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Role of primary and secondary bile acids as feedback inhibitors of bile acid synthesis in the rat in vivo.

机译:伯和仲胆汁酸作为大鼠体内胆汁酸合成的反馈抑制剂的作用。

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摘要

The effect of various primary and secondary bile acids on the rates of synthesis of all major bile acids was studied in the live rat with an extracorporal bile duct. Bile acid synthesis was determined using HPLC based on mass or by isotope dilution. Derepressed rates of bile acid synthesis (30-54 h) were inhibited by an infusion of taurocholic acid only at a supraphysiological dose of 500 mumol/kg per h, but not at 300 mumol/kg per h, which approximates the initial bile acid secretion (250 mumol/kg per h). When administered together with taurocholic acid (200 mumol/kg per h) only a high dose of taurochenodeoxycholic acid (100 mumol/kg per h) decreased taurocholic but not tauromuricholic or taurochenodeoxycholic acid synthesis. The only bile acid suppressing taurocholic acid (36-71%) and taurochenodeoxycholic acid (up to 33%) formation at an infusion rate close to the normal portal flux was deoxy- or taurodeoxycholic acid at 15-50 mumol/kg per h. It may be concluded that deoxycholic acid and possibly other secondary bile acids are much more potent inhibitors than primary bile acids.
机译:在具有体外胆管的活大鼠中研究了各种伯,仲胆汁酸对所有主要胆汁酸合成速率的影响。使用基于质量的HPLC或通过同位素稀释确定胆汁酸的合成。牛磺胆酸的超生理剂量仅以每小时500μmol/ kg的超生理学剂量输注牛磺酸,抑制胆汁酸合成的降低速率(30-54 h),而以每小时300μmol/ kg的超生理学剂量抑制,这近似于最初的胆汁酸分泌(250摩尔/千克/小时)。当与牛磺胆酸(每小时200摩尔/千克)一起施用时,仅高剂量的牛磺去氧胆酸(100摩尔/千克/小时)可降低牛磺胆酸的含量,但不能减少牛磺胆酸或牛磺去氧胆酸的合成。输注速率接近正常门户通量的唯一抑制胆汁酸的牛磺胆酸(36-71%)和牛磺去氧胆酸(高达33%)是脱氧-或牛磺脱氧胆酸,每小时15-50μmol/ kg。可以得出结论,脱氧胆酸和其他可能的仲胆汁酸比伯胆汁酸更有效。

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