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可注射化疗微球与胶质瘤I:植入减瘤肿瘤腔壁后生存期延长

Injectable chemotherapeutic microspheres and glioma I: enhanced survival following implantation into the cavity wall of debulked tumors.

作者信息

Emerich D F, Winn S R, Hu Y, Marsh J, Snodgrass P, LaFreniere D, Wiens T, Hasler B P, Bartus R T

机构信息

Alkermes, Inc., Cambridge, Massachusetts 02139, USA.

出版信息

Pharm Res. 2000 Jul;17(7):767-75. doi: 10.1023/a:1007576405039.

Abstract

PURPOSE

Implantation of biodegradable polymers provides a powerful method to deliver high, sustained concentrations of chemotherapeutics to brain tumors. The present studies examined the ability of injectable polymeric microspheres, formulated to release carboplatin or BCNU for 2-3 weeks, to enhance survival in a rodent model of surgically-resected glioma.

METHODS

Rat glioma (RG2) cells were implanted into the cortex of rats and allowed to grow for 10 days prior to surgical resection. Rats were given either surgical resection only, bolus injection (100 microg) or microspheres containing 10, 50, or 100 microg of carboplatin or BCNU. The microspheres were implanted, via hypodermic injection, either directly into the surgical cavity or into the tissue along the perimeter of the cavity.

RESULTS

The order of survival among treatment groups was: no resection < resection only < bolus chemotherapy < sustained release chemotherapy. Carboplatin and BCNU did not differ in this respect and in each case, the enhanced survival achieved with sustained release was dose-related. However, the enhanced survival achieved with carboplatin was substantially greater when the microspheres were implanted into the perimeter wall of the resection cavity, compared to implantation into the cavity itself. The enhanced survival produced by carboplatin implants along the resection perimeter was associated with a significant attenuation of regrowth of the tumor. Finally, in a separate study in non-tumor brain, atomic absorption spectrophotometry revealed that while the microspheres produced significantly prolonged tissue levels of carboplatin relative to a bolus injection, carboplatin diffusion was limited to brain tissue extending primarily 0.5 mm from the injection site.

CONCLUSIONS

These data demonstrate: (1) that sustained delivery of chemotherapy is superior to equipotent bolus doses following tumor resection, and (2) that direct injection of sustained release microspheres into the tissue surrounding a growing tumor mass may provide superior effects over injections into the surgical cavity. They also suggest that successful implementation of this approach in humans may require measures or circumstances that improve upon the limited spatial drug diffusion from the implantation site.

摘要

目的

植入可生物降解聚合物为向脑肿瘤递送高浓度、持续的化疗药物提供了一种有力方法。本研究考察了经配制可释放卡铂或卡莫司汀2至3周的可注射聚合物微球在手术切除的胶质瘤啮齿动物模型中提高生存率的能力。

方法

将大鼠胶质瘤(RG2)细胞植入大鼠皮层,在手术切除前让其生长10天。大鼠接受仅手术切除、大剂量注射(100微克)或含10、50或100微克卡铂或卡莫司汀的微球治疗。微球通过皮下注射直接植入手术腔或腔周组织。

结果

各治疗组的生存顺序为:未切除<仅切除<大剂量化疗<缓释化疗。卡铂和卡莫司汀在这方面无差异,且在每种情况下,缓释实现的生存改善与剂量相关。然而,与植入手术腔本身相比,当微球植入切除腔周壁时,卡铂实现的生存改善显著更大。沿切除周边的卡铂植入物产生的生存改善与肿瘤再生长的显著减弱相关。最后,在一项针对非肿瘤脑的单独研究中,原子吸收分光光度法显示,相对于大剂量注射,微球使卡铂在组织中的水平显著延长,但卡铂扩散仅限于主要从注射部位延伸0.5毫米的脑组织。

结论

这些数据表明:(1)肿瘤切除后化疗的持续递送优于等效的大剂量给药,(2)将缓释微球直接注射到生长肿瘤块周围的组织中可能比注射到手术腔中产生更好的效果。它们还表明,在人类中成功实施这种方法可能需要改善从植入部位有限的空间药物扩散的措施或情况。

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