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结肠细胞对吡哆醇的摄取:一种特定的、受调控的载体介导过程。

Pyridoxine uptake by colonocytes: a specific and regulated carrier-mediated process.

作者信息

Said Zainab M, Subramanian Veedamali S, Vaziri Nosratola D, Said Hamid M

机构信息

Department of Medicine and Physiology, University of California, Irvine, California, USA.

出版信息

Am J Physiol Cell Physiol. 2008 May;294(5):C1192-7. doi: 10.1152/ajpcell.00015.2008. Epub 2008 Mar 19.

Abstract

The water-soluble vitamin B6 (pyridoxine) is important for normal cellular functions, growth, and development. The vitamin is obtained from two exogenous sources: a dietary source, which is absorbed in the small intestine, and a bacterial source, where the vitamin is synthesized in significant quantities by the normal microflora of the large intestine. Evidence exists to suggest the bioavailability of the latter source of the vitamin, but nothing is known about the mechanism involved and its regulation. In this study, we addressed these issues using young adult mouse colonic epithelial (YAMC) cells and human colonic apical membrane vesicles (AMV) as models and using [3H]pyridoxine as the uptake substrate. The results showed the initial rate of [3H]pyridoxine uptake by YAMC cells to be 1) energy- and temperature- (but not Na-) dependent and to occur without metabolic alteration in the transported substrate; 2) saturable as a function of concentration with an apparent Km and Vmax of 2.1 +/- 0.5 muM and 53.4 +/- 4.3 pmol.mg protein(-1).3 min(-1), respectively; 3) cis-inhibited by unlabeled pyridoxine and its structural analogs, but not by the unrelated compounds theophylline, penicillamine, and isoniazid; 4) trans-stimulated by unlabeled pyridoxine; 5) amiloride sensitive; and 6) regulated by extracellular and intracellular factors. Uptake of pyridoxine by native human colonic AMV was also found to involve a carrier-mediated process. These studies demonstrate, for the first time, the functional existence of a specific and regulatable carrier-mediated process for pyridoxine uptake by mammalian colonocytes.

摘要

水溶性维生素B6(吡哆醇)对正常细胞功能、生长和发育至关重要。该维生素有两个外源来源:一是饮食来源,在小肠中被吸收;二是细菌来源,大肠中的正常微生物群可大量合成该维生素。有证据表明后一种来源的维生素具有生物利用度,但对其涉及的机制及其调节尚不清楚。在本研究中,我们以年轻成年小鼠结肠上皮(YAMC)细胞和人结肠顶端膜囊泡(AMV)为模型,以[3H]吡哆醇作为摄取底物,探讨了这些问题。结果显示,YAMC细胞对[3H]吡哆醇的初始摄取速率为:1)能量和温度依赖性(但非钠依赖性),且转运底物无代谢改变;2)作为浓度的函数呈饱和状态,表观Km和Vmax分别为2.1±0.5μM和53.4±4.3 pmol·mg蛋白-1·3 min-1;3)被未标记的吡哆醇及其结构类似物顺式抑制,但不受无关化合物茶碱、青霉胺和异烟肼抑制;4)被未标记的吡哆醇反式刺激;5)对氨氯地平敏感;6)受细胞外和细胞内因子调节。还发现天然人结肠AMV对吡哆醇的摄取涉及载体介导过程。这些研究首次证明了哺乳动物结肠细胞摄取吡哆醇存在一种特异性且可调节的载体介导过程。

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