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首页> 外文期刊>American Journal of Physiology >Cellular localization of divalent metal transporter DMT-1 in rat kidney.
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Cellular localization of divalent metal transporter DMT-1 in rat kidney.

机译:大鼠肾脏中二价金属转运体DMT-1的细胞定位。

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We have demonstrated that the kidney plays an important role in iron balance and that metabolically significant reabsorption of this ion occurs in the loop of Henle and the collecting ducts [Wareing M, Ferguson CJ, Green R, Riccardi D, and Smith CP. J Physiol (Lond) 524: 581-586, 2000]. To test the possibility that the divalent metal transporter DMT1 (Gunshin H, Mackenzie B, Berger UV, Gunshin Y, Romero MF, Boron WF, Nussberger S, Gollan JL, and Hediger MA. Nature 388: 482-488, 1997) could represent the apical route for iron entry in the kidney, we raised and affinity-purified an anti-DMT-1 polyclonal antibody and determined DMT-1 distribution in rat kidney by Western analysis, immunofluorescence, and confocal microscopy. The strongest DMT1-specific (i.e., peptide-protectable) immunoreactivity was found in the collecting ducts, in both principal and intercalated cells. Thick ascending limbs of Henle's loop and, more intensely, distal convoluted tubules exhibited apical immunostaining. Considerable intracellular DMT-1 immunoreactivity was seen throughout the nephron, particularly in S3 segments. The described distribution of DMT-1 protein is in agreement with our previous identification of nephron sites of iron reabsorption, suggesting that DMT-1 provides the molecular mechanism for apical iron entry in the distal nephron but not in the proximal tubule. Basolateral iron exit may be facilitated by a different system.
机译:我们已经证明肾脏在铁平衡中起重要作用,并且该离子的代谢显着重吸收发生在Henle和收集管的环中[Wareing M,Ferguson CJ,Green R,Riccardi D和Smith Smith CP。 J Physiol(Lond)524:581-586,2000]。为了测试二价金属转运体DMT1(Gunshin H,Mackenzie B,Berger UV,Gunshin Y,Romero MF,Boron WF,Nussberger S,Gollan JL和Hediger MA.Nature 388:482-488,1997)的可能性作为肾脏中铁进入的根尖途径,我们提出了抗DMT-1多克隆抗体并进行了亲和纯化,并通过Western分析,免疫荧光和共聚焦显微镜确定了大鼠肾脏中DMT-1的分布。在主细胞和插层细胞中,在收集管中发现了最强的DMT1特异性(即肽可保护的)免疫反应性。亨利环的粗大上升肢,以及远端弯曲的小管更强烈地表现出顶端免疫染色。在整个肾单位,特别是在S3节段中观察到相当大的细胞内DMT-1免疫反应性。所描述的DMT-1蛋白分布与我们先前鉴定的铁重吸收肾单位相吻合,这表明DMT-1提供了远端铁而不是近端肾小管中根尖铁进入的分子机制。基底外侧铁出口可以通过不同的系统来促进。

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