首页> 美国卫生研究院文献>The British Journal of Cancer. Supplement >Induction of DT-diaphorase by 12-dithiole-3-thione and increase of antitumour activity of bioreductive agents.
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Induction of DT-diaphorase by 12-dithiole-3-thione and increase of antitumour activity of bioreductive agents.

机译:12-二硫代-3-硫酮诱导DT-黄递酶的存在并增强生物还原剂的抗肿瘤活性。

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摘要

Bioreductive antitumour agents are an important new class of anticancer drugs that require activation by reduction. The two-electron reducing enzyme, DT-diaphorase, has been shown to be an important activating enzyme for the bioreductive agents, mitomycin C (MMC) and EO9. Incubation of L5178Y murine lymphoma cells in vitro with 1,2-dithiole-3-thione (D3T) increased the level of DT-diaphorase activity in these cells 22-fold. In contrast, D3T had no effect on the DT-diaphorase level in normal mouse bone marrow cells. Combination therapy with D3T and MMC or EO9, produced a 2- or 7-fold enhancement, respectively, of the cytotoxic activity of these antitumour agents in L5178Y cells. By comparison, D3T did not enhance the activity of MMC in marrow cells and produced only a small increase in EO9 cytotoxicity in these cells. The DT-diaphorase inhibitor, dicoumarol, inhibited the effect of D3T on the antitumour activity of the bioreductive agents, supporting the proposal that the enhanced anticancer activity was due to the elevated enzyme level. These findings suggest that D3T, or other inducers of DT-diaphorase, could be used to enhance the antitumour efficacy of bioreductive antitumour agents.
机译:生物还原抗肿瘤剂是一类重要的新型抗癌药物,需要通过还原来激活。二电子还原酶DT-黄递酶已被证明是生物还原剂丝裂霉素C(MMC)和EO9的重要活化酶。 L1178Y鼠淋巴瘤细胞与1,2-二硫代-3-硫酮(D3T)的体外孵育使这些细胞中DT-黄递酶活性的水平提高了22倍。相反,D3T对正常小鼠骨髓细胞中的DT-黄递酶水平没有影响。 D3T和MMC或EO9的联合治疗分别使L5178Y细胞中这些抗肿瘤药的细胞毒性活性提高了2倍或7倍。相比之下,D3T在骨髓细胞中并未增强MMC的活性,而在这些细胞中仅使EO9细胞毒性产生了小幅增加。 DT-心肌黄酶抑制剂双香豆酚抑制D3T对生物还原剂的抗肿瘤活性的作用,从而支持了抗癌活性增强是由于酶水平升高的建议。这些发现表明,D3T或DT-黄递酶的其他诱导剂可用于增强生物还原抗肿瘤剂的抗肿瘤功效。

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