of demyelination was studied via a modified Hodgkin–Huxley model, because some types of demyelinating disease, i.e., primary progressive and secondary progressive multiple sclerosis, are difficult to be distinguished by magnetic resonance imaging (MRI), we focused on the differences in signal conduction between two different demyelinated axons, such as the first-level demyelination and the second-level demyelination. The spatio-temporal distribution of action potentials along demyelinated axons and conduction properties including the refractory period and frequency encoding in these two patterns were investigated. The results showed that demyelination could induce the decrease both in the amplitude of action potentials and the ability of frequency coding. Furthermore, the signal conduction velocity in the second-level demyelination was about 21% slower than that in the first-level demyelination. The refractory period in the second-level demyelination was about 32% longer than the first-level. Thus, detecting the signal conduction in demyelinated axons by action-potential-encoded optical SHG could greatly improve the assessment of demyelinating disorders to classify the patients. This technique also offers a potential fast and noninvasive optical approach for monitoring membrane potential.

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Effect of Several Cations on Transmembrane Potentials of Cardiac Muscle

American Journal of Physiology-Legacy Content ◽

10.1152/ajplegacy.1956.186.2.317 ◽

1956 ◽

Vol 186 (2) ◽

pp. 317-324 ◽

Cited By ~ 140

Author(s):

Brian F. Hoffman ◽

E. E. Suckling

Keyword(s):

Action Potential ◽

Cardiac Muscle ◽

Action Potentials ◽

Time Course ◽

Pacemaker Activity ◽

Transmembrane Potentials ◽

High K ◽

Intracellular Microelectrodes ◽

Simultaneous Decrease ◽

Low K

The effects of changes in the extracellular concentrations of Ca, K and Mg on the transmembrane resting and action potentials of single fibers of the auricle, ventricle and specialized conducting system of the dog heart have been studied by means of intracellular microelectrodes. With respect to Ca, the three tissues exhibit quite different sensitivities. Changes in concentration of this ion alter the time course of the action potential recorded from auricle and ventricle but have little effect on the action potential configuration of the Purkinje fiber. In the latter tissue, on the other hand, pacemaker activity is most strongly enhanced by Ca depletion and excitability is lost at Ca concentrations permitting normal propagation in papillary muscle. The effect of K on the resting transmembrane potential is dependent on the simultaneous Ca concentration. The interrelationship is such that the depolarizing effect of high K is decreased by elevated Ca and the depolarization produced by low K is diminished by low levels of Ca. Changes in the concentration of Mg have little effect on the transmembrane potentials of cardiac muscle unless the level of Ca is low. Under this condition a simultaneous decrease in Mg gives rise to a marked prolongation of the action potential duration of both auricle and ventricle. Some evidence for the basic similarity of the processes underlying repolarization in these three tissues is presented and it is thought the normally encountered differences in their action potentials may be related to the sensitivity of each tissue to extracellular Ca.

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Posttetanic hyperpolarization produced by electrogenic Na(+)-K+ pump in lizard axons impaled near their motor terminals

Journal of Neurophysiology ◽

10.1152/jn.1993.70.5.1874 ◽

1993 ◽

Vol 70 (5) ◽

pp. 1874-1884 ◽

Cited By ~ 58

Author(s):

K. Morita ◽

G. David ◽

J. N. Barrett ◽

E. F. Barrett

Keyword(s):

