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背侧迷走神经复合体中PYY偏好性受体及其在大鼠中对PYY刺激胃酸分泌的参与作用。

PYY-preferring receptor in the dorsal vagal complex and its involvement in PYY stimulation of gastric acid secretion in rats.

作者信息

Yang H, Li W P, Reeve J R, Rivier J, Taché Y

机构信息

CURE: Digestive Diseases Research Center, West Los Angeles Veterans Affairs Medical Center, UCLA, CA 90073, USA.

出版信息

Br J Pharmacol. 1998 Apr;123(8):1549-54. doi: 10.1038/sj.bjp.0701767.

Abstract
  1. Microinjection of peptide YY (PYY, 7-46 pmol) into the dorsal vagal complex (DVC) stimulated gastric acid secretion in urethane-anaesthetized rats. Using a variety of neuropeptide Y (NPY) and PYY derivatives, we characterized the pharmacological profile of the receptor mediating the acid secretory response to PYY. 2. [Pro34]rat(r)/porcine(p)PYY and [Pro34]human(h)PYY (23-117 pmol), microinjected unilaterally into the DVC resulted in a similar maximal increase in net acid secretion reaching 68+/-11 and 89+/-31 micromol 90 min(-1) respectively. 3. Rat/hNPY and pNPY (47 pmol) microinjected into the DVC induced a similar net gastric acid secretion (27+/-8 and 23+/-8 micromol 90 min(-1) respectively) and a higher dose (116 pmol) tended to reduce the response. 4. Pancreatic polypeptide (PP, 4-46 pmol), [Leu31,Pro34]r/hNPY (47 and 117 pmol) and the Y2 selective agonists, hPYY3-36, pNPY5-36 and PNPY13-36 (25-168 pmol) microinjected into the DVC failed to influence basal gastric acid secretion. 5. The rank order of potency of PYY > or = [Pro34]r/pPYY = [Pro34]hPYY> r/hNPY = pNPY to stimulate gastric acid secretion upon injection into the DVC and the ineffectiveness of PP, [Leu31,Pro34]NPY and C-terminal NPY/PYY fragments suggest that a PYY-preferring receptor subtype may be involved in mediating the stimulating effect.
摘要
  1. 向氨基甲酸乙酯麻醉的大鼠迷走神经背核(DVC)微量注射肽YY(PYY,7 - 46皮摩尔)可刺激胃酸分泌。我们使用多种神经肽Y(NPY)和PYY衍生物,对介导PYY酸分泌反应的受体的药理学特征进行了表征。2. 单侧微量注射到DVC中的[Pro34]大鼠(r)/猪(p)PYY和[Pro34]人(h)PYY(23 - 117皮摩尔)分别导致净酸分泌的最大增加相似,分别在90分钟时达到68±11和89±31微摩尔。3. 微量注射到DVC中的大鼠/人NPY和猪NPY(47皮摩尔)诱导了相似的净胃酸分泌(分别为27±8和23±8微摩尔/90分钟),更高剂量(116皮摩尔)倾向于降低反应。4. 向DVC微量注射胰多肽(PP,4 - 46皮摩尔)、[Leu31,Pro34]大鼠/人NPY(47和117皮摩尔)以及Y2选择性激动剂hPYY3 - 36、猪NPY5 - 36和PNPY13 - 36(25 - 168皮摩尔)未能影响基础胃酸分泌。5. 注射到DVC中刺激胃酸分泌的效力顺序为PYY≥[Pro34]大鼠/猪PYY = [Pro34]人PYY>大鼠/人NPY = 猪NPY,以及PP、[Leu31,Pro34]NPY和C末端NPY/PYY片段无效表明,可能涉及一种更倾向于PYY的受体亚型来介导刺激作用。

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