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顺铂和卡铂抑制细胞存活恢复的有效性:治疗顺序的影响。

Effectiveness in inhibition of recovery of cell survival by cisplatin and carboplatin: influence of treatment sequence.

作者信息

Schwachöfer J H, Crooijmans R P, Hoogenhout J, Kal H B, Theeuwes A G

机构信息

Department of Radiotherapy, University Hospital Nijmegen, The Netherlands.

出版信息

Int J Radiat Oncol Biol Phys. 1991 Jun;20(6):1235-41. doi: 10.1016/0360-3016(91)90233-t.

Abstract

Clinical protocols have been designed to combine platinum-based drugs and radiation in the treatment of cancer. The rationale for this approach has been developed from preclinical studies demonstrating that platinum compounds can potentiate the cytotoxic effects of radiation toward cells. In the present study multicellular spheroids derived from squamous cell carcinoma cell line HN-1 have been used to study the effects of both cisplatin and carboplatin when administered prior to, concurrently, and after irradiation treatment. To study the influence of platinum compounds on sublethal damage repair, single and split doses of radiation were applied. Growth delay and proportion cured spheroids served as endpoints. Both cisplatin and carboplatin had no potentiating effect when administered 24 hr prior to irradiation. When administered 3 hr after completion of irradiation procedures, growth delay after single and split doses were enhanced to the same extent. The drug enhancement ratio for cisplatin was larger (1.5) than for carboplatin (1.2). Both single and split doses were enhanced by the same factor, which was interpreted as no effect on sublethal damage repair. When platinum compounds were present in the target cells at the time of irradiation, especially the split dose radiation response was strongly enhanced: the drug enhancement ratio was 3.9 for cisplatin and 3.2 for carboplatin. Recovery from sublethal damage was totally repressed. This study shows that platinum compounds can potentiate radiation and that for maximum effect the sequence of the two treatment modalities is of utmost importance. Moreover, these results may in part explain the heterogeneous outcomes of trials combining platinum compounds and radiation.

摘要

临床方案已设计用于联合铂类药物和放疗来治疗癌症。这种方法的理论依据源于临床前研究,该研究表明铂化合物可增强放疗对细胞的细胞毒性作用。在本研究中,源自鳞状细胞癌细胞系HN - 1的多细胞球体被用于研究顺铂和卡铂在放疗前、放疗期间和放疗后给药时的效果。为了研究铂化合物对亚致死损伤修复的影响,采用了单次和分次放疗剂量。生长延迟和治愈球体的比例作为终点指标。在放疗前24小时给药时,顺铂和卡铂均无增强作用。在放疗程序完成后3小时给药时,单次和分次剂量后的生长延迟均得到相同程度的增强。顺铂的药物增强比(1.5)大于卡铂(1.2)。单次和分次剂量均以相同倍数增强,这被解释为对亚致死损伤修复无影响。当在放疗时靶细胞中存在铂化合物时,尤其是分次剂量放疗反应会强烈增强:顺铂的药物增强比为3.9,卡铂为3.2。亚致死损伤的恢复被完全抑制。本研究表明铂化合物可增强放疗效果,并且为达到最大效果,两种治疗方式的顺序至关重要。此外,这些结果可能部分解释了联合铂化合物和放疗试验结果的异质性。

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