4.4 Article

Age-dependent effects of the cannabinoid CB1 antagonist SR141716A on food intake, body weight change, and pruritus in rats

期刊

PSYCHOPHARMACOLOGY
卷 206, 期 1, 页码 155-165

出版社

SPRINGER
DOI: 10.1007/s00213-009-1592-6

关键词

Cannabinoid; CB1; Age; Development; Food intake; Body weight; Scratching; Itch; SR141716A; Ketanserin

资金

  1. NIH [RO1-DA014673, F32DA01931]
  2. Health Research Formula Fund PA
  3. NATIONAL INSTITUTE ON DRUG ABUSE [R01DA014673] Funding Source: NIH RePORTER

向作者/读者索取更多资源

The cannabinoid CB1 selective antagonist SR141716A (Rimonabant) has been shown to decrease body weight in laboratory animals and humans. Furthermore, SR141716A can elicit scratching behavior in rodents, a behavior that has been hypothesized to contribute to SR141716A-induced decrease in food intake. Although childhood obesity is a rising health issue, it is unknown whether SR141716A is equipotent at modulating food intake and other CB1-mediated behaviors in younger subjects. To determine whether CB1 receptor blockade is equipotent at modulating food and water intake, body weight, and scratching behavior, the effect of a range of SR141716A doses on these behaviors in food-restricted postnatal day (P) 18, 28, and 60 male rats was investigated. Brain concentrations of SR141716A were determined in each age group. SR141716A dose- and age-dependently suppressed food and water intake and body weight gain and elicited head scratching, with the most potent effects observed in P18 and P28 rats. Brain concentrations of SR141716A were significantly elevated in P18 rats relative to P28 and P60 rats. SR141716A-elicited head scratching was attenuated by the 5-HT2A/2C antagonist ketanserin. SR141716A is more potent at modulating food intake and head scratching in very young animals; these differences can be attributed to an increase in brain penetration of SR141716A for P18 but not for P28 and P60 rats. In addition, SR141716-elicited head scratching is modulated by 5HT receptor antagonism and is not a contributing factor to SR141716A's anorectic effects.

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