Distinct changes in the behavioural effects of morphine and naloxone in CCK2 receptor-deficient mice

Kertu Rünkorg; Alar Veraksitš; Kaido Kurrikoff; Hendrik Luuk; Sirli Raud; Urho Abramov; Toshimitsu Matsui; Michel Bourin; Sulev Kõks; Eero Vasar

doi:10.1016/S0166-4328(03)00070-6

Distinct changes in the behavioural effects of morphine and naloxone in CCK₂ receptor-deficient mice

Kertu Rünkorg, Alar Veraksitš, Kaido Kurrikoff, Hendrik Luuk, Sirli Raud, Urho Abramov, Toshimitsu Matsui, Michel Bourin, Sulev Kõks, Eero Vasar

Research output: Contribution to journal › Article › peer-review

14 Scopus citations

Abstract

The effects of morphine, μ-opioid receptor agonist, and naloxone, a non-selective opioid receptor antagonist, in the locomotor activity and place conditioning tests were studied in the CCK₂ receptor-deficient male mice. The exposure of mice to the motility boxes for 3 consecutive days induced a significant inhibition of locomotor activity in the wild-type (+/+) mice compared to homozygous (-/-) animals. The administration of naloxone (10mg/kg i.p.) to animals, adapted to the motility boxes, induced a significant reduction of locomotor activity in the homozygous (-/-), but not in the wild-type (+/+) mice. Treatment of habituated mice with morphine (10mg/kg i.p.) caused a stronger increase of locomotor activity in the wild-type (+/+) mice compared to the homozygous (-/-) littermates. In the place preference test the pairing of the preferred side with naloxone (1 and 10mg/kg i.p.) induced a dose-dependent place aversion in the wild-type (+/+) mice. The treatment with naloxone was less effective in the homozygous (-/-) mice, because the high dose of naloxone (10mg/kg) tended to shift the preference. The pairing of morphine (3mg/kg i.p.) injections with the non-preferred side induced a significant place preference both in the wild-type (+/+) and homozygous (-/-) mice. The increased density of opioid receptors was established in the striatum of homozygous (-/-) mice, but not in the other forebrain structures. In conclusion, the targeted invalidation of CCK₂ receptors induces a dissociation of behavioural effects of morphine and naloxone. Morphine-induced place preference remained unchanged, whereas hyper-locomotion was less pronounced in the mutant mice compared to the wild-type (+/+) littermates. By contrast, naloxone-induced place aversion was weaker, but naloxone caused a stronger inhibition of locomotor activity in the homozygous (-/-) mice than in the wild-type (+/+) animals. These behavioural alterations can be explained in the light of data that the targeted mutation of CCK₂ receptors induces distinct changes in the properties of opioid receptors in various brain structures.

Original language	English
Pages (from-to)	125-135
Number of pages	11
Journal	Behavioural Brain Research
Volume	144
Issue number	1-2
DOIs	https://doi.org/10.1016/S0166-4328(03)00070-6
State	Published - 15 Sep 2003
Externally published	Yes

Keywords

CCK receptors
Homozygous
Locomotor activity
Morphine
Mouse
Naloxone
Opioid receptors
Place conditioning
Targeted mutagenesis
Wild-type

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10.1016/S0166-4328(03)00070-6

Cite this

@article{2fc234c5e0d445aaa64bc4b9b24a9808,

title = "Distinct changes in the behavioural effects of morphine and naloxone in CCK2 receptor-deficient mice",

abstract = "The effects of morphine, μ-opioid receptor agonist, and naloxone, a non-selective opioid receptor antagonist, in the locomotor activity and place conditioning tests were studied in the CCK2 receptor-deficient male mice. The exposure of mice to the motility boxes for 3 consecutive days induced a significant inhibition of locomotor activity in the wild-type (+/+) mice compared to homozygous (-/-) animals. The administration of naloxone (10mg/kg i.p.) to animals, adapted to the motility boxes, induced a significant reduction of locomotor activity in the homozygous (-/-), but not in the wild-type (+/+) mice. Treatment of habituated mice with morphine (10mg/kg i.p.) caused a stronger increase of locomotor activity in the wild-type (+/+) mice compared to the homozygous (-/-) littermates. In the place preference test the pairing of the preferred side with naloxone (1 and 10mg/kg i.p.) induced a dose-dependent place aversion in the wild-type (+/+) mice. The treatment with naloxone was less effective in the homozygous (-/-) mice, because the high dose of naloxone (10mg/kg) tended to shift the preference. The pairing of morphine (3mg/kg i.p.) injections with the non-preferred side induced a significant place preference both in the wild-type (+/+) and homozygous (-/-) mice. The increased density of opioid receptors was established in the striatum of homozygous (-/-) mice, but not in the other forebrain structures. In conclusion, the targeted invalidation of CCK2 receptors induces a dissociation of behavioural effects of morphine and naloxone. Morphine-induced place preference remained unchanged, whereas hyper-locomotion was less pronounced in the mutant mice compared to the wild-type (+/+) littermates. By contrast, naloxone-induced place aversion was weaker, but naloxone caused a stronger inhibition of locomotor activity in the homozygous (-/-) mice than in the wild-type (+/+) animals. These behavioural alterations can be explained in the light of data that the targeted mutation of CCK2 receptors induces distinct changes in the properties of opioid receptors in various brain structures.",

keywords = "CCK receptors, Homozygous, Locomotor activity, Morphine, Mouse, Naloxone, Opioid receptors, Place conditioning, Targeted mutagenesis, Wild-type",

author = "Kertu R{\"u}nkorg and Alar Veraksit{\v s} and Kaido Kurrikoff and Hendrik Luuk and Sirli Raud and Urho Abramov and Toshimitsu Matsui and Michel Bourin and Sulev K{\~o}ks and Eero Vasar",

note = "Funding Information: This study was supported by the James S. McDonnell Foundation (USA) and by grant no. 3922 of the Estonian Science Foundation.",

year = "2003",

month = sep,

day = "15",

doi = "10.1016/S0166-4328(03)00070-6",

language = "English",

volume = "144",

pages = "125--135",

journal = "Behavioural Brain Research",

issn = "0166-4328",

publisher = "Elsevier B.V.",

number = "1-2",

}

TY - JOUR

T1 - Distinct changes in the behavioural effects of morphine and naloxone in CCK2 receptor-deficient mice

