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实验性诱导肠病大鼠对51铬-乙二胺四乙酸的肠道通透性

Intestinal permeability to 51Cr-EDTA in rats with experimentally induced enteropathy.

作者信息

Bjarnason I, Smethurst P, Levi A J, Peters T J

出版信息

Gut. 1985 Jun;26(6):579-85. doi: 10.1136/gut.26.6.579.

Abstract

Intestinal permeability has been investigated in the normal rat by measuring the five hour urine excretion of 51Cr-EDTA after intragastric administration. Twelve control animals excreted 2.06% +/- 0.22 (mean +/- SE) of the administered dose. Prolonged intestinal transit times with atropine had no significant effect on the apparent permeability with a urine excretion 2.31% +/- 0.36. The concomitant administration of a hypertonic, but rapidly absorbed glycerol solution, was accompanied by increased urinary excretion (3.05% +/- 0.33) while the administration of a poorly absorbed sugar, lactulose, significantly decreased the apparent permeability (urine excretion 0.61% +/- 0.14) showing that passive intestinal permeability estimations are affected by test dose composition. Enteropathy was induced by ethanol, cetrimide, or methotrexate and each was associated with increased permeability, with urine excretions of 4.19% +/- 0.47, 4.20% +/- 0.66 and 3.97% +/- 0.49 respectively. It is thus suggested that the normal rat mucosa is maximally resistant to the absorption of foreign compounds such as 51Cr-EDTA and intestinal damage will disrupt this barrier.

摘要

通过测量灌胃给予51Cr-EDTA后正常大鼠5小时的尿排泄量,对肠道通透性进行了研究。12只对照动物排泄了给药剂量的2.06%±0.22(平均值±标准误)。阿托品导致肠道转运时间延长,但对表观通透性无显著影响,尿排泄量为2.31%±0.36。同时给予高渗但吸收迅速的甘油溶液,会使尿排泄增加(3.05%±0.33),而给予吸收不良的糖乳果糖,则会显著降低表观通透性(尿排泄量为0.61%±0.14),这表明被动性肠道通透性评估受测试剂量组成的影响。用乙醇、西曲溴铵或甲氨蝶呤诱导肠病,每种情况均与通透性增加有关,尿排泄量分别为4.19%±0.47、4.20%±0.66和3.9(7)%±0.49。因此提示,正常大鼠黏膜对诸如51Cr-EDTA等外来化合物的吸收具有最大抵抗力,而肠道损伤会破坏这一屏障。

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