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含硼多胺作为脑肿瘤中子俘获治疗潜在药物的合成与生物学评价

Synthesis and biological evaluation of boron-containing polyamines as potential agents for neutron capture therapy of brain tumors.

作者信息

Zhuo J C, Cai J, Soloway A H, Barth R F, Adams D M, Ji W, Tjarks W

机构信息

College of Pharmacy and Department of Pathology, The Ohio State University, Columbus, Ohio 43210, USA.

出版信息

J Med Chem. 1999 Apr 8;42(7):1282-92. doi: 10.1021/jm980703f.

Abstract

New boron-containing spermidine/spermine (SPD/SPM) analogues have been synthesized: N5-[4-(2-aminoethyl-o-carboranyl)butyl] and N5-{4-[(2,3-dihydroxypropyl)-o-carboranyl]butyl} SPD/SPM derivatives (ASPD-5, ASPM-5, DHSPD-5, and DHSPM-5) as well as N5-{[4-(dihydroxyboryl)phenyl]methyl}spermidine (BBSPD-5). These boronated polyamines retain their ability to displace ethidium bromide from calf thymus DNA and are rapidly taken up in vitro by F98 rat glioma cells. The in vitro toxicities of ASPD-5, ASPM-5, DHSPD-5, and DHSPM-5 are lower than those previously reported for N5-[4-(o-carboranyl)butyl] SPD/SPM derivatives (SPD-5 and SPM-5) but similar to those of native SPD and SPM. Very low toxicity was also observed for BBSPD-5. In vivo studies of ASPD-5 and BBSPD-5 were performed in mice bearing intracerebral implants of the GL261 glioma and subcutaneous implants of the B16 melanoma. The biodistribution data found in both tumor models suggest that the polyamines synthesized to date do not appear to be suitable boron agents for BNCT.

摘要

新型含硼亚精胺/精胺(SPD/SPM)类似物已被合成:N5-[4-(2-氨基乙基-邻碳硼烷基)丁基]和N5-{4-[(2,3-二羟基丙基)-邻碳硼烷基]丁基}SPD/SPM衍生物(ASPD-5、ASPM-5、DHSPD-5和DHSPM-5)以及N5-{[4-(二羟基硼基)苯基]甲基}亚精胺(BBSPD-5)。这些硼化多胺保留了从 calf胸腺DNA中置换溴化乙锭的能力,并在体外被F98大鼠胶质瘤细胞迅速摄取。ASPD-5、ASPM-5、DHSPD-5和DHSPM-5的体外毒性低于先前报道的N5-[4-(邻碳硼烷基)丁基]SPD/SPM衍生物(SPD-5和SPM-5),但与天然SPD和SPM相似。BBSPD-5的毒性也非常低。在携带GL261胶质瘤脑内植入物和B16黑色素瘤皮下植入物的小鼠中对ASPD-5和BBSPD-5进行了体内研究。在两种肿瘤模型中发现的生物分布数据表明,迄今为止合成的多胺似乎不是适合硼中子俘获疗法(BNCT)的硼剂。

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