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酶模式导向化疗:3-去氮尿苷与D-半乳糖胺的协同相互作用。

Enzyme pattern-directed chemotherapy: synergistic interaction of 3-deazauridine with D-galactosamine.

作者信息

Jackson R C, Williams J C, Weber G

出版信息

Cancer Treat Rep. 1976 Jul;60(7):835-43.

PMID:188552
Abstract

We tested an experimental approach in which the specialized enzymatic pattern characteristic of the tissue of origin of a tumor might be exploited to target and enhance drug selectivity. In the present work, the D-galactosamine-induced depletion of uridine 5'-triphosphate (primarily a hepatic event) was employed to enhance the growth inhibition caused by 3-deazauridine. As predicted, the drug effect was most pronounced in the slower growing, well differentiated hepatoma lines where the activities of certain hepatic metabolic pathways and enzymes, though decreased, were still operative. The interactions of D-galactosamine and cytosine arabinoside with 3-deazauridine were examined in vitro in four liver tumor cell lines and two nonhepatic lines. The effects of D-galactosamine and 3-deazauridine on the growth of the Morris hepatoma cell lines 3924A, 8999S,AND 8999R were strongly synergistic; on the Novikoff hepatoma and the nonhepatic cell lines they were only additive. The combination of 3-deazauridine with cytosine arabinoside gave approximately additive growth inhibition with all cell types, without selective toxicity towards the hepatocellular lines. Results of growth-inhibition studies with the combination of D-galactosamine and cytosine arabinoside and with combinations of all three agents are also presented. These results are analyzed in the context of the regulation of hepatic pyrimidine nucleotide metabolism and our design of enzyme pattern directed drug selectivity.

摘要

我们测试了一种实验方法,即利用肿瘤起源组织特有的特殊酶模式来靶向并提高药物选择性。在本研究中,利用D-半乳糖胺诱导的尿苷5'-三磷酸耗竭(主要发生在肝脏)来增强3-去氮尿苷引起的生长抑制作用。正如所预测的,药物效应在生长较慢、分化良好的肝癌细胞系中最为明显,在这些细胞系中,某些肝脏代谢途径和酶的活性虽然降低,但仍有作用。在四种肝癌细胞系和两种非肝癌细胞系中,体外研究了D-半乳糖胺和阿糖胞苷与3-去氮尿苷的相互作用。D-半乳糖胺和3-去氮尿苷对莫里斯肝癌细胞系3924A、8999S和8999R生长的影响具有强烈的协同作用;对诺维科夫肝癌细胞系和非肝癌细胞系的影响仅为相加作用。3-去氮尿苷与阿糖胞苷联合使用对所有细胞类型均产生近似相加的生长抑制作用,对肝细胞系无选择性毒性。还给出了D-半乳糖胺和阿糖胞苷联合使用以及三种药物联合使用的生长抑制研究结果。在肝脏嘧啶核苷酸代谢调节以及我们针对酶模式的药物选择性设计的背景下,对这些结果进行了分析。

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