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柠檬酸盐对前列腺上皮细胞中高亲和力天冬氨酸转运的调节作用

Citrate modulation of high-affinity aspartate transport in prostate epithelial cells.

作者信息

Costello L C, Lao L, Franklin R

机构信息

Department of Physiology, Dental School, University of Maryland, Baltimore 21201.

出版信息

Cell Mol Biol (Noisy-le-grand). 1993 Jul;39(5):515-24.

PMID:8104067
Abstract

Prostate secretory epithelial cells have the unique and highly specialized function of accumulating and secreting extraordinarily high levels of citrate. Aspartate is a major four-carbon source of oxaloacetate required for the net synthesis of citrate by these cells. The prostate epithelial cells contain a Na(+)-coupled, high-affinity aspartate transporter which permits the cells to accumulate aspartate from circulation against a large concentration gradient. Because of this unique relationship between aspartate and citrate, it was important to determine if citrate modulated the high-affinity transport of aspartate into prostate epithelial cells. The current studies with freshly prepared prostate epithelial cells obtained from rat ventral prostate demonstrated that citrate exerted two effects on aspartate transport. Physiological levels of extracellular citrate (i.e., equivalent to circulating levels) markedly inhibited (cis-inhibitory effect) aspartate transport. In contrast, intracellular citrate at concentrations associated with normal in situ cells resulted in two levels of stimulation of aspartate transport. A 4-fold increase in aspartate transport occurred when the intracellular citrate was increased up to 500 nmols/g, and an 11-fold increase resulted when the intracellular citrate concentration was elevated to 1800 nmols/g (which is uniquely characteristic of prostate cells). The combined effect of the cis-inhibitory and trans-stimulatory actions of citrate was a consistent 1-2 fold increase in aspartate transport. These studies support the concept that citrate is a physiological regulator of the high-affinity transport of aspartate into prostate secretory epithelial cells in association with the unique and highly specialized function of net citrate production and secretion.

摘要

前列腺分泌上皮细胞具有独特且高度专业化的功能,即积累和分泌极高水平的柠檬酸盐。天冬氨酸是这些细胞净合成柠檬酸盐所需草酰乙酸的主要四碳来源。前列腺上皮细胞含有一种钠偶联的高亲和力天冬氨酸转运体,它使细胞能够逆着较大的浓度梯度从循环中积累天冬氨酸。由于天冬氨酸和柠檬酸盐之间存在这种独特关系,因此确定柠檬酸盐是否调节天冬氨酸向前列腺上皮细胞的高亲和力转运非常重要。目前对从大鼠腹侧前列腺获得的新鲜制备的前列腺上皮细胞的研究表明,柠檬酸盐对天冬氨酸转运有两种作用。细胞外柠檬酸盐的生理水平(即相当于循环水平)显著抑制(顺式抑制作用)天冬氨酸转运。相比之下,与原位正常细胞相关浓度的细胞内柠檬酸盐导致天冬氨酸转运有两个刺激水平。当细胞内柠檬酸盐增加至500 nmol/g时,天冬氨酸转运增加4倍,而当细胞内柠檬酸盐浓度升高至1800 nmol/g(这是前列腺细胞特有的特征)时,天冬氨酸转运增加11倍。柠檬酸盐的顺式抑制和反式刺激作用的综合效应是天冬氨酸转运持续增加1至2倍。这些研究支持这样一种概念,即柠檬酸盐是天冬氨酸向前列腺分泌上皮细胞高亲和力转运的生理调节剂,这与柠檬酸盐净产生和分泌的独特且高度专业化功能相关。

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