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用铁螯合剂探究大鼠肝细胞铁动力学。

Hepatocyte iron kinetics in the rat explored with an iron chelator.

作者信息

Pippard M J, Johnson D K, Finch C A

出版信息

Br J Haematol. 1982 Oct;52(2):211-24. doi: 10.1111/j.1365-2141.1982.tb03883.x.

Abstract

The hepatocyte metabolism of 59Fe-labelled ferritin, haemoglobin-haptoglobin and transferrin has been examined in rats. All three forms of 59Fe became transiently available to desferrioxamine (DF) at the time they would otherwise have entered storage or alternative pathways of iron metabolism. However, differences in both the patterns of spontaneous 59Fe reutilization by normal and iron deficient rats and the partition of chelate iron excretion between bile and urine, suggested that iron in transit within hepatocytes did not behave as a single common pool. Ferritin 59Fe, entering a pool of non-radioactive iron the size of which is determined by liver iron stores, was chelated predominantly into the bile. Transferrin 59Fe was distinguished by a greater reflux to the erythron in iron deficient rats, and by excretion of a larger proportion of 59Fe chelated by DF in the urine. Haemoglobin-haptoglobin 59Fe followed a metabolic pathway which was relatively independent of both the iron stores and DF. If the heterogeneous behaviour of rat hepatocyte transit iron has a parallel in man, alterations in the size of similar chelatable iron pools could explain the dependence of DF-induced urine and faecal iron excretion on both liver iron stores and the level of erythropoiesis.

摘要

已在大鼠中研究了59Fe标记的铁蛋白、血红蛋白-触珠蛋白和转铁蛋白的肝细胞代谢情况。在这三种形式的59Fe原本会进入铁代谢的储存或其他途径时,它们都能短暂地被去铁胺(DF)利用。然而,正常和缺铁大鼠自发再利用59Fe的模式以及胆汁和尿液中螯合铁排泄的分配存在差异,这表明肝细胞内转运的铁并非表现为单一的共同池。铁蛋白59Fe进入一个由肝脏铁储存量决定大小的非放射性铁池,主要螯合进入胆汁。转铁蛋白59Fe的特点是在缺铁大鼠中更多地回流到红细胞生成中,并且DF螯合的59Fe有更大比例经尿液排泄。血红蛋白-触珠蛋白59Fe遵循一条相对独立于铁储存和DF的代谢途径。如果大鼠肝细胞转运铁的异质性在人类中有类似情况,那么类似可螯合铁池大小的改变可以解释DF诱导的尿液和粪便铁排泄对肝脏铁储存和红细胞生成水平的依赖性。

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