AU - Rünkorg, Kertu

AU - Veraksitš, Alar

AU - Kurrikoff, Kaido

AU - Luuk, Hendrik

AU - Raud, Sirli

AU - Abramov, Urho

AU - Matsui, Toshimitsu

AU - Bourin, Michel

AU - Kõks, Sulev

AU - Vasar, Eero

N1 - Funding Information: This study was supported by the James S. McDonnell Foundation (USA) and by grant no. 3922 of the Estonian Science Foundation.

PY - 2003/9/15

Y1 - 2003/9/15

N2 - The effects of morphine, μ-opioid receptor agonist, and naloxone, a non-selective opioid receptor antagonist, in the locomotor activity and place conditioning tests were studied in the CCK2 receptor-deficient male mice. The exposure of mice to the motility boxes for 3 consecutive days induced a significant inhibition of locomotor activity in the wild-type (+/+) mice compared to homozygous (-/-) animals. The administration of naloxone (10mg/kg i.p.) to animals, adapted to the motility boxes, induced a significant reduction of locomotor activity in the homozygous (-/-), but not in the wild-type (+/+) mice. Treatment of habituated mice with morphine (10mg/kg i.p.) caused a stronger increase of locomotor activity in the wild-type (+/+) mice compared to the homozygous (-/-) littermates. In the place preference test the pairing of the preferred side with naloxone (1 and 10mg/kg i.p.) induced a dose-dependent place aversion in the wild-type (+/+) mice. The treatment with naloxone was less effective in the homozygous (-/-) mice, because the high dose of naloxone (10mg/kg) tended to shift the preference. The pairing of morphine (3mg/kg i.p.) injections with the non-preferred side induced a significant place preference both in the wild-type (+/+) and homozygous (-/-) mice. The increased density of opioid receptors was established in the striatum of homozygous (-/-) mice, but not in the other forebrain structures. In conclusion, the targeted invalidation of CCK2 receptors induces a dissociation of behavioural effects of morphine and naloxone. Morphine-induced place preference remained unchanged, whereas hyper-locomotion was less pronounced in the mutant mice compared to the wild-type (+/+) littermates. By contrast, naloxone-induced place aversion was weaker, but naloxone caused a stronger inhibition of locomotor activity in the homozygous (-/-) mice than in the wild-type (+/+) animals. These behavioural alterations can be explained in the light of data that the targeted mutation of CCK2 receptors induces distinct changes in the properties of opioid receptors in various brain structures.

AB - The effects of morphine, μ-opioid receptor agonist, and naloxone, a non-selective opioid receptor antagonist, in the locomotor activity and place conditioning tests were studied in the CCK2 receptor-deficient male mice. The exposure of mice to the motility boxes for 3 consecutive days induced a significant inhibition of locomotor activity in the wild-type (+/+) mice compared to homozygous (-/-) animals. The administration of naloxone (10mg/kg i.p.) to animals, adapted to the motility boxes, induced a significant reduction of locomotor activity in the homozygous (-/-), but not in the wild-type (+/+) mice. Treatment of habituated mice with morphine (10mg/kg i.p.) caused a stronger increase of locomotor activity in the wild-type (+/+) mice compared to the homozygous (-/-) littermates. In the place preference test the pairing of the preferred side with naloxone (1 and 10mg/kg i.p.) induced a dose-dependent place aversion in the wild-type (+/+) mice. The treatment with naloxone was less effective in the homozygous (-/-) mice, because the high dose of naloxone (10mg/kg) tended to shift the preference. The pairing of morphine (3mg/kg i.p.) injections with the non-preferred side induced a significant place preference both in the wild-type (+/+) and homozygous (-/-) mice. The increased density of opioid receptors was established in the striatum of homozygous (-/-) mice, but not in the other forebrain structures. In conclusion, the targeted invalidation of CCK2 receptors induces a dissociation of behavioural effects of morphine and naloxone. Morphine-induced place preference remained unchanged, whereas hyper-locomotion was less pronounced in the mutant mice compared to the wild-type (+/+) littermates. By contrast, naloxone-induced place aversion was weaker, but naloxone caused a stronger inhibition of locomotor activity in the homozygous (-/-) mice than in the wild-type (+/+) animals. These behavioural alterations can be explained in the light of data that the targeted mutation of CCK2 receptors induces distinct changes in the properties of opioid receptors in various brain structures.

KW - CCK receptors

KW - Homozygous

KW - Locomotor activity

KW - Morphine

KW - Mouse

KW - Naloxone

KW - Opioid receptors

KW - Place conditioning

KW - Targeted mutagenesis

KW - Wild-type

UR - https://www.scopus.com/pages/publications/17744410286

U2 - 10.1016/S0166-4328(03)00070-6

DO - 10.1016/S0166-4328(03)00070-6

M3 - Article

C2 - 12946603

AN - SCOPUS:17744410286

SN - 0166-4328

VL - 144

SP - 125

EP - 135

JO - Behavioural Brain Research

JF - Behavioural Brain Research

IS - 1-2