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使用缓释载体泊洛尼克凝胶增强重组白细胞介素2对可移植大鼠纤维肉瘤的治疗效果。

Enhancement of therapeutic effects of recombinant interleukin 2 on a transplantable rat fibrosarcoma by the use of a sustained release vehicle, pluronic gel.

作者信息

Morikawa K, Okada F, Hosokawa M, Kobayashi H

出版信息

Cancer Res. 1987 Jan 1;47(1):37-41.

PMID:3491675
Abstract

We have tested the feasibility of pluronic F-127 gel (PLF-127; a polyoxyethylene-polyoxypropylene surface active block copolymer) as a sustained release vehicle for topical administration of interleukin 2 (IL-2) in order to enhance the therapeutic effects of IL-2 against a rat fibrosarcoma, KMT-17. Injection of human DNA recombinant IL-2 (3 X 10(4) units s.c.) in 30% (w/w) PLF-127 into rats provided detectable serum IL-2 levels for up to 10 h, while injection of IL-2 alone provided detectable IL-2 levels for 3 h. When, following s.c. inoculation with 1 X 10(5) KMT-17 tumor cells into rats, IL-2 (6 X 10(4) units/day) in PLF-127 gels was injected s.c. around the growing tumor inoculum every 2 days for 10 days from Day 1 to Day 19, the survival days of rats were more prolonged [mean survival day, 32.3 +/- 5.4 (SD)] as compared with that of rats treated with saline [20.7 +/- 2.1] than mean survival days of rats treated with IL-2 alone [27.3 +/- 4.5] or PLF-127 alone [22.9 +/- 3.3]. Moreover, the span of mean survival days of rats treated with IL-2 in PLF-127 locally (31.7 +/- 5.9) was much longer than that of rats given IL-2 in PLF-127 systemically (22.8 +/- 3.4). By means of a Winn assay, stronger tumor neutralizing activities were observed in regional lymph node cells obtained from tumor bearing rats treated with IL-2 in PLF-127 than were observed in lymph node cells from rats treated with IL-2 alone or PLF-127 alone (percentage of inhibition, 90.3, 12.2, and -15.5%, respectively). The therapeutic effects of IL-2 were thus found to be consistent with the antitumor activity in regional lymph node cells. These results suggest that the enhanced therapeutic effects of IL-2 in PLF-127 are due to enhancement of antitumor immune responses induced by sustained IL-2 activity at the tumor sites.

摘要

我们测试了普朗尼克F - 127凝胶(PLF - 127;一种聚氧乙烯 - 聚氧丙烯表面活性嵌段共聚物)作为白细胞介素2(IL - 2)局部给药缓释载体的可行性,以增强IL - 2对大鼠纤维肉瘤KMT - 17的治疗效果。将人DNA重组IL - 2(3×10⁴单位,皮下注射)注射到含30%(w/w)PLF - 127的大鼠体内,可使血清IL - 2水平在长达10小时内保持可检测,而单独注射IL - 2时,可检测的IL - 2水平仅持续3小时。在给大鼠皮下接种1×10⁵个KMT - 17肿瘤细胞后,从第1天到第19天,每2天在生长的肿瘤接种部位周围皮下注射含IL - 2(6×10⁴单位/天)的PLF - 127凝胶,与用生理盐水处理的大鼠[平均存活天数,20.7±2.1]相比,大鼠的存活天数延长更多[平均存活天数,32.3±5.4(标准差)],比单独用IL - 2处理的大鼠[27.3±4.5]或单独用PLF - 127处理的大鼠[22.9±3.3]的平均存活天数都长。此外,局部给予含IL - 2的PLF - 127的大鼠平均存活天数范围(31.7±5.9)比全身给予含IL - 2的PLF - 127的大鼠(22.8±3.4)长得多。通过Winn试验,在接受含IL - 2的PLF - 127治疗的荷瘤大鼠的区域淋巴结细胞中观察到比单独用IL - 2或单独用PLF - 127处理的大鼠的淋巴结细胞更强的肿瘤中和活性(抑制百分比分别为90.3%、12.2%和 - 15.5%)。因此发现IL - 2的治疗效果与区域淋巴结细胞中的抗肿瘤活性一致。这些结果表明,IL - 2在PLF - 127中的治疗效果增强是由于肿瘤部位IL - 2持续活性诱导的抗肿瘤免疫反应增强所致。

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