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首页> 外文期刊>European journal of clinical investigation >The effects of ABT-229 and octreotide on interdigestive small bowel motility, bacterial overgrowth and bacterial translocation in rats.
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The effects of ABT-229 and octreotide on interdigestive small bowel motility, bacterial overgrowth and bacterial translocation in rats.

机译:ABT-229和奥曲肽对大鼠消化道小肠蠕动,细菌过度生长和细菌易位的影响。

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BACKGROUND: Interdigestive small bowel motility has a regulatory function on the microflora of the upper small bowel. Here we investigate the effects of ABT-229 and octreotide on morphine-induced dysmotility, the accompanying bacterial overgrowth and bacterial translocation. METHODS: Rats were fitted with jejunal myoelectrodes and a subcutaneous cannula for continuous infusion of saline or morphine. Fasting motility was measured for 6 h on four occasions: one control measurement (day 0) and three measurements on consecutive days (days 1-3) while receiving saline alone (group A), morphine alone (group B), saline + ABT-229 (group C), morphine + ABT-229 (group D), saline + octreotide (group E) or morphine + octreotide (group F). Samples from the mesenteric lymph node complex (MLN), liver, spleen, duodenum and ileum were taken for quantitative microbial culturing on day 4. RESULTS: Neither ABT-229 nor octreotide increased the number of propagated activity fronts during saline infusion. During morphine-induced dysmotility, ABT-229 induced more propagated activity fronts in group D (13.4, 9.8 and 8.8 per 6 h) than in group B (7.0, 4.5, 3.8 per 6 h) on days 1, 2 and 3 (P < 0.05 for all days) Octreotide did not induce more propagated activity fronts. Disruption of small bowel motility by morphine led to bacterial overgrowth in the duodenum. ABT-229 and octreotide did not reduce the bacterial growth levels. The total incidence of bacterial translocation was significantly higher in the morphine-treated animals than in the saline-treated animals. Neither ABT-229 nor octreotide reduced the bacterial translocation incidence. The number of propagated activity fronts on day 3 and duodenal bacterial growth correlated significantly in groups A, E and F. CONCLUSIONS: ABT-229, but not octreotide, reduced morphine induced dysmotility. Small bowel bacterial overgrowth and bacterial translocation were not prevented. Fasting small bowel motility has a regulatory function on the intestinal microflora of the upper small bowel.
机译:背景:消化小肠蠕动对上部小肠的菌群具有调节功能。在这里,我们研究了ABT-229和奥曲肽对吗啡诱导的运动障碍,伴随的细菌过度生长和细菌移位的影响。方法:给大鼠安装空肠肌电极和皮下插管,以连续输注盐水或吗啡。在四种情况下分别测量空腹运动6小时:一次对照测量(第0天)和连续几天(1-3天)进行三个测量,同时单独接受盐水(A组),单独吗啡(B组),盐水+ ABT- 229(C组),吗啡+ ABT-229(D组),生理盐水+奥曲肽(E组)或吗啡+奥曲肽(F组)。在第4天,从肠系膜淋巴结复合物(MLN),肝脏,脾脏,十二指肠和回肠取样进行定量微生物培养。结果:在盐水注入过程中,ABT-229和奥曲肽均未增加传播的活动前沿数量。在吗啡引起的运动障碍期间,在第1、2和3天,ABT-229诱导的D组(13.4、9.8和8.8每6小时)比B组(7.0、4.5、3.8每6小时)传播更多的活动前沿(P所有天均<0.05)奥曲肽没有诱导更多的传播活动前沿。吗啡对小肠蠕动的破坏导致十二指肠细菌过度生长。 ABT-229和奥曲肽没有降低细菌的生长水平。在吗啡处理的动物中,细菌移位的总发生率显着高于盐水处理的动物。 ABT-229和奥曲肽均未降低细菌易位发生率。 A,E和F组在第3天传播的活动前沿的数量与十二指肠细菌的生长显着相关。结论:ABT-229降低了吗啡引起的运动障碍,但奥曲肽没有。小肠细菌的过度生长和细菌移位都没有得到预防。空腹小肠蠕动对上部小肠的肠道菌群有调节作用。

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