Leptin responses to glucose infusions in obesity-prone rats

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Leptin responses to glucose infusions in obesity-prone rats

James R. Levy¹^,², John Lesko¹, Richard J. Krieg Jr.², Robert A. Adler¹^,², and Wayne Stevens¹

¹ Section of Endocrinology and Metabolism, McGuire Veterans Administration Medical Center and ² Medical College of Virginia/Virginia Commonwealth University, Richmond, Virginia 23249

The secretion of leptin is dually regulated. In fasting animals, plasma leptin concentrations reflect body fat stores, whereasthe incremental leptin response to fasting or refeeding most likelyreflects insulin-mediated energy flux and metabolism within adipocytes.Impaired secretion of leptin in either pathway could result inobesity. We therefore measured plasma leptin concentrations infasted animals and plasma leptin concentrations after an intravenousglucose infusion in a rat model of obesity. Young Sprague-Dawley(S-D) and Fischer 344 (F344) rats had similar percent body fatand fasting glucose and fasting leptin concentrations. However,F344 animals had higher insulin concentrations and leptin responsesto intravenous glucose than did the S-D animals. The animals werethen fed a control or high-fat diet for 6 wk. High-fat fed animalsgained more weight and body fat than did the control fed animals.Control and high-fat fed F344 animals gained ~40% (P < 0.0001)more weight and >100% (P < 0.01) more body fat than did the S-Danimals. Fasting leptin concentrations and leptin concentrationsafter intravenous glucose infusions and feeding were more thandouble (P < 0.05) in F344 animals compared with S-D animals. Whetheran animal is fed a control or high-fat diet had little effecton the leptin response to intravenous glucose. In conclusion,young, lean F344 animals, before the onset of obesity, demonstrateda greater acute leptin response to intravenous glucose than similarlylean S-D animals. After a 6-wk diet, F344 animals had a greaterpercent increase in body weight and insulin resistance and exhibitedhigher fasting leptin concentrations and a greater absolute leptinresponse to intravenous glucose compared with the S-D animals.The chronic diet (control or high fat) had little impact on theacute leptin response to intravenous glucose. F344 animals exhibitleptin resistance in young, lean animals and after aging and fataccumulation.

secretion; Fischer 344; body fat

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