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铁蛋白转运蛋白中离子转运和抑制的结构基础。

Structural basis of ion transport and inhibition in ferroportin.

机构信息

Verna and Marrs McLean Department of Biochemistry and Molecular Biology, Baylor College of Medicine, Houston, TX, 77030, USA.

Department of Molecular Biology, Princeton University, Princeton, NJ, 08544, USA.

出版信息

Nat Commun. 2020 Nov 10;11(1):5686. doi: 10.1038/s41467-020-19458-6.

Abstract

Ferroportin is an iron exporter essential for releasing cellular iron into circulation. Ferroportin is inhibited by a peptide hormone, hepcidin. In humans, mutations in ferroportin lead to ferroportin diseases that are often associated with accumulation of iron in macrophages and symptoms of iron deficiency anemia. Here we present the structures of the ferroportin from the primate Philippine tarsier (TsFpn) in the presence and absence of hepcidin solved by cryo-electron microscopy. TsFpn is composed of two domains resembling a clamshell and the structure defines two metal ion binding sites, one in each domain. Both structures are in an outward-facing conformation, and hepcidin binds between the two domains and reaches one of the ion binding sites. Functional studies show that TsFpn is an electroneutral H/Fe antiporter so that transport of each Fe is coupled to transport of two H in the opposite direction. Perturbing either of the ion binding sites compromises the coupled transport of H and Fe. These results establish the structural basis of metal ion binding, transport and inhibition in ferroportin and provide a blueprint for targeting ferroportin in pharmacological intervention of ferroportin diseases.

摘要

铁蛋白是一种将细胞内铁释放到循环中的必需铁输出蛋白。铁蛋白受一种肽激素——hepcidin 抑制。在人类中,铁蛋白基因突变导致铁蛋白病,常伴有巨噬细胞中铁的积累和缺铁性贫血的症状。本文通过冷冻电镜解析了食蟹猴铁蛋白(TsFpn)在 hepcidin 存在和不存在两种状态下的结构。TsFpn 由两个类似于蛤壳的结构域组成,结构定义了两个金属离子结合位点,每个结构域一个。两种结构都呈向外开放构象,hepcidin 结合在两个结构域之间并到达一个离子结合位点。功能研究表明,TsFpn 是一种电中性的 H/Fe 反向转运体,因此每个 Fe 的转运都与相反方向的两个 H 的转运偶联。干扰任何一个离子结合位点都会破坏 H 和 Fe 的偶联转运。这些结果确立了铁蛋白中铁离子结合、转运和抑制的结构基础,并为铁蛋白病的铁蛋白靶向药物干预提供了蓝图。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ce9b/7655804/8e7741ee9838/41467_2020_19458_Fig1_HTML.jpg

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