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吗啡对小肠和大肠蠕动抑制作用的差异:小鼠中枢和外周μ-阿片受体的参与

Differences in the morphine-induced inhibition of small and large intestinal transit: Involvement of central and peripheral μ-opioid receptors in mice.

作者信息

Matsumoto Kenjiro, Umemoto Hiroyuki, Mori Tomohisa, Akatsu Ryuya, Saito Shinichiro, Tashima Kimihito, Shibasaki Masahiro, Kato Shinichi, Suzuki Tsutomu, Horie Syunji

机构信息

Laboratory of Pharmacology, Faculty of Pharmaceutical Sciences, Josai International University, 1 Gumyo, Togane, Chiba 283-8555, Japan; Division of Pathological Sciences, Department of Pharmacology and Experimental Therapeutics, Kyoto Pharmaceutical University, Misasagi, Ymashina, Kyoto 607-8414, Japan.

Laboratory of Pharmacology, Faculty of Pharmaceutical Sciences, Josai International University, 1 Gumyo, Togane, Chiba 283-8555, Japan.

出版信息

Eur J Pharmacol. 2016 Jan 15;771:220-8. doi: 10.1016/j.ejphar.2015.12.033. Epub 2015 Dec 19.

Abstract

Constipation is the most common side effect of morphine. Morphine acts centrally and on peripheral sites within the enteric nervous system. There are a few comprehensive studies on morphine-induced constipation in the small and large intestine by the activation of central and peripheral μ-opioid receptors. We investigated the differences in the inhibition of the small and large intestinal transit in normal and morphine-tolerant mice. Morphine reduced the geometric center in the fluorescein isothiocyanate-dextran assay and prolonged the bead expulsion time in a dose-dependent manner. The inhibitory effects of morphine were blocked by μ-opioid antagonist β-funaltrexamine, but not by δ- and κ-opioid antagonists. The peripheral opioid receptor antagonist, naloxone methiodide, partially blocked morphine's effect in the small intestine and completely blocked its effect in the large intestine. The intracerebroventricular administration of naloxone significantly reversed the delay of small intestinal transit but did not affect morphine-induced inhibition of large intestinal transit. Naloxone methiodide completely reversed the inhibition of large intestinal transit in normal and morphine-tolerant mice. Naloxone methiodide partially reversed the morphine-induced inhibition of small intestinal transit in normal mice but completely reversed the effects of morphine in tolerant mice. Chronic treatment with morphine results in tolerance to its inhibitory effect on field-stimulated contraction in the isolated small intestine but not in the large intestine. These results suggest that peripheral and central opioid receptors are involved in morphine-induced constipation in the small and large intestine during the early stage of treatment, but the peripheral receptors mainly regulate constipation during long-term morphine treatment.

摘要

便秘是吗啡最常见的副作用。吗啡作用于中枢以及肠神经系统的外周部位。关于通过激活中枢和外周μ-阿片受体导致吗啡引起的小肠和大肠便秘,有一些全面的研究。我们研究了正常小鼠和吗啡耐受小鼠中小肠和大肠运输抑制的差异。在异硫氰酸荧光素-葡聚糖试验中,吗啡降低了几何中心,并以剂量依赖的方式延长了珠子排出时间。吗啡的抑制作用被μ-阿片拮抗剂β-芬太尼环已胺阻断,但未被δ-和κ-阿片拮抗剂阻断。外周阿片受体拮抗剂甲硫氨酸纳洛酮部分阻断了吗啡在小肠中的作用,并完全阻断了其在大肠中的作用。脑室内注射纳洛酮显著逆转了小肠运输的延迟,但不影响吗啡引起的大肠运输抑制。甲硫氨酸纳洛酮完全逆转了正常小鼠和吗啡耐受小鼠中大肠运输的抑制。甲硫氨酸纳洛酮部分逆转了正常小鼠中吗啡引起的小肠运输抑制,但完全逆转了耐受小鼠中吗啡的作用。长期用吗啡治疗会导致对其对离体小肠场刺激收缩的抑制作用产生耐受性,但对大肠则不会。这些结果表明,在治疗早期,外周和中枢阿片受体参与了吗啡引起的小肠和大肠便秘,但在长期吗啡治疗期间,外周受体主要调节便秘。

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