The distribution of spinal primary afferent terminals labeled
transganglionically with the choleratoxin B subunit (CTB) or
its conjugates changes profoundly after perineural treatment
with capsaicin. Injection of CTB conjugated with horseradish
peroxidase (HRP) into an intact nerve labels somatotopically
related areas in the ipsilateral dorsal horn with the
exceptions of the marginal zone and the substantia
gelatinosa, whereas injection of this tracer into a
capsaicin-pretreated nerve also results in massive labeling
of these most superficial layers of the dorsal horn. The
present study was initiated to clarify the role of C-fiber
primary afferent neurons in this phenomenon. In L5 dorsal
root ganglia, analysis of the size frequency distribution of
neurons labeled after injection of CTB-HRP into the
ipsilateral sciatic nerve treated previously with capsaicin
or resiniferatoxin revealed a significant increase in the
proportion of small neurons. In the spinal dorsal horn,
capsaicin or resiniferatoxin pretreatment resulted in intense
CTB-HRP labeling of the marginal zone and the substantia
gelatinosa. Electron microscopic histochemistry disclosed a
dramatic, approximately 10-fold increase in the proportion of
CTB-HRP-labeled unmyelinated dorsal root axons following
perineural capsaicin or resiniferatoxin. The present results
indicate that CTB-HRP labeling of C-fiber dorsal root
ganglion neurons and their central terminals after perineural
treatment with vanilloid compounds may be explained by their
phenotypic switch rather than a sprouting response of thick
myelinated spinal afferents which, in an intact nerve, can be
labeled selectively with CTB-HRP. The findings also suggest a
role for GM1 ganglioside in the modulation of nociceptor
function and pain
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