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卵巢癌细胞敏感性体外测试的药代动力学方法

Pharmacokinetic approach to in vitro testing of ovarian cancer cell sensitivity.

作者信息

Morasca L, Balconi G, Erba E, D'Incalci M, Ottolenghi L, Salmona A, Garattini S

出版信息

Oncology. 1980;37(3):169-73. doi: 10.1159/000225428.

Abstract

Cell populations obtained from ovarian cancer specimens were seeded in primary culture and morphologically identified as cancer cells. Methotrexate, cytosine arabinoside, 5-fluorouracil, antinomycin D, melphalan, and adriamycin were added to the culture medium at different concentrations and for various periods of time. The results are discussed in relation to the pharmacokinetic availability of drugs in the plasma compartment of patients treated by different therapuetic regimens. Totally inactive drugs can be identified by comparing plasma levels with active concentrations while for drugs active in vitro at concentrations in the range of pharmacokinetic levels, the percentage of responders among patients might be explained by the intrinsic variability of cancer cells.

摘要

从卵巢癌标本中获取的细胞群体接种于原代培养物中,并在形态学上鉴定为癌细胞。将甲氨蝶呤、阿糖胞苷、5-氟尿嘧啶、放线菌素D、美法仑和阿霉素以不同浓度添加到培养基中,并作用不同时间。结合不同治疗方案治疗的患者血浆中药物的药代动力学可及性对结果进行了讨论。通过比较血浆水平和活性浓度可鉴定出完全无活性的药物,而对于在药代动力学水平范围内的浓度下体外具有活性的药物,患者中反应者的百分比可能由癌细胞的内在变异性来解释。

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