β-galactoside prodrugs of doxorubicin for application in antibody directed enzyme prodrug therapy/prodrug monotherapy

被引:32
作者
Devalapallya, HariKrishna
Navath, Raghavendra Swamy
Yenamandra, Venkateshwarlu
Akkinepally, RaghuRam Rao
Devarakonda, Rama Krishna [1 ]
机构
[1] Kakatiya Univ, Univ Coll Pharmaceut Sci, Drug Metab Pharmacokinet Canc & Aging Res Div, Warangal 9, Andhra Pradesh, India
[2] Kakatiya Univ, Univ Coll Pharmaceut Sci, Med Chem Res Div, Warangal 9, Andhra Pradesh, India
[3] Indian Inst Chem Technol, Organ Div 1, Nat Prod Lab, Hyderabad 7, Andhra Pradesh, India
关键词
prodrugs; doxorubicin; stability; hydrolysis; release kinetics; in vitro cytotoxicity; ANTICANCER PRODRUGS; SELECTIVE ACTIVATION; THERAPY; ANTHRACYCLINES; CONJUNCTION; ADEPT;
D O I
10.1007/BF02977634
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Anthracycline antibiotics, particularly doxorubicin and daunorubicin, have been used extensively in the treatment of human malignancies. However cardiotoxicity and multidrug resistance are significant problems that limit the clinical efficacy of such agents. Rational design to avoid these side effects includes strategies such as drug targeting and prodrug synthesis. Described here are the synthesis and preliminary biological evaluation of the enzymatically activated two new prodrugs (6 & 11) of doxorubicin. These prodrugs were designed as potential candidates for selective chemotherapy in ADEPT or PMT strategies. They are constituted of a galactose moiety, a spacer and the cytotoxic drug and they differ by the type of spacer. The prodrugs were stable in a buffer, and the in vitro studies showed good detoxification and hydrolysis kinetics. As prodrug 11 was readily hydrolyzed, this could be a valuable candidate for further development.
引用
收藏
页码:723 / 732
页数:10
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