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首页> 外文期刊>Chemical research in toxicology >Formation of Tamoxifen-DNA Adducts in Human Endometrial Explants Exposed to alpha-Hydroxytamoxifen
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Formation of Tamoxifen-DNA Adducts in Human Endometrial Explants Exposed to alpha-Hydroxytamoxifen

机译:暴露于α-羟基他莫昔芬的人子宫内膜外植体中他莫昔芬-DNA加合物的形成

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摘要

An increased risk of developing endometrial cancer has been observed in women receiving tamoxifen (TAM) endocrine therapy and chemoprevention.The genotoxic damage induced by TAM metabolites may be involved in the development of endometrial cancer.To investigate the capability of endometrial tissues to form TAM-DNA adducts,primary cultured human endometrial explants were exposed to a-hydroxytamoxifen (alpha-OHTAM) and used for quantitative analysis of TAM-DNA adducts,using ~(32)P-postlabeling/HPLC analysis.A trans isoform of alpha-(N~2-deoxyguanosinyl)tamoxifen (dG-N~2-TAM) was detected as the major adduct in eight of nine endometrial explants exposed to 100 muM alpha-OHTAM at levels of 7.7 +- 5.3 (mean +- SD) adducts/10~7 nucleotides.Approximately 25- and 37-fold lower amounts of the cis form of dG-N-TAM and another trans isoform were also detected.The dG-N~2-TAM adduct (3.3 adducts/ 10~7 nucleotides) was detected in one of three endometrial explants exposed to 25 muM alpha-OHTAM.No TAM-DNA adducts were detected in any unexposed tissues.These results indicate that TAM-DNA adducts are capable of forming through O-sulfonation and/or O-acetylation of alpha-OHTAM in the endometrium.The endometrial explant culture can be used as a model system to explore the genotoxic mechanism of antiestrogens for humans.
机译:在接受他莫昔芬(TAM)内分泌治疗和化学预防的妇女中发现发生子宫内膜癌的风险增加.TAM代谢物诱导的遗传毒性损害可能与子宫内膜癌的发展有关。研究子宫内膜组织形成TAM-的能力DNA加合物,原代培养的人子宫内膜外植体暴露于α-羟基他莫昔芬(α-OHTAM),并通过〜(32)P后标记/ HPLC分析用于TAM-DNA加合物的定量分析.α-(N在暴露于100μMα-OHTAM的9种子宫内膜外植体中,有8种被检出的〜2-脱氧鸟苷基)他莫昔芬(dG-N〜2-TAM)是主要加合物,水平为7.7 +-5.3(平均值+-SD)加合物/ 10 〜7个核苷酸。还检测到dG-N-TAM的顺式和另一种反式异构体的量分别降低了25和37倍.dG-N〜2-TAM加合物(3.3个加合物/ 10〜7个核苷酸)为在暴露于25μMα-OHTAM的三种子宫内膜外植体之一中检测到。在任何未暴露的组织中均检测到M-DNA加合物,这些结果表明TAM-DNA加合物能够通过子宫内膜中α-OHTAM的O磺化和/或O-乙酰化而形成。模型系统探索抗雌激素对人类的遗传毒性机制。

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