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罗丹明123在体外对癌细胞的选择性毒性。

Selective toxicity of rhodamine 123 in carcinoma cells in vitro.

作者信息

Lampidis T J, Bernal S D, Summerhayes I C, Chen L B

出版信息

Cancer Res. 1983 Feb;43(2):716-20.

PMID:6848187
Abstract

The study of mitochondria in situ has recently been facilitated through the use of rhodamine 123, a mitochondrial-specific fluorescent dye. It has been found to be nontoxic when applied for short periods to a variety of cell types and has thus become an invaluable tool for examining mitochondrial morphology and function in the intact living cell. In this report, however, we demonstrate that with continuous exposure, rhodamine 123 selectively kills carcinoma as compared to normal epithelial cells grown in vitro. At doses of rhodamine 123 which were toxic to carcinoma cells, the conversion of mitochondrial-specific to cytoplasmic-nonspecific localization of the drug was observed prior to cell death. At 10 microgram/ml, greater than 50% cell death occurred within 7 days in all nine of the carcinoma cell types and lines of different origin studied, while six of six normal epithelial cell types and lines remained unaffected. Cotreating carcinoma cells with 2-deoxyglucose and rhodamine 123 enhanced the inhibition of growth by rhodamine 123 alone in clonogenic survival assays. The observation of the selective toxicity of rhodamine 123 appears to be unique in view of the absence of selective toxicity reported in vitro for the various antitumor agents currently in clinical use. Preliminary results with rhodamine 123 in animal tumor systems indicate antitumor activity for carcinomas.

摘要

近年来,通过使用若丹明123(一种线粒体特异性荧光染料),线粒体原位研究得到了促进。已发现,短时间应用于多种细胞类型时,它是无毒的,因此已成为检查完整活细胞中线粒体形态和功能的宝贵工具。然而,在本报告中,我们证明,与体外培养的正常上皮细胞相比,持续暴露于若丹明123时,它能选择性杀死癌细胞。在对癌细胞有毒性的若丹明123剂量下,在细胞死亡之前观察到该药物从线粒体特异性定位转变为细胞质非特异性定位。在10微克/毫升的浓度下,所研究的所有九种不同来源的癌细胞类型和细胞系中,超过50%的细胞在7天内死亡,而六种正常上皮细胞类型和细胞系中有六种不受影响。在克隆存活试验中,用2-脱氧葡萄糖和若丹明123共同处理癌细胞增强了若丹明123单独对生长的抑制作用。鉴于目前临床使用的各种抗肿瘤药物在体外未报道有选择性毒性,若丹明123的选择性毒性观察似乎是独特的。若丹明123在动物肿瘤系统中的初步结果表明对癌具有抗肿瘤活性。

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