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生氰糖苷扁桃苷的主要代谢产物苦杏仁苷的小肠转运机制。

Small-intestinal transfer mechanism of prunasin, the primary metabolite of the cyanogenic glycoside amygdalin.

作者信息

Strugala G J, Stahl R, Elsenhans B, Rauws A G, Forth W

机构信息

Walther Straub-Institut für Pharmakologie und Toxikologie, Ludwig-Maximilians-Universität München, Germany.

出版信息

Hum Exp Toxicol. 1995 Nov;14(11):895-901. doi: 10.1177/096032719501401107.

Abstract
  1. The small-intestinal transfer of prunasin (D-mandelo-nitrile-beta-D-glucoside), the primary metabolite of amygdalin which is not absorbed in the small intestine as such, was studied in rat jejunum and ileum in vitro. 2. As shown by high pressure liquid chromatography, prunasin is transferred essentially intact across the intestinal wall, without cleavage of the glycosidic bond and thus no formation of benzaldehyde or cyanide during the mucosal passage. 3. Only the jejunal transfer of prunasin followed saturation kinetics (vmax = 1.6 mumol cm-1 min-1; KT = 460 mumol l-1) and exhibited a clearsodium-ion dependence. As indicated by the temperature dependence, only the jejunal mucosa-to-serosa transfer and the corresponding tissue uptake of prunasin required apparently high activation energies. Transfer in the terminal ileum showed diffusion characteristics. 4. Jejunal methyl alpha-D-glucoside transfer was inhibited by the presence of prunasin. Furthermore, the tissue uptake of methyl alpha-D-glucoside in rat jejunum was competitively inhibited by prunasin. 5. The results indicate that prunasin is absorbed unmetabolised in the jejunum of the rat via the transport system of glucose.
摘要
  1. 苦杏仁苷的主要代谢产物苦杏仁素(D-扁桃腈-β-D-葡萄糖苷)本身在小肠中不被吸收,本研究在大鼠空肠和回肠中对其小肠转运进行了体外研究。2. 高压液相色谱分析表明,苦杏仁素基本上完整地穿过肠壁,糖苷键未断裂,因此在穿过黏膜的过程中不会形成苯甲醛或氰化物。3. 只有苦杏仁素的空肠转运遵循饱和动力学(最大转运速率vmax = 1.6 μmol·cm⁻¹·min⁻¹;转运常数KT = 460 μmol·L⁻¹),并且表现出明显的钠离子依赖性。从温度依赖性来看,只有苦杏仁素的空肠黏膜到浆膜的转运以及相应的组织摄取明显需要较高的活化能。回肠末端的转运表现出扩散特征。4. 苦杏仁素的存在会抑制空肠中α-D-甲基葡萄糖苷的转运。此外,苦杏仁素会竞争性抑制大鼠空肠中α-D-甲基葡萄糖苷的组织摄取。5. 结果表明,苦杏仁素在大鼠空肠中通过葡萄糖转运系统未被代谢地吸收。

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