Sugar and amino acid transport in animal cells.

U Hopfer
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Abstract

The molecular basis of intracellular metabolism of nutrients and its control is quite well understood in animal cells. Comparable knowledge about solute entry into cells is still lacking, as, in contrast to metabolism, no chemical reactions seem to be directly associated with the known nutrient transport. Nevertheless, translocations of sugars and amino acids across the plasma membrane are specific and controlled processes, biologically as well as chemically. Recent advances in techniques for isolation of plasma membranes have made it feasible to study transport properties of animal cells without the complications encoutered in viable cells. This approach has been applied to sugar and amino acid transport in plasma membranes of several tissues, and intact transport systems for D-glucose, D-fructose, neutral L-amino acids, and dipeptides have been demonstrated. This demonstration of intact transport systems in an in vitro setting accomplishes the first step in the direction of molecular isolation of transport systems. Furthermore, the information obtained about the transport mechanism catalyzed by some systems has settled controversies on active nutrient transport. For example, electrogenic cotransport of sodium and D-glucose or of sodium and neutral L-amino acids has been shown to form the basis for active, sodium-dependent absorption of these nutrients. A consequence of this type of mechanism is interaction between sugar and amino acid transport via the common charged cosubstrate sodium. Moreover, different types of transport systems for the same substrate have been demonstrated in the luminal and contraluminal regions of the plasma membrane of epithelial cells, which explains unidirectional transepithelial transport. The luminal membrane contains sodium-dependent, active transport systems, and the contraluminal membrane passive, facilitated diffusion systems. In vivo, the lower intracellular sodium potential would result in concentrative nutrient uptake from the lumen, but would not influence exit on the contraluminal side. Variations in the electrical components of the sodium potential, which have not been measured, may explain apparently contradicting results on active sugar and amino acid transport with various tissue preparations.

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糖和氨基酸在动物细胞中的运输。
在动物细胞中,细胞内营养物质代谢及其控制的分子基础已被很好地理解。关于溶质进入细胞的可比知识仍然缺乏,因为与代谢相反,似乎没有化学反应与已知的营养物质运输直接相关。尽管如此,糖和氨基酸在质膜上的易位是特定的和受控的过程,在生物学和化学上都是如此。质膜分离技术的最新进展使研究动物细胞的转运特性成为可能,而不会遇到在活细胞中遇到的并发症。该方法已被应用于糖和氨基酸在几种组织的质膜中的运输,并且已经证明了d -葡萄糖、d -果糖、中性l -氨基酸和二肽的完整运输系统。在体外环境中完整转运系统的演示完成了转运系统分子分离方向的第一步。此外,对某些系统催化的转运机制的研究也解决了有关营养物质活性转运的争议。例如,钠和d -葡萄糖或钠和中性l -氨基酸的电致共转运已被证明是这些营养物质的活性、钠依赖性吸收的基础。这种机制的结果是糖和氨基酸之间的相互作用,通过共同带电的共底物钠进行运输。此外,在上皮细胞的质膜的管腔区和管腔区,已经证明了相同底物的不同类型的运输系统,这解释了单向的跨上皮运输。管腔膜包含钠依赖、主动转运系统和对管膜被动、促进扩散系统。在体内,较低的细胞内钠电位会导致从腔内集中摄取营养,但不会影响对腔侧的排出。钠电位的电成分的变化尚未被测量,这可能解释了不同组织制剂对活性糖和氨基酸运输的明显矛盾的结果。
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