New Bicyclam−AZT Conjugates:  Design, Synthesis, Anti-HIV Evaluation, and Their Interaction with CXCR-4 Coreceptor

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 replicat...

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Bibliographic Details
Published in:Journal of medicinal chemistry 1999-01, Vol.42 (2), p.229-241
Main Authors: Dessolin, Jean, Galea, Pascale, Vlieghe, Patrick, Chermann, Jean-Claