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转铁蛋白结合铁功能异质性的体内证据。I. 对正常大鼠的研究。

In vivo evidence for the functional heterogeneity of transferrin-bound iron. I. Studies in normal rats.

作者信息

Awai M, Chipman B, Brown E B

出版信息

J Lab Clin Med. 1975 May;85(5):769-84.

PMID:1123558
Abstract

Functional heterogeneity of iron atoms bound to transferrin as postulated by Fletcher and Huehns was demonstrated by in vivo studies in rats. Serum transferrin was selectively double-labeled by adding 59Fe to 90 per cent saturation of iron binding capacity, incubation with rat reticulocytes to reduce the saturation to 50 per cent or less, and then adding back 55Fe. Rats were killed at various times after intravenous injection of this double-labeled transferrin, and the ratios of 55Fe to 59Fe were measured in plasma, circulating erythrocytes, bone marrow and spleen heme, whole liver and isolated hepatic Kupffer and parenchymal cells, and in small intestinal segments. Selective uptake of erythroblast-oriented 55Fe was observed in red cells and heme from marrow and spleen; storage-oriented 59Fe was selectively removed by liver cells and small intestine. Greater polarization was achieved by using Fe3+-nitrilotriacetic acid instead of ferrous ammonium sulfate and by injecting transferrin selectively double-labeled at less than 50 per cent saturation. These studies confirm the hypothesis of Fletcher and Huehns that the iron atoms of transferrin are functionally different and support the concept that transferrin plays a selective role in the distribution of iron to tissues in the rat.

摘要

弗莱彻和休恩斯所假定的与转铁蛋白结合的铁原子的功能异质性,在大鼠体内研究中得到了证实。通过将59Fe添加至铁结合能力的90%饱和度,与大鼠网织红细胞孵育以将饱和度降低至50%或更低,然后再添加55Fe,对血清转铁蛋白进行选择性双标记。在静脉注射这种双标记转铁蛋白后的不同时间点处死大鼠,并测量血浆、循环红细胞、骨髓和脾脏血红素、全肝以及分离的肝库普弗细胞和实质细胞以及小肠段中55Fe与59Fe的比率。在来自骨髓和脾脏的红细胞和血红素中观察到了向成红细胞定向的55Fe的选择性摄取;向储存定向的59Fe被肝细胞和小肠选择性清除。通过使用Fe3 + -次氮基三乙酸代替硫酸亚铁铵,并通过注射饱和度低于50%的选择性双标记转铁蛋白,实现了更大的极化。这些研究证实了弗莱彻和休恩斯的假设,即转铁蛋白的铁原子在功能上是不同的,并支持转铁蛋白在大鼠体内铁向组织的分布中起选择性作用的概念。

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