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正常叶酸肠肝循环的动力学

Kinetics of the normal folate enterohepatic cycle.

作者信息

Steinberg S E, Campbell C L, Hillman R S

出版信息

J Clin Invest. 1979 Jul;64(1):83-8. doi: 10.1172/JCI109467.

Abstract

Detailed studies were undertaken to better define the role of the liver and the folate enterohepatic cycle in folate homeostasis. Three isotopes of folate were employed in a rat model to study several parameters: (a) intestinal transport; (b) variation in hepatic uptake after different routes of administration; (c) hepatic reduction, methylation, and polyglutamate formation; (d) biliary excretion; (e) transport of folate to tissue and its return to liver for re-entry into the enterohepatic cycle. Folate absorption was not affected by the type of folate administered, but subsequent liver accumulation was greater when PteGlu(1) was given rather than CH(3)H(4)PteGlu(1). After liver uptake, CH(3)H(4)PteGlu(1) is rapidly and quantitatively excreted into bile, whereas nonmethylated folates are either methylated and transported into bile or incorporated into a hepatic polyglutamate pool. Bile folate is then reabsorbed for distribution to both tissue and liver, completing the enterohepatic cycle. The importance of this cycle was demonstrated by long-term bile drainage and by transport studies with two isotopes of CH(3)H(4)PteGlu(1). With bile drainage, serum folate levels fell to 30-40% of normal within 6 h, a much more dramatic drop than that seen with folate-free diets alone. Studies with labeled CH(3)H(4)PteGlu(1) demonstrated that about one-third was taken up by tissue, demethylated, and returned to liver for remethylation and recirculation through the bile and gut. This establishes the enterohepatic cycle as a major factor in folate homeostasis and, for the first time, demonstrates a transport pathway between tissue and liver for nonmethylated folate.

摘要

开展了详细研究以更好地界定肝脏和叶酸肠肝循环在叶酸稳态中的作用。在大鼠模型中使用了三种叶酸同位素来研究几个参数:(a)肠道转运;(b)不同给药途径后肝脏摄取的变化;(c)肝脏还原、甲基化和多聚谷氨酸形成;(d)胆汁排泄;(e)叶酸向组织的转运及其返回肝脏以重新进入肠肝循环。叶酸的吸收不受所给药叶酸类型的影响,但给予PteGlu(1)而非CH(3)H(4)PteGlu(1)时,随后肝脏的蓄积量更大。肝脏摄取后,CH(3)H(4)PteGlu(1)迅速且定量地排泄到胆汁中,而非甲基化叶酸要么被甲基化并转运到胆汁中,要么被纳入肝脏多聚谷氨酸池。然后胆汁中的叶酸被重新吸收以分布到组织和肝脏,从而完成肠肝循环。长期胆汁引流以及用两种CH(3)H(4)PteGlu(1)同位素进行的转运研究证明了这个循环的重要性。进行胆汁引流时,血清叶酸水平在6小时内降至正常水平的30 - 40%,下降幅度比仅采用无叶酸饮食时更为显著。用标记的CH(3)H(4)PteGlu(1)进行的研究表明,约三分之一被组织摄取、去甲基化,然后返回肝脏进行再甲基化,并通过胆汁和肠道进行再循环。这确立了肠肝循环是叶酸稳态的一个主要因素,并且首次证明了非甲基化叶酸在组织和肝脏之间的转运途径。

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