A carrier-mediated mechanism for pyridoxine uptake by human intestinal epithelial Caco-2 cells: regulation by a PKA-mediated pathway.

IF 4.7 2区生物学 Q2 CELL BIOLOGY

American journal of physiology. Cell physiology Pub Date : 2003-11-01 Epub Date: 2003-07-16 DOI:10.1152/ajpcell.00204.2003

Hamid M Said, Alvaro Ortiz, Thomas Y Ma

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引用次数: 86

Abstract

Vitamin B6 is essential for cellular functions and growth due to its involvement in important metabolic reactions. Humans and other mammals cannot synthesize vitamin B6 and thus must obtain this micronutrient from exogenous sources via intestinal absorption. The intestine, therefore, plays a central role in maintaining and regulating normal vitamin B6 homeostasis. Due to the water-soluble nature of vitamin B6 and the demonstration that transport of other water-soluble vitamins in intestinal epithelial cells involves specialized carrier-mediated mechanisms, we hypothesized that transport of vitamin B6 in these cells is also carrier mediated in nature. To test this hypothesis, we examined pyridoxine transport in a model system for human enterocytes, the human-derived intestinal epithelial Caco-2 cells. The results showed pyridoxine uptake to be 1) linear with time for up to 10 min of incubation and to occur with minimal metabolic alteration in the transported substrate, 2) temperature and energy dependent but Na+ independent, 3) pH dependent with higher uptake at acidic compared with alkaline pHs, 4) saturable as a function of concentration (at buffer pH 5.5 but not 7.4) with an apparent Michaelis-Menten constant (Km) of 11.99 +/- 1.41 microM and a maximal velocity (Vmax) of 67.63 +/- 3.87 pmol. mg protein-1. 3 min-1, 5) inhibited by pyridoxine structural analogs (at buffer pH 5.5 but not 7.4) but not by unrelated compounds, and 6) inhibited in a competitive manner by amiloride with an apparent inhibitor constant (Ki) of 0.39 mM. We also examined the possible regulation of pyridoxine uptake by specific intracellular regulatory pathways. The results showed that whereas modulators of PKC, Ca+2/calmodulin (CaM), and nitric oxide (NO)-mediated pathways had no effect on pyridoxine uptake, modulators of PKA-mediated pathway were found to cause significant reduction in pyridoxine uptake. This reduction was mediated via a significant inhibition in the Vmax, but not the apparent Km, of the pyridoxine uptake process. These results demonstrate, for the first time, the involvement of a specialized carrier-mediated mechanism for pyridoxine uptake by intestinal epithelial cells. This system is pH dependent and amiloride sensitive and appears to be under the regulation of an intracellular PKA-mediated pathway.

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人肠上皮Caco-2细胞对吡哆醇摄取的载体介导机制:pka介导途径的调控

维生素B6是细胞功能和生长所必需的，因为它参与重要的代谢反应。人类和其他哺乳动物不能合成维生素B6，因此必须通过肠道吸收从外源性来源获得这种微量营养素。因此，肠道在维持和调节正常的维生素B6体内平衡中起着核心作用。由于维生素B6的水溶性以及其他水溶性维生素在肠上皮细胞中的转运涉及特殊的载体介导机制，我们假设维生素B6在这些细胞中的转运本质上也是载体介导的。为了验证这一假设，我们在人肠细胞模型系统中检测了吡哆醇的转运，人源性肠上皮Caco-2细胞。结果表明，吡哆醇的摄取与时间呈线性关系，最长可达10分钟，并且在运输的底物中代谢变化最小;2)温度和能量依赖但不依赖于Na+; 3) pH依赖于酸性，与碱性pH相比，酸性pH的摄取更高。4)可饱和(缓冲液pH为5.5而非7.4)，表观Michaelis-Menten常数(Km)为11.99 +/- 1.41 μ m，最大流速(Vmax)为67.63 +/- 3.87 pmol。毫克蛋白1。3分钟- 1,5)被吡哆醇结构类似物(缓冲pH为5.5但不是7.4)抑制，但不被无关的化合物抑制，6)被阿米洛利以竞争方式抑制，其明显的抑制剂常数(Ki)为0.39 mM。我们还研究了通过特定的细胞内调节途径对吡哆醇摄取的可能调节。结果表明，PKC、Ca+2/钙调素(CaM)和一氧化氮(NO)介导途径的调节剂对吡哆醇摄取没有影响，而pka介导途径的调节剂可显著降低吡哆醇摄取。这种减少是通过显著抑制Vmax介导的，而不是明显的Km，吡哆醇摄取过程。这些结果首次证明了肠上皮细胞对吡哆醇摄取的特殊载体介导机制的参与。该系统是pH依赖性和阿米洛利敏感的，似乎是在细胞内pka介导的途径的调节下。

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来源期刊

American journal of physiology. Cell physiology 生物-生理学

CiteScore

9.10

自引率

1.80%

发文量

252

审稿时长

1 months

期刊介绍： The American Journal of Physiology-Cell Physiology is dedicated to innovative approaches to the study of cell and molecular physiology. Contributions that use cellular and molecular approaches to shed light on mechanisms of physiological control at higher levels of organization also appear regularly. Manuscripts dealing with the structure and function of cell membranes, contractile systems, cellular organelles, and membrane channels, transporters, and pumps are encouraged. Studies dealing with integrated regulation of cellular function, including mechanisms of signal transduction, development, gene expression, cell-to-cell interactions, and the cell physiology of pathophysiological states, are also eagerly sought. Interdisciplinary studies that apply the approaches of biochemistry, biophysics, molecular biology, morphology, and immunology to the determination of new principles in cell physiology are especially welcome.