TY - JOUR
T1 - Role of spinal mu opioid receptors in the development of morphine tolerance and dependence
AU - DeLander, G. E.
AU - Portoghese, P. S.
AU - Takemori, A. E.
PY - 1984
Y1 - 1984
N2 - We previously demonstrated that the spinal cord is a primary site for the development of morphine-induced tolerance and dependence. In the current investigation, we have determined the significance of mu opioid receptors in the spinal cord in tolerance and dependence induced by systematically administered morphine. Rats surgically implanted with intrathecal (i.t.) catheters were injected i.t. with various doses of β-funaltrexamine (β-FNA), a specific irreversible mu opioid receptor antagonist. β-FNA (i.t.) dose-dependently antagonized morphine-induced analgesia (i.p.) with approximately one-half the potency of β-chlornaltrexamine, a nonselective irreversible opioid receptor antagonist. Rats injected with saline i.t. 24 h before implanting morphine pellets developed a significant degree of tolerance and dependence 72 h after morphine administration. Tolerance did not develop in similarly treated animals that received i.t. injections of 4.5 nmol β-FNA. Signs of naloxone-precipitated withdrawal were also significantly antagonized in all instances, except weight loss, in animals pretreated with β-FNA (i.t.). We conclude that i.t. injections of β-FNA significantly antagonized in all instances, except weight loss, in animals pretreated with β-FNA (i.t.). We conclude that i.t. injections of β-FNA significantly antagonized the development of tolerance and dependence induced by systemically administered morphine. Therefore, our results indicate that mu opioid receptors within the spinal cord, and probably throughout the central nervous system, play a primary role in morphine-induced tolerance and dependence.
AB - We previously demonstrated that the spinal cord is a primary site for the development of morphine-induced tolerance and dependence. In the current investigation, we have determined the significance of mu opioid receptors in the spinal cord in tolerance and dependence induced by systematically administered morphine. Rats surgically implanted with intrathecal (i.t.) catheters were injected i.t. with various doses of β-funaltrexamine (β-FNA), a specific irreversible mu opioid receptor antagonist. β-FNA (i.t.) dose-dependently antagonized morphine-induced analgesia (i.p.) with approximately one-half the potency of β-chlornaltrexamine, a nonselective irreversible opioid receptor antagonist. Rats injected with saline i.t. 24 h before implanting morphine pellets developed a significant degree of tolerance and dependence 72 h after morphine administration. Tolerance did not develop in similarly treated animals that received i.t. injections of 4.5 nmol β-FNA. Signs of naloxone-precipitated withdrawal were also significantly antagonized in all instances, except weight loss, in animals pretreated with β-FNA (i.t.). We conclude that i.t. injections of β-FNA significantly antagonized in all instances, except weight loss, in animals pretreated with β-FNA (i.t.). We conclude that i.t. injections of β-FNA significantly antagonized the development of tolerance and dependence induced by systemically administered morphine. Therefore, our results indicate that mu opioid receptors within the spinal cord, and probably throughout the central nervous system, play a primary role in morphine-induced tolerance and dependence.
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M3 - Article
C2 - 6092607
AN - SCOPUS:0021162578
SN - 0022-3565
VL - 231
SP - 91
EP - 96
JO - Journal of Pharmacology and Experimental Therapeutics
JF - Journal of Pharmacology and Experimental Therapeutics
IS - 1
ER -