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Binding and uptake of H-ferritin are mediated by human transferrin receptor-1

铁蛋白 转铁蛋白受体 转铁蛋白 受体 内体 生物化学 体外 化学 细胞生物学 结合位点 细胞 生物
作者
Li Li,Celia J. Fang,James C. Ryan,Eréne C. Niemi,José Antonio Lebrón,Pamela J. Björkman,Hisashi Arase,Frank M. Torti,Suzy V. Torti,Mary C. Nakamura,William E. Seaman
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [National Academy of Sciences]
卷期号:107 (8): 3505-3510 被引量:482
标识
DOI:10.1073/pnas.0913192107
摘要

Ferritin is a spherical molecule composed of 24 subunits of two types, ferritin H chain (FHC) and ferritin L chain (FLC). Ferritin stores iron within cells, but it also circulates and binds specifically and saturably to a variety of cell types. For most cell types, this binding can be mediated by ferritin composed only of FHC (HFt) but not by ferritin composed only of FLC (LFt), indicating that binding of ferritin to cells is mediated by FHC but not FLC. By using expression cloning, we identified human transferrin receptor-1 (TfR1) as an important receptor for HFt with little or no binding to LFt. In vitro, HFt can be precipitated by soluble TfR1, showing that this interaction is not dependent on other proteins. Binding of HFt to TfR1 is partially inhibited by diferric transferrin, but it is hindered little, if at all, by HFE. After binding of HFt to TfR1 on the cell surface, HFt enters both endosomes and lysosomes. TfR1 accounts for most, if not all, of the binding of HFt to mitogen-activated T and B cells, circulating reticulocytes, and all cell lines that we have studied. The demonstration that TfR1 can bind HFt as well as Tf raises the possibility that this dual receptor function may coordinate the processing and use of iron by these iron-binding molecules.

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