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裸鼠体内的人脑肿瘤异种移植作为化疗模型。

Human brain tumor xenografts in nude mice as a chemotherapy model.

作者信息

Houchens D P, Ovejera A A, Riblet S M, Slagel D E

出版信息

Eur J Cancer Clin Oncol. 1983 Jun;19(6):799-805. doi: 10.1016/0277-5379(83)90012-3.

Abstract

Two human brain tumors which were previously established in nude mice were used to determine antitumor efficacy of various therapeutic agents. These tumors were a medulloblastoma (TE-671) and a glioma (U-251) with mass doubling times of 3.5 and 5.5 days respectively as subcutaneous implants in nude mice. Intracranial (i.c.) tumor challenge was accomplished by inoculating tissue culture-grown cells of either tumor into the right cerebral hemisphere to a depth of 3 mm. Median survival time (MST) in untreated mice with 10(5) i.c. injected TE-671 cells was approximately 30 days and 53 days in the U-251 tumor. With 2 X 10(5) U-251 tumor cells the MST was 27-31 days. Groups of mice which had been inoculated with tumor were treated with various doses and schedules of antineoplastic compounds by the i.p. route. The TE-671 tumor responded to AZQ treatment with an increase in life span (ILS) of 37% compared to untreated controls and an ILS of 30% with CCNU treatment. BCNU and PCNU were ineffective. With the U-251 tumor BCNU produced an ILS of greater than 60%, with 75% cures, greater than 112% ILS with PCNU and 49% ILS with CCNU. Neither tumor responded to procarbazine, PALA, dianhydrogalactitol, D-O-norleucine or dibromodulcitol. The U-251 tumor was treated on various schedules and doses with BCNU and found to respond well on late as well as early treatment. A new drug (rapamycin) being investigated by the NCI was found to be very effective against the U-251 tumor. This model system should prove valuable in assessing the effects of various chemotherapeutic modalities against brain tumors.

摘要

使用两个先前在裸鼠体内建立的人脑肿瘤来确定各种治疗药物的抗肿瘤疗效。这些肿瘤分别是髓母细胞瘤(TE - 671)和胶质瘤(U - 251),作为皮下植入物在裸鼠体内时,其质量倍增时间分别为3.5天和5.5天。通过将两种肿瘤的组织培养生长细胞接种到右大脑半球3毫米深处来完成颅内(i.c.)肿瘤攻击。用10⁵个颅内注射的TE - 671细胞接种的未治疗小鼠的中位生存时间(MST)约为30天,而U - 251肿瘤小鼠的MST为53天。接种2×10⁵个U - 251肿瘤细胞时,MST为27 - 31天。接种肿瘤的小鼠组通过腹腔注射途径接受各种剂量和给药方案的抗肿瘤化合物治疗。TE - 671肿瘤对AZQ治疗有反应,与未治疗的对照组相比,寿命延长(ILS)37%,CCNU治疗的ILS为30%。BCNU和PCNU无效。对于U - 251肿瘤,BCNU产生的ILS大于60%,治愈率为75%,PCNU的ILS大于112%,CCNU的ILS为49%。两种肿瘤对丙卡巴肼、PALA、双脱水半乳糖醇、D - O - 正亮氨酸或二溴卫矛醇均无反应。用BCNU对U - 251肿瘤进行了各种给药方案和剂量的治疗,发现无论早期还是晚期治疗,反应都良好。美国国立癌症研究所正在研究的一种新药(雷帕霉素)被发现对U - 251肿瘤非常有效。该模型系统在评估各种化疗方式对脑肿瘤的影响方面应具有重要价值。

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