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乳铁蛋白和转铁蛋白与人原单核细胞系U937的结合。对铁摄取和释放的影响。

Binding of lactoferrin and transferrin to the human promonocytic cell line U937. Effect on iron uptake and release.

作者信息

Ismail M, Brock J H

机构信息

University Department of Immunology, Western Infirmary, Glasgow, Scotland, United Kingdom.

出版信息

J Biol Chem. 1993 Oct 15;268(29):21618-25.

PMID:8408013
Abstract

We have compared the ability of lactoferrin and transferrin to interact with and donate iron to the monocytic cell line U937. About 10 times more lactoferrin was bound than transferrin, but most lactoferrin bound nonspecifically, and the degree of specific binding was similar for both proteins (2-3 x 10(6) sites/cell). The binding affinity for lactoferrin (83 nM) was about 4-fold lower than for transferrin (21 nM). Lactoferrin did not inhibit binding of transferrin, or vice versa. Binding of lactoferrin was not inhibited by 30 mM glucose or fucose nor by incubating the cells with heparinase. Transferrin, but not lactoferrin, was internalized, and 3 mM primaquine caused intracellular accumulation of transferrin but not lactoferrin. The cells rapidly acquired iron from transferrin, but uptake from lactoferrin was 10-fold slower and probably resulted from transfer of 59Fe from lactoferrin to unlabeled transferrin during culture. Lactoferrin, but not transferrin, released iron to the extracellular medium when bound to U937 cells. Lactoferrin inhibited cellular uptake of iron from Fe-nitrilotriacetate but not from transferrin. It is concluded that transferrin, but not lactoferrin, acts as an iron donor to U937 cells. Lactoferrin may regulate uptake of potentially toxic non-transferrin-bound iron.

摘要

我们比较了乳铁蛋白和转铁蛋白与单核细胞系U937相互作用并向其提供铁的能力。乳铁蛋白的结合量比转铁蛋白多约10倍,但大多数乳铁蛋白是非特异性结合,两种蛋白质的特异性结合程度相似(2 - 3×10⁶个位点/细胞)。乳铁蛋白的结合亲和力(83 nM)比转铁蛋白(21 nM)低约4倍。乳铁蛋白不抑制转铁蛋白的结合,反之亦然。30 mM葡萄糖或岩藻糖以及用肝素酶处理细胞均不抑制乳铁蛋白的结合。转铁蛋白可被内化,但乳铁蛋白不能,3 mM伯氨喹导致转铁蛋白在细胞内蓄积,但不影响乳铁蛋白。细胞能迅速从转铁蛋白获取铁,但从乳铁蛋白的摄取速度慢10倍,可能是由于培养过程中59Fe从乳铁蛋白转移至未标记的转铁蛋白所致。当与U937细胞结合时,乳铁蛋白可将铁释放到细胞外培养基中,但转铁蛋白不能。乳铁蛋白抑制细胞从次氮基三乙酸铁摄取铁,但不抑制从转铁蛋白摄取铁。结论是,转铁蛋白而非乳铁蛋白可作为U937细胞的铁供体。乳铁蛋白可能调节对潜在有毒的非转铁蛋白结合铁的摄取。

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