首页> 外文期刊>Obesity Surgery >Peptide YY(1-36) and Peptide YY(3-36): Part II. Changes after Gastrointestinal Surgery and Bariatric Surgery: Part I. Distribution, Release and Actions appeared in the last issue (May 2006)
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Peptide YY(1-36) and Peptide YY(3-36): Part II. Changes after Gastrointestinal Surgery and Bariatric Surgery: Part I. Distribution, Release and Actions appeared in the last issue (May 2006)

机译:肽YY(1-36)和肽YY(3-36):第二部分。胃肠外科和减肥手术后的变化:第一部分。分布,释放和作用出现在上一期(2006年5月)中

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摘要

Peptide YY (PYY) is secreted as a 36 amino acid, straight chain polypeptide, and is found in greatest concentrations in the terminal ileum, colon and rectum. After secretion, dipeptidyl peptidase IV (DPP-IV) cleaves the N-terminal Tyrosine-Proline residues from PYY(1-36), producing PYY(3-36). PYY(1-36) acts at all four human Y receptors, Y1, Y2, Y4 and Y5, while PYY(336) is a specific Y2 receptor agonist. PYY participates in the regulation of appetite and weight balance through hypothalamic-based mechanisms. PYY(1-36) stimulates appetite and weight gain through Y1 and Y5 receptors. PYY(3-36) suppresses appetite and stimulates weight loss through Y2 receptors. GI diseases that cause malabsorption increase both basal and meal-stimulated PYY levels. In contrast, obesity decreases both basal and meal-stimulated PYY levels. Mutations in the human PYY and Y2 receptor genes may contribute to the development of obesity. Small bowel resection elevates PYY levels in humans. Colon resections increase PYY levels in animal models but not in man. PYY changes following bariatric operations are incompletely studied. Vertical banded gastroplasty, open Roux-en-Y gastric bypass and jejunoileal bypass significantly elevate basal and meal-stimulated PYY levels. In dogs with Pavlov pouches, Roux-en-Y duodenojejunostomy (duodenal switch) increases PYY levels compared to Roux-en-Y gastrojejunostomy. DPP-IV activity is increased in obese individuals and remains increased after biliopancreatic diversion. Thus, diseases or operations which cause malabsorption, elevate basal and meal-stimulated PYY levels. Bariatric operations also increase basal and meal-stimulated PYY levels. This suggests that the combination of increased PYY levels and elevated levels of DPP-IV observed after bariatric operations may generate increased circulating levels of PYY(3-36), leading to hypothalamic-mediated suppression of appetite and promotion of weight loss through Y2 receptor mediated mechanisms.
机译:YY肽(PYY)以36个氨基酸的直链多肽形式分泌,在回肠末端,结肠和直肠中浓度最高。分泌后,二肽基肽酶IV(DPP-IV)从PYY(1-36)切割N端酪氨酸-脯氨酸残基,产生PYY(3-36)。 PYY(1-36)作用于所有四个人类Y受体Y1,Y2,Y4和Y5,而PYY(336)是一种特定的Y2受体激动剂。 PYY通过下丘脑机制参与食欲和体重平衡的调节。 PYY(1-36)通过Y1和Y5受体刺激食欲和体重增加。 PYY(3-36)抑制食欲,并通过Y2受体刺激体重减轻。引起吸收不良的胃肠道疾病会增加基础和膳食刺激的PYY水平。相反,肥胖会降低基础和进餐刺激的PYY水平。人类PYY和Y2受体基因的突变可能有助于肥胖症的发展。小肠切除会提高人体的PYY水平。结肠切除术会增加动物模型中的PYY水平,但不会增加人模型中的PYY水平。减肥手术后PYY的变化尚未完全研究。垂直条带化胃成形术,开放的Roux-en-Y胃旁路手术和空肠油旁路手术可显着提高基础和进餐刺激的PYY水平。在具有Pavlov袋的狗中,与Roux-en-Y胃空肠吻合术相比,Roux-en-Y十二指肠空肠吻合术(十二指肠开关)增加了PYY水平。 DPP-IV活性在肥胖个体中增加,并且在胆胰转移后仍保持增加。因此,引起吸收不良的疾病或手术会升高基础和膳食刺激的PYY水平。减肥手术还会增加基础和膳食刺激的PYY水平。这表明减肥手术后观察到PYY水平升高和DPP-IV水平升高可能会增加PYY的循环水平(3-36),从而导致下丘脑介导的食欲抑制和通过Y2受体介导的体重减轻机制。

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