2008
DOI: 10.1038/oby.2008.223
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Effects of a Novel Y5 Antagonist in Obese Mice: Combination With Food Restriction or Sibutramine

Abstract: Objective:To further address the function of the Y5 receptor in energy homeostasis, we investigated the effects of a novel spironolactone Y5 antagonist in diet-induced obese (DIO) mice. Methods and Procedures: Male C57BL/6 or Npy5r −/− mice were adapted to high-fat (HF) diet for 6-10 months and were submitted to three experimental treatments. First, the Y5 antagonist at a dose of 10 or 30 mg/kg was administered for 1 month to DIO C57BL/6 or Npy5r −/− mice. Second, the Y5 antagonist at 30 mg/kg was administered… Show more

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Cited by 26 publications
(19 citation statements)
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“…In order to validate the HE-fed DIO rat as a useful animal model of obesity, we examined the body weight lowering effect of the well-known anti-obesity agent sibutramine and the once-daily human GLP-1 analog liraglutide. The findings of a transient (7 day) effect on food intake and a approximate 10% weight loss following 28 days of treatment with sibutramine is in agreement with data reported previously from other rodent DIO models (Boozer et al 2001, Bush et al 2006, Mashiko et al 2008 as well as in a previous study in the DIO rat (Levin & Dunn-Meynell 2000). The body weight loss of w10% seen in rodent models of obesity translates into an approximate 5% sustained weight loss in humans (Bray et al 1999, James et al 2000.…”
Section: Discussionsupporting
confidence: 81%
“…In order to validate the HE-fed DIO rat as a useful animal model of obesity, we examined the body weight lowering effect of the well-known anti-obesity agent sibutramine and the once-daily human GLP-1 analog liraglutide. The findings of a transient (7 day) effect on food intake and a approximate 10% weight loss following 28 days of treatment with sibutramine is in agreement with data reported previously from other rodent DIO models (Boozer et al 2001, Bush et al 2006, Mashiko et al 2008 as well as in a previous study in the DIO rat (Levin & Dunn-Meynell 2000). The body weight loss of w10% seen in rodent models of obesity translates into an approximate 5% sustained weight loss in humans (Bray et al 1999, James et al 2000.…”
Section: Discussionsupporting
confidence: 81%
“…Six-week-old Sprague-Dawley rats were offered a two-choice diet consisting of standard rodent chow diet or the gubra diet, a highly palatable high-fat, high-sugar diet. After a six-month feeding period, body weight changes, ingestive responses and feeding behaviors were examined following daily administration of sibutramine and liraglutide for 23 d. Compared to the vehicle control, chronic administration of either sibutramine or liraglutide to high-fat/sugar-fed DIO-rats caused significant reductions in body weight gain, which is in agreement with previously reported data using other rodent DIO models [14,15,[31][32][33][34] . The body weight loss observed in both groups was mainly caused by decreasing levels of total fat mass as revealed by the weekly measurements of whole body composition.…”
Section: Wwwchinapharcom Hansen G Et Alsupporting
confidence: 80%
“…Specifically, data on EI and BW in the mouse are reported for rimonabant 10 mg/kg/day,35 sibutramine 10 mg/kg/day,36 and topiramate 66 mg/kg/day (only BW; Figure 3 a,c ). Data on EI and BW in the rat are reported for rimonabant 10 mg/kg/day,37 taranabant 3 mg/kg/day,37 sibutramine 5 mg/kg/day,38 and lorcaserin 4 mg/kg/day39 ( Figure 3 b,d ).…”
Section: Methodsmentioning
confidence: 99%