Intrinsic Neuromodulation in the Tritonia Swim CPG: Serotonin Mediates Both
Neuromodulation and Neurotransmission by the Dorsal Swim Interneurons.
Katz, Paul S. and William N. Frost.
Department of Neurobiology and Anatomy, University of Texas Medical School,
Houston, TX 77030 USA.
APStracts 2:0204N, 1995.
SUMMARY AND CONCLUSIONS
1. Neuromodulation has previously been shown to be intrinsic to the central
pattern generator (CPG) circuit that generates the escape swim of the
nudibranch mollusc, Tritonia diomedea ; the dorsal swim interneurons (DSIs)
make conventional monosynaptic connections and evoke neuromodulatory effects
within the swim motor circuit. The conventional synaptic potentials evoked by
a DSI onto cerebral neuron 2 (C2) and onto the dorsal flexion neurons (DFNs)
consist of a fast excitatory post-synaptic potential (fast EPSP) followed by a
prolonged slow EPSP. In their neuromodulatory role, the DSIs produce an
enhancement of the monosynaptic connections made by C2 onto other CPG circuit
interneurons and onto efferent flexion neurons. Previous work showed that the
DSIs are immunoreactive for serotonin (5-hydroxytryptamine, 5-HT). Here we
provide evidence that both the neurotransmission and the neuromodulation
evoked by the DSIs are produced by serotonin, and that these effects may be
pharmacologically separable.2. Previously, it was shown that bath-applied
serotonin both mimics and occludes the modulation of the C2 synapses by the
DSIs. Here we find that pressure-applied puffs of serotonin mimic both the
fast and slow EPSPs evoked by a DSI onto a DFN while high concentrations of
bath-applied serotonin occlude both of these synaptic components. 3.
Consistent with the hypothesis that serotonin mediates the actions of the
DSIs, the serotonin reuptake inhibitor imipramine prolongs the duration of the
fast DSI-DFN EPSP, increases the amplitude of the slow DSI-DFN EPSP, and
increases both the amplitude and duration of the modulation of the C2-DFN
synapse by the DSIs. 4. Two serotonergic antagonists were found which block
the actions of the DSIs. Gramine blocks the fast DSI-DFN EPSP, and has far
less of an effect on the slow EPSP and the modulation. Gramine also diminishes
the depolarization evoked by pressure-applied serotonin, showing that it is a
serotonin antagonist in this system. In contrast, methysergide greatly reduces
both the slow EPSP and the modulation evoked by the DSIs, but has mixed
effects on the fast EPSP. Methysergide also blocks the ability of exogenous
serotonin to enhance the C2-DFN EPSP demonstrating that it antagonizes the
serotonin receptors responsible for this modulation. 5. Taken together with
previous work, these results indicate that serotonin is likely to be
responsible for all three actions of the DSIs that were examined: the fast and
slow DSI-DFN EPSPs and the neuromodulation of the C2-DFN synapse. These
results also indicate that the conventional and neuromodulatory effects of the
DSIs may be pharmacologically separable. In future work it may be possible to
determine the functional role of each in the swim circuit.
Received 24 October 1995; accepted in final form 5 July 1995.
APS Manuscript Number J666-4.
Article publication pending J. Neurophysiol.
ISSN 1080-4757 Copyright 1995 The American Physiological Society.
Published in APStracts on 30 July 1995.