首页> 外文OA文献 >Uptake of a nido-carboranylporphyrin by human glioma xenografts in athymic nude mice and by syngeneic ovarian carcinomas in immunocompetent mice.
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Uptake of a nido-carboranylporphyrin by human glioma xenografts in athymic nude mice and by syngeneic ovarian carcinomas in immunocompetent mice.

机译:人神经胶质瘤异种移植在无胸腺裸鼠中和同基因卵巢癌在免疫活性小鼠中对Nido-carboranylporphyrin的摄取。

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摘要

A tetraphenylporphyrin bearing four dicarbollide ([B9C2H11]-) cages linked to the o-phenyl ring positions by anilide bonds, known as boronated tetraphenylporphyrin (BTPP), has been synthesized in excellent yield from tetra-(o-aminophenyl) porphyrin and carborane carbonyl chloride followed by base-assisted cage opening and ion exchange to give the highly water-soluble potassium salt. Preliminary studies showed that BTPP accumulates in liver and in a syngeneic ovarian carcinoma, but not in normal brain parenchyma, of mice infused with BTPP subcutaneously for 6 or 7 days via surgically implanted osmotic minipumps. In this study, the uptake of boron was measured in human gliomas xenografted subcutaneously to athymic nude mice in which BTPP was infused intraperitoneally or subcutaneously or both for 3 or 7 days by using similar minipumps. Immunocompetent mice bearing a syngeneic ovarian carcinoma were similarly infused to provide comparative data. Bulk concentrations of boron up to 18 micrograms/g of glioma and up to 45 micrograms/g of carcinoma were observed when up to 102 micrograms/g of tissue was present in the liver after 7 days of BTPP infusion. Glioma boron concentrations were increased by approximately 80% on the average (up to 33 micrograms/g) when correspondingly greater amounts of BTPP were infused in only 3 days. Cell counts and chemical tests on blood samples from individual mice indicate that BTPP causes moderate hepatotoxicity and thrombocytopenia. This hepatohematic toxicity syndrome should be taken into account if BTPP or a similar agent is used for boron neutron-capture therapy (BNCT) of human malignancies.
机译:由四-(邻-氨基苯基)卟啉和碳硼烷羰基化合物以优异的收率合成了带有四个通过苯胺键与邻苯环位置连接到邻苯环位置的二咔唑([B9C2H11]-)笼的四苯基卟啉氯化物,然后碱辅助的笼子打开并进行离子交换,得到高度水溶性的钾盐。初步研究表明,通过外科植入的渗透性微型泵皮下注射BTPP的小鼠,在6或7天之内,BTPP会积聚在肝脏和同基因卵巢癌中,但不会在正常的脑实质中积聚。在这项研究中,在皮下移植到无胸腺裸鼠的人神经胶质瘤中,通过使用类似的微型泵将BTPP腹膜内或皮下或两者同时注入3天或7天,测量了硼的摄取。类似地,输注携带同基因卵巢癌的免疫活性小鼠以提供比较数据。当BTPP输注7天后肝脏中存在高达102微克/克的组织时,观察到硼的最高浓度为18微克/克的神经胶质瘤和高达45微克/克的癌。当仅在3天内注入相应量的BTPP时,胶质瘤硼的浓度平均增加大约80%(最高33微克/克)。对单个小鼠血液样本的细胞计数和化学测试表明,BTPP引起中度肝毒性和血小板减少。如果将BTPP或类似药物用于人体恶性肿瘤的硼中子捕获治疗(BNCT),则应考虑这种肝血液毒性综合征。

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