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Effects of acute agonist treatment on subcellular distribution of κ opioid receptor in rat spinal cord

✍ Scribed by Yulin Wang; Wei Xu; Peng Huang; Charles Chavkin; Elisabeth J. Van Bockstaele; Lee-Yuan Liu-Chen


Publisher
John Wiley and Sons
Year
2009
Tongue
English
Weight
668 KB
Volume
87
Category
Article
ISSN
0360-4012

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✦ Synopsis


Abstract

We investigated whether acute treatment with agonists affected the subcellular distribution of κ opioid receptor (KOPR) in the dorsal horn of the rat lumbar spinal cord by using immunoelectron microscopy. Rats were injected intrathecally (i.t.) with U50,488H (100 nmole), dynorphin A(1–17) (15 nmole), or vehicle. The doses chosen have been shown to induce antinociception. Rats were perfused transcardially 30 min later, and lumbar spinal cords were removed and processed for electron microscopic analysis. KOPR was stained with KT‐2, a specific polyclonal antibody against the rat/mouse KOPR(371–380) peptide, followed by gold‐labeled secondary antibody and silver intensification. The silver grains were present in axons, terminals, dendrites, and somata, and the association with plasma membranes was quantified in dendrites, because KOPR immunoreactivity was most frequently observed in these profiles. In vehicle‐treated rats, ∼27% of KOPR immunoreactivity was associated with plasma membranes. U50,488H, i.t., did not cause a significant change in the percentage of KOPR present on plasma membranes, whereas dynorphin A, i.t., significantly decreased cell surface KOPR to ∼19%. In summary, these data indicate that U50,488H and dynorphin A differentially regulate the subcellular distribution of endogenous KOPR. © 2009 Wiley‐Liss, Inc.


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