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大鼠腹腔内顺铂治疗联合区域热疗的优化

Optimisation of intraperitoneal cisplatin therapy with regional hyperthermia in rats.

作者信息

Los G, Sminia P, Wondergem J, Mutsaers P H, Havemen J, ten Bokkel Huinink D, Smals O, Gonzalez-Gonzalez D, McVie J G

机构信息

The Netherlands Cancer Institute, Division of Experimental Chemotherapy, Amsterdam.

出版信息

Eur J Cancer. 1991;27(4):472-7. doi: 10.1016/0277-5379(91)90389-u.

Abstract

The purpose of this study was to optimise intraperitoneal chemotherapy by combining this modality with regional hyperthermia. In vitro data demonstrated that both the uptake of cisplatin into CC531 tumour cells and cytotoxicity were increased at temperatures of 40 degrees C (factor 4) and 43 degrees C (factor 6) compared to 37 degrees C. The increase of intracellular platinum concentration correlated well with the decrease in survival of these cells. In vivo, rats were treated intraperitoneally with cisplatin (5 mg/kg) in combination with regional hyperthermia of the abdomen (41.5 degrees C, 1 h). The mean (S.D.) temperature in the peritoneal cavity was 41.5 (0.3) degrees C and outside the peritoneal cavity 40.5 (0.3) degrees C. Enhanced platinum concentrations were found in peritoneal tumours (factor 4.1) and kidney, liver, spleen and lung (all around a factor 2.0), after combined cisplatin-hyperthermia treatment. The platinum distribution in peritoneal tumours was more homogeneous after the combined treatment than after cisplatin alone, possibly due to increased penetration of cisplatin into peritoneal tumours. Pharmacokinetic data demonstrated an increased tumour exposure for unfiltered platinum in the peritoneal cavity (area under the curve [AUC] increased from 339 mumol/l/min to 486 mumol/l/min at 37 degrees C and 41.5 degrees C, respectively), and for total and ultrafiltered platinum in the blood. The AUC for total platinum increased from 97.9 to 325.8 mumol/min and for ultrafiltered platinum from 22.2 to 107 mumol/l/min at 37 degrees C and 41.5 degrees C respectively. The latter might be due to a slower elimination of platinum from the blood. The combined treatment, intraperitoneal cisplatin and regional hyperthermia, also increased toxicity. The thermal enhancement ratio (TER) using lethality as endpoint was 1.8.

摘要

本研究的目的是通过将腹腔内化疗与区域热疗相结合来优化这种治疗方式。体外数据表明,与37℃相比,在40℃(增加4倍)和43℃(增加6倍)时,顺铂进入CC531肿瘤细胞的摄取量和细胞毒性均增加。细胞内铂浓度的增加与这些细胞存活率的降低密切相关。在体内,大鼠腹腔内注射顺铂(5mg/kg)并结合腹部区域热疗(41.5℃,1小时)。腹腔内平均(标准差)温度为41.5(0.3)℃,腹腔外为40.5(0.3)℃。顺铂-热疗联合治疗后,在腹膜肿瘤中发现铂浓度升高(增加4.1倍),在肾脏、肝脏、脾脏和肺中也升高(均约为2.0倍)。联合治疗后腹膜肿瘤中的铂分布比单独使用顺铂时更均匀,这可能是由于顺铂进入腹膜肿瘤的渗透率增加所致。药代动力学数据表明,腹腔内未过滤铂的肿瘤暴露增加(曲线下面积[AUC]在37℃和41.5℃时分别从339μmol/l/min增加到486μmol/l/min),血液中总铂和超滤铂的暴露也增加。总铂的AUC在37℃和41.5℃时分别从97.9增加到325.8μmol/min,超滤铂的AUC从22.2增加到107μmol/l/min。后者可能是由于铂从血液中的清除较慢。腹腔内顺铂和区域热疗的联合治疗也增加了毒性。以致死率为终点的热增强比(TER)为1.8。

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