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白细胞介素12与化疗在小鼠MB - 49膀胱癌和B16黑色素瘤中的最佳给药方案

Optimal scheduling of interleukin 12 and chemotherapy in the murine MB-49 bladder carcinoma and B16 melanoma.

作者信息

Teicher B A, Ara G, Buxton D, Leonard J, Schaub R G

机构信息

Dana-Farber Cancer Institute and Joint Center for Radiation Therapy, Boston, MA 02115, USA.

出版信息

Clin Cancer Res. 1997 Sep;3(9):1661-7.

PMID:9815857
Abstract

The antitumor activity of interleukin (IL)-12, a naturally occurring cytokine, has been demonstrated in several murine solid tumors. Animals bearing established B16 melanoma or MB-49 bladder carcinoma were used to study the most effective scheduling of recombinant murine IL-12 (rmIL-12), along with systemic chemotherapy. rmIL-12 (0. 45, 4.5, or 45 microgram/kg) was more effective as a single agent when administered to mice bearing the MB-49 bladder carcinoma at the highest dose for 11 doses rather than for 5 doses. In combination with chemotherapy (Adriamycin, cyclophosphamide, or 5-fluorouracil), rmIL-12 administration did not increase the toxicity of the chemotherapy, and there was increased antitumor activity with each rmIL-12-drug combination. Administering rmIL-12 (45 microgram/kg) on days 4-14, along with Adriamycin, cyclophosphamide, or 5-fluorouracil on days 7-11, resulted in 2.2-2.7-fold increases in tumor growth delay, compared with the chemotherapy alone against the primary tumor, and a marked decrease in the number of lung metastases on day 20. Because the B16 melanoma grows more slowly than the MB-49 bladder carcinoma, allowing multiple courses of chemotherapy, cyclophosphamide could be administered. The rmIL-12 (45 microgram/kg)-cyclophosphamide combination regimen that was most effective overlapped 2 days with the terminal portion of the chemotherapy treatment. There was a parallel increase in the response of the primary tumor and metastatic disease to the lungs. Administration of rmIL-12 to animals bearing the MB-49 bladder carcinoma or the B16 melanoma was compatible with coadministration of chemotherapy at full dose without additional toxicity.

摘要

白细胞介素(IL)-12是一种天然存在的细胞因子,其抗肿瘤活性已在多种小鼠实体瘤中得到证实。携带已形成的B16黑色素瘤或MB-49膀胱癌的动物被用于研究重组小鼠IL-12(rmIL-12)与全身化疗联合使用时的最有效给药方案。当以最高剂量(0.45、4.5或45微克/千克)给携带MB-49膀胱癌的小鼠注射11剂而非5剂时,rmIL-12作为单一药物更有效。与化疗药物(阿霉素、环磷酰胺或5-氟尿嘧啶)联合使用时,rmIL-12的给药并未增加化疗的毒性,且每种rmIL-12与药物的联合使用均增强了抗肿瘤活性。在第4至14天给予rmIL-12(45微克/千克),同时在第7至11天给予阿霉素、环磷酰胺或5-氟尿嘧啶,与单独使用化疗药物相比,原发性肿瘤的肿瘤生长延迟增加了2.2至2.7倍,并且在第20天时肺转移灶数量显著减少。由于B16黑色素瘤的生长速度比MB-49膀胱癌慢,因此可以进行多疗程化疗,可给予环磷酰胺。最有效的rmIL-12(45微克/千克)-环磷酰胺联合治疗方案与化疗治疗末期部分重叠2天。原发性肿瘤和肺部转移性疾病的反应呈平行增加。给携带MB-49膀胱癌或B16黑色素瘤的动物注射rmIL-12与全剂量化疗药物联合使用是相容的,且不会增加额外毒性。

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