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转铁蛋白受体1

Transferrin receptor 1.

作者信息

Aisen Philip

机构信息

Department of Physiology and Biophysics, Albert Einstein College of Medicine, 1300 Morris Park Avenue, Bronx, NY 10461, USA.

出版信息

Int J Biochem Cell Biol. 2004 Nov;36(11):2137-43. doi: 10.1016/j.biocel.2004.02.007.

Abstract

With the discovery that transferrin serves as the iron source for hemoglobin-synthesizing immature red blood cells came the demonstration that a cell surface receptor, now known as transferrin receptor 1, is required for iron delivery from transferrin to cells. (A recently described second transferrin receptor, with as yet poorly understood function, will not be discussed in this brief review.) In succeeding years transferrin receptor 1 was established as a gatekeeper for regulating iron uptake by most cells, and the transferrin-to-cell endocytic pathway characterized in detail. HFE, the protein incriminated in the pathogenesis of hereditary hemochromatosis, a disorder of progressive and toxic iron overload, competes with transferrin for binding to receptor, thereby impeding the uptake of iron from transferrin. Mutation of HFE destroys this competition, thus facilitating access of transferrin and its iron to cells. Availability of the crystal structure of transferrin receptor 1, along with those of transferrin and HFE, opened research on molecular mapping of the transferrin-HFE- transferrin receptor interfaces by correlated synchrotron-generated hydroxyl radical footprinting and cryo-electron microscopy. The emerging challenge is to relate structure to the functional effects of receptor binding on the iron-binding and iron-releasing properties of transferrin within the iron-dependent cell.

摘要

随着转铁蛋白作为合成血红蛋白的未成熟红细胞的铁源这一发现,人们证实了一种细胞表面受体(现称为转铁蛋白受体1)是铁从转铁蛋白传递至细胞所必需的。(本文简要综述不讨论最近描述的第二种转铁蛋白受体,其功能尚不清楚。)在随后的几年里,转铁蛋白受体1被确立为大多数细胞调节铁摄取的守门人,并且详细描述了转铁蛋白至细胞的内吞途径。HFE是一种与遗传性血色素沉着症(一种进行性毒性铁过载疾病)发病机制有关的蛋白质,它与转铁蛋白竞争结合受体,从而阻碍铁从转铁蛋白的摄取。HFE的突变破坏了这种竞争,从而促进了转铁蛋白及其铁进入细胞。转铁蛋白受体1的晶体结构以及转铁蛋白和HFE的晶体结构的可得性,开启了通过相关的同步加速器产生的羟基自由基足迹法和冷冻电子显微镜对转铁蛋白-HFE-转铁蛋白受体界面进行分子图谱研究。新出现的挑战是将结构与受体结合对铁依赖性细胞内转铁蛋白的铁结合和铁释放特性的功能影响联系起来。

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