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Activity- and schedule-dependent interactions of paclitaxel, etoposide and hydroperoxy-ifosfamide in cisplatin-sensitive and -refractory human ovarian carcinoma cell lines.

机译:紫杉醇,依托泊苷和氢过氧化物-异环磷酰胺在顺铂敏感和难治性人类卵巢癌细胞系中的活性和时间表依赖性相互作用。

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摘要

Paclitaxel has demonstrated broad clinical activity in a variety of malignancies both alone and in combination with other chemotherapeutic agents. The in vitro cytotoxicity of a 2 h exposure to paclitaxel, hydroperoxy-ifosfamide and etoposide alone, in combination and in sequence, was evaluated against established cisplatin-sensitive and cisplatin-refractory human ovarian carcinoma cell lines using isobologram analysis. The combinations of either paclitaxel-hydroperoxy-ifosfamide or paclitaxel-etoposide were found to be additive or synergistic when the drugs were given simultaneously or when paclitaxel was given 24 h before hydroperoxy-ifosfamide or etoposide respectively. However, when etoposide or hydroperoxy-ifosfamide were given before paclitaxel, antagonistic interactions were observed. With regard to etoposide this antagonism was evident for up to 24 h. In agreement with our data with the schedule-dependent interactions of paclitaxel and cisplatin in human gastric and ovarian carcinoma cell lines, these data demonstrate that the interactions of paclitaxel, etoposide and hydroperoxy-ifosfamide are also highly schedule dependent and applications of etoposide or ifosfamide before paclitaxel may result in pronounced antagonism. These findings could have implications for the design of further clinical protocols.
机译:紫杉醇已单独或与其他化学治疗剂联合使用,在多种恶性肿瘤中显示出广泛的临床活性。单独和组合使用紫杉醇,氢过氧化物-异环磷酰胺和依托泊苷暴露2 h的体外细胞毒性,通过等效线图分析评估了对已建立的顺铂敏感和顺铂难治性人类卵巢癌细胞系的毒性。紫杉醇-氢过氧-异环磷酰胺或紫杉醇-依托泊苷的组合被发现是当药物同时给药时或分别在氢过氧-异环磷酰胺或依托泊苷给药前24小时给予紫杉醇时是加和或协同的。然而,当在紫杉醇之前给予依托泊苷或氢过氧异环磷酰胺时,观察到拮抗作用。对于依托泊苷,这种拮抗作用长达24小时是明显的。与我们的数据以及紫杉醇和顺铂在人胃和卵巢癌细胞系中的依赖于时间表的相互作用相一致,这些数据表明紫杉醇,依托泊苷和氢过氧化物-异环磷酰胺的相互作用也高度依赖于时间表,并且依托泊苷或异环磷酰胺的应用之前紫杉醇可能导致明显的拮抗作用。这些发现可能对进一步临床方案的设计有影响。

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