A leu-enkephalin depresses transmission from muscle and skin non-nociceptors to first-order feline spinal neurones

The effects of an opioid (D-Ser-Leu-enkephalin-Thr; DSLET) were tested on synaptic actions of non-nociceptive afferents: group I and II muscle afferents and low-threshold skin afferents. They were tested on population EPSPs (field potentials) evoked in the dorsal horn and the intermediate zone of mi...

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Bibliographic Details
Published in:The Journal of physiology 1998-07, Vol.510 (2), p.513-525
Main Authors: Jankowska, E., Schomburg, E. D.
Format: Article
Language:English
Subjects:
Afferent
Analgesics
Analgesics - pharmacology
analogs & derivatives
Animals
Cats
Chemical
cytology
Depression
Depression, Chemical
drug effects
Electric Stimulation
Electrophysiology
Enkephalin
Enkephalin, Leucine - analogs & derivatives
Enkephalin, Leucine - pharmacology
Fysiologi
innervation
Interneurons
Interneurons - drug effects
Interneurons - physiology
Leucine
Membrane Potentials
Membrane Potentials - physiology
Muscle
Muscle, Skeletal - drug effects
Muscle, Skeletal - innervation
Naloxone
Naloxone - pharmacology
Narcotic Antagonists
Narcotic Antagonists - pharmacology
Neurons
Neurons, Afferent - drug effects
Neurons, Afferent - physiology
Nociceptors
Nociceptors - drug effects
Original
Patch-Clamp Techniques
pharmacology
Physiology
Skeletal
Spinal Cord
Spinal Cord - cytology
Spinal Cord - drug effects
Synaptic Transmission
Synaptic Transmission - drug effects
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Summary:The effects of an opioid (D-Ser-Leu-enkephalin-Thr; DSLET) were tested on synaptic actions of non-nociceptive afferents: group I and II muscle afferents and low-threshold skin afferents. They were tested on population EPSPs (field potentials) evoked in the dorsal horn and the intermediate zone of mid-lumbar segments, and on monosynaptically evoked responses of single interneurones at the same locations. DSLET was applied locally (ionophoretically) at locations at which the field potentials were maximal and close to the selected neurones. DSLET potently depressed transmission from group II muscle afferents and from low-threshold skin afferents. Transmission to neurones located in the dorsal horn or in the intermediate zone was depressed to a similar extent. The depression was readily antagonized by naloxone. Transmission from group Ia or Ib muscle afferents to neurones located in the intermediate zone was not affected, or was facilitated by DSLET. The results show that DSLET has similar depressive actions on spinal neurones to monoamines, but its actions are more widespread. Like monoamines it affects transmission from nociceptors and group II muscle afferents, but in addition it gates transmission from low-threshold cutaneous afferents. Furthermore its effects do not appear to be restricted to interneurones at particular locations since it depressed responses of dorsal horn interneurones (gated by serotonin) as well as intermediate zone interneurones (gated by noradrenaline).
ISSN:0022-3751
1469-7793
DOI:10.1111/j.1469-7793.1998.513bk.x