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两性霉素B和霍乱毒素对大鼠肠道转运的影响。二羟基胆汁酸和脂肪酸对肠道转运影响的体内模型。

Effects of amphotericin B and cholera toxin on intestinal transport in the rat. An in vivo model for the effects of dihydroxy bile acids and fatty acids on intestinal transport.

作者信息

Ammon H V, Walter L G, Loeffler R F

出版信息

J Lab Clin Med. 1983 Oct;102(4):509-21.

PMID:6413628
Abstract

In vivo perfusion experiments were performed in the rat jejunum and colon to test the hypothesis that the changes in intestinal solute transport induced by dihydroxy bile acids and fatty acids are the result of the combined effects of fluid secretion and enhancement of mucosal permeability. The hypothesis predicts that absorption of organic solutes will be reduced in inverse relationship to the absorption rates under control conditions and that absorption of small, nonabsorbable solutes such as mannitol will be enhanced by these agents. Fluid secretion was induced either by administering cholera toxin or by increasing the osmolality of the perfusion solution to 365 mOsm/L. Permeability was enhanced by adding amphotericin B, 50 micrograms/ml, to the perfusion solutions. The isotonic perfusion solutions contained 11.2 mM glucose and 4 mM triethylene, tetraethylene, pentaethylene, and hexaethylene glycol or mannitol as probes of passive permeability. In the jejunum cholera toxin induced fluid and electrolyte secretion and reduced organic solute absorption to a small but significant degree (p less than 0.05). Amphotericin B alone enhanced absorption of organic solutes, water, and electrolytes (p less than 0.01). In the presence of fluid secretion induced by an osmotic load, only absorption of triethylene and pentaethylene glycol was reduced. Addition of amphotericin B after exposure to cholera toxin or to the hypertonic solutions resulted in a further significant reduction of absorption of glucose and ethylene glycols (p less than 0.05). The combination of amphotericin B and cholera toxin resulted in enhanced absorption of mannitol (p less than 0.02). Similarly, 5 mM deoxycholate enhanced jejunal absorption of mannitol (p less than 0.01) and reduced the absorption of glucose and the low-molecular-weight ethylene glycols (p less than 0.01). In the colon the administration of amphotericin B after the exposure to cholera toxin resulted in enhanced absorption of glucose (p less than 0.05) in spite of continuing fluid secretion. The combination of fluid secretion and enhancement of mucosal permeability, therefore, reproduced all in vivo effects of bile acids and fatty acids on intestinal transport of organic solutes.

摘要

在大鼠空肠和结肠中进行了体内灌注实验,以检验以下假设:二羟基胆汁酸和脂肪酸诱导的肠道溶质转运变化是液体分泌和黏膜通透性增强共同作用的结果。该假设预测,有机溶质的吸收将与对照条件下的吸收速率呈反比降低,并且这些物质会增强甘露醇等小的、不可吸收溶质的吸收。通过给予霍乱毒素或将灌注溶液的渗透压提高到365 mOsm/L来诱导液体分泌。通过向灌注溶液中添加50微克/毫升的两性霉素B来增强通透性。等渗灌注溶液含有11.2 mM葡萄糖和4 mM三乙烯、四乙烯、五乙烯和六乙烯二醇或甘露醇作为被动通透性的探针。在空肠中,霍乱毒素诱导液体和电解质分泌,并使有机溶质吸收略有但显著降低(p<0.05)。单独使用两性霉素B可增强有机溶质、水和电解质的吸收(p<0.01)。在由渗透压负荷诱导的液体分泌存在的情况下,只有三乙烯和五乙烯二醇的吸收降低。在接触霍乱毒素或高渗溶液后添加两性霉素B会导致葡萄糖和乙二醇的吸收进一步显著降低(p<0.05)。两性霉素B和霍乱毒素的组合导致甘露醇吸收增强(p<0.02)。同样,5 mM脱氧胆酸盐增强了空肠对甘露醇的吸收(p<0.01),并降低了葡萄糖和低分子量乙二醇的吸收(p<0.01)。在结肠中,尽管持续有液体分泌,但在接触霍乱毒素后给予两性霉素B导致葡萄糖吸收增强(p<0.05)。因此,液体分泌和黏膜通透性增强的组合重现了胆汁酸和脂肪酸对肠道有机溶质转运的所有体内效应。

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