Multiple Contributions of an Input-Representing Neuron to the Dynamics of the Aplysia Feeding Network

In Aplysia, mutually antagonistic ingestive and egestive behaviors are produced by the same multifunctional central pattern generator (CPG) circuit. Interestingly, higher-order inputs that activate the CPG do not directly specify whether the resulting motor program is ingestive or egestive because the slow dynamics of the network intervene. One input, the commandlike cerebral–buccal interneuron 2 (CBI-2), slowly drives the motor output toward ingestion, whereas another input, the esophageal nerve (EN), drives the motor output toward egestion. When the input is switched from EN to CBI-2, the motor output does not switch immediately and remains egestive. Here, we investigated how these slow dynamics are implemented on the interneuronal level. We found that activity of two CPG interneurons, B20 and B40, tracked the motor output regardless of the input, whereas activity of another CPG interneuron, B65, tracked the input regardless of the motor output. Furthermore, we show that the slow dynamics of the network are implemented, at least in part, in the slow dynamics of the interaction between the input-representing and the output-representing neurons. We conclude that 1) a population of CPG interneurons, recruited during a particular motor program, simultaneously encodes both the input that is used to elicit the motor program and the output elicited by this input; and 2) activity of the input-representing neurons may serve to bias the future motor programs.

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B64, a newly identified central pattern generator element producing a phase switch from protraction to retraction in buccal motor programs of Aplysia californica

Journal of Neurophysiology ◽

10.1152/jn.1996.75.4.1327 ◽

1996 ◽

Vol 75 (4) ◽

pp. 1327-1344 ◽

Cited By ~ 53

Author(s):

I. Hurwitz ◽

A. J. Susswein

Keyword(s):

Phase Shift ◽

Central Pattern Generator ◽

Motor Program ◽

Pattern Generator ◽

Synaptic Activity ◽

Excitatory Postsynaptic Potential ◽

Motor Programs ◽

Identified Neuron ◽

Protraction Phase ◽

Two Phases

1. Buccal motor programs in Aplysia are characterized by two phases of activity, which represent protraction and retraction of the radula in intact animals. The shift from protraction to retraction is caused by synaptic activity inhibiting neurons that are active during protraction and exciting neurons that are active during retraction. 2. B64, a newly identified neuron present bilaterally in the buccal ganglia, is partially responsible for the phase shift. Stimulating a single B64 causes bilateral inhibition of neurons B31/B32 and other neurons active during protraction and cause bilateral excitation of neurons B4/B5 and other neurons active during retraction. B64 is active throughout retraction. The amplitude and waveforms of the synaptic potentials caused by firing B64 are similar, but not identical, to those seen during retraction. 3. Some of the effects of B64 on B31/B32 and on B4/B5 are monosynaptic, as shown by their maintained presence in high divalent cation seawater, which blocks polysynaptic activity. 4. A brief depolarization of B64 leads to a long-lasting depolarization and firing. The ability of B64 to respond in this way is at least partially caused by an endogenous plateau potential, as this property is still seen after synaptic transmission is blocked. 5. Hyperpolarization of B64 bilaterally and preventing the somata from firing unmasks a large excitatory postsynaptic potential in B64. This procedure does not block the shift from protraction to retraction, indicating that spiking in the B64 somata is not necessary for the phase shift. 6. The firing pattern and synaptic connections of B64 are consistent with the hypothesis that the neuron is part of a central pattern generator underlying buccal motor programs. B64 is monosynaptically inhibited by neurons that are active along with B31/B32, which are responsible for producing the protraction phase of a buccal motor program. During the later portion of the protraction phase B64 is excited. In addition, firing B64 can phase advance and phase delay buccal motor programs. 7. Regulating the firing of B64 can regulate the expression of buccal motor programs. Stimulation of B64 at frequencies of 0.5-1.0 Hz leads to complete inhibition of buccal motor programs, whereas steady-state depolarization of B64 can lead to repetitive bursts of activity.

