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Phosphate transporters and their function

机译:磷酸盐转运蛋白及其功能

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Plasma phosphate concentration is maintained within a relatively narrow range by control of renal reabsorption of filtered inorganic phosphate (Pi). Pi reabsorption is a transcellular process that occurs along the proximal tubule. Pi flux at the apical (luminal) brush border membrane represents the rate-limiting step and is mediated by three Na+-dependent Pi cotransporters (members of the SLC34 and SLC20 families). The putative proteins responsible for basolateral Pi flux have not been identified. The transport mechanism of the two kidney-specific SLC34 proteins (NaPi-IIa and NaPi-IIc) and of the ubiquitously expressed SLC20 protein (PiT-2) has been studied by heterologous expression to reveal important differences in kinetics, stoichiometry, and substrate specificity. Studies on the regulation of the abundance of the respective proteins highlight significant differences in the temporal responses to various hormonal and nonhormonal factors that can influence Pi homeostasis. The phenotypes of mice deficient in NaPi-IIa and NaPi-IIc indicate that NaPi-IIa is responsible for most Pi renal reabsorption. In contrast, in the human kidney, NaPi-IIc appears to have a relatively greater role. The physiological relevance of PiT-2 to Pi reabsorption remains to be elucidated.
机译:通过控制肾脏对已过滤的无机磷酸盐(Pi)的重吸收,可使血浆磷酸盐浓度保持在相对狭窄的范围内。 Pi重吸收是沿近端小管发生的跨细胞过程。顶端(管腔)刷状缘膜上的Pi通量代表了限速步骤,并由三个依赖Na +的Pi共转运蛋白(SLC34和SLC20家族的成员)介导。尚未确定负责基底外侧Pi通量的推定蛋白。通过异源表达研究了两种肾脏特异性SLC34蛋白(NaPi-IIa和NaPi-IIc)和普遍表达的SLC20蛋白(PiT-2)的转运机制,以揭示动力学,化学计量和底物特异性方面的重要差异。有关各种蛋白质丰度调节的研究突显了对各种可能影响Pi动态平衡的激素和非激素因子的时间反应的显着差异。 NaPi-IIa和NaPi-IIc缺陷型小鼠的表型表明,NaPi-IIa导致大部分Pi肾重吸收。相反,在人的肾脏中,NaPi-IIc似乎具有相对更大的作用。 PiT-2与Pi重吸收的生理相关性尚待阐明。

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