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十二氢-闭式-十二硼酸盐含磷衍生物用于神经胶质瘤和肉瘤硼中子俘获治疗的体内评估

In vivo evaluation of phosphorous-containing derivatives of dodecahydro-closo-dodecaborate for boron neutron capture therapy of gliomas and sarcomas.

作者信息

Tjarks W, Barth R F, Rotaru J H, Adams D M, Yang W, Kultyshev R G, Forrester J, Barnum B A, Soloway A H, Shore S G

机构信息

College of Pharmacy, Ohio State University, 500 W. 12th Ave, Columbus, Ohio 43210, USA.

出版信息

Anticancer Res. 2001 Mar-Apr;21(2A):841-6.

Abstract

The in vivo uptake of dodecahydro-closo-dodecaborate derivatives substituted with phosphate- and bisphosphonate groups was evaluated in two different experimental tumor model systems and compared to other boronated and non-boronated compounds. These phosphorous-containing boron clusters may have potential for use in boron neutron capture therapy, a chemoradiotherapeutic form of cancer treatment. Using the F98 rat glioma as a brain tumor model in syngeneic Fischer rats, there was selective tumor uptake of the phosphate derivative with 21.5 micrograms boron/g tumor versus 5.2 micrograms/g normal brain and a tumor:blood ratio of 2.7. However, this compound was toxic to test animals and lethal at relatively low doses. The uptake of the bisphosphonate by the murine K8 osteosarcoma was approximately 18 micrograms boron/g tumor with a T:Bl ratio of 7.6 and a tumor:bone ratio of 1.5. This compound was non toxic to the test animals. The results indicate that phosphate- and bisphosphonate derivatives of dodecahydro-closo-dodecaborate may have potential for BNCT of gliomas and osteosarcomas, respectively.

摘要

在两种不同的实验肿瘤模型系统中评估了用磷酸酯和双膦酸酯基团取代的十二氢-闭-十二硼酸盐衍生物的体内摄取情况,并与其他硼化和非硼化化合物进行了比较。这些含磷硼簇可能有潜力用于硼中子俘获疗法,这是一种癌症的化学放射治疗形式。以F98大鼠胶质瘤作为同基因Fischer大鼠的脑肿瘤模型,磷酸酯衍生物在肿瘤中有选择性摄取,肿瘤中硼含量为21.5微克/克,而正常脑中为5.2微克/克,肿瘤与血液的比率为2.7。然而,该化合物对实验动物有毒,在相对低剂量时具有致死性。小鼠K8骨肉瘤对双膦酸酯的摄取量约为18微克硼/克肿瘤,肿瘤与血液比率为7.6,肿瘤与骨骼比率为1.5。该化合物对实验动物无毒。结果表明,十二氢-闭-十二硼酸盐的磷酸酯和双膦酸酯衍生物可能分别有潜力用于胶质瘤和骨肉瘤的硼中子俘获疗法。

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