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Synthesis and evaluation of fluoromycin: a novel fluorescence-labeled derivative of talisomycin S10b.

作者信息

Mistry J S, Jani J P, Morris G, Mujumdar R B, Reynolds I J, Sebti S M, Lazo J S

机构信息

Department of Pharmacology, University of Pittsburgh, School of Medicine, Pennsylvania 15261.

出版信息

Cancer Res. 1992 Feb 1;52(3):709-18.

PMID:1370650
Abstract

We have synthesized fluoromycin (FLM), a novel fluorescein-labeled derivative of talisomycin S10b (TLM S10b), and used it to evaluate cellular drug accumulation and distribution in bleomycin (BLM)-sensitive and -resistant cell lines. The fluorescence intensity of FLM was 300- to 400-fold greater than that of BLM A2, TLM S10b, or the lipophilic BLM analogue, liblomycin. FLM possessed an antiproliferative potency similar to liblomycin in BLM-sensitive human A-253 squamous carcinoma cells but was less potent than BLM A2 or TLM S10b. C-10E cells, a clone of A-253 cells with 40- to 50-fold resistance to BLM A2 and TLM S10b, were 50-fold resistant to FLM. A partially revertant cell population (C-10E ND) regained sensitivity to BLM A2, TLM S10b, and FLM. FLM like BLM cleaved pGEM-3Z plasmid DNA in vitro in a concentration-dependent manner. Flow cytometric analysis of FLM content in C-10E and C-10E ND cell lines showed 4-fold and 2-fold lower fluorescence intensity, respectively, compared with A-253 cells. Similar results were seen by fluorescence spectrophotometry with cell extracts. Fluorescence microscopy indicated heterogeneous distribution among A-253 cells with at least 50% of the cells exhibiting marked nuclear fluorescence localization. In contrast, C-10E cells displayed lower cellular fluorescence and predominantly cytoplasmic localization. C-10E ND cells exhibited a mixed population of nuclear and cytoplasmic vesicular localization with fluorescence levels that were intermediate between A-253 and C-10E cells. Thus, BLM-resistant cells have reduced levels of FLM and appear to have a lower nuclear:cytoplasmic ratio of FLM. FLM may be useful in studying the intracellular fate of BLM-like drugs as well as providing a tool to detect and isolate BLM-resistant cells.

摘要

相似文献

1
Synthesis and evaluation of fluoromycin: a novel fluorescence-labeled derivative of talisomycin S10b.
Cancer Res. 1992 Feb 1;52(3):709-18.
2
Characteristics of bleomycin-resistant phenotypes of human cell sublines and circumvention of bleomycin resistance by liblomycin.人细胞亚系博来霉素耐药表型的特征及利博霉素对博来霉素耐药的规避
Cancer Res. 1989 Jan 1;49(1):185-90.
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Liblomycin-mediated DNA cleavage in human head and neck squamous carcinoma cells and purified DNA.利博霉素介导的人头颈鳞状癌细胞和纯化DNA中的DNA切割。
Cancer Res. 1990 Mar 15;50(6):1732-7.
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Lidocaine potentiation of bleomycin A2 cytotoxicity and DNA strand breakage in L1210 and human A-253 cells.利多卡因增强博来霉素A2对L1210细胞和人A - 253细胞的细胞毒性及DNA链断裂作用。
Cancer Res. 1985 May;45(5):2103-9.
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