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Interneuronal and Peptidergic Control of Motor Pattern Switching in Aplysia

Journal of Neurophysiology ◽

10.1152/jn.00438.2001 ◽

2002 ◽

Vol 87 (1) ◽

pp. 49-61 ◽

Cited By ~ 54

Author(s):

Peter T. Morgan ◽

Jian Jing ◽

Ferdinand S. Vilim ◽

Klaudiusz R. Weiss

Keyword(s):

Motor Pattern ◽

Electrical Coupling ◽

Motor Program ◽

Pattern Generator ◽

Higher Order ◽

Pattern Selection ◽

Motor Programs ◽

Additional Support ◽

Selection Of ◽

Stimulation Of

It has been proposed that a choice of specific behaviors can be mediated either by activation of behavior-specific higher order neurons or by distinct combinations of such neurons in different behaviors. We examined the role that two higher order neurons, CBI-2 and CBI-3, play in the selection of motor programs that correspond to ingestion and egestion, two stimulus-dependent behaviors that are generated by a single central pattern generator (CPG) of Aplysia. We found that CBI-2 could evoke either ingestive, egestive, or ambiguous motor programs depending on the regime of stimulation. When CBI-2 recruited CBI-3 firing via electrical coupling, the motor program tended to be ingestive. In the absence of CBI-3 activation, the program was usually egestive. When CBI-2 was stimulated to produce ingestive programs, hyperpolarization of CBI-3 converted the programs to egestive or ambiguous. When CBI-2 was stimulated to produce egestive or ambiguous programs, co-stimulation of CBI-3 converted them into ingestive. These findings are consistent with the idea that combinatorial commands are responsible for the choice of specific behaviors. Additional support for this view comes from the observations that appropriate stimulus conditions exist both for activation of CBI-2 together with CBI-3, and for activation of CBI-2 without a concomitant activation of CBI-3. The ability of CBI-3 to convert egestive and ambiguous programs into ingestive ones was mimicked by application of APGWamide, a neuropeptide that we have detected in CBI-3 by immunostaining. Thus combinatorial actions of higher order neurons that underlie pattern selection may involve the use of modulators released by specific higher order neurons.

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Release of a single neurotransmitter from an identified interneuron coherently affects motor output on multiple time scales

Journal of Neurophysiology ◽

10.1152/jn.01079.2012 ◽

2013 ◽

Vol 109 (9) ◽

pp. 2327-2334 ◽

Cited By ~ 4

Author(s):

Andrew M. Dacks ◽

Klaudiusz R. Weiss

Keyword(s):

Time Scales ◽

Motor Program ◽

Gaba Release ◽

Motor Output ◽

Multiple Time Scales ◽

Multiple Time ◽

Intrinsic Properties ◽

Buccal Ganglion ◽

Motor Programs ◽

Pattern Characteristic

Neurotransmitters can have diverse effects that occur over multiple time scales often making the consequences of neurotransmission difficult to predict. To explore the consequences of this diversity, we used the buccal ganglion of Aplysia to examine the effects of GABA release by a single interneuron, B40, on the intrinsic properties and motor output of the radula closure neuron B8. B40 induces a picrotoxin-sensitive fast IPSP lasting milliseconds in B8 and a slow EPSP lasting seconds. We found that the excitatory effects of this slow EPSP are also mediated by GABA. Together, these two GABAergic actions structure B8 firing in a pattern characteristic of ingestive programs. Furthermore, we found that repeated B40 stimulation induces a persistent increase in B8 excitability that was occluded in the presence of the GABA B receptor agonist baclofen, suggesting that GABA affects B8 excitability over multiple time scales. The phasing of B8 activity during the feeding motor programs determines the nature of the behavior elicited during that motor program. The persistent increase in B8 excitability induced by B40 biased the activity of B8 during feeding motor programs causing the motor programs to become more ingestive in nature. Thus, a single transmitter released from a single interneuron can have consequences for motor output that are expressed over multiple time scales. Importantly, despite the differences in their signs and temporal characteristics, the three actions of B40 are coherent in that they promote B8 firing patterns that are characteristic of ingestive motor outputs.

