beta -Endorphin-Induced Feeding: Pharmacological Characterization Using Selective Opioid Antagonists and Antisense Probes in Rats

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Vol. 297, Issue 2, 590-596, May 2001

$beta$ -Endorphin-Induced Feeding: Pharmacological Characterization Using Selective Opioid Antagonists and Antisense Probes in Rats

Robert M. Silva, Maria M. Hadjimarkou, Grace C. Rossi , Gavril W. Pasternak and Richard J. Bodnar

Department of Psychology and Neuropsychology Doctoral Sub-Program, Queens College, City University of New York, Flushing, New York (R.M.S., M.M.H., R.J.B.); Department of Psychology, CW Post College, Long Island University, Brookville, New York (G.C.R.); and The George C. Cotzias Laboratory of Neuro-Oncology, Memorial Sloan-Kettering Cancer Center, New York, New York (G.C.R., G.W.P.)

Ventricular administration of the opioid $beta$ END induces feeding in rats. Since its pharmacological characterization has notbeen fully identified, the present study examined whether equimolardoses of general and selective opioid antagonists as well as ASODN opioid probes altered spontaneous daytime feeding over a 4-htime course elicited by $beta$ END. $beta$ END-induced feeding was significantlyreduced by moderate (20-40-nmol, i.c.v.) doses of general (naltrexone)opioid antagonists, and lower (0.5-40-nmol) doses of selectiveµ ( $beta$ -funaltrexamine)-antagonists. Correspondingly, AS ODN probesdirected against either exons 1, 3, or 4, but not exon 2, of theµ-opioid receptor clone reduced $beta$ END-induced feeding; a missenseODN control probe was ineffective. The $delta$ -antagonist Nti (20-40nmol) reduced $beta$ END-induced feeding to a lesser degree, and ASODN probes targeting exon 1, but not 2 or 3, of the $delta$ -opioid receptorclone significantly reduced $beta$ END-induced feeding. Although theselective $kappa$ ₁-receptor antagonist NBNI (20-40 nmol) significantlyreduced $beta$ END-induced feeding, this response was not altered byAS ODN probes directed against either exons 1, 2, or 3 of eitherthe KOR-1 clone or the $kappa$ ₃-like opioid receptor clone. These convergingantagonist and AS ODN data firmly implicate the µ-opioid receptorin the mediation of $beta$ END-induced feeding. The relative lack ofconvergence between the lesser effectiveness of Nti and NBNI inreducing $beta$ END-induced feeding, and the lack of effectiveness oftheir corresponding AS ODN probes suggest that $delta$ - and $kappa$ -receptorsplay a minimal role in the mediation of thisresponse.

0022-3565/01/2972-0590$03.00/0
THE JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS
Copyright © 2001 by The American Society for Pharmacology and Experimental Therapeutics

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