首页> 外文期刊>Kidney and blood pressure research >Arginine transport is augmented, through modulation of cationic amino acid transporter-1, in obstructive uropathy in rats.
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Arginine transport is augmented, through modulation of cationic amino acid transporter-1, in obstructive uropathy in rats.

机译:在大鼠阻塞性尿毒症中,通过调节阳离子氨基酸转运蛋白-1来增加精氨酸转运。

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BACKGROUND: The decrease in glomerular filtration rate (GFR), which is characteristic of obstructive uropathy, was suggested to be associated with attenuated nitric oxide (NO) generation. Since availability of L-arginine, the sole precursor for NO, governs NO synthesis, we aimed to determine the role of glomerular arginine transport in rats subjected to 24 h of bilateral ureteral ligation (BUO). METHODS: Glomerular arginine transport was measured by uptake of radiolabeled arginine ([(3)H]-L-arginine), cationic amino acid transporters (CAT)-1 and -2 and arginases I and II mRNA expression were determined using reverse transcription-polymerase chain reaction. CAT-1, arginase I, and arginase II protein contents were evaluated by Western blotting. RESULTS: L-Arginine transport by freshly harvested glomeruli from BUO rats was significantly augmented than in controls. The aforementioned findings were associated with a significant increase in glomerular CAT-1 mRNA expression, while CAT-2 mRNA was unchanged. Western blotting demonstrated a significant increase in CAT-1 abundance in BUO. Expression of both glomerular arginase I and II mRNA and protein content were significantly elevated in BUO. CONCLUSIONS: BUO induces an increase in glomerular arginine transport via upregulation of CAT-1, probably due to increase in arginine utilization by a non-NO pathway.
机译:背景:肾小球滤过率(GFR)的降低是阻塞性尿病的特征,建议与一氧化氮(NO)的产生减少有关。由于L-精氨酸(NO的唯一前体)的可用性决定着NO的合成,因此我们旨在确定肾小球精氨酸转运在双侧输尿管结扎(BUO)24小时大鼠中的作用。方法:通过摄取放射性标记的精氨酸([(3)H] -L-精氨酸),测量肾小球精氨酸的转运,阳离子氨基酸转运蛋白(CAT)-1和-2,并通过逆转录测定精氨酸I和II mRNA的表达。聚合酶链反应。通过蛋白质印迹法评估CAT-1,精氨酸酶I和精氨酸酶II的蛋白质含量。结果:BUO大鼠新鲜收获的肾小球转运L-精氨酸比对照组明显增加。上述发现与肾小球CAT-1 mRNA表达的显着增加有关,而CAT-2 mRNA则没有变化。 Western印迹显示BUO中CAT-1的丰度显着增加。 BUO中肾小球精氨酸酶I和II的mRNA表达和蛋白质含量均显着升高。结论:BUO通过上调CAT-1诱导肾小球精氨酸转运的增加,可能是由于非NO途径精氨酸利用率的增加。

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