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Slc39a14基因编码ZIP14,一种金属/碳酸氢盐共转运蛋白:与ZIP8转运蛋白的相似性。

Slc39a14 gene encodes ZIP14, a metal/bicarbonate symporter: similarities to the ZIP8 transporter.

作者信息

Girijashanker Kuppuswami, He Lei, Soleimani Manoocher, Reed Jodie M, Li Hong, Liu Zhiwei, Wang Bin, Dalton Timothy P, Nebert Daniel W

机构信息

Department of Environmental Health, University of Cincinnati Medical Center, P.O. Box 670056, Cincinnati, OH 45267-0056, USA.

出版信息

Mol Pharmacol. 2008 May;73(5):1413-23. doi: 10.1124/mol.107.043588. Epub 2008 Feb 12.

Abstract

The mouse and human genomes contain 14 highly conserved SLC39 genes. Viewed from an evolutionary perspective, SLC39A14 and SLC39A8 are the most closely related, each having three noncoding exons 1. However, SLC39A14 has two exons 4, giving rise to Zrt- and Irt-related protein (ZIP)ZIP14A and ZIP14B alternatively spliced products. C57BL/6J mouse ZIP14A expression is highest in liver, duodenum, kidney, and testis; ZIP14B expression is highest in liver, duodenum, brain, and testis; and ZIP8 is highest in lung, testis, and kidney. We studied ZIP14 stably retroviral-infected mouse fetal fibroblast cultures and transiently transfected Madin-Darby canine kidney (MDCK) polarized epithelial cells. Our findings include: 1) ZIP14-mediated cadmium uptake is proportional to cell toxicity, but manganese is not; 2) ZIP14B has a higher affinity than ZIP14A toward Cd(2+) (K(m) = 0.14 versus 1.1 microM) and Mn(2+) uptake (K(m) = 4.4 versus 18.2 microM); 3) ZIP14A- and ZIP14B-mediated Cd(2+) uptake is most inhibited by Zn(2+), and next by Mn(2+) and Cu(2+); 4) like ZIP8, ZIP14A- and ZIP14B-mediated Cd(2+) uptake is dependent on extracellular HCO(3)(-); 5) like ZIP8, ZIP14 transporters are localized on the apical surface of MDCK-ZIP cells; and 6) like ZIP8, ZIP14 proteins are glycosylated. Tissues such as intestine and liver, located between the environment and the animal, show high levels of ZIP14; given the high affinity for ZIP14, Cd(2+) is likely to act as a rogue hitchhiker-displacing Zn(2+) or Mn(2+) and entering the body to cause unwanted cell damage and disease.

摘要

小鼠和人类基因组包含14个高度保守的溶质载体家族39(SLC39)基因。从进化的角度来看,SLC39A14和SLC39A8关系最为密切,每个都有三个非编码外显子1。然而,SLC39A14有两个外显子4,产生了锌转运蛋白(Zrt)和铁调节转运蛋白(Irt)相关蛋白(ZIP)ZIP14A和ZIP14B的可变剪接产物。C57BL/6J小鼠中ZIP14A在肝脏、十二指肠、肾脏和睾丸中表达最高;ZIP14B在肝脏、十二指肠、大脑和睾丸中表达最高;而ZIP8在肺、睾丸和肾脏中表达最高。我们研究了稳定逆转录病毒感染的小鼠胎儿成纤维细胞培养物以及瞬时转染的犬肾(MDCK)极化上皮细胞中的ZIP14。我们的研究结果包括:1)ZIP14介导的镉摄取与细胞毒性成正比,但锰摄取并非如此;2)ZIP14B对Cd(2+)(K(m)=0.14对1.1微摩尔)和Mn(2+)摄取(K(m)=4.4对18.2微摩尔)的亲和力高于ZIP14A;3)ZIP14A和ZIP14B介导的Cd(2+)摄取受Zn(2+)抑制作用最强,其次是Mn(2+)和Cu(2+);4)与ZIP8一样,ZIP14A和ZIP14B介导的Cd(2+)摄取依赖于细胞外HCO(3)(-);5)与ZIP8一样,ZIP14转运蛋白定位于MDCK-ZIP细胞的顶端表面;6)与ZIP8一样,ZIP14蛋白是糖基化的。肠道和肝脏等位于环境与动物之间的组织中ZIP14水平较高;鉴于ZIP14对镉有高亲和力,Cd(2+)可能作为一个“不速之客”——取代Zn(2+)或Mn(2+)并进入体内,导致不必要的细胞损伤和疾病。

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