生理氧环境对人肺癌多细胞肿瘤球体药物致死性的影响。

S Inoue, T Ohnuma
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引用次数: 4

摘要

某些组织学类型的晚期恶性肿瘤包含缺氧和坏死的核心。多细胞球状肿瘤(MTS)具有中心慢性缺氧细胞的特征。我们研究了生理氧环境对多柔比星(DXR)和顺铂(DDP)对MTS生长及细胞致死率的影响。2种人肺癌细胞系制备MTS;PC-6小细胞癌和PC-10鳞状细胞癌,分别生长2、3、4周;在5% CO2/空气或5% 02/5% CO2/90% N2中均可。将小鼠暴露于不同浓度的DXR中1小时,通过克隆致死性试验测定细胞的致死率。在生理氧环境下,两种细胞系的MTS生长均受到抑制。生理氧环境下生长的PC-6 MTS对DXR的敏感性高于空气环境下生长的PC-6 MTS。敏感性差异在2周大的MTS时最为明显,随着MTS大小的增加而逐渐缩小。生理氧环境下生长的PC-10 MTS比空气环境下生长的PC-10 MTS更耐DXR;在2周龄的MTS中,差异再次最为明显。无论细胞处于单层或MTS中,生长在空气中或生理氧环境中,DDP的细胞杀伤效果几乎没有差异。这些观察结果与PC-6 MTS细胞几乎不受生理氧环境的影响,但容易受到DXR的影响的解释一致,而PC-10 MTS细胞则相反。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effects of physiological oxygen environment on drug-induced cell lethality of multicellular tumor spheroids from human lung cancer.

Advanced malignant tumors of certain histological types contain a hypoxic and necrotic core. Multicellular tumor spheroids (MTS) have the characteristics of chronically hypoxic cells in the center. We studied the effects of physiological oxygen environment on MTS growth and the cell lethality produced by doxorubicin (DXR) and cisplatin (DDP). MTS were made from 2 human lung cancer cell lines; PC-6 small cell and PC-10 squamous cell carcinoma, and grown for 2, 3 or 4 weeks; either in 5% CO2/air or 5% 02/5% CO2/90% N2. They were exposed to graded concentrations of DXR for 1 hr and cell lethality was determined by clonogenic assay. In the physiological oxygen environment MTS growth was retarded for both cell lines. PC-6 MTS grown in physiological oxygen environment were more sensitive to DXR than those developed in air. The differential sensitivity was most pronounced with the 2 week old MTS and gradually narrowed with increasing MTS size. In contrast, PC-10 MTS developed in the physiological oxygen environment were more resistant to DXR than those in air; the differences were again most pronounced in 2 week old MTS. There were little differences in cell kill effects of DDP, irrespective of cells being in monolayer or in MTS and growing in air or in physiological oxygen environment. These observations are consistent with the interpretation that cells in PC-6 MTS are scarcely affected by the physiological oxygen environment but easily affected by DXR, whereas cells in PC-10 MTS responded vice versa.

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