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体外培养的胎鼠心脏中牛磺酸载体介导转运系统的特性研究

Characterization of a carrier-mediated transport system for taurine in the fetal mouse heart in vitro.

作者信息

Grosso D S, Roeske W R, Bressler R

出版信息

J Clin Invest. 1978 Apr;61(4):944-52. doi: 10.1172/JCI109019.

Abstract

Cardiac taurine levels are elevated in hypertension and congestive heart failure. A possible mechanism for this increase in taurine is an alteration of its uptake. We sought to identify and characterize a carrier-mediated transport system for taurine in the mammalian myocardium utilizing the fetal mouse heart in organ culture. Hearts from fetuses of 16-19 days gestational age used in these studies had an endogenous taurine content of 14.1+/-0.5 nmol/mg tissue. The uptake of [(3)H]taurine was linear for up to 8 h. Taurine was accumulated against a concentration gradient as demonstrated by a net increase in taurine concentration when hearts were incubated in 0.5 mM taurine. [(3)H]Taurine uptake was saturable, K(m) = 0.44 mM, temperature dependent, and required sodium. The close structural analogues, hypotaurine and beta-alanine, reduced [(3)H]taurine uptake by 87% when present in 100-fold excess. The alpha-amino acids alanine, alpha-aminoisobutyric acid, glycine, leucine, and threonine did not inhibit uptake. Other taurine analogues tested were guanidinotaurine, guanidinopropionic acid, gamma-aminobutyric acid, 2-aminoethane phosphonic acid, aminomethane sulfonic acid, 3-aminopropane sulfonic acid, N-acetyltaurine, and isethionic acid. We conclude that a carrier-mediated transport system for taurine exists in the fetal mouse heart based on the demonstration of (a) temperature dependence, (b) saturability, and (c) structural selectivity of the uptake process. Transport was demonstrated to be mediated by a beta-amino acid uptake system. In addition, taurine uptake was observed to be sodium dependent, energy dependent, and capable of accumulating taurine against a concentration gradient.

摘要

高血压和充血性心力衰竭患者的心脏牛磺酸水平会升高。牛磺酸水平升高的一种可能机制是其摄取发生改变。我们试图利用器官培养中的胎鼠心脏,识别和表征哺乳动物心肌中牛磺酸的载体介导转运系统。这些研究中使用的孕龄为16 - 19天胎儿的心脏,其 endogenous taurine含量为14.1±0.5 nmol/mg组织。 [3H]牛磺酸的摄取在长达8小时内呈线性。如在0.5 mM牛磺酸中孵育心脏时牛磺酸浓度净增加所示,牛磺酸是逆浓度梯度积累的。 [3H]牛磺酸摄取是可饱和的, Km = 0.44 mM,依赖于温度,并需要钠。紧密的结构类似物亚牛磺酸和β-丙氨酸,当以100倍过量存在时,会使 [3H]牛磺酸摄取减少87%。α-氨基酸丙氨酸、α-氨基异丁酸、甘氨酸、亮氨酸和苏氨酸不抑制摄取。测试的其他牛磺酸类似物有胍基牛磺酸、胍基丙酸、γ-氨基丁酸、2-氨基乙烷磺酸、氨基甲烷磺酸、3-氨基丙烷磺酸、N-乙酰牛磺酸和羟乙基磺酸。我们得出结论,基于摄取过程的(a)温度依赖性、(b)可饱和性和(c)结构选择性,胎鼠心脏中存在牛磺酸的载体介导转运系统。已证明转运是由β-氨基酸摄取系统介导的。此外,观察到牛磺酸摄取依赖于钠、能量,并能够逆浓度梯度积累牛磺酸。

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本文引用的文献

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