Effect of interstitial and/or systemic delivery of tirapazamine on the radiosensitivity of human glioblastoma multiforme in nude mice.

R M Cardinale, L E Dillehay, J A Williams, K Tabassi, H Brem, D J Lee
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引用次数: 8

Abstract

The purpose of this study was to investigate the feasibility and the efficacy of administering tirapazamine by a slow-releasing polymer disc that was implanted interstitially into a U251 (human glioblastoma multiforme) tumor grown in nude mice. Tumor-bearing animals, with a tumor nodule 0.8 cm3 in size, were distributed to groups receiving combinations of empty or drug-containing polymer implants in the tumor or contralateral leg, intraperitoneal (i.p.) drug, and/or irradiation. The drug (i.p.) alone (14 mg/kg x6) or in combination with tumor drug implant (2 mg) did not significantly increase the tumor volume doubling time compared to that of control animals. Given with 12 Gy of irradiation in twice a day 2-Gy fractions, combined i.p. drug and tumor drug implant significantly delayed tumor growth compared to irradiation alone, which was not achieved with either drug treatment alone added to irradiation. Toxicity, as manifested by transient weight loss, was primarily seen in animals receiving radiation and i.p. tirapazamine. These results indicated that a slow-releasing tirapazamine disc can be produced and the addition of an interstitially implanted tirapazamine disc further increased the effectiveness of i.p. tirapazamine.

间质和/或全身给药替拉帕嗪对裸鼠人多形性胶质母细胞瘤放射敏感性的影响。
本研究的目的是探讨在裸鼠生长的U251(人多形性胶质母细胞瘤)肿瘤中植入缓释聚合物盘给药替拉帕嗪的可行性和有效性。荷瘤动物,肿瘤结节大小为0.8 cm3,分为两组,分别在肿瘤或对侧腿内植入空的或含药物的聚合物植入物,腹腔内(i.p)药物和/或照射。与对照动物相比,单独给药(14 mg/kg x6)或与肿瘤药物植入物(2 mg)联合用药均未显著增加肿瘤体积倍增时间。给予12 Gy的每日两次2 Gy分量的照射,与单独照射相比,联合i.p.药物和肿瘤药物植入物显著延迟肿瘤生长,而单独添加任何一种药物治疗都无法达到这一效果。毒性,表现为短暂的体重减轻,主要见于接受辐射和口服替拉巴胺的动物。上述结果表明,可以制备缓释的替拉帕胺盘,并在间质植入替拉帕胺盘后,进一步提高了滴注替拉帕胺的有效性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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