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用全身或瘤内甲氨蝶呤或放疗治疗实验性胶质瘤。

Therapy of an experimental glioma with systemic or intraneoplastic methotrexate or radiation.

作者信息

Tator C H, Wassenaar W, Day A, So W S

出版信息

J Neurosurg. 1977 Feb;46(2):175-84. doi: 10.3171/jns.1977.46.2.0175.

Abstract

An intracranial mouse glioma model was used to study the effectiveness of chemotherapy with methotrexate )MTX) or radiotherapy. Maximum tolerable doses of MTX were established by toxicity studies in nontumor-bearing mice for the intraperitoneal and intracerebral routes of drug administration with and without leucovorin as an antidote. These maximum tolerable doses were then given either by the intraperitoneal route or directly into the tumor to mice bearing intracerebral tumors. The glioma model proved to be extremely useful for assessing the modalities studied, including repeated intraneoplastic injection of MTX. Dosage schedules were successfully developed for administering large amount of MTX and for preventing systemic toxicity by the administration of the antidote. Radiotherapy in single doses and 800 rads delayed the median day of death and produced several long-term survivors. Higher doses were toxic. Intraperitoneal or intraneoplastic MTX was completely ineffective as a chemotherapeutic agent for this tumor, even though very large amounts could be delivered due to the protection from systemic toxicity afforded by leucovorin. It is concluded that MTX is a poor chemotherapeutic agent for this experimental brain tumor, but that the technique of intraneoplastic administration of chemotherapeutic agents is feasible with this model system and should be studied further.

摘要

使用颅内小鼠胶质瘤模型来研究甲氨蝶呤(MTX)化疗或放疗的效果。通过在无肿瘤小鼠中进行毒性研究,确定了腹腔内和脑内给药途径(有无亚叶酸作为解毒剂)时MTX的最大耐受剂量。然后将这些最大耐受剂量通过腹腔内途径或直接注射到患有脑肿瘤的小鼠肿瘤内。结果证明,该胶质瘤模型对于评估所研究的治疗方式非常有用,包括在肿瘤内重复注射MTX。成功制定了给药方案,用于给予大量MTX并通过给予解毒剂来预防全身毒性。单次800拉德的放疗延迟了中位死亡天数,并产生了几名长期存活者。更高剂量则具有毒性。腹腔内或肿瘤内注射MTX作为该肿瘤的化疗药物完全无效,尽管由于亚叶酸提供的全身毒性保护,可以给予非常大量的MTX。结论是,MTX作为这种实验性脑肿瘤的化疗药物效果不佳,但在该模型系统中肿瘤内给药化疗药物的技术是可行的,应进一步研究。

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