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己烯雌酚及其单磷酸酯和二磷酸酯对前列腺癌细胞的细胞毒性活性评估。

Evaluation of the cytotoxic activity of diethylstilbestrol and its mono- and diphosphate towards prostatic carcinoma cells.

作者信息

Schulz P, Bauer H W, Brade W P, Keller A, Fittler F

机构信息

Institut für Physiologische Chemie der Universität München, Germany.

出版信息

Cancer Res. 1988 May 15;48(10):2867-70.

PMID:2834049
Abstract

To evaluate a possible direct cytotoxic effect of diethylstilbestrol diphosphate (DESDP) in the treatment of prostate cancer we exposed three prostatic carcinoma cell lines (LNCaP, DU 145, and PC-3), 2 nonprostatic neoplastic cell lines (KB and EJ), and one nontransformed cell line (MRC-5) to diethylstilbestrol (DES), diethylstilbestrol monophosphate, and DESDP at levels occurring in patients' sera during p.o. DES therapy (2 to 5 ng/ml) or DESDP infusions (1 to 20 micrograms/ml), respectively. With 5 ng/ml of DES no effect was seen in LNCaP cells, even after 14 days of exposure. In contrast, drug levels attained during DESDP infusions showed marked, dose-dependent cytotoxicity towards all cell lines under study. Prostatic cells were not exceptionally sensitive. High-dose DES slightly stimulated the synthesis of prostatic acid phosphatase in LNCaP cells. Formation of foci of polygonal cells was induced by 5 micrograms/ml of DES in cultures of MRC-5 fibroblasts. We conclude that, at high doses, DES liberated from DESDP acts upon a regulatory or metabolic mechanism common to many if not all human cells. Preferential sensitivity of prostate cancer cells in vivo may be due to high local phosphatase activity and/or DES accumulation in prostatic tissue.

摘要

为评估己烯雌酚二磷酸酯(DESDP)在治疗前列腺癌时可能存在的直接细胞毒性作用,我们将三种前列腺癌细胞系(LNCaP、DU 145和PC - 3)、两种非前列腺肿瘤细胞系(KB和EJ)以及一种未转化细胞系(MRC - 5)分别暴露于己烯雌酚(DES)、己烯雌酚单磷酸酯和DESDP中,其浓度分别为口服DES治疗期间患者血清中出现的浓度(2至5 ng/ml)或DESDP输注期间的浓度(1至20 μg/ml)。对于LNCaP细胞,即使暴露14天,5 ng/ml的DES也未见任何作用。相比之下,DESDP输注期间达到的药物浓度对所有研究的细胞系均显示出明显的、剂量依赖性的细胞毒性。前列腺细胞并非特别敏感。高剂量DES轻微刺激了LNCaP细胞中前列腺酸性磷酸酶的合成。在MRC - 5成纤维细胞培养物中,5 μg/ml的DES诱导了多边形细胞灶的形成。我们得出结论,在高剂量下,从DESDP释放的DES作用于许多(如果不是所有)人类细胞共有的调节或代谢机制。前列腺癌细胞在体内的优先敏感性可能归因于前列腺组织中高局部磷酸酶活性和/或DES积累。

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