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阿片肽对犬十二指肠环行肌的作用。

Effect of opioid peptides on circular muscle of canine duodenum.

作者信息

Bauer A J, Szurszewski J H

机构信息

Department of Physiology and Biophysics, Mayo Medical School, Rochester, MN 55905.

出版信息

J Physiol. 1991 Mar;434:409-22. doi: 10.1113/jphysiol.1991.sp018477.

Abstract
  1. The effects of opioid peptides on inhibitory transmission in the circular muscle layer of canine duodenum were investigated in vitro using simultaneous mechanical and intracellular electrical recording techniques. 2. Exogenously added [Met5]enkephalin, [Leu5]enkephalin and dynorphin (1-13) decreased the amplitude of non-adrenergic, non-cholinergic inhibitory junction potentials (IJPs) evoked by transmural nerve stimulation. 3. A selective delta-receptor agonist, DPDPE ([D-Pen2, D-Pen5]enkephalin), and a selective mu-receptor agonist, PL017 (Try-Pro-NMePhe-D-Pro-NH2), decreased the amplitude of IJPs whereas a selective kappa-receptor agonist, U-50,488H ([trans-3,4-dichloro-N-methyl-N-(2-91-pyrolidinyl)-cyclohexyl]- benzeneacetamide methanesulphonate), in large doses (1 microM) produced only a small reduction. 4. A selective delta-receptor antagonist, ICI-174,864, blocked the effect of DPDPE but not that of PL017 suggesting the presence of distinct delta- and mu-opioid receptors on inhibitory motor nerves. 5. Exogenously added dynorphin (1-13) decreased the amplitude of IJPs. delta-Opioid receptors appeared to be involved because ICI-174,864, a selective delta-antagonist, blocked the inhibitory effect of exogenously added dynorphin (1-13). 6. The inhibitory effect of the opioid peptides was still observed in preparations of circular muscle devoid of myenteric and submucosal plexuses, indicating that the site of action was on inhibitory motor nerve fibres located within the circular muscle layer and not on neuronal cell bodies in the enteric plexuses. 7. It was concluded that in the canine small intestine, opioid peptides could modulate release of inhibitory transmitter(s) at or near nerve terminals of inhibitory motor nerves innervating circular muscle cells.
摘要
  1. 采用同步机械和细胞内电记录技术,在体外研究了阿片肽对犬十二指肠环行肌层抑制性传递的影响。2. 外源性添加的[Met5]脑啡肽、[Leu5]脑啡肽和强啡肽(1 - 13)降低了经壁神经刺激诱发的非肾上腺素能、非胆碱能抑制性接头电位(IJPs)的幅度。3. 选择性δ受体激动剂DPDPE([D - Pen2,D - Pen5]脑啡肽)和选择性μ受体激动剂PL017(Try - Pro - NMePhe - D - Pro - NH2)降低了IJPs的幅度,而选择性κ受体激动剂U - 50,488H([反式 - 3,4 - 二氯 - N - 甲基 - N - (2 - 吡咯烷基) - 环己基] - 苯乙酰胺甲磺酸盐)在大剂量(1μM)时仅产生微小的降低。4. 选择性δ受体拮抗剂ICI - 174,864阻断了DPDPE的作用,但未阻断PL017的作用,提示在抑制性运动神经上存在不同的δ和μ阿片受体。5. 外源性添加的强啡肽(1 - 13)降低了IJPs的幅度。δ阿片受体似乎参与其中,因为选择性δ拮抗剂ICI - 174,864阻断了外源性添加的强啡肽(1 - 13)的抑制作用。6. 在没有肌间和黏膜下神经丛的环行肌制备物中仍观察到阿片肽的抑制作用,表明作用部位是位于环行肌层内的抑制性运动神经纤维,而不是肠神经丛中的神经元细胞体。7. 得出结论,在犬小肠中,阿片肽可调节支配环行肌细胞的抑制性运动神经末梢处或其附近抑制性递质的释放。

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