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Intrinsic and Extrinsic Modulation of a Single Central Pattern Generating Circuit

Journal of Neurophysiology ◽

10.1152/jn.2000.84.3.1186 ◽

2000 ◽

Vol 84 (3) ◽

pp. 1186-1193 ◽

Cited By ~ 47

Author(s):

Peter T. Morgan ◽

Ray Perrins ◽

Philip E. Lloyd ◽

Klaudiusz R. Weiss

Keyword(s):

Neural Circuits ◽

Central Pattern Generators ◽

Motor Program ◽

Pattern Generator ◽

Motor Programs ◽

Appetitive Behavior ◽

Protraction Phase ◽

Pattern Generators ◽

Rhythmic Behaviors ◽

Appetitive Behaviors

Intrinsic and extrinsic neuromodulation are both thought to be responsible for the flexibility of the neural circuits (central pattern generators) that control rhythmic behaviors. Because the two forms of modulation have been studied in different circuits, it has been difficult to compare them directly. We find that the central pattern generator for biting in Aplysia is modulated both extrinsically and intrinsically. Both forms of modulation increase the frequency of motor programs and shorten the duration of the protraction phase. Extrinsic modulation is mediated by the serotonergic metacerebral cell (MCC) neurons and is mimicked by application of serotonin. Intrinsic modulation is mediated by the cerebral peptide-2 (CP-2) containing CBI-2 interneurons and is mimicked by application of CP-2. Since the effects of CBI-2 and CP-2 occlude each other, the modulatory actions of CBI-2 may be mediated by CP-2 release. Although the effects of intrinsic and extrinsic modulation are similar, the neurons that mediate them are active predominantly at different times, suggesting a specialized role for each system. Metacerebral cell (MCC) activity predominates in the preparatory (appetitive) phase and thus precedes the activation of CBI-2 and biting motor programs. Once the CBI-2s are activated and the biting motor program is initiated, MCC activity declines precipitously. Hence extrinsic modulation prefacilitates biting, whereas intrinsic modulation occurs during biting. Since biting inhibits appetitive behavior, intrinsic modulation cannot be used to prefacilitate biting in the appetitive phase. Thus the sequential use of extrinsic and intrinsic modulation may provide a means for premodulation of biting without the concomitant disruption of appetitive behaviors.

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Fast Synaptic Connections From CBIs to Pattern-Generating Neurons in Aplysia: Initiation and Modification of Motor Programs

Journal of Neurophysiology ◽

10.1152/jn.00497.2002 ◽

2003 ◽

Vol 89 (4) ◽

pp. 2120-2136 ◽

Cited By ~ 31

Author(s):

Itay Hurwitz ◽

Irving Kupfermann ◽

Klaudiusz R. Weiss

Keyword(s):

Central Pattern Generator ◽

Motor Pattern ◽

Aplysia Californica ◽

Pattern Generator ◽

Synaptic Connections ◽

Motor Patterns ◽

Motor Programs ◽

Postsynaptic Potentials ◽

Buccal Ganglia ◽

Very High

Consummatory feeding movements in Aplysia californica are organized by a central pattern generator (CPG) in the buccal ganglia. Buccal motor programs similar to those organized by the CPG are also initiated and controlled by the cerebro-buccal interneurons (CBIs), interneurons projecting from the cerebral to the buccal ganglia. To examine the mechanisms by which CBIs affect buccal motor programs, we have explored systematically the synaptic connections from three of the CBIs (CBI-1, CBI-2, CBI-3) to key buccal ganglia CPG neurons (B31/B32, B34, and B63). The CBIs were found to produce monosynaptic excitatory postsynaptic potentials (EPSPs) with both fast and slow components. In this report, we have characterized only the fast component. CBI-2 monosynaptically excites neurons B31/B32, B34, and B63, all of which can initiate motor programs when they are sufficiently stimulated. However, the ability of CBI-2 to initiate a program stems primarily from the excitation of B63. In B31/B32, the size of the EPSPs was relatively small and the threshold for excitation was very high. In addition, preventing firing in either B34 or B63 showed that only a block in B63 firing prevented CBI-2 from initiating programs in response to a brief stimulus. The connections from CBI-2 to the buccal ganglia neurons showed a prominent facilitation. The facilitation contributed to the ability of CBI-2 to initiate a BMP and also led to a change in the form of the BMP. The cholinergic blocker hexamethonium blocked the fast EPSPs induced by CBI-2 in buccal ganglia neurons and also blocked the EPSPs between a number of key CPG neurons within the buccal ganglia. CBI-2 and B63 were able to initiate motor patterns in hexamethonium, although the form of a motor pattern was changed, indicating that non-hexamethonium-sensitive receptors contribute to the ability of these cells to initiate bursts. By contrast to CBI-2, CBI-1 excited B63 but inhibited B34. CBI-3 excited B34 and not B63. The data indicate that CBI-1, -2, and -3 are components of a system that initiates and selects between buccal motor programs. Their behavioral function is likely to depend on which combination of CBIs and CPG elements are activated.

