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神经肽Y、神经肽Y片段13 - 36、肽YY和胰多肽对大鼠十二指肠和结肠运动及动脉血压的外周调节:胆碱能机制

Peripheral modulation of duodenal and colonic motility and arterial pressure by neuropeptide Y, neuropeptide Y fragment 13-36, peptide YY, and pancreatic polypeptide in rats: cholinergic mechanisms.

作者信息

Wager-Pagé S A, Raizada E, Veale W, Davison J S

机构信息

Faculty of Medicine, Department of Medical Physiology, University of Calgary, Canada.

出版信息

Can J Physiol Pharmacol. 1993 Oct-Nov;71(10-11):768-75. doi: 10.1139/y93-115.

Abstract

The pancreatic polypeptide-fold (PP-fold) peptides neuropeptide Y (NPY), peptide YY (PYY), and pancreatic polypeptide (PP) (500 pmol/kg) increased duodenal and colonic intraluminal pressure of urethane-anesthesized rats following intravenous (i.v.) bolus injections. Increases in mean arterial pressure (MAP) accompanied the excitatory effects of NPY and PYY on gastrointestinal motility in these rats during the same time period. Atropine attenuated PYY's excitatory effect on duodenal pressure of rats. Excitatory effects of NPY, PYY, and PP (i.v.) on rat colon were not mediated via the muscarinic receptors. In the presence of hexamethonium, a nicotinic antagonist, PP (i.v.) increased colonic pressure to a greater extent than when administered alone. This observation suggested that PP had an inhibitory effect on colonic motility, which was not apparent as a result of the larger excitatory component. The nicotinic antagonist did not modulate the effects of peripherally administered NPY or PYY on duodenal or colonic motility in anesthetized rats. The Y2 receptor ligand, NPY (13-36) (i.v.) (500 pmol/kg), increased duodenal and colonic pressure in rats to the same extent as the full NPY molecule. Therefore, the peripheral effect of PYY and NPY on duodenal and colonic motility in rats may be mediated via Y2 receptors. NPY and PYY (i.v.) initially increased MAP, which then return to baseline values. Unlike NPY and PYY (i.v.) which produced short-term hypertensive effects PP (i.v. decreased MAP. Atropine did not attenuate the hypertensive effects of PYY and NPY (i.v.); however, the hypotensive effect of PP (i.v.) was blocked by atropine. The effects of the PP-fold peptides on MAP were not altered in the presence of hexamethonium.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

胰多肽折叠(PP-折叠)肽神经肽Y(NPY)、肽YY(PYY)和胰多肽(PP)(500 pmol/kg)在静脉推注后,可使氨基甲酸乙酯麻醉大鼠的十二指肠和结肠腔内压力升高。在同一时期,NPY和PYY对这些大鼠胃肠动力的兴奋作用伴随着平均动脉压(MAP)的升高。阿托品减弱了PYY对大鼠十二指肠压力的兴奋作用。NPY、PYY和PP(静脉注射)对大鼠结肠的兴奋作用不是通过毒蕈碱受体介导的。在存在烟碱拮抗剂六甲铵的情况下,PP(静脉注射)比单独给药时更能增加结肠压力。这一观察结果表明,PP对结肠动力有抑制作用,由于较大的兴奋成分,这种抑制作用并不明显。烟碱拮抗剂并未调节外周给予的NPY或PYY对麻醉大鼠十二指肠或结肠动力的作用。Y2受体配体NPY(13-36)(静脉注射)(500 pmol/kg)使大鼠十二指肠和结肠压力升高的程度与完整的NPY分子相同。因此,PYY和NPY对大鼠十二指肠和结肠动力的外周作用可能是通过Y2受体介导的。NPY和PYY(静脉注射)最初使MAP升高,随后恢复到基线值。与产生短期高血压作用的NPY和PYY(静脉注射)不同,PP(静脉注射)使MAP降低。阿托品并未减弱PYY和NPY(静脉注射)的高血压作用;然而,PP(静脉注射)的降压作用被阿托品阻断。在存在六甲铵的情况下,PP-折叠肽对MAP的作用未改变。(摘要截短于250字)

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