Literature DB >> 20026311

Genetic variance contributes to dopamine and opioid receptor antagonist-induced inhibition of intralipid (fat) intake in inbred and outbred mouse strains.

Cheryl T Dym1, Veronica S Bae, Tamar Kraft, Yakov Yakubov, Amanda Winn, Anthony Sclafani, Richard J Bodnar.   

Abstract

Preference for and intake of solid and emulsified fat (intralipid) solutions vary across different mouse strains. Fat intake in rodents is inhibited by dopamine and opioid receptor antagonists, but any variation in these responses as a function of genetic background is unknown. Therefore, the present study compared the ability of dopamine D1-like (SCH23390) and general opioid (naltrexone) receptor antagonism to alter intake of fat emulsions (intralipid) in mice. Two-hour intakes of 5% intralipid were measured (5-120 min) in seven inbred (BALB/c, C57BL/6, C57BL/10, DBA/2, SJL, SWR, 129P3) and one outbred (CD-1) mouse strains following treatment with vehicle, SCH23390 (50-1600 nmol/kg, ip) and naltrexone (0.001-5 mg/kg, sc). SCH23390 significantly, dose-dependently and differentially reduced intralipid intake at all five (DBA/2, SWR, CD-1), four (SJL, C57BL/6), three (129P3) and one (C57BL/10) of the doses tested, but failed to affect intralipid intake in BALB/c mice. Naltrexone significantly, dose-dependently and differentially reduced intralipid intake at all four (DBA/2), three (SWR, SJL), two (CD-1, C57BL/10) and one (C57BL/6, 129P3) of the doses tested, and also failed to affect intralipid intake in BALB/cJ mice. SCH23390 and naltrexone were respectively 13.3-fold and 9.3-fold more potent in inhibiting intralipid intake in the most sensitive (DBA/2) relative to the least sensitive (BALB/c) mouse strains. A strong positive relationship (r=0.91) was observed for the abilities of SCH23390 and naltrexone to inhibit intralipid intake across strains. These findings indicate that dopaminergic and opioid signaling mechanisms differentially control intralipid intake across different mouse strains, suggesting important genetic and pharmacological interactions in the short-term control of rewarding and post-ingestive consequences of fat intake. (c) 2009 Elsevier B.V. All rights reserved.

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Year:  2009        PMID: 20026311      PMCID: PMC2822056          DOI: 10.1016/j.brainres.2009.12.021

Source DB:  PubMed          Journal:  Brain Res        ISSN: 0006-8993            Impact factor:   3.252


  48 in total

Review 1.  Opioids for hedonic experience and dopamine to get ready for it.

Authors:  M Flavia Barbano; Martine Cador
Journal:  Psychopharmacology (Berl)       Date:  2006-10-10       Impact factor: 4.530

2.  Quantitative trait Loci for regional adiposity in mouse lines divergently selected for food intake.

Authors:  Kellie A Rance; Catherine Hambly; Gillian Dalgleish; Jean-Michel Fustin; Lutz Bünger; John R Speakman
Journal:  Obesity (Silver Spring)       Date:  2007-12       Impact factor: 5.002

Review 3.  'Liking' and 'wanting' food rewards: brain substrates and roles in eating disorders.

Authors:  Kent C Berridge
Journal:  Physiol Behav       Date:  2009-03-29

4.  Macronutrient diet selection in thirteen mouse strains.

Authors:  B K Smith; P K Andrews; D B West
Journal:  Am J Physiol Regul Integr Comp Physiol       Date:  2000-04       Impact factor: 3.619

5.  Fat and sugar flavor preference and acceptance in C57BL/6J and 129 mice: experience attenuates strain differences.

Authors:  Anthony Sclafani
Journal:  Physiol Behav       Date:  2007-01-08

6.  In vivo regulation of mu-opioid receptor density and gene expression in CXBK and outbred Swiss Webster mice.

Authors:  A Duttaroy; B C Yoburn
Journal:  Synapse       Date:  2000-08       Impact factor: 2.562

7.  Baclofen, raclopride, and naltrexone differentially reduce solid fat emulsion intake under limited access conditions.

Authors:  R E Rao; F H E Wojnicki; J Coupland; S Ghosh; R L W Corwin
Journal:  Pharmacol Biochem Behav       Date:  2008-02-15       Impact factor: 3.533

8.  Contribution of orosensory stimulation to strain differences in oil intake by mice.

Authors:  John I Glendinning; Natalie Feld; Leora Goodman; Rouane Bayor
Journal:  Physiol Behav       Date:  2008-07-17

9.  Activation of mesolimbic dopamine neurons during novel and daily limited access to palatable food is blocked by the opioid antagonist LY255582.

Authors:  Allison E Sahr; Dana K Sindelar; Jesline T Alexander-Chacko; Brian J Eastwood; Charles H Mitch; Michael A Statnick
Journal:  Am J Physiol Regul Integr Comp Physiol       Date:  2008-06-04       Impact factor: 3.619

10.  Genetic variance contributes to dopamine receptor antagonist-induced inhibition of sucrose intake in inbred and outbred mouse strains.

Authors:  Cheryl T Dym; Alexander Pinhas; Magdalena Robak; Anthony Sclafani; Richard J Bodnar
Journal:  Brain Res       Date:  2008-12-25       Impact factor: 3.252
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  3 in total

1.  Roles of dopamine D1 and D2 receptors in the acquisition and expression of fat-conditioned flavor preferences in rats.

Authors:  J A D Dela Cruz; D Icaza-Cukali; H Tayabali; C Sampson; V Galanopoulos; D Bamshad; K Touzani; A Sclafani; R J Bodnar
Journal:  Neurobiol Learn Mem       Date:  2012-02-25       Impact factor: 2.877

2.  Double-dissociation of D1 and opioid receptor antagonism effects on the acquisition of sucrose-conditioned flavor preferences in BALB/c and SWR mice.

Authors:  Cheryl T Dym; Tamar T Kraft; Veronica S Bae; Yakov Yakubov; Khalid Touzani; Anthony Sclafani; Richard J Bodnar
Journal:  Pharmacol Biochem Behav       Date:  2012-08-07       Impact factor: 3.533

3.  Critical role of NMDA but not opioid receptors in the acquisition of fat-conditioned flavor preferences in rats.

Authors:  J A D Dela Cruz; V S Bae; D Icaza-Cukali; C Sampson; D Bamshad; A Samra; S Singh; N Khalifa; K Touzani; A Sclafani; R J Bodnar
Journal:  Neurobiol Learn Mem       Date:  2012-10-24       Impact factor: 2.877
  3 in total

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