Inhibition of food intake in response to intestinal  lipid is mediated by cholecystokinin in humans

Matzinger, Daniel; Gutzwiller, Jean‐Pierre; Drewe, Jürgen; Orban, Amar; Engel, Reto; D’Amato, Massimo; Rovati, Lucio C.; Beglinger, Christoph

doi:10.1152/ajpregu.1999.277.6.r1718

Cited by 76 publications

(84 citation statements)

References 34 publications

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“…Conversely, loxiglumide, a specific CCK-A receptor antagonist, stimulates calorie intake and feelings of hunger, and delays fullness. [4][5][6][7] These studies therefore provide evidence for a physiological role of CCK, acting via peripheral CCK-A receptors, in mediating satiation signals that reduce meal size and energy intake.…”

Section: Introductionmentioning

confidence: 72%

“…4 Conversely, loxiglumide, a specific CCK-A receptor antagonist, stimulates calorie intake and feelings of hunger, and delays fullness. [4][5][6][7] However, as already discussed, hydrolysis of dietary triglycerides by pancreatic lipase is necessary for the release and, presumably, the function of endogenous CCK. Indeed, Matzinger et al 7 demonstrated that intraduodenal administration of fat reduced the amount of food eaten at a subsequent meal (60 min after starting the perfusion) by 20%, corresponding to a 23% reduction in calorie intake.…”

Section: Discussionmentioning

confidence: 91%

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Effects of a lipase inhibitor (Orlistat) on cholecystokinin and appetite in response to a high-fat meal

et al. 2003

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OBJECTIVE:To examine the short-term effects of a lipase inhibitor (Orlistat) on physiological and behavioural measures of appetite in response to a high-fat meal. DESIGN: Randomised, single blind, placebo-controlled, crossover trial. SUBJECTS: A total of 19 healthy nonobese male subjects. PROCEDURES: After an overnight fast, subjects ingested a test meal of 2940 kJ (60% fat, 30% CHO, 10% protein) with Orlistat (120 mg) or a placebo, separated by 2 weeks. Appetite, as assessed by a standard line scale, and plasma cholecystokinin (CCK) concentrations were measured prior to and every hour after the test meal for 4 h. Thereafter, subjects ingested a quantified, but self-selected portion of a standardised lunch (15% protein, 37% fat and 45% CHO), before completing a final line scale questionnaire. RESULTS: The CCK response to the test meal was negatively correlated with BMI in both the Orlistat and placebo trials (R ¼ À0.69 and À0.65, Po0.01). Orlistat administration did not significantly alter the CCK response to the test meal (6.3073.27 vs 7.3673.94 pM min, for Orlistat and placebo, P ¼ 0.193). Similarly, the line scale measures of appetite and subsequent intake (5207205 vs 5547197 g, P ¼ 0.48) were not different between the trials. CONCLUSION: Orlistat administration did not alter short-term physiological or behavioural measures of satiety in response to a high-fat meal in healthy, nonobese subjects. The CCK response to a test meal may be partly determined by BMI.

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Section: Introductionmentioning

confidence: 72%

Section: Discussionmentioning

confidence: 91%

Effects of a lipase inhibitor (Orlistat) on cholecystokinin and appetite in response to a high-fat meal

et al. 2003

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“…Dietary protein is the most satiating macronutrient in experimental meal settings (Poppitt et al, 1998), with high-protein meals increasing blood concentrations of CCK (Blom et al, 2006;Bowen et al, 2006). Fat (Matzinger et al, 1999) and to a lesser extent carbohydrate (Holt et al, 1992;Parker et al, 2005) also stimulate CCK production from I cells in the duodenum and jejunum (Buffa et al, 1978).…”

