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中枢介导的蛙皮素对胃肠运动的影响。

Centrally-mediated bombesin effects on gastrointestinal motility.

作者信息

Porreca F, Burks T F, Koslo R J

出版信息

Life Sci. 1985 Jul 15;37(2):125-34. doi: 10.1016/0024-3205(85)90415-1.

DOI:10.1016/0024-3205(85)90415-1
PMID:2409425
Abstract

Administration of bombesin into the lateral cerebral ventricle (i.c.v.) of rats results in a dose-related delay in gastric emptying and small intestinal transit. Recordings of intestinal intraluminal pressure in this species show that the i.c.v. peptide produces a dose-related increase in the frequency of duodenal contractions, and a complex inhibitory/excitatory jejunal effect at low and high doses, respectively. Intrathecal (i.th.) or i.c., but not intraperitoneal (i.p.), bombesin produces a dose-related slowing of gastrointestinal and colonic transit in mice. I.c.v. bombesin is 13.5 and 3406 times more potent in inhibition of gastrointestinal transit than when given by the i.th. or i.p. routes, respectively. Similarly, the i.c.v. peptide is 1.54 and over 11000 times more potent in slowing mouse colonic transit than when given by the i.th. or i.p. routes, respectively. The substance P analogue, D-Arg1, D-Pro2, D-Trp7,9, Leu11-Substance P (DAPTL-SP)(a reported bombesin antagonist in vitro) was not effective in blocking the gastrointestinal transit effects of the peptide in vivo. Transection of the spinal cord at the level of the second thoracic vertebra (T2) eliminates the gastrointestinal and colonic effects of i.th., but not i.c.v. bombesin. Thus, bombesin can affect motor function of the gut via activity within the brain or spinal cord of rats and mice; the activity of the peptide when given at the supraspinal level depends on an intact vagus nerve and adrenal-pituitary axis, while the activity of the peptide given at the spinal level appears to depend on the integrity of ascending spinal-supraspinal pathways.

摘要

向大鼠侧脑室(脑室内)注射蛙皮素会导致胃排空和小肠转运出现剂量相关的延迟。对该物种肠腔内压力的记录表明,脑室内注射该肽会使十二指肠收缩频率出现剂量相关的增加,并且在低剂量和高剂量时分别对空肠产生复杂的抑制/兴奋作用。鞘内注射(鞘内)或脑室内注射,但不是腹腔内注射(腹腔内),蛙皮素会使小鼠的胃肠和结肠转运出现剂量相关的减慢。脑室内注射蛙皮素在抑制胃肠转运方面的效力分别比鞘内注射或腹腔内注射高13.5倍和3406倍。同样,脑室内注射该肽在减慢小鼠结肠转运方面的效力分别比鞘内注射或腹腔内注射高1.54倍和超过11000倍。P物质类似物D-Arg1、D-Pro2、D-Trp7,9、Leu11-P物质(DAPTL-SP)(一种体外报道的蛙皮素拮抗剂)在体内不能有效阻断该肽对胃肠转运的影响。在第二胸椎(T2)水平横断脊髓可消除鞘内注射蛙皮素对胃肠和结肠的影响,但不能消除脑室内注射蛙皮素的影响。因此,蛙皮素可通过大鼠和小鼠脑内或脊髓内的活动影响肠道的运动功能;该肽在脊髓上水平给药时的活性取决于完整的迷走神经和肾上腺-垂体轴,而在脊髓水平给药时的活性似乎取决于脊髓-脊髓上上行通路的完整性。

相似文献

1
Centrally-mediated bombesin effects on gastrointestinal motility.中枢介导的蛙皮素对胃肠运动的影响。
Life Sci. 1985 Jul 15;37(2):125-34. doi: 10.1016/0024-3205(85)90415-1.
2
Centrally administered bombesin affects gastrointestinal transit and colonic bead expulsion through supraspinal mechanisms.中枢给予的蛙皮素通过脊髓上机制影响胃肠转运和结肠小珠排出。
J Pharmacol Exp Ther. 1986 Jul;238(1):62-7.
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Effects of bombesin on behavior.
Life Sci. 1985 Jul 15;37(2):135-45. doi: 10.1016/0024-3205(85)90416-3.
4
Pituitary-adrenal mediation of bombesin-induced inhibition of gastrointestinal transit in rats.大鼠中蛙皮素诱导的胃肠运输抑制的垂体 - 肾上腺介导作用
Regul Pept. 1984 Nov;9(4):299-304. doi: 10.1016/0167-0115(84)90082-x.
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Bombesin stimulates small intestinal motility after intracerebroventricular administration to rats.向大鼠脑室内注射蛙皮素后,其可刺激小肠蠕动。
Eur J Pharmacol. 1985 Aug 15;114(2):167-73. doi: 10.1016/0014-2999(85)90624-7.
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A comparison of the central gastrointestinal antitransit effects of morphine and bombesin in the mouse.小鼠体内吗啡与蛙皮素对胃肠道中枢性抗转运作用的比较。
Life Sci. 1987 Nov 30;41(22):2455-61. doi: 10.1016/0024-3205(87)90671-0.
7
Intrathecal bombesin in rats: effects on behaviour and gastrointestinal transit.大鼠鞘内注射蛙皮素:对行为和胃肠转运的影响。
Eur J Pharmacol. 1983 Oct 14;94(1-2):141-3. doi: 10.1016/0014-2999(83)90451-x.
8
Centrally administered bombesin affects gastric emptying and small and large bowel transit in the rat.中枢给予蛙皮素会影响大鼠的胃排空以及小肠和大肠的转运。
Gastroenterology. 1983 Aug;85(2):313-7.
9
Centrally administered bombesin modulates gastric motility.中枢给予蛙皮素可调节胃动力。
Peptides. 1987 Sep-Oct;8(5):887-91. doi: 10.1016/0196-9781(87)90076-3.
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Central nervous system action of bombesin to inhibit gastric acid secretion.蛙皮素抑制胃酸分泌的中枢神经系统作用。
Life Sci. 1985 Jul 15;37(2):115-23. doi: 10.1016/0024-3205(85)90414-x.

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