4.5 Article

Food intake in lean and obese mice after peripheral administration of glucagon-like peptide 2

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JOURNAL OF ENDOCRINOLOGY
卷 213, 期 3, 页码 277-284

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BIOSCIENTIFICA LTD
DOI: 10.1530/JOE-12-0092

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  1. Ministero dell'Universita e della Ricerca Scientifica, Italy

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We investigated the potential anorectic action of peripherally administered glucagon-like peptide 2 (GLP2) in lean and diet-induced obese (DIO) mice. Mice, fasted for 16 h, were injected i.p. with native GLP2 or [Gly(2)]GLP2, stable analog of GLP2, before or after GLP2 (3-33), a GLP2 receptor (GLP2R) antagonist, or exendin (9-39), a GLP1R antagonist. Food intake was measured at intervals 1, 2, 4, 8, and 24 h postinjection. In addition, we tested in lean mice the influence of [Gly(2)]GLP2 on gastric emptying and the effects of GLP1 alone or in combination with [Gly(2)]GLP2 on food intake. [Gly(2)]GLP2 dose dependently and significantly inhibited food intake in lean and DIO mice. The reduction of food intake occurred in the first hour postinjection and it was sustained until 4 h postinjection in lean mice while it was sustained until 2 h postinjection in DIO mice. GLP2 significantly inhibited food intake in both lean and DIO mice but only in the first hour postinjection. The efficiency of [Gly(2)]GLP2 or GLP2 in suppressing food intake was significantly weaker in DIO mice compared with lean animals. The [Gly(2)]GLP2 anorectic actions were blocked by the GLP2R antagonist GLP2 (3-33) or by the GLP1R antagonist exendin (9-39). The coadministration of [Gly(2)]GLP2 and GLP1 did not cause additive effects. [Gly(2)]GLP2 decreased the gastric emptying rate. Results suggest that GLP2 can reduce food intake in mice in the short term, likely acting at a peripheral level. DIO mice are less sensitive to the anorectic effect of the peptide. Journal of Endocrinology (2012) 213, 277-284

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