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培养的人成纤维细胞对二碱基氨基酸、胱氨酸和色氨酸的转运:胱氨酸尿症和哈特纳普病无缺陷

Transport of dibasic amino acids, cystine, and tryptophan by cultured human fibroblasts: absence of a defect in cystinuria and Hartnup disease.

作者信息

Groth U, Rosenberg L E

出版信息

J Clin Invest. 1972 Aug;51(8):2130-42. doi: 10.1172/JCI107020.

Abstract

Transport of lysine, arginine, cystine, and tryptophan was studied in cultured skin fibroblasts from normal controls and from patients with cystinuria and Hartnup disease. Each of these amino acids was accumulated against concentration gradients by energy-dependent, saturable mechanisms. Lysine and arginine were each transported by two distinct processes which they shared with each other and with ornithine. In contrast, cystine was taken up by a different transport system with no demonstrable affinity for the dibasic amino acids. The time course and Michaelis-Menten kinetics of lysine and cystine uptake by cells from three cystinuric patients differed in no way from those found in control cells. Similarly, the characteristics of tryptophan uptake by cells from a child with Hartnup disease were identical to those noted in control cells. These findings indicate that the specific transport defects observed in gut and kidney in cystinuria and Hartnup disease are not expressed in cultured human fibroblasts, thus providing additional evidence of the important role that cellular differentiation plays in the regulation of expression of the human genome.

摘要

对来自正常对照以及胱氨酸尿症和哈特纳普病患者的培养皮肤成纤维细胞中的赖氨酸、精氨酸、胱氨酸和色氨酸转运进行了研究。这些氨基酸中的每一种都是通过能量依赖的、可饱和的机制逆浓度梯度积累的。赖氨酸和精氨酸各自通过两种不同的过程进行转运,它们彼此之间以及与鸟氨酸共享这些过程。相比之下,胱氨酸通过一种不同的转运系统被摄取,对二碱基氨基酸没有明显的亲和力。来自三名胱氨酸尿症患者的细胞摄取赖氨酸和胱氨酸的时间进程和米氏动力学与对照细胞中发现的情况没有任何差异。同样,来自一名哈特纳普病患儿的细胞摄取色氨酸的特征与对照细胞中观察到的特征相同。这些发现表明,在胱氨酸尿症和哈特纳普病中在肠道和肾脏中观察到的特定转运缺陷在培养的人成纤维细胞中并未表现出来,从而提供了额外的证据,证明细胞分化在人类基因组表达调控中所起的重要作用。

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