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硼中子俘获疗法候选化合物5-二羟基硼基-6-丙基-2-硫尿嘧啶(BPTU)在荷黑素瘤小鼠体内的药代动力学

Pharmacokinetics in melanoma-bearing mice of 5-dihydroxyboryl-6-propyl-2-thiouracil (BPTU), a candidate compound for boron neutron capture therapy.

作者信息

Verrijk R, Smolders I J, Huiskamp R, Gavin P R, Philipp K H, Begg A C

机构信息

The Netherlands Cancer Institute, Division of Experimental Therapy, Amsterdam.

出版信息

Br J Cancer. 1994 Apr;69(4):641-7. doi: 10.1038/bjc.1994.125.

Abstract

Blood pharmacokinetics and tissue distribution of 5-dihydroxyboryl-6-propyl-2-thiouracil (BPTU), a boron carrier with postulated melanin-seeking properties for boron neutron capture therapy, were determined in C57/BL mice with subcutaneous pigmented or non-pigmented B16 melanomas. Borocaptate sodium (BSH) was used as a boron compound without melanin-seeking properties in a comparative biodistribution study in the same animal tumour models. Administration of single doses showed that BPTU was retained better in the pigmented B16 tumour than in the non-pigmented variant. BPTU was found in large concentrations in kidney and liver. Brain boron was approximately 10-fold lower than tumour boron. On a molar basis, BPTU demonstrated higher affinity for B16 tumours than BSH. Owing to solubility limits, tumour boron concentrations in this mouse study were too low for effective application of BNCT. However, the high tumour-to-blood and tumour-to-normal tissues ratios indicate that, with appropriate formulation, BPTU could be a promising candidate for clinical BNCT.

摘要

在患有皮下色素沉着或无色素B16黑色素瘤的C57/BL小鼠中,测定了5-二羟基硼基-6-丙基-2-硫脲(BPTU)的血液药代动力学和组织分布。BPTU是一种硼载体,假定具有用于硼中子俘获疗法的黑色素靶向特性。在相同动物肿瘤模型的比较生物分布研究中,硼酸钠(BSH)被用作不具有黑色素靶向特性的硼化合物。单剂量给药表明,BPTU在色素沉着的B16肿瘤中的保留率高于无色素变体。在肾脏和肝脏中发现了高浓度的BPTU。脑硼含量比肿瘤硼含量低约10倍。以摩尔计,BPTU对B16肿瘤的亲和力高于BSH。由于溶解度限制,该小鼠研究中的肿瘤硼浓度过低,无法有效应用硼中子俘获疗法。然而,高肿瘤与血液以及肿瘤与正常组织的比率表明,通过适当的制剂,BPTU可能是临床硼中子俘获疗法的有前途的候选者。

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