Involvement of opioid receptor subtypes in rat feeding behavior

Donald A. Simone; Richard J. Bodnar; Ellen J. Goldman; Gavril W. Pasternak

doi:10.1016/0024-3205(85)90206-1

Involvement of opioid receptor subtypes in rat feeding behavior

Donald A. Simone, Richard J. Bodnar, Ellen J. Goldman, Gavril W. Pasternak

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73 Scopus citations

Abstract

The short-acting opiate antagonist naloxone decreases food intake in three models of ingestive behavior: free feeding, food-deprivation induced feeding and deoxyglucose-induced feeding. Twenty-four hours after administration, the long-acting, mu₁ selective antagonist naloxonazine inhibits food intake to the same extent as naloxone in freely feeding and food-deprived rats, but not in animals treated with 2-deoxyglucose. These results indicate that 1) opiates modulate feeding through multiple opioid receptor mechanisms, one of which is the mu subtype, and 2) the feeding observed in various experimental paradigms are modulated by different receptor subtypes. Furthermore, these results illustrate the usefulness of naloxone in defining a behavior as opioid but point out its limitations in discriminating between opioid receptor subtypes.

Original language	English
Pages (from-to)	829-833
Number of pages	5
Journal	Life Sciences
Volume	36
Issue number	9
DOIs	https://doi.org/10.1016/0024-3205(85)90206-1
State	Published - 4 Mar 1985
Externally published	Yes

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@article{4dfd4d4dbd164463a86772881475c72b,

title = "Involvement of opioid receptor subtypes in rat feeding behavior",

abstract = "The short-acting opiate antagonist naloxone decreases food intake in three models of ingestive behavior: free feeding, food-deprivation induced feeding and deoxyglucose-induced feeding. Twenty-four hours after administration, the long-acting, mu1 selective antagonist naloxonazine inhibits food intake to the same extent as naloxone in freely feeding and food-deprived rats, but not in animals treated with 2-deoxyglucose. These results indicate that 1) opiates modulate feeding through multiple opioid receptor mechanisms, one of which is the mu subtype, and 2) the feeding observed in various experimental paradigms are modulated by different receptor subtypes. Furthermore, these results illustrate the usefulness of naloxone in defining a behavior as opioid but point out its limitations in discriminating between opioid receptor subtypes.",

author = "Simone, \{Donald A.\} and Bodnar, \{Richard J.\} and Goldman, \{Ellen J.\} and Pasternak, \{Gavril W.\}",

note = "Funding Information: We thank Drs. Posner, Shapiro and Hahn for their assistance with these studies and Endo Laboratories for their generous gift of naloxone. This work was supported by a PSC/CUNY grant (RIB) and grants from NIDA (DA02615) and the American Cancer Society (PDT169) (GWP).",

year = "1985",

month = mar,

day = "4",

doi = "10.1016/0024-3205(85)90206-1",

language = "English",

volume = "36",

pages = "829--833",

journal = "Life Sciences",

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publisher = "Elsevier Inc.",

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T1 - Involvement of opioid receptor subtypes in rat feeding behavior

AU - Simone, Donald A.

AU - Bodnar, Richard J.

AU - Goldman, Ellen J.

AU - Pasternak, Gavril W.

N1 - Funding Information: We thank Drs. Posner, Shapiro and Hahn for their assistance with these studies and Endo Laboratories for their generous gift of naloxone. This work was supported by a PSC/CUNY grant (RIB) and grants from NIDA (DA02615) and the American Cancer Society (PDT169) (GWP).

PY - 1985/3/4

Y1 - 1985/3/4

N2 - The short-acting opiate antagonist naloxone decreases food intake in three models of ingestive behavior: free feeding, food-deprivation induced feeding and deoxyglucose-induced feeding. Twenty-four hours after administration, the long-acting, mu1 selective antagonist naloxonazine inhibits food intake to the same extent as naloxone in freely feeding and food-deprived rats, but not in animals treated with 2-deoxyglucose. These results indicate that 1) opiates modulate feeding through multiple opioid receptor mechanisms, one of which is the mu subtype, and 2) the feeding observed in various experimental paradigms are modulated by different receptor subtypes. Furthermore, these results illustrate the usefulness of naloxone in defining a behavior as opioid but point out its limitations in discriminating between opioid receptor subtypes.

AB - The short-acting opiate antagonist naloxone decreases food intake in three models of ingestive behavior: free feeding, food-deprivation induced feeding and deoxyglucose-induced feeding. Twenty-four hours after administration, the long-acting, mu1 selective antagonist naloxonazine inhibits food intake to the same extent as naloxone in freely feeding and food-deprived rats, but not in animals treated with 2-deoxyglucose. These results indicate that 1) opiates modulate feeding through multiple opioid receptor mechanisms, one of which is the mu subtype, and 2) the feeding observed in various experimental paradigms are modulated by different receptor subtypes. Furthermore, these results illustrate the usefulness of naloxone in defining a behavior as opioid but point out its limitations in discriminating between opioid receptor subtypes.

UR - https://www.scopus.com/pages/publications/0021921080

U2 - 10.1016/0024-3205(85)90206-1

DO - 10.1016/0024-3205(85)90206-1

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AN - SCOPUS:0021921080

SN - 0024-3205

VL - 36

SP - 829

EP - 833

JO - Life Sciences

JF - Life Sciences

IS - 9

ER -

Involvement of opioid receptor subtypes in rat feeding behavior

Abstract

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