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鉴定一种新型的钠偶联柠檬酸铁转运系统,该系统不同于哺乳动物的INDY,用于哺乳动物细胞摄取柠檬酸。

Identification of a novel Na-coupled Fe-citrate transport system, distinct from mammalian INDY, for uptake of citrate in mammalian cells.

作者信息

Ogura Jiro, Babu Ellappan, Miyauchi Seiji, Ramachandran Sabarish, Nemeth Elizebeta, Bhutia Yangzom D, Ganapathy Vadivel

机构信息

Department of Cell Biology and Biochemistry, Texas Tech University Health Sciences Center, Lubbock, TX, 79430, USA.

Department of Pharmaceutics, Toho University, Funabashi, Chiba, 274-8510, Japan.

出版信息

Sci Rep. 2018 Feb 6;8(1):2519. doi: 10.1038/s41598-018-20620-w.

Abstract

NaCT is a Na-coupled transporter for citrate expressed in hepatocytes and neurons. It is the mammalian ortholog of INDY (I'm Not Dead Yet), a transporter which modifies lifespan in Drosophila. Here we describe a hitherto unknown transport system for citrate in mammalian cells. When liver and mammary epithelial cells were pretreated with the iron supplement ferric ammonium citrate (FAC), uptake of citrate increased >10-fold. Iron chelators abrogated the stimulation of citrate uptake in FAC-treated cells. The iron exporter ferroportin had no role in this process. The stimulation of citrate uptake also occurred when Fe was added during uptake without pretreatment. Similarly, uptake of Fe was enhanced by citrate. The Fe-citrate uptake was coupled to Na. This transport system was detectable in primary hepatocytes and neuronal cell lines. The functional features of this citrate transport system distinguish it from NaCT. Loss-of-function mutations in NaCT cause early-onset epilepsy and encephalopathy; the newly discovered Na-coupled Fe-citrate transport system might offer a novel treatment strategy for these patients to deliver citrate into affected neurons independent of NaCT. It also has implications to iron-overload conditions where circulating free iron increases, which would stimulate cellular uptake of citrate and consequently affect multiple metabolic pathways.

摘要

NaCT是一种在肝细胞和神经元中表达的用于转运柠檬酸盐的钠偶联转运蛋白。它是INDY(我还没死)在哺乳动物中的直系同源物,INDY是一种能改变果蝇寿命的转运蛋白。在此,我们描述了一种哺乳动物细胞中迄今未知的柠檬酸盐转运系统。当肝和乳腺上皮细胞用铁补充剂柠檬酸铁铵(FAC)预处理时,柠檬酸盐的摄取增加了10倍以上。铁螯合剂消除了FAC处理细胞中对柠檬酸盐摄取的刺激作用。铁输出蛋白铁转运蛋白在此过程中不起作用。在没有预处理的摄取过程中添加铁时,也会发生对柠檬酸盐摄取的刺激作用。同样,柠檬酸盐可增强铁的摄取。铁-柠檬酸盐的摄取与钠偶联。这种转运系统在原代肝细胞和神经元细胞系中均可检测到。这种柠檬酸盐转运系统的功能特性使其有别于NaCT。NaCT功能丧失突变会导致早发性癫痫和脑病;新发现的钠偶联铁-柠檬酸盐转运系统可能为这些患者提供一种新的治疗策略,即不依赖NaCT将柠檬酸盐输送到受影响的神经元中。它也与铁过载情况有关,在铁过载时循环游离铁增加,这会刺激细胞对柠檬酸盐的摄取,从而影响多种代谢途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5403/5802838/46a8756e0bb0/41598_2018_20620_Fig1_HTML.jpg

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