Abstract

Many studies have shown that brain stem regions such as the nucleus raphe magnus and periaqueductal gray can control the inflow of sensory information to the spinal cord. It has recently been found that selective analgesia may result from stimulating these brain centers and that morphine analgesia may be mediated by the same mechanisms. Pathways implicated in this """"""""descending control"""""""" extend from enkephalin-containing neurons in the mesencephalic central gray which project to serotonergic neurons in the nucleus raphe magnus, which in turn project to the spinal cord marginal zone (MZ) (lamina I), substantia gelatinosa (SG) (lamina II), and nucleus proprius (lamina V). However, many questions still remain unanswered, including: 1) the types of neurotransmitters involved at the central nervous system (CNS) level and 2) the morphological and physiological substrates by which these descending pathways produce their effects.
The aim of this research proposal is to explore these issues by studying: 1) the morphology of MZ and SG neurons and identified projection neurons that are modulated by focal brainstem stimulation; 2) the synaptic conductance changes evoked by focal brainstem stimulation; 3) the types of neurotransmitters released by brainstem neurons. Conventional single unit recordings, both extra and intracellular, will be used to physiologically identify interneurons and projection neurons. Iontophoresis of intracellular labels will be used to identify the recorded neurons for examination at light and EM levels. Microiontophoresis and pressure injection will be used to locally apply specific antagonists to putative neurotransmitters, and finally, immunocytochemistry combined with anatomical tracers will be used to establish the relationship between descending connections and the various putative neurotransmitters found in the spinal SG. The results of these studies should lead to a basic understanding of the mechanisms whereby the CNS can modulate somatosensory information at the spinal level.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS016433-07
Application #
3396871
Study Section
Communication Sciences and Disorders (CMS)
Project Start
1980-07-01
Project End
1989-06-30
Budget Start
1986-07-01
Budget End
1987-06-30
Support Year
7
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
Schools of Medicine
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Eckert 3rd, William A; McNaughton, Kirk K; Light, Alan R (2003) Morphology and axonal arborization of rat spinal inner lamina II neurons hyperpolarized by mu-opioid-selective agonists. J Comp Neurol 458:240-56
Chattipakorn, Siriporn Chattipakorn; Sigurdsson, Asgeir; Light, Alan R et al. (2002) Trigeminal c-Fos expression and behavioral responses to pulpal inflammation in ferrets. Pain 99:61-9
Eckert 3rd, W A; Willcockson, H H; Light, A R (2001) Interference of biocytin with opioid-evoked hyperpolarization and membrane properties of rat spinal substantia gelatinosa neurons. Neurosci Lett 297:117-20
Fu, K Y; Light, A R; Maixner, W (2000) Relationship between nociceptor activity, peripheral edema, spinal microglial activation and long-term hyperalgesia induced by formalin. Neuroscience 101:1127-35
Light, A R; Willcockson, H H (1999) Spinal laminae I-II neurons in rat recorded in vivo in whole cell, tight seal configuration: properties and opioid responses. J Neurophysiol 82:3316-26
Vierck Jr, C J; Light, A R (1999) Effects of combined hemotoxic and anterolateral spinal lesions on nociceptive sensitivity. Pain 83:447-57
Chattipakorn, S C; Light, A R; Willcockson, H H et al. (1999) The effect of fentanyl on c-fos expression in the trigeminal brainstem complex produced by pulpal heat stimulation in the ferret. Pain 82:207-15
Madison, R D; Robinson, G A (1998) lambda RNA internal standards quantify sensitivity and amplification efficiency of mammalian gene expression profiling. Biotechniques 25:504-8, 510, 512, passim
Schneider, S P; Eckert 3rd, W A; Light, A R (1998) Opioid-activated postsynaptic, inward rectifying potassium currents in whole cell recordings in substantia gelatinosa neurons. J Neurophysiol 80:2954-62
Robinson, G A (1996) Changes in the expression of transcription factors ATF-2 and Fra-2 after axotomy and during regeneration in rat retinal ganglion cells. Brain Res Mol Brain Res 41:57-64

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