与颅脑照射序列和强化化疗给药相关的长期毒性和神经病理学。

Long-term toxicity and neuropathology associated with the sequencing of cranial irradiation and enhanced chemotherapy delivery.

作者信息

Remsen L G, McCormick C I, Sexton G, Pearse H D, Garcia R, Mass M, Roman-Goldstein S, Neuwelt E A

机构信息

Department of Neurology, Oregon Health Sciences University, Portland, USA.

出版信息

Neurosurgery. 1997 May;40(5):1034-40; discussion 1040-2. doi: 10.1097/00006123-199705000-00030.

DOI:10.1097/00006123-199705000-00030

PMID:9149262

Abstract

OBJECTIVE

The goal was to evaluate, at 1 year, 75 Long-Evans rats for survival rates and toxicity associated with the sequencing of cranial irradiation and enhanced chemotherapy delivery.

METHODS

Seventy-five Long-Evans rats were randomized into four groups and evaluated at 1 year for survival rates and toxicity associated with the sequencing of cranial irradiation and enhanced chemotherapy delivery. Radiation (2,000 cGy) was administered as a single fraction, by using parallel opposed portals, 30 days before chemotherapy (Group 1), 24 hours before chemotherapy (Group 2), 30 days after chemotherapy (Group 3), or without chemotherapy or without radiation (control group, Group 4). Five subgroups within each treatment group included rats receiving intra-arterially administered methotrexate (1 g/m2) or intravenously administered etoposide (200 mg/m2) combined with intra-arterially administered carboplatin (200 mg/m2), administered with or without osmotic blood-rain barrier disruption, and a group receiving normal saline solution after blood-brain barrier disruption.

RESULTS

There was a significant increase in total toxic effects when the three experimental groups were compared with the control group (P = 0.001, 0.006, and 0.013 for Groups 1, 2, and 3, respectively). All groups receiving radiation and chemotherapy (particularly carboplatin and etoposide) had an increased incidence of hind limb paralysis, resembling experimental allergic neuritis (P = 0.053). Statistical analysis showed a trend toward increased mortality rates in Group 1 (antecedent radiation), compared with the control group (P = 0.082), and an increased incidence of intracerebral calcification (P = 0.019). No differences in mortality rates were observed for Group 2 or 3, compared with the control group.

CONCLUSION

Radiation before chemotherapy was a more toxic sequence and, surprisingly, carboplatin/etoposide administered in combination with radiotherapy was more detrimental than methotrexate. Additional studies are in progress to evaluate the toxicity and efficacy of sequences of cranial irradiation and enhanced chemotherapy in tumor-bearing rats.

摘要

目的

本研究旨在评估75只Long-Evans大鼠在接受头颅照射和强化化疗联合治疗1年后的生存率及毒性反应。

方法

将75只Long-Evans大鼠随机分为四组，在1年后评估其与头颅照射和强化化疗联合治疗顺序相关的生存率和毒性反应。放疗（2000 cGy）采用平行相对野单次照射，分别在化疗前30天（第1组）、化疗前24小时（第2组）、化疗后30天（第3组）进行，或不进行化疗及放疗（对照组，第4组）。每个治疗组内的五个亚组包括接受动脉内注射甲氨蝶呤（1 g/m²）或静脉注射依托泊苷（200 mg/m²）联合动脉内注射卡铂（200 mg/m²）的大鼠，注射时伴或不伴有渗透性血脑屏障破坏，以及一组在血脑屏障破坏后接受生理盐水的大鼠。

结果

与对照组相比，三个实验组的总毒性效应显著增加（第1组、第2组和第3组的P值分别为0.001、0.006和0.013）。所有接受放疗和化疗（尤其是卡铂和依托泊苷）的组后肢麻痹发生率增加，类似于实验性过敏性神经炎（P = 0.053）。统计分析显示，与对照组相比，第1组（先行放疗）的死亡率有增加趋势（P = 0.082），脑内钙化发生率增加（P = 0.019）。与对照组相比，第2组和第3组的死亡率无差异。