肠内而非肠外给予菜豆凝集素可诱导哺乳大鼠肠道生长和早熟。

Biology of the neonate Pub Date : 2006-01-01 Epub Date: 2005-09-26 DOI:10.1159/000088563
Ann Linderoth, Olena Prykhod'ko, Stefan G Pierzynowski, Bjorn R Westrom
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引用次数: 25

摘要

背景:凝集素植物血凝素(PHA)已被证明可以诱导哺乳大鼠胃肠道的生长和功能成熟。目的:探讨给药途径的影响,以及是否需要肠内暴露于PHA以诱导功能成熟。方法:14日龄大鼠每天经胃灌胃(0.05 mg PHA/g BW)或皮下注射(0.05或0.005 mg PHA/g BW)给予PHA,连续3 d,对照组经胃灌胃给予生理盐水。在17日龄时,分析脏器重量、肠道和胰腺功能以及血浆皮质酮水平。此外,14日龄的幼犬接受单剂量PHA(肠内或肠外),12小时后处死,用免疫组织化学检测器官PHA结合情况。结果:肠内PHA暴露导致PHA与小肠上皮结合,促进胃肠道生长,减少肠道大分子吸收,改变二糖酶表达,使其向成人样模式转变,增加胰腺蛋白和胰蛋白酶含量。相反,肠外PHA暴露(高剂量)导致PHA在肠外器官结合,肝脏和脾脏重量增加,胸腺重量减少。肠道麦芽糖酶活性适度升高,BSA向血浆的转移部分减少。两种PHA治疗均导致血浆皮质酮水平升高。结论:这些结果表明,肠内暴露于PHA是诱导胃肠道和胰腺早熟的必要条件,而肠外给药则影响肠外器官。此外,肠内效应可能不是通过皮质类固醇依赖途径介导的。
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Enterally but not parenterally administered Phaseolus vulgaris lectin induces growth and precocious maturation of the gut in suckling rats.

Background: The lectin, phytohemagglutinin (PHA) has been shown to induce growth and functional maturation of the gastrointestinal (GI) tract in suckling rats.

Objectives: To investigate the effect of the administration route, and whether enteral exposure to PHA was necessary to induce functional maturation.

Methods: Fourteen-day-old rats were daily administered PHA via orogastric feeding (0.05 mg PHA/g BW) or via subcutaneous injection (0.05 or 0.005 mg PHA/g BW) for 3 days, while the controls received saline orogastrically. At 17 days of age, organ weight, intestinal and pancreatic function, and plasma corticosterone levels were analyzed. Moreover, 14-days old pups receiving a single dose of PHA, enterally or parenterally, were sacrificed after 12 h and examined for organ PHA binding using immunohistochemistry.

Results: Enteral PHA exposure resulted in PHA binding in the epithelial lining of the small intestine, increased gastrointestinal growth, reduced intestinal macromolecular absorption, altered the disaccharidase expression towards an adult-like pattern, and increased the pancreatic protein and trypsin contents. In contrast, parenteral PHA exposure (high dose) resulted in PHA-binding in extra-intestinal organs, increased liver and spleen weight, and decreased thymus weight. Moreover, the intestinal maltase activity increased moderately, and the transfer of BSA to blood plasma was partially reduced. Both PHA treatments led to elevated plasma corticosterone levels.

Conclusion: These results demonstrated that enteral exposure to PHA was necessary to induce the precocious maturation of the GI tract and the pancreas, while parenteral administration affects the extra-intestinal organs. Furthermore, the enteral effects were probably not mediated via a corticosteroid dependent pathway.

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