首页> 外文期刊>Scandinavian journal of gastroenterology. >Intestinal nitric oxide synthase activity changes during experimental colon obstruction.
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Intestinal nitric oxide synthase activity changes during experimental colon obstruction.

机译:在实验性结肠梗阻过程中肠一氧化氮合酶活性发生变化。

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OBJECTIVE: The experiments in this study were designed to follow the time course of nitric oxide (NO) synthesis in the large bowel during acute mechanical ileus. MATERIAL AND METHODS: Occlusion of the mid-transverse colon was maintained for 420 min in anesthetized dogs. Strain-gauge transducers were used to analyze motility changes on the hepatic and lienal flexures, respectively. Constitutive NO synthase (cNOS) and inducible NOS (iNOS) activities were determined in tissue biopsies, and plasma nitriteitrate (NOx) level was measured in the portal blood. Following completion of the baseline studies, the animals were treated with either 7-nitroindazole (7-NI, selective neuronal NOS inhibitor), or N-nitro-L-arginine (NNA, non-selective NOS inhibitor). RESULTS: In the sham-operated group the cNOS activities differed significantly in the oral and aboral tissue samples (oral: 102.9; versus aboral: 62.1 fmol/mg protein/min). The obstruction elicited a significant increase in portal NOx and elevated tissue inducible NO synthase (iNOS) activity. NNA treatment decreased the motility index in both intestinal segments for 60 min, but 120 min later the motility index was significantly elevated (2.5-fold increase in the oral part, and 1.8-fold enhancement in the aboral segment, respectively). Treatment with 7-NI decreased the cNOS activity in the oral and aboral parts by approximately 40% and 70%, respectively, and suppressed the motility increase in the aboral colon segment. CONCLUSIONS: The motility of the colon was either significantly increased or decreased, depending on the type and selectivity of the NOS inhibitor compounds applied. NO of neuronal origin is a transmitter that stimulates peristaltic activity; but an increased iNOSNOS ratio significantly moderates the obstruction-induced motility increase.
机译:目的:本研究旨在追踪急性机械性肠梗阻期间大肠中一氧化氮(NO)合成的时间过程。材料与方法:在麻醉犬中,将中横结肠闭塞420分钟。应变计换能器分别用于分析肝和肠弯曲的运动性变化。在组织活检中确定组成型NO合酶(cNOS)和诱导型NOS(iNOS)活性,并在门静脉血中测量血浆亚硝酸盐/硝酸盐(NOx)水平。完成基线研究后,用7-硝基吲唑(7-NI,选择性神经元NOS抑制剂)或N-硝基-L-精氨酸(NNA,非选择性NOS抑制剂)治疗动物。结果:在假手术组中,口腔和鼻腔组织样品中的cNOS活性差异显着(口腔:102.9;鼻腔:62.1 fmol / mg蛋白/ min)。梗阻引起门NOx显着增加,组织诱导型NO合酶(iNOS)活性升高。 NNA治疗可降低两个肠段的运动指数60分钟,但120分钟后,运动指数显着升高(口腔部分分别增加2.5倍和北侧部分增加1.8倍)。用7-NI进行治疗分别使口腔和鼻腔部分的cNOS活性降低了约40%和70%,并抑制了鼻腔结肠部分的运动性增加。结论:结肠运动明显增加或减少,取决于所应用的NOS抑制剂化合物的类型和选择性。神经元来源的NO是刺激蠕动的递质。但是增加的iNOS / nNOS比例可显着缓解阻塞引起的运动性增加。

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