首页> 美国卫生研究院文献>The Journal of Clinical Investigation >The effect of sodium taurocholate on the hepatic metabolism of sulfobromophthalein sodium (BSP). The role of bile flow
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The effect of sodium taurocholate on the hepatic metabolism of sulfobromophthalein sodium (BSP). The role of bile flow

机译:牛磺胆酸钠对磺基溴酞钠(BSP)肝脏代谢的影响。胆汁流的作用

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摘要

The influence of bile salts on the hepatic metabolism of sulfobromophthalein sodium (BSP) was studied in the perfused rat liver. During sodium taurocholate infusions, hepatic uptake of BSP from plasma was increased and appeared to be related to an enhanced transit of BSP from liver into bile. BSP-glutathione conjugation was not affected by the bile salt infusions, although bile salts inhibited the enzyme system in vitro.The major effect of bile salts was to increase the BSP transport maximum (Tm). When sodium taurocholate was infused in saline at a rate of 30 μmoles/hr, both bile flow and the BSP Tm increased, and remained at peak levels of 1.5 ±0.12 μl/min per g liver and 21 ±3.0 μg/min per g liver, respectively. In contrast, during saline infusion alone both levels were significantly lower (1.06 ±0.17 μl/min per g liver and 15.8 ±4.16 μg/min per g liver, respectively), and both fell progressively after the 2nd hr of perfusion. This decline in bile flow and BSP Tm was associated with a decrease in biliary bile salt excretion and was reversed by adding bile salts to the perfusate. Since the biliary concentration of BSP remained within a narrow range in all experiments, the BSP Tm was primarily determined by the rate of bile flow.Dependence of BSP Tm on the rate of bile production was further confirmed by changing the temperature of the perfusate during a constant infusion of taurocholate. BSP Tm paralleled temperature-induced changes in bile flow irrespective of changes in the level of bile salt excretion.Since the biliary concentration of BSP remained within a narrow range in all experiments, the concentrating capacity for BSP in bile may be the major limiting factor in BSP transport. Thus two independent factors appear to determine the BSP Tm: the bile BSP concentration, and the rate of bile production.Because taurocholate enhanced BSP transport only when it increased bile production, its effect on the BSP Tm appears to be attributable to its choleretic properties.
机译:在灌注的大鼠肝脏中研究了胆盐对磺基溴酞钠(BSP)肝代谢的影响。在牛磺胆酸钠输注期间,肝脏从血浆中摄取BSP的量增加,并且似乎与BSP从肝脏向胆汁的转运增加有关。尽管胆盐在体外抑制了酶系统,但BSP-谷胱甘肽的结合不受胆盐输注的影响。胆盐的主要作用是增加BSP转运最大值(Tm)。当牛磺胆酸钠以30μmoles/ hr的速度注入盐水中时,胆汁流量和BSP Tm均增加,并保持在每g肝1.5±0.12μl/ min和每g肝21±3.0μg/ min的峰值水平, 分别。相比之下,在单独输注盐水期间,两个水平均显着降低(分别为每g肝脏1.06±0.17μl/ min和每g肝脏15.8±4.16μg/ min),并且在灌注第二小时后均逐渐下降。胆汁流量和BSP Tm的下降与胆汁胆汁盐排泄的减少有关,并通过向灌注液中添加胆汁盐来逆转。由于在所有实验中BSP的胆汁浓度都保持在狭窄的范围内,因此BSP Tm主要由胆汁流速决定.BSP Tm对胆汁产生速率的依赖性进一步通过在灌装过程中改变灌流液温度来确定。不断输注牛磺胆酸盐。 BSP Tm与温度引起的胆汁流量变化平行,而与胆汁盐排泄水平的变化无关。由于在所有实验中BSP的胆汁浓度均保持在狭窄范围内,因此BSP在胆汁中的浓缩能力可能是胆汁中主要的限制因素。 BSP传输。因此,似乎有两个独立的因素决定了BSP Tm:胆汁BSP浓度和胆汁生成速率。由于牛磺胆酸盐仅在胆汁产量增加时才增强BSP转运,因此其对BSP Tm的作用似乎归因于其胆汁特性。

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