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A Newly Identified Buccal Interneuron Initiates and Modulates Feeding Motor Programs in Aplysia

Journal of Neurophysiology ◽

10.1152/jn.00173.2003 ◽

2003 ◽

Vol 90 (4) ◽

pp. 2190-2204 ◽

Cited By ~ 17

Author(s):

N. C. Dembrow ◽

J. Jing ◽

A. Proekt ◽

A. Romero ◽

F. S. Vilim ◽

...

Keyword(s):

Central Pattern Generator ◽

Pattern Generator ◽

Considerable Progress ◽

Buccal Ganglion ◽

Motor Programs ◽

Cerebral Ganglia ◽

Full Complement ◽

Electrophysiological Characterization

Despite considerable progress in characterizing the feeding central pattern generator (CPG) in Aplysia, the full complement of neurons that generate feeding motor programs has not yet been identified. The distribution of neuropeptide-containing neurons in the buccal and cerebral ganglia can be used as a tool to identify additional elements of the feeding circuitry by providing distinctions between otherwise morphologically indistinct neurons. For example, our recent study revealed a unique and potentially interesting unpaired PRQFVamide (PRQFVa)-containing neuron in the buccal ganglion. In this study, we describe the morphological and electrophysiological characterization of this novel neuron, which we designate as B50. We found that activation of B50 is capable of producing organized rhythmic output of the feeding CPG. The motor programs elicited by B50 exhibit some similarities as well as differences to motor programs elicited by the command-like cerebral-to-buccal interneuron CBI-2. In addition to activating the feeding CPG, B50 may act as a program modulator.

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Isoflurane Disrupts Central Pattern Generator Activity and Coordination in the Lamprey Isolated Spinal Cord

Anesthesiology ◽

10.1097/00000542-200509000-00020 ◽

2005 ◽

Vol 103 (3) ◽

pp. 567-575 ◽

Cited By ~ 24

Author(s):

Steven L. Jinks ◽

Richard J. Atherley ◽

Carmen L. Dominguez ◽

Karen A. Sigvardt ◽

Joseph F. Antognini

Keyword(s):

Spinal Cord ◽

Central Pattern Generator ◽

Motor Neurons ◽

Central Pattern Generators ◽

Volatile Anesthetics ◽

Pattern Generator ◽

Motor Output ◽

Petroleum Jelly ◽

Burst Frequency ◽

Generator Activity

Background Although volatile anesthetics such as isoflurane can depress sensory and motor neurons in the spinal cord, movement occurring during anesthesia can be coordinated, involving multiple limbs as well as the head and trunk. However, it is unclear whether volatile anesthetics depress locomotor interneurons comprising central pattern generators or disrupt intersegmental central pattern generator coordination. Methods Lamprey spinal cords were excised during anesthesia and placed in a bath containing artificial cerebrospinal fluid and D-glutamate to induce fictive swimming. The rostral, middle, and caudal regions were bath-separated using acrylic partitions and petroleum jelly, and in each compartment, the authors recorded ventral root activity. The authors selectively delivered isoflurane (0.5, 1, and 1.5%) only to the middle segments of the spinal cord. Spectral analyses were then used to assess isoflurane effects on central pattern generator activity and coordination. Results Isoflurane dose-dependently reduced fictive locomotor activity in all three compartments, with 1.5% isoflurane nearly eliminating activity in the middle compartment and reducing spectral amplitudes in the anesthetic-free rostral and caudal compartments to 23% and 31% of baseline, respectively. Isoflurane decreased burst frequency in the caudal compartment only, to 53% of baseline. Coordination of central pattern generator activity between the rostral and caudal compartments was also dose-dependently decreased, to 42% of control at 1.5% isoflurane. Conclusion Isoflurane disrupts motor output by reducing interneuronal central pattern generator activity in the spinal cord. The effects of isoflurane on motor output outside the site of isoflurane application were presumably independent of effects on sensory or motor neurons.

