S Desbène, H D Van, S Michel, M Koch, F Tillequin, G Fournier, N Farjaudon, C Monneret
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引用次数: 0
摘要
以(4-羟基甲基-2-硝基苯基2,3,4-三- o -乙酰- β - d -葡萄糖吡喃苷)脲酸甲酯(5)和阿霉素为原料制备了3种新的亲水前药2、3和4。它们的细胞毒性低,经β -d -葡萄糖醛酸酶水解后可有效释放阿霉素,并且在pH 7.2下2和3的稳定性满足了它们用于抗体导向酶前药治疗或前药单药治疗的初步要求。
Doxorubicin prodrugs with reduced cytotoxicity suited for tumour-specific activation.
The three new hydrophilic prodrugs 2, 3 and 4 have been prepared from methyl (4-hydroxymethyl-2-nitrophenyl 2,3,4-tri-O-acetyl-beta-D-glucopyranosid)uronate (5) and doxorubicin. Their low cytotoxicity, efficient release of doxorubicin after hydrolysis by beta-D-glucuronidase, and in the cases of 2 and 3 stability at pH 7.2 fulfil the preliminary requirement for their use in antibody-directed enzyme prodrug therapy or prodrug monotherapy.
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