Section: Introductionmentioning

confidence: 99%

Effect of the glycemic index of carbohydrates on day-long (10 h) profiles of plasma glucose, insulin, cholecystokinin and ghrelin

et al. 2008

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Background: Low glycemic index (GI) carbohydrates have been linked to increased satiety. The drive to eat may be mediated by postprandial changes in glucose, insulin and gut peptides. Objective: To investigate the effect of a low and a high GI diet on day-long (10 h) blood concentrations of glucose, insulin, cholecystokinin (CCK) and ghrelin (GHR). Design: Subjects (n ¼ 12) consumed a high and a low GI diet in a randomized, crossover design, consisting of four meals that were matched for macronutrients and fibre, and differed only in carbohydrate quality (GI). Blood was sampled every 30-60 min and assayed for glucose, insulin, CCK and GHR. Results: The high GI diet resulted in significantly higher glucose and insulin mean incremental areas under the curve (IAUC, P ¼ 0.027 and P ¼ 0.001 respectively). CCK concentration was 59% higher during the first 7 h of the low GI diet (394 ± 95 pmol/ l min) vs the high GI diet (163 ± 38 pmol/l min, P ¼ 0.046), but there was no difference over 10 h (P ¼ 0.224). GHR concentration was inversely correlated with insulin concentration (Pearson correlation À0.48, P ¼ 0.007), but did not differ significantly between the low and high GI diets. Conclusions: Mixed meals of lower GI are associated with lower day-long concentrations of glucose and insulin, and higher CCK after breakfast, morning tea and lunch. This metabolic profile could mediate differences in satiety and hunger seen in some, but not all, studies.

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“…Numerous studies have demonstrated a role for CCK and other gut peptides in the reduction of food intake and the activation of satiety mechanisms following intraintetsinal infusions of fatty acids. These robust effects have been ameliorated by both vagotomy and CCK-A receptor antagonism (7,8,15,32). Taken together, these novel findings both demonstrate the potential clinical relevance of gut-initiated satiety mechanisms in the treatment of obesity, and suggest important information on the means to best initiate them.…”

Section: Discussionmentioning

confidence: 73%

“…Numerous studies have described a reduction in food intake following infusion of fatty acids directly into the small intestine: French et al demonstrated that upper intestinal infusions of 20% oil emulsions enriched with either stearic, oleic, or linoleic acid significantly reduced food intake compared controls infused with saline, and that this reduction in food intake was accompanied with increased plasma CCK concentrations (9); Meyer et al described reductions in food intake following intraintestinal infusions of either fatty or amino acids (16); Cox et al have reported that jejunal infusions of linoleic or oleic acid elicit increased satiety, decreased food intake and decreased body weight in rats (6). Matzinger et al demonstrated that this effect is mediated by cholecystokinin, abolishing the effects of intraduodenal fat infusions on food intake with a specific CCK-A receptor antagonist (15).…”

Section: Introductionmentioning

confidence: 99%

Voluntary consumption of ethyl oleate reduces food intake and body weight in rats

Kemp

D’Alessio

Scott

et al. 2008

Physiology & Behavior

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Previous studies have shown that administration of the fatty acids, linoleic and oleic acid, either by intragastric or intraintestinal infusion, suppresses food intake and body weight in rats. While still not fully understood, gut-mediated satiety mechanisms likely are potential effectors of this robust response to gastrointestinal fatty acid infusions. The objective of this study was to assess the effects of voluntary access to an oleic acid derivative, ethyl oleate (EO), on subsequent food intake and body weight in rats. Animals were randomized either to a 12.5% EO diet or a soybean oil diet as a "breakfast," followed either by two one-hour or one five-hour access periods to standard rodent diet, and food intake and body weights were collected. Across 14 days access, rats consuming EO on both feeding schedules gained less weight and consumed less total kilocalories than rats consuming the SO diet. Further, plasma levels of glucose and insulin were comparable in both EO and SO diet groups. In summary, EO was found to increase weight loss in rats maintained on a 75% foodrestriction regimen, and attenuate weight-gain upon resumption of an ad-libitum feeding regimen. These data indicate that voluntary access to EO promoted short-term satiety, compared to SO diet, and that these effects contributed to a important and novel attenuated weight gain in EO-fed animals.

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Inhibition of food intake in response to intestinal lipid is mediated by cholecystokinin in humans

Cited by 76 publications

References 34 publications

Effects of a lipase inhibitor (Orlistat) on cholecystokinin and appetite in response to a high-fat meal

Effects of a lipase inhibitor (Orlistat) on cholecystokinin and appetite in response to a high-fat meal

Effect of the glycemic index of carbohydrates on day-long (10 h) profiles of plasma glucose, insulin, cholecystokinin and ghrelin

Voluntary consumption of ethyl oleate reduces food intake and body weight in rats

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