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Apical ammonia transport by the mouse inner medullary collecting duct cell (mIMCD-3).

机译:小鼠内髓样集合管细胞(mIMCD-3)的顶端氨运输。

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摘要

The collecting duct is the primary site of urinary ammonia secretion; the current study determines whether apical ammonia transport in the mouse inner medullary collecting duct cell (mIMCD-3) occurs via nonionic diffusion or a transporter-mediated process and, if the latter, presents the characteristics of this apical ammonia transport. We used confluent cells on permeable support membranes and examined apical uptake of the ammonia analog [(14)C]methylammonia ([(14)C]MA). mIMCD-3 cells exhibited both diffusive and saturable, transporter-mediated, nondiffusive apical [(14)C]MA transport. Transporter-mediated [(14)C]MA uptake had a K(m) of 7.0 +/- 1.5 mM and was competitively inhibited by ammonia with a K(i) of 4.3 +/- 2.0 mM. Transport activity was stimulated by both intracellular acidification and extracellular alkalinization, and it was unaltered by changes in membrane voltage, thereby functionally identifying an apical, electroneutral NH(4)(+)/H(+) exchange activity. Transport was bidirectional, consistent with a role in ammonia secretion. In addition, transport was not altered by Na(+) or K(+) removal, not inhibited by luminal K(+), and not mediated by apical H(+)-K(+)-ATPase, Na(+)-K(+)-ATPase, or Na(+)/H(+) exchange. Finally, mIMCD-3 cells express the recently identified ammonia transporter family member Rh C glycoprotein (RhCG) at its apical membrane. These studies indicate that the renal collecting duct cell mIMCD-3 has a novel apical, electroneutral Na(+)- and K(+)-independent NH(4)(+)/H(+) exchange activity, possibly mediated by RhCG, that is likely to mediate important components of collecting duct ammonia secretion.
机译:收集管是尿液氨分泌的主要部位。当前的研究确定了小鼠内髓收集管细胞(mIMCD-3)中的根尖氨转运是否通过非离子扩散或转运蛋白介导的过程发生,如果是后者,则表现出这种根尖氨转运的特征。我们在可渗透的支持膜上使用汇合的细胞,并检查了氨类似物[(14)C]甲基氨([(14)C] MA)的顶端吸收。 mIMCD-3细胞既具有扩散性又具有饱和性,是转运蛋白介导的非扩散性心尖[(14)C] MA转运。转运蛋白介导的[(14)C] MA摄取的K(m)为7.0 +/- 1.5 mM,并被氨竞争性抑制,其K(i)为4.3 +/- 2.0 mM。运输活性受到细胞内酸化和细胞外碱化的刺激,并且不受膜电压变化的影响,从而在功能上确定了根尖的,电子中性的NH(4)(+)/ H(+)交换活性。转运是双向的,与氨分泌中的作用一致。此外,转运不会因Na(+)或K(+)去除而改变,不受腔K(+)的抑制,并且不受顶端H(+)-K(+)-ATPase,Na(+)- K(+)-ATPase或Na(+)/ H(+)交换。最后,mIMCD-3细胞在其顶膜表达最近鉴定的氨转运蛋白家族成员Rh C糖蛋白(RhCG)。这些研究表明,肾脏收集导管细胞mIMCD-3具有可能由RhCG介导的新型心尖,电中性Na(+)-和K(+)独立的NH(4)(+)/ H(+)交换活性,可能会介导收集管道氨分泌的重要成分。

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