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钠氢和钠锂交换由人类红细胞中的同一膜转运蛋白介导:一项核磁共振研究。

Na(+)-H+ and Na(+)-Li+ exchange are mediated by the same membrane transport protein in human red blood cells: an NMR investigation.

作者信息

Chi Y, Mo S, Mota de Freitas D

机构信息

Department of Chemistry, Loyola University of Chicago, Illinois 60626, USA.

出版信息

Biochemistry. 1996 Sep 24;35(38):12433-42. doi: 10.1021/bi960814l.

Abstract

Na(+)-H+ exchange is a transport system present in erythrocytes which plays an important role in the regulation of intracellular pH, cellular volume, and transmembrane ion transport. Na(+)-Li+ exchange has received much attention and has been investigated in more detail than have any of the other ion transport systems, because of its high reproducibility. Both red blood cell (RBC) Na(+)-H+ and Na(+)-Li+ exchange are elevated in essential hypertensive patients relative to normotensive individuals. RBC Na(+)-Li+ exchange may be a mode of operation of Na(+)-H+ exchange. Amiloride and its analogue, 5-(N,N-hexamethylene)amiloride (HMA), are well-known inhibitors of Na(+)-H+ exchange, whereas phloretin strongly inhibits Na(+)-Li+ exchange. In this study, we tested the effects of amiloride, HMA, and phloretin on Na(+)-Li+ exchange activity in intact RBCs by using atomic absorption. We investigated by using 7Li nuclear magnetic resonance (NMR) spectroscopy the effects of HMA and phloretin inhibition on Li+ efflux across resealed H(+)- and Li(+)-loaded RBC ghosts in the absence and presence of pH gradients. Amiloride inhibitory activities on both Na+ and Li+ binding to exposed RBC membranes under different pH conditions were also studied by 23Na and 7Li NMR relaxation time measurements. We found that Na(+)-Li+ exchange activity was inhibited by amiloride, HMA, and phloretin in suspensions of intact RBCs and of resealed RBC ghosts. Li+ efflux rates across resealed H(+)- and Li(+)-loaded RBC ghosts were significantly lower when a pH gradient was present, presumably because of the competition between Li+ and H+ for transport by the same transport protein. Amiloride had similar inhibitory constants on both Na+ and Li+ binding to RBC membranes (1021 +/- 48 M-1 vs 964 +/- 40 M-1 at pH 8.0; 731 +/- 147 M-1 vs 716 +/- 27 M-1 at pH 7.0). These results suggest that Na(+)-H+ exchange and Na(+)-Li+ exchange are mediated by the same RBC membrane transport protein.

摘要

钠氢交换是一种存在于红细胞中的转运系统,在细胞内pH值、细胞体积和跨膜离子转运的调节中起重要作用。钠锂交换因其高重复性而备受关注,并且比其他任何离子转运系统都得到了更详细的研究。与血压正常的个体相比,原发性高血压患者的红细胞(RBC)钠氢交换和钠锂交换均升高。红细胞钠锂交换可能是钠氢交换的一种运作模式。氨氯吡脒及其类似物5-(N,N-六亚甲基)氨氯吡脒(HMA)是众所周知的钠氢交换抑制剂,而根皮素强烈抑制钠锂交换。在本研究中,我们通过原子吸收法测试了氨氯吡脒、HMA和根皮素对完整红细胞中钠锂交换活性的影响。我们使用7Li核磁共振(NMR)光谱研究了在有无pH梯度的情况下,HMA和根皮素抑制对锂通过重新封闭的、加载了H+和Li+的红细胞血影流出的影响。我们还通过23Na和7Li NMR弛豫时间测量研究了在不同pH条件下氨氯吡脒对Na+和Li+与暴露的红细胞膜结合的抑制活性。我们发现,在完整红细胞悬浮液和重新封闭的红细胞血影中,氨氯吡脒、HMA和根皮素均抑制钠锂交换活性。当存在pH梯度时,锂通过重新封闭的、加载了H+和Li+的红细胞血影的流出速率显著降低,这可能是因为Li+和H+竞争同一转运蛋白进行转运。氨氯吡脒对Na+和Li+与红细胞膜结合的抑制常数相似(在pH 8.0时为1021±48 M-1对964±40 M-1;在pH 7.0时为731±147 M-1对716±27 M-1)。这些结果表明,钠氢交换和钠锂交换由同一红细胞膜转运蛋白介导。

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