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谷胱甘肽、谷胱甘肽-S-转移酶与铂类药物和美法仑在八种人卵巢癌细胞系中的细胞毒性之间的关系。

The relationships between glutathione, glutathione-S-transferase and cytotoxicity of platinum drugs and melphalan in eight human ovarian carcinoma cell lines.

作者信息

Mistry P, Kelland L R, Abel G, Sidhar S, Harrap K R

机构信息

Drug Development Section, Institute of Cancer Research, Sutton, Surrey, UK.

出版信息

Br J Cancer. 1991 Aug;64(2):215-20. doi: 10.1038/bjc.1991.279.

Abstract

The role of glutathione (GSH) and GSH-S-transferase (GST) activity in modulating the cytotoxicity of four platinum drugs and melphalan was evaluated in eight human ovarian carcinoma cell lines. The cell lines were established from solid and ascitic tumours from pretreated and untreated patients, and showed a wide spectrum of sensitivity to several platinum II and platinum IV drugs; cisplatin, carboplatin, CHIP and tetraplatin. Intracellular glutathione concentration measured in the cell lines showed a significant (P = 0.05) correlation with IC50 values for cisplatin (r = 0.91), carboplatin (r = 0.87) and CHIP (r = 0.88). The correlation between GSH levels and IC50 values for melphalan (r = 0.76) or tetraplatin (r = 0.60) was not as significant. GST activity showed no correlation with IC50 values, for the four platinum drugs. To determine the significance of the elevated GSH concentration in the refractory cell lines, the effect of D,L-buthionine-S, R-sulfoximine (BSO) mediated GSH depletion on platinum drug cytotoxicity was examined in one of the most sensitive (CH1) and two of the least sensitive (relatively resistant; SKOV-3, HX/62) cell lines. Comparison was made with the effect of GSH depletion on melphalan cytotoxicity in these three lines. These lines were differentially sensitive to BSO, with the two most platinum drug resistant lines being more tolerant to BSO than the sensitive CH1 line. Depletion of cellular GSH, ranging between 61 and 88%, had a differential effect on the sensitivity to PtII vs PtIV drugs in the three cell lines: cytotoxicity of the PtIV drugs, tetraplatin and CHIP, was substantially enhanced in both the resistant and sensitive cell lines; in contrast, the cytotoxicity of the PtII drugs, cisplatin and carboplatin, was only significantly increased in one of the two relatively resistant lines (SKOV-3) and in the sensitive (CH1) line after GSH depletion. Moreover the dose modification factor (DMF) for the PtII agents were lower than those for PtIV agents in the three cell lines. The dose modification factor for tetraplatin after BSO treatment was similar to that observed for melphalan in all three cell lines. In the SKOV-3 cell line extending the BSO pretreatment period to 48 h from 24 h marginally reduced the cytotoxicity of cisplatin, whereas the cytotoxicity of the other three drugs remained similar to that observed after 24 h BSO pretreatment. In contrast, extending the BSO treatment to 24 h after drug exposure potentiated the cytotoxicity of cisplatin, CHIP and tetraplatin.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在8种人卵巢癌细胞系中评估了谷胱甘肽(GSH)和谷胱甘肽-S-转移酶(GST)活性在调节4种铂类药物和美法仑细胞毒性中的作用。这些细胞系源自预处理和未处理患者的实体瘤和腹水瘤,对几种铂II和铂IV药物表现出广泛的敏感性;顺铂、卡铂、CHIP和四铂。在细胞系中测得的细胞内谷胱甘肽浓度与顺铂(r = 0.91)、卡铂(r = 0.87)和CHIP(r = 0.88)的IC50值呈显著(P = 0.05)相关。GSH水平与美法仑(r = 0.76)或四铂(r = 0.60)的IC50值之间的相关性不那么显著。对于4种铂类药物,GST活性与IC50值无相关性。为了确定难治性细胞系中GSH浓度升高的意义,在最敏感的细胞系之一(CH1)和最不敏感的两个细胞系(相对耐药;SKOV-3、HX/62)中研究了D,L-丁硫氨酸-S,R-亚砜亚胺(BSO)介导的GSH耗竭对铂类药物细胞毒性的影响。并与这三种细胞系中GSH耗竭对美法仑细胞毒性的影响进行了比较。这些细胞系对BSO的敏感性不同,两种对铂类药物耐药性最强的细胞系比敏感的CH1细胞系对BSO更耐受。细胞内GSH耗竭61%至88%对三种细胞系中对PtII与PtIV药物的敏感性产生了不同影响:在耐药和敏感细胞系中,PtIV药物四铂和CHIP的细胞毒性均显著增强;相比之下,PtII药物顺铂和卡铂的细胞毒性仅在两个相对耐药的细胞系之一(SKOV-3)和敏感细胞系(CH1)中在GSH耗竭后显著增加。此外,在这三种细胞系中,PtII药物的剂量修正因子低于PtIV药物。在所有三种细胞系中,BSO处理后四铂的剂量修正因子与美法仑观察到的相似。在SKOV-3细胞系中,将BSO预处理时间从24小时延长至48小时,顺铂的细胞毒性略有降低,而其他三种药物的细胞毒性与24小时BSO预处理后观察到的相似。相反,在药物暴露后将BSO处理延长至24小时可增强顺铂、CHIP和四铂的细胞毒性。(摘要截断于400字)

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