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铁、锰和钴通过位于质膜上表达的Nramp1(Slc11a1)和Nramp2(Slc11a2)进行转运。

Iron, manganese, and cobalt transport by Nramp1 (Slc11a1) and Nramp2 (Slc11a2) expressed at the plasma membrane.

作者信息

Forbes John R, Gros Philippe

机构信息

Department of Biochemistry, McGill University, 3655 Sir William Osler Promenade, Montreal, QC, Canada, H3G1Y6.

出版信息

Blood. 2003 Sep 1;102(5):1884-92. doi: 10.1182/blood-2003-02-0425. Epub 2003 May 15.

Abstract

Mutations in the Nramp1 gene (Slc11a1) cause susceptibility to infection by intracellular pathogens. The Nramp1 protein is expressed at the phagosomal membrane of macrophages and neutrophils and is a paralog of the Nramp2 (Slc11a2) iron transporter. The Nramp1 transport mechanism at the phagosomal membrane has remained controversial. An Nramp1 protein modified by insertion of a hemagglutinin epitope into the predicted TM7/8 loop was expressed at the plasma membrane of Chinese hamster ovary cells as demonstrated by immunofluorescence and surface biotinylation. Experiments in Nramp1HA transfectants using the metal-sensitive fluorophors calcein and Fura2 showed that Nramp1HA can mediate Fe2+, Mn2+, and Co2+ uptake. Similar results were obtained in transport studies using radioisotopic 55Fe2+ and 54Mn2+. Nramp1HA transport was dependent on time, temperature, and acidic pH, occurring down the proton gradient. These experiments suggest that Nramp1HA may be a more efficient transporter of Mn2+ compared to Fe2+ and a more efficient Mn2+ transporter than Nramp2HA. The membrane topology and transport properties of Nramp1HA and Nramp2HA were indistinguishable, suggesting that Nramp1 divalent-metal transport at the phagosomal membrane is mechanistically similar to that of Nramp2 at the membrane of acidified endosomes. These results clarify the mechanism by which Nramp1 contributes to phagocyte defenses against infections.

摘要

Nramp1基因(Slc11a1)的突变会导致对细胞内病原体感染的易感性。Nramp1蛋白在巨噬细胞和中性粒细胞的吞噬体膜上表达,是Nramp2(Slc11a2)铁转运蛋白的旁系同源物。Nramp1在吞噬体膜上的转运机制一直存在争议。通过免疫荧光和表面生物素化证明,将血凝素表位插入预测的TM7/8环修饰的Nramp1蛋白在中国仓鼠卵巢细胞的质膜上表达。使用金属敏感荧光染料钙黄绿素和Fura2对Nramp1HA转染子进行的实验表明,Nramp1HA可以介导Fe2+、Mn2+和Co2+的摄取。使用放射性同位素55Fe2+和54Mn2+进行的转运研究也得到了类似的结果。Nramp1HA转运依赖于时间、温度和酸性pH,沿质子梯度发生。这些实验表明,与Fe2+相比,Nramp1HA可能是一种更有效的Mn2+转运体,并且比Nramp2HA更有效地转运Mn2+。Nramp1HA和Nramp2HA的膜拓扑结构和转运特性无法区分,这表明Nramp1在吞噬体膜上的二价金属转运机制与Nramp2在酸化内体膜上的转运机制在机械上相似。这些结果阐明了Nramp1对吞噬细胞抗感染防御作用的机制。

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