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硼化卟啉(BOPP)和巯基硼氢化物(BSH)在RG2大鼠胶质瘤模型中的药代动力学和生物分布的比较研究。

A comparative study on the pharmacokinetics and biodistribution of boronated porphyrin (BOPP) and sulfhydryl boron hydride (BSH) in the RG2 rat glioma model.

作者信息

Ceberg C P, Brun A, Kahl S B, Koo M S, Persson B R, Salford L G

机构信息

Department of Radiation Physics, Lund University Hospital, Sweden.

出版信息

J Neurosurg. 1995 Jul;83(1):86-92. doi: 10.3171/jns.1995.83.1.0086.

DOI:10.3171/jns.1995.83.1.0086
PMID:7782856
Abstract

Boron neutron capture therapy is a treatment modality for cancer that depends on the specific uptake of boron by the tumor cells. The infiltrative growth of malignant gliomas requires that boron reach and accumulate in migrating cells outside the margin of the tumor; thus, it is important that the biodistribution of new boron compounds is also studied in the surrounding healthy brain tissue. This study is undertaken in the present work, in which the biodistribution and pharmacokinetics of sulfhydryl boron hydride (BSH) and boronated porphyrin (BOPP) in the RG2 rat glioma model are investigated. This model mimics the characteristics of human glioma with cells migrating into the surrounding brain. The animals were infused intravenously with either BSH (25 micrograms or 175 micrograms of boron per gram of body weight) or BOPP (12 micrograms of boron per gram body weight). For the low dose of BSH, the maximum tumor-boron content was 8 ppm at approximately 9 hours after the infusion with a tumor-to-blood ratio of 0.6. At the higher dose, the corresponding figures were 15 ppm after 12 hours with a tumor-to-blood ratio of 0.5. For BOPP, a tumor-boron concentration of 81 ppm was achieved 24 hours after the infusion and sustained in that range for at least 72 hours. The tumor-to-blood ratio at 24 hours was slightly above 6, but continued to increase as the blood was cleared. These results indicate that both compounds are spread into the normal brain tissue following the same pathways as the migrating tumor cells and in this way can be taken up even in distant tumor cell foci.

摘要

硼中子俘获疗法是一种癌症治疗方式,它依赖于肿瘤细胞对硼的特异性摄取。恶性胶质瘤的浸润性生长要求硼到达并积聚在肿瘤边缘外迁移的细胞中;因此,研究新型硼化合物在周围健康脑组织中的生物分布也很重要。本研究即为此目的而开展,其中研究了巯基硼氢化物(BSH)和硼化卟啉(BOPP)在RG2大鼠胶质瘤模型中的生物分布和药代动力学。该模型模拟了人类胶质瘤细胞迁移至周围脑组织的特征。给动物静脉注射BSH(每克体重25微克或175微克硼)或BOPP(每克体重12微克硼)。对于低剂量的BSH,输注后约9小时最大肿瘤硼含量为8 ppm,肿瘤与血液的比率为0.6。在较高剂量下,相应的数据是输注12小时后为15 ppm,肿瘤与血液的比率为0.5。对于BOPP,输注后24小时肿瘤硼浓度达到81 ppm,并在该范围内持续至少72小时。24小时时肿瘤与血液的比率略高于6,但随着血液清除而持续增加。这些结果表明,这两种化合物都通过与迁移肿瘤细胞相同的途径扩散到正常脑组织中,因此即使在远处的肿瘤细胞灶中也能被摄取。

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