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New bicyclam-AZT conjugates: Design, synthesis, anti-HIV evaluation, and their interaction with CXCR-4 coreceptor

被引:35
作者
Dessolin, J
Galea, P
Vlieghe, P
Chermann, JC
Kraus, JL
机构
[1] Univ Mediterranee, Lab Chim Biomol, Fac Sci Luminy, F-13288 Marseille 9, France
[2] INSERM, U322, F-13273 Marseille, France
来源
JOURNAL OF MEDICINAL CHEMISTRY | 1999年 / 42卷 / 02期
关键词
D O I
10.1021/jm980358u
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
We report the synthesis of mono- and bis-tetraazamacrocycle-AZT conjugates. All new compounds were screened for their ability to inhibit HIV-1 replication in MT4 cell line and were compared to AZT alone. It appears that N-protected covalent prodrugs are equipotent to AZT as inhibitor of HIV replication, while N-deprotected analogues exhibit both higher activity and selectivity against HIV-infected cells. The most active antiviral compounds 27, 28, 34, and 35 were then tested for their binding capability to CXCR-4 receptor. N-Boc analogues 27 and 34 were only weakly effective; in contrast, N-deprotected conjugates 28 and 35 were antagonists to 12G5 mAb binding until 0.05 and 5 mu g/mL, respectively. The stability of compound 28 in human plasma was evaluated, and half-life was found to be approximately 8 h in the described conditions. All these results seem to demonstrate the confidence of our prodrug approach, with analogue 28 emerging as the best candidate as lead compound in HIV-1 polytherapy perspective.
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收藏
页码:229 / 241
页数:13
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