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L1210细胞中载体介导的叶酸化合物转运。在生理阴离子存在下,叶酸和5-甲基四氢高叶酸非对映异构体的初始速率动力学及进入途径的双重性程度。

Carrier-mediated transport of folate compounds in L1210 cells. Initial rate kinetics and extent of duality of entry routes for folic acid and diastereomers of 5-methyltetrahydrohomofolate in the presence of physiological anions.

作者信息

Sirotnak F M, Goutas L J, Jacobsen D M, Mines L S, Barrueco J R, Gaumont Y, Kisliuk R L

出版信息

Biochem Pharmacol. 1987 May 15;36(10):1659-67. doi: 10.1016/0006-2952(87)90051-7.

Abstract

Comparison of the kinetic parameters for influx of highly purified [3H]folic acid versus [3H]methotrexate in L1210 cells under anionic buffer conditions showed a marked discordancy. In addition, the kinetics for influx of [3H]folic acid were unchanged in variant L1210 cells defective in [3H]methotrexate transport. In these variant cells, the Vmax for methotrexate was reduced 17-fold and the Km was increased 3-fold. The results show that [3H]folic acid influx is mediated by a system which has a low affinity, but a 20-fold higher capacity, for folate compounds than the classical high-affinity system mediating [3H]methotrexate influx. Since the latter system also exhibits very low affinity for [3H]folic acid, it would not be expected to contribute significantly to the total influx of [3H]folic acid. The high-capacity system for [3H]folic acid influx is different from that believed to mediate pterin influx in L1210 cells since it was not inhibited by adenine, a potent inhibitor of pterin influx. However, exposure of cells to [3H]folic acid in a nonanionic buffer resulted in marked stimulation of initial influx, and a fraction of influx under these conditions was inhibited by methotrexate. These results suggest that anions modulate the extent of multiplicity of [3H]folic acid influx by their known effects on the high-affinity, reduced folate/methotrexate system. The diastereomers, at carbon 6, of [14C]5-methyltetrahydrohomofolate shared both transport systems. The influx Km for the natural diastereomer was one-half that of the unnatural form for both transport systems. Both diastereomers showed a much greater differential in affinity between the two transport systems than did [3H]folic acid. Our results suggest that an analog which could be effectively transported by the low-affinity/high-capacity route may be useful in the treatment of tumors resistant to methotrexate due to a defective high-affinity/low capacity influx system. We also found that incubation of L1210 cells with [3H]folic acid or the natural diastereomer [14C]5-methyltetrahydrohomofolate for 10 min resulted in the formation of a nonexchangeable fraction of radioactivity amounting to 20-40% of the total accumulation. This non-exchangeable fraction may be explained by the accumulation of metabolites other than polyglutamates. Preloading of cells with methotrexate prior to incubation with [3H]folic acid prevented the accumulation of radioactivity as a nonexchangeable fraction.

摘要

在阴离子缓冲条件下,对L1210细胞中高纯度[3H]叶酸与[3H]甲氨蝶呤流入的动力学参数进行比较,结果显示出明显的不一致。此外,在[3H]甲氨蝶呤转运存在缺陷的L1210变异细胞中,[3H]叶酸流入的动力学没有变化。在这些变异细胞中,甲氨蝶呤的Vmax降低了17倍,而Km增加了3倍。结果表明,[3H]叶酸的流入是由一个系统介导的,该系统对叶酸化合物的亲和力较低,但容量比介导[3H]甲氨蝶呤流入的经典高亲和力系统高20倍。由于后一个系统对[3H]叶酸的亲和力也非常低,预计它对[3H]叶酸的总流入贡献不大。介导[3H]叶酸流入的高容量系统与被认为介导L1210细胞中蝶呤流入的系统不同,因为它不受腺嘌呤(一种有效的蝶呤流入抑制剂)的抑制。然而,在非阴离子缓冲液中将细胞暴露于[3H]叶酸会导致初始流入的显著刺激,并且在这些条件下的一部分流入会被甲氨蝶呤抑制。这些结果表明,阴离子通过其对高亲和力、还原型叶酸/甲氨蝶呤系统的已知作用来调节[3H]叶酸流入的多重性程度。[14C]5-甲基四氢高同型叶酸在碳6处的非对映异构体共享这两种转运系统。对于两种转运系统,天然非对映异构体的流入Km是非天然形式的一半。两种非对映异构体在两种转运系统之间的亲和力差异比[3H]叶酸大得多。我们的结果表明,一种可以通过低亲和力/高容量途径有效转运的类似物可能有助于治疗由于高亲和力/低容量流入系统缺陷而对甲氨蝶呤耐药的肿瘤。我们还发现,将L??1210细胞与[3H]叶酸或天然非对映异构体[14C]5-甲基四氢高同型叶酸孵育10分钟会导致形成一种不可交换的放射性部分,其占总积累量的20 - 40%。这种不可交换部分可能是由多聚谷氨酸以外的代谢产物积累所解释的。在用[3H]叶酸孵育之前用甲氨蝶呤对细胞进行预加载可防止放射性以不可交换部分的形式积累。

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