Li X, Bynum T, Hayashida K, Eisenach JC (2005) Role of IB4-containing afferents in the effect of IT clonidine. Neuroscience 2005 Abstracts 171.22. Society for Neuroscience, Washington, DC.
Summary: Alpha2 adrenoceptors diminish pain transmission in animals with normal condition. Our previous data demonstrated clonidine, an Alpha2 adrenoceptor agonist, inhibited calcium influx after an electrical stimulation in the acutely cultured DRG cells from normal animal, 80% of which are Isolectin B4 (IB4) positive. Therefore we assume intrathecal clonidine produces antinociception primarily by actions on IB4-expressing afferents, and clonidine effect will be decreased with the loss of IB4 containing afferents. In the current report, normal rats received an intra-nerve injection of 2 μg of saporin conjugated IB4 (Sap-IB4), a targeted cytotoxin to IB4-expressing neurons, or a 6 μg of saporin as the control in the rat sciatic nerve. Effects of 30 μg intrathecal clonidine were observed for antinociception to thermal and mechanical stimuli in both ipsi- and contra- lateral side to the injection weekly, before and after Sap-IB4 injection for three weeks. Immunocitochemistry study demonstrated that three weeks of Sap-IB4 treatment dramatically decreased IB4 expression in DRG cells or spinal afferent fibers in the ipslateral side. The basal thermal withdrawal latency and mechanical withdrawal threshold were slightly increased by Sap-IB4 in the ipsilateral side one week after injection, which were returned to normal three weeks later. Additionally, the effeccy of 30 μg clonidine for antinociception to thermal and mechanical stimuli was significantly decreased at the end of treatment. These observations suggested IB4 containing afferents may play a very important role in intrathecal clonidine mediated antinociception.
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