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人顺铂耐药细胞系中对甲氨蝶呤和金属的交叉耐药源于这些化合物积累中的多效性缺陷,这与质膜结合蛋白减少有关。

Cross-resistance to methotrexate and metals in human cisplatin-resistant cell lines results from a pleiotropic defect in accumulation of these compounds associated with reduced plasma membrane binding proteins.

作者信息

Shen D, Pastan I, Gottesman M M

机构信息

Laboratory of Cell Biology, National Cancer Institute, NIH, Bethesda, Maryland 20892-4255, USA.

出版信息

Cancer Res. 1998 Jan 15;58(2):268-75.

PMID:9443404
Abstract

Cross-resistance to a wide array of toxic chemicals is a common phenomenon in cisplatin-resistant cell lines. In this study, two independently isolated cisplatin-resistant cell lines derived from a human hepatoma and a cervical adenocarcinoma were shown to be cross-resistant to methotrexate (MTX) and several metal salts, such as sodium arsenite, sodium arsenate, antimony potassium tartrate, and cadmium chloride. A pleiotropic defect resulting in reduced accumulation of cisplatin, 3[H]MTX, 73As3+, and 73As5+ was found in both cisplatin-resistant cell lines. Analysis by immunoblot, indirect immunofluorescence, and Northern hybridization showed dramatically reduced expression of the folate binding protein that mediates MTX uptake in both human cisplatin-resistant cell lines. By photoaffinity labeling with UV irradiation, specific binding proteins of Mr 230,000 and Mr 48,000 for 73As3+ and Mr 190,000 for 73As5+ were found in enriched plasma membrane of both human cisplatin-sensitive parental cell lines. Expression of these specific binding proteins was decreased in cells selected for cisplatin resistance. A protein band at Mr 36,000 that binds to 73As3+ was overexpressed in both human cisplatin-resistant cell lines. The finding of loss of distinct binding proteins for MTX, arsenate, and arsenite in association with decreased accumulation of these agents in cisplatin-resistant cells suggests a pleiotropic, possibly regulatory, alteration in these cells.

摘要

对多种有毒化学物质产生交叉耐药性是顺铂耐药细胞系中的常见现象。在本研究中,从人肝癌细胞系和宫颈腺癌细胞系中独立分离出的两个顺铂耐药细胞系,显示出对甲氨蝶呤(MTX)以及几种金属盐(如亚砷酸钠、砷酸钠、酒石酸锑钾和氯化镉)具有交叉耐药性。在这两个顺铂耐药细胞系中均发现了一种多效性缺陷,导致顺铂、3[H]MTX、73As3 +和73As5 +的积累减少。通过免疫印迹、间接免疫荧光和Northern杂交分析表明,在两个人顺铂耐药细胞系中,介导MTX摄取的叶酸结合蛋白的表达显著降低。通过紫外线照射进行光亲和标记,在两个人顺铂敏感亲本细胞系的富集质膜中发现了分子量为230,000和48,000的73As3 +特异性结合蛋白以及分子量为19,000的73As5 +特异性结合蛋白。在选择获得顺铂耐药性的细胞中,这些特异性结合蛋白的表达降低。在两个人顺铂耐药细胞系中,分子量为36,000的与73As3 +结合的蛋白条带均过表达。在顺铂耐药细胞中,与MTX、砷酸盐和亚砷酸盐的积累减少相关的不同结合蛋白的缺失,表明这些细胞中存在多效性、可能是调节性的改变。

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