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HFE与转铁蛋白在溶液中和细胞表面直接竞争转铁蛋白受体。

HFE and transferrin directly compete for transferrin receptor in solution and at the cell surface.

作者信息

Giannetti Anthony M, Björkman Pamela J

机构信息

Graduate Option in Biochemistry and Molecular Biophysics, California Institute of Technology, Pasadena, CA 91125, USA.

出版信息

J Biol Chem. 2004 Jun 11;279(24):25866-75. doi: 10.1074/jbc.M401467200. Epub 2004 Mar 31.

Abstract

Transferrin receptor (TfR) is a dimeric cell surface protein that binds both the serum iron transport protein transferrin (Fe-Tf) and HFE, the protein mutated in patients with the iron overload disorder hereditary hemochromatosis. HFE and Fe-Tf can bind simultaneously to TfR to form a ternary complex, but HFE binding to TfR lowers the apparent affinity of the Fe-Tf/TfR interaction. This apparent affinity reduction could result from direct competition between HFE and Fe-Tf for their overlapping binding sites on each TfR polypeptide chain, from negative cooperativity, or from a combination of both. To explore the mechanism of the affinity reduction, we constructed a heterodimeric TfR that contains mutations such that one TfR chain binds only HFE and the other binds only Fe-Tf. Binding studies using a heterodimeric form of soluble TfR demonstrate that TfR does not exhibit cooperativity in heterotropic ligand binding, suggesting that some or all of the effects of HFE on iron homeostasis result from competition with Fe-Tf for TfR binding. Experiments using transfected cell lines demonstrate a physiological role for this competition in altering HFE trafficking patterns.

摘要

转铁蛋白受体(TfR)是一种二聚体细胞表面蛋白,它能结合血清铁转运蛋白转铁蛋白(Fe-Tf)以及遗传性血色素沉着症(一种铁过载疾病)患者体内发生突变的蛋白质HFE。HFE和Fe-Tf可以同时与TfR结合形成三元复合物,但HFE与TfR的结合会降低Fe-Tf/TfR相互作用的表观亲和力。这种表观亲和力的降低可能是由于HFE和Fe-Tf在每个TfR多肽链上重叠的结合位点存在直接竞争、负协同效应或两者兼而有之。为了探究亲和力降低的机制,我们构建了一种异源二聚体TfR,其中一个TfR链只结合HFE,另一个只结合Fe-Tf。使用可溶性TfR的异源二聚体形式进行的结合研究表明,TfR在异源配体结合中不表现出协同性,这表明HFE对铁稳态的部分或全部影响是由于与Fe-Tf竞争TfR结合所致。使用转染细胞系进行的实验证明了这种竞争在改变HFE运输模式方面的生理作用。

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