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新型吲哚醌EO9对缺氧非小细胞肺癌细胞系的细胞毒性

Cytotoxicity of a novel indoloquinone eo9 in hypoxic non-small-cell lung-cancer cell-lines.

作者信息

Bando T, Kasahara K, Shibata K, Numata Y, Heki U, Shirasaki H, Iwasa K, Fujimura M, Matsuda T

出版信息

Int J Oncol. 1995 Oct;7(4):789-93. doi: 10.3892/ijo.7.4.789.

Abstract

3-Hydroxymethyl-5-aziridinyl-1-methyl-[1H-indole-4,7-dione]-prop-beta-en -alpha-ol (EO9) is a bioreductive anticancer agent active for non-small cell lung cancer (NSCLC) and structurally related to mitomycin C (MMC). DT-diaphorase (DTD) is regarded as a two electron reductase that plays an important role in the biotransformation of MMC to antitumor metabolites. To evaluate the role of DTD as a bioactivator of EO9 in NSCLC cell lines under oxic and hypoxic conditions, we examined the inhibitory effect of dicumarol which was regarded as a selective inhibitor of DTD on the sensitivity to EO9 in vitro. In this study, we used an MMC-resistant NSCLC cell line (PC-9/MC4) which was established from a PC-9 cell line as a parent cell line by continuous exposure to MMC in our laboratory. We reported previously that the subline PC-9/MC4 was 6.7-fold more resistant to MMC than PC-9 with decreased DTD activity. The IC50 value of PC-9 against EO9 was significantly increased by co-incubation with dicumarol under oxic conditions. EO9 was more cytotoxic against PC-9/MC4 than against PC-9 cells and the enhancement was impaired by tempol under hypoxic conditions. These findings suggest a suppressive role of DTD against one-electron reduction pathway in the bioactivation of EO9 under hypoxic conditions and EO9 may be more active against oxygen-deficient solid tumors especially in MMC-resistant NSCLC cells with low levels of DTD activity.

摘要

3-羟甲基-5-氮丙啶基-1-甲基-[1H-吲哚-4,7-二酮]-丙-β-烯-α-醇(EO9)是一种对非小细胞肺癌(NSCLC)有活性的生物还原抗癌剂,其结构与丝裂霉素C(MMC)相关。DT-黄递酶(DTD)被认为是一种双电子还原酶,在MMC生物转化为抗肿瘤代谢物的过程中起重要作用。为了评估DTD作为EO9在有氧和缺氧条件下对NSCLC细胞系的生物激活剂的作用,我们研究了被视为DTD选择性抑制剂的双香豆素对体外EO9敏感性的抑制作用。在本研究中,我们使用了一种MMC耐药的NSCLC细胞系(PC-9/MC4),它是我们实验室通过将PC-9细胞系作为亲本细胞系连续暴露于MMC而建立的。我们之前报道过,亚系PC-9/MC4对MMC的耐药性是PC-9的6.7倍,且DTD活性降低。在有氧条件下,双香豆素与PC-9共同孵育可显著提高其对EO9的IC50值。在缺氧条件下,EO9对PC-9/MC4的细胞毒性比对PC-9细胞更强,而tempol会削弱这种增强作用。这些发现表明,在缺氧条件下,DTD对EO9生物激活中的单电子还原途径具有抑制作用,并且EO9可能对缺氧实体瘤更具活性,尤其是在DTD活性较低的MMC耐药NSCLC细胞中。

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