Action Potential ◽

Action Potentials ◽

Time Course ◽

Input Resistance ◽

Peak Amplitude ◽

Resting Potential ◽

Tetanic Stimulation ◽

Train Duration ◽

Consistent Change ◽

Nodal Voltage

1. The hyperpolarization that follows tetanic stimulation was recorded intra-axonally from the internodal region of intramuscular myelinated motor axons. 2. The peak amplitude of the posttetanic hyperpolarization (PTH) that followed stimulation at 20-100 Hz for < or = 35 s increased with increasing train duration, reaching a maximum of 22 mV. PTH decayed over a time course that increased from tens to hundreds of seconds with increasing train duration. For a given frequency of stimulation the time integral of PTH was proportional to the number of stimuli in the train, averaging 3-4 mV.s per action potential. 3. Ouabain (0.1-1 mM) and cyanide (1 mM) depolarized the resting potential and abolished PTH. Tetanic stimulation in ouabain was followed by a slowly decaying depolarization (probably due to extra-axonal K+ accumulation) whose magnitude and duration increased as the duration of the train increased. 4. Axonal input resistance showed no consistent change during PTH in normal solution but increased during PTH in the presence of 3 mM Cs+ (which blocks axonal inward rectifier currents). 5. PTH was abolished when bath Na+ was replaced by Li+ or choline. PTH persisted after removal of bath Ca2+ and addition of 2 mM Mn2+. 6. Removal of bath K+ abolished the PTH recorded after brief stimulus trains and greatly reduced the duration of PTH recorded after longer stimulus trains. 7. A brief application of 10 mM K+, which normally depolarizes axons, produced a ouabain-sensitive hyperpolarization in axons bathed in K(+)-free solution. 8. These observations suggest that in these myelinated axons PTH is produced mainly by activation of an electrogenic Na(+)-K(+)-ATPase, rather than by changes in K+ permeability or transmembrane [K+] gradients. This conclusion is supported by calculations showing agreement between estimates of Na+ efflux/impulse based on PTH measurements and estimates of Na+ influx/impulse based on nodal voltage-clamp measurements. Pump activity also appears to contribute to the resting potential. 9. The stimulus intensity required to initiate a propagating action potential increased during PTH but decreased during the posttetanic depolarization recorded in ouabain. Thus changes in axonal excitability after tetanic stimulation correlate with changes in the posttetanic membrane potential. 10. Action potentials that propagated during PTH had a larger peak amplitude and were followed by a larger and longer depolarizing afterpotential than action potentials elicited at the resting potential. This enhancement of the depolarizing afterpotential is consistent with previous reports of an increased superexcitable period after action potentials evoked during PTH.

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Contribution of Na+/Ca2+ exchange to action potential of human atrial myocytes

AJP Heart and Circulatory Physiology ◽

10.1152/ajpheart.1996.271.3.h1151 ◽

1996 ◽

Vol 271 (3) ◽

pp. H1151-H1161 ◽

Cited By ~ 12

Author(s):

A. Benardeau ◽

S. N. Hatem ◽

C. Rucker-Martin ◽

B. Le Grand ◽

L. Mace ◽

...

Keyword(s):

Action Potential ◽

Action Potentials ◽

Time Course ◽

Significant Proportion ◽

Type A ◽

Plateau Phase ◽

Type B ◽

Atrial Myocytes ◽

Human Atrial Myocytes ◽

Delayed Afterdepolarizations

The Ca2+ dye indo 1 was used to record internal Ca2+ (Cai) transients in order to investigate the role of the Na+/Ca2+ exchange current (INa/Ca) in whole cell patch-clamped human atrial myocytes After the activation of the L-type Ca2+ current by test pulses (20 ms) at +20 mV, a tail current (I(tail)) was activated at a holding potential of -80 mV with a density of -1.29 +/- 0.06 pA/pF. The time course of I(tail) followed that of Cai transients I(tail) was suppressed by dialyzing cells with ethylene glycol-bis(beta-aminoethyl ether)-N,N,N',N'-tetraacetic acid, applying 5 mM caffeine, or substituting external Na+ with Li+, indicating that this current was mainly generated by INa/Ca. Two types of action potential were recorded: type A, which is characterized by a narrow early plateau followed by a late low plateau phase, and type B, which is characterized by a small initial peak followed by a prolonged high plateau phase. Type B action potentials were found in larger cells than type A action potentials (membrane capacitance 81.8 +/- 4.5 and 122.4 +/- 7.0 pF in types A and B, respectively, P < 0.001). Substitution of external Na+ with Li+ shortened the late plateau of the type A action potential and the prolonged plateau of the type B action potential. Suppression of Cai transients by caffeine shortens the late part of both types of action potentials, whereas its lengthening effect on the initial phase of action potentials can result from several different mechanisms. The beat-to-beat dependent relationship between Cai transients and action potentials could be mediated by Ina/Ca- Delayed afterdepolarizations were present in a significant proportion of atrial myocytes in our experimental conditions. They were reversibly suppressed by Li+ substitution for Na+, suggesting that they are generated by INa/Ca. We conclude that INa/Ca plays a major role in the development of action potentials and delayed afterdepolarizations in isolated human atrial myocytes.