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An interneurone mediating motor programme switching in the ventilatory system of the crab

Journal of Experimental Biology ◽

10.1242/jeb.154.1.517 ◽

1990 ◽

Vol 154 (1) ◽

pp. 517-535

Author(s):

R. A. DiCaprio

Keyword(s):

Central Pattern Generator ◽

Water Flow ◽

Pattern Generator ◽

Current Injection ◽

Motor Output ◽

Current Step ◽

Motor Neurones ◽

Motor Programme

The central pattern generator controlling ventilation in the crab can generate two distinct motor programmes, which determine the direction of water flow during irrigation of the gills. An interneurone has been identified that depolarizes when the ventilatory motor output switches from forward to reverse ventilation and remains depolarized for the duration of the reverse motor programme. Depolarization of this neurone by intracellular current injection causes a switch in the motor programme from forward to reverse ventilation, which persists for the duration of the current step. Hyperpolarization of this cell during reverse ventilation terminates the reverse motor programme. The possible role of this reversal switch interneurone is considered in the context of the observed changes in the activity of other ventilatory interneurones and motor neurones during reverse ventilation.

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Repetition priming of motor activity mediated by a central pattern generator: the importance of extrinsic vs. intrinsic program initiators

Journal of Neurophysiology ◽

10.1152/jn.00365.2016 ◽

2016 ◽

Vol 116 (4) ◽

pp. 1821-1830 ◽

Cited By ~ 9

Author(s):

Michael J. Siniscalchi ◽

Elizabeth C. Cropper ◽

Jian Jing ◽

Klaudiusz R. Weiss

Keyword(s):

Motor Activity ◽

Central Pattern Generator ◽

Repetition Priming ◽

Second Messengers ◽

Pattern Generator ◽

Motor Programs ◽

Chemical Coding ◽

The Core ◽

Mediating Mechanisms ◽

Intrinsic Program

Repetition priming is characterized by increased performance as a behavior is repeated. Although this phenomenon is ubiquitous, mediating mechanisms are poorly understood. We address this issue in a model system, the feeding network of Aplysia. This network generates both ingestive and egestive motor programs. Previous data suggest a chemical coding model: ingestive and egestive inputs to the feeding central pattern generator (CPG) release different modulators, which act via different second messengers to prime motor activity in different ways. The ingestive input to the CPG (neuron CBI-2) releases the peptides feeding circuit activating peptide and cerebral peptide 2, which produce an ingestive pattern of activity. The egestive input to the CPG (the esophageal nerve) releases the peptide small cardioactive peptide. This model is based on research that focused on a single aspect of motor control (radula opening). Here we ask whether repetition priming is observed if activity is triggered with a neuron within the core CPG itself and demonstrate that it is not. Moreover, previous studies demonstrated that effects of modulatory neurotransmitters that induce repetition priming persist. This suggests that it should be possible to “prime” motor programs triggered from within the CPG by first stimulating extrinsic modulatory inputs. We demonstrate that programs triggered after ingestive input activation are ingestive and programs triggered after egestive input activation are egestive. We ask where this priming occurs and demonstrate modifications within the CPG itself. This arrangement is likely to have important consequences for “task” switching, i.e., the cessation of one type of motor activity and the initiation of another.

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Na+/K+ pump interacts with the h-current to control bursting activity in central pattern generator neurons of leeches

eLife ◽

10.7554/elife.19322 ◽

2016 ◽

Vol 5 ◽

Cited By ~ 17

Author(s):

Daniel Kueh ◽

William H Barnett ◽

Gennady S Cymbalyuk ◽

Ronald L Calabrese

Keyword(s):

Central Pattern Generator ◽

Ionic Currents ◽

Pump Current ◽

Pattern Generator ◽

Motor Output ◽

Animal Cells ◽

Monensin A ◽

Bursting Activity

The dynamics of different ionic currents shape the bursting activity of neurons and networks that control motor output. Despite being ubiquitous in all animal cells, the contribution of the Na+/K+ pump current to such bursting activity has not been well studied. We used monensin, a Na+/H+ antiporter, to examine the role of the pump on the bursting activity of oscillator heart interneurons in leeches. When we stimulated the pump with monensin, the period of these neurons decreased significantly, an effect that was prevented or reversed when the h-current was blocked by Cs+. The decreased period could also occur if the pump was inhibited with strophanthidin or K+-free saline. Our monensin results were reproduced in model, which explains the pump’s contributions to bursting activity based on Na+ dynamics. Our results indicate that a dynamically oscillating pump current that interacts with the h-current can regulate the bursting activity of neurons and networks.

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