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生物还原剂RH1的细胞毒性及其与辐射的无相互作用

Cytotoxicity of the bioreductive agent RH1 and its lack of interaction with radiation.

作者信息

Kim Joo-Young, West C M L, Valentine H, Ward T H, Patterson A V, Stratford I J, Roberts S A, Hendry J H

机构信息

Cancer Research UK Groups of Experimental Radiation Oncology, Paterson Institute for Cancer Research, Christie Hospital NHS Trust, Manchester, UK.

出版信息

Radiother Oncol. 2004 Mar;70(3):311-7. doi: 10.1016/j.radonc.2003.12.008.

Abstract

BACKGROUND AND PURPOSE

RH1 is a new bioreductive agent that was developed as a cytotoxic agent with selectivity for tumour cells expressing high levels of the enzyme DT-diaphorase (DTD). The aim of the present study was to investigate the cytotoxicity of RH1 in relation to cellular levels of reducing enzymes and any interaction of RH1 with ionizing radiation under oxic and hypoxic conditions.

PATIENTS AND METHODS

The MB-MDA231 human breast cancer cell line (WT) and WT cells transfected with the NQO1 gene encoding DTD (the D7 cell line) were used to examine the dependency of RH1's cytotoxicity on cellular DTD activity. The role of the 1-electron reducing enzyme P450 reductase was also studied using a P450 reductase-transfected isogenic cell line (R4). A clonogenic assay was used to investigate the cytotoxicity of RH1 with and without irradiation in air and in nitrogen. In all cases drug exposure was for 3 h.

RESULTS

DTD levels were around 300-fold higher in D7 compared to WT and R4 cells. RH1 was cytotoxic at nanomolar concentrations to all the cell lines, and was 2-3 times more toxic in the D7 cells with high DTD than in the other two cell lines. Doses of RH1 was around 2-fold more effective in hypoxic than in oxic WT cells, but not by as much in D7 cells. RH1 did not radiosensitise the cells but showed an additive effect when combined with irradiation under oxic and hypoxic conditions.

CONCLUSIONS

RH1 shows high clonogenic cytotoxicity to MDA231 cells with high DTD activity but its selectivity based on the presence of DTD is much less than as shown in previous reports. RH1 showed an additive cell killing effect when combined with irradiation under both oxic and hypoxic conditions.

摘要

背景与目的

RH1是一种新型生物还原剂,作为一种细胞毒性剂开发,对表达高水平酶DT-二氢硫辛酰胺脱氢酶(DTD)的肿瘤细胞具有选择性。本研究的目的是研究RH1在有氧和缺氧条件下的细胞毒性与还原酶细胞水平的关系,以及RH1与电离辐射的任何相互作用。

患者与方法

使用MB-MDA231人乳腺癌细胞系(WT)和转染了编码DTD的NQO1基因的WT细胞(D7细胞系)来检测RH1细胞毒性对细胞DTD活性的依赖性。还使用转染了P450还原酶的同基因细胞系(R4)研究了单电子还原酶P450还原酶的作用。采用克隆形成试验研究了在空气和氮气中有无照射情况下RH1的细胞毒性。在所有情况下,药物暴露时间均为3小时。

结果

与WT和R4细胞相比,D7细胞中的DTD水平高约300倍。RH1在纳摩尔浓度下对所有细胞系均具有细胞毒性,在DTD含量高的D7细胞中的毒性是其他两个细胞系的2至3倍。在缺氧的WT细胞中,RH1的剂量效果比在有氧时高约2倍,但在D7细胞中则没有那么明显。RH1不会使细胞产生放射增敏作用,但在有氧和缺氧条件下与照射联合使用时显示出相加效应。

结论

RH1对具有高DTD活性的MDA231细胞表现出高克隆形成细胞毒性,但其基于DTD存在的选择性远低于先前报道。在有氧和缺氧条件下,RH1与照射联合使用时均显示出相加的细胞杀伤作用。

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