N-PHOSPHORYL DERIVATIVES OF BISANTRENE - ANTITUMOR PRODRUGS WITH ENHANCED SOLUBILITY AND REDUCED POTENTIAL FOR TOXICITY

被引:10
|
作者
MURDOCK, KC
LEE, VJ
CITARELLA, RV
DURR, FE
NICOLAU, G
KOHLBRENNER, M
机构
[1] AMER CYANAMID CO,DEPT CHEM INFECT DIS,DIV MED RES,PEARL RIVER,NY 10965
[2] AMER CYANAMID CO,CHEMOTHERAPY RES DEPT,DIV MED RES,PEARL RIVER,NY 10965
[3] AMER CYANAMID CO,METAB RES DEPT,DIV MED RES,PEARL RIVER,NY 10965
关键词
D O I
10.1021/jm00067a007
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
The selective phosphorylation of bisantrene (1) affords bis(phosphonoguanidinic acid) 6, a prodrug with enhanced aqueous solubility (as sodium salt 7) at physiological pH. Unlike 1, in a rat tail vein model, no precipitation was observed when bis(phosphonoguanidinic acid) 6 was injected. While in rats 6 hydrolyzed to monophosphonoguanidinic acid 9 with a half-life of ca. 12 min., complete hydrolysis to bisantrene required several hours. The corresponding monophosphonoguanidinic acid 9 was synthesized from bisantrene and also showed good solubility and antitumor activity. While the antitumor activities of 6 in mice were comparable to bisantrene against B-16 melanoma and P-388 and L-1210 leukemias, it was inactive in vitro vs several tumor cell types. Thus, its activity in vivo resulted from its ability to serve as a prodrug for bisantrene.
引用
收藏
页码:2098 / 2101
页数:4
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