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Two Components of the Cardiac Action Potential

The Journal of General Physiology ◽

10.1085/jgp.54.5.607 ◽

1969 ◽

Vol 54 (5) ◽

pp. 607-635 ◽

Cited By ~ 117

Author(s):

Antonio Paes de Carvalho ◽

Brian Francis Hoffman ◽

Marilene de Paula Carvalho

Keyword(s):

Action Potential ◽

Action Potentials ◽

Time Course ◽

Slow Component ◽

Slow Inward Current ◽

Equilibrium Potential ◽

Slow Phase ◽

Positive Equilibrium ◽

Cardiac Action

Transmembrane potentials recorded from the rabbit heart in vitro were displayed as voltage against time (V, t display), and dV/dt against voltage (V, V or phase-plane display). Acetylcholine was applied to the recording site by means of a hydraulic system. Results showed that (a) differences in time course of action potential upstroke can be explained in terms of the relative magnitude of fast and slow phases of depolarization; (b) acetylcholine is capable of depressing the slow phase of depolarization as well as the plateau of the action potential; and (c) action potentials from nodal (SA and AV) cells seem to lack the initial fast phase. These results were construed to support a two-component hypothesis for cardiac electrogenesis. The hypothesis states that cardiac action potentials are composed of two distinct and physiologically separable "components" which result from discrete mechanisms. An initial fast component is a sodium spike similar to that of squid nerve. The slow component, which accounts for both a slow depolarization during phase 0 and the plateau, probably is dependent on the properties of a slow inward current having a positive equilibrium potential, coupled to a decrease in the resting potassium conductance. According to the hypothesis, SA and AV nodal action potentials are due entirely or almost entirely to the slow component and can therefore be expected to exhibit unique electrophysiological and pharmacological properties.

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The Effect of Aconitine on the Giant Axon of the Squid

The Journal of General Physiology ◽

10.1085/jgp.47.4.719 ◽

1964 ◽

Vol 47 (4) ◽

pp. 719-733 ◽

Cited By ~ 30

Author(s):

W. H. Herzog ◽

R. M. Feibel ◽

S. H. Bryant

Keyword(s):

Membrane Potential ◽

Action Potential ◽

Action Potentials ◽

Giant Axon ◽

Membrane Resistance ◽

Repetitive Stimulation ◽

Resting Membrane Potential ◽

Sustained Activity ◽

Frequency Of Stimulation ◽

Sodium And Potassium

In the giant axon of Loligo pealii, "aconitine potent" Merck added to the bath (10-7 to 1.25 x 10-6 gm/ml) (a) had no effect on resting membrane potential, membrane resistance and rectification, membrane response to subthreshold currents, critical depolarization, or action potential, but (b) on repetitive stimulation produced oscillations of membrane potential after the spike, depolarization, and decrease of membrane resistance. The effect sums with successive action potentials; it increases with concentration of aconitine, time of exposure, and frequency of stimulation. When the oscillations are large enough and the membrane potential is 51.6 ± SD 1.5 mv a burst of self-sustained activity begins; it usually lasts 20 to 70 sec. and at its end the membrane potential is 41.5 ± SD 1.9 mv. Repolarization occurs with a time constant of 2.5 to 11.1 min. Substitution of choline for external sodium after a burst hyperpolarizes the membrane to -70 mv, and return to normal external sodium depolarizes again beyond the resting membrane potential. The effect of aconitine on the membrane is attributed to an increase of sodium and potassium or chloride conductances following the action potential.

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Properties of tetraethylammonium ion-resistant K+ channels in the photoreceptor membrane of the giant barnacle.

The Journal of General Physiology ◽

10.1085/jgp.77.6.629 ◽

1981 ◽

Vol 77 (6) ◽

pp. 629-646 ◽

Cited By ~ 8

Author(s):

D R Edgington ◽

A E Stuart

Keyword(s):

Action Potential ◽

Action Potentials ◽

Cardiac Glycosides ◽

Time Course ◽

Photoreceptor Membrane ◽

K Channels ◽

Na Pump ◽

Tetraethylammonium Ion ◽

Electrogenic Na Pump ◽

Time Courses

After the offset of illumination, barnacle photoreceptors undergo a large hyperpolarization that lasts seconds or minutes. We studied the mechanisms that generate this afterpotential by recording afterpotentials intracellularly from the medial photoreceptors of the giant barnacle Balanus nubilus. The afterpotential has two components with different time-courses: (a) an earlier component due to an increase in conductance to K+ that is not blocked by extracellular tetraethylammonium ion (TEA+) or 3-aminopyridine (3-AP) and (b) a later component that is sensitive to cardiac glycosides and that requires extracellular K+, suggesting that it is due to an electrogenic Na+ pump. The K+ conductance component increases in amplitude with increasing CA++ concentration and is inhibited by extracellular Co++; the Co++ inhibition can be overcome by increasing the Ca++ concentration. Thus, the K+ conductance component is Ca++ dependent. An afterpotential similar to that evoked by a brief flash of light is generated by depolarization with current in the dark and by eliciting Ca++ action potentials in the presence of TEA+ in the soma, axon, or terminal regions of the photoreceptor. The action potential undershoot is generated by an increase in conductance to K+ that is resistant to TEA+ and 3-AP and inhibited by Co++. The similarity in time-course and pharmacology of the hyperpolarization afterpotentials elicited by (a) a brief flash of light, (b) depolarization with current, and (c) an action potential indicates that Ca++-dependent K+ channels throughout the photoreceptor membrane are responsible for all three hyperpolarizing events.

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Transmural recording of monophasic action potentials

AJP Heart and Circulatory Physiology ◽

10.1152/ajpheart.01172.2000 ◽

2002 ◽

Vol 282 (3) ◽

pp. H855-H861 ◽

Cited By ~ 7

Author(s):

Xiaohong Zhou ◽

Jian Huang ◽

Raymond E. Ideker

Keyword(s):

Guinea Pig ◽

Action Potential ◽

Refractory Period ◽

Time Course ◽

Monophasic Action Potential ◽

Papillary Muscles ◽

Transmembrane Potentials ◽

Potential Map ◽

Monophasic Action Potentials ◽

Injury Potential

To investigate the possibility of transmural recording of repolarization through the ventricular wall, KCl monophasic action potential (MAP) electrodes positioned along plunge needles were developed and tested. The MAP electrode consists of a silver wire surrounded by agarose gel containing KCl, which slowly eluted into the adjacent tissue to depolarize it. In six dogs, a plunge needle containing three KCl MAP electrodes was inserted into the left ventricle to simultaneously record from the subepicardium, midwall, and subendocardium. In six pigs, eight plunge needles containing three KCl MAP electrodes and two plunge needles containing similar electrodes except for the absence of KCl were inserted into the ventricles. In three guinea pig papillary muscles, a KCl electrode was used to record MAPs along with two microelectrodes for recording transmembrane potentials. Transmural MAP recordings could be made for >1 h in dogs and >2 h in pigs with a significant decrease in MAP amplitude over time but without a significant change in MAP duration. With the electrodes without KCl in pigs, the injury potentials subsided in <30 min. When the pacing rate was changed to alter the action potential duration and refractory period in dogs, the MAP duration correlated with the local effective refractory period ( r = 0.94). The time course of the MAP duration recorded with a KCl MAP electrode in guinea pig papillary muscles corresponded well with that of the transmembrane potential recorded with an adjacent microelectrode. It is possible to record transmural repolarization of the ventricles with KCl MAP electrodes on plunge needles. The MAP is caused by the KCl rather than being a nonspecific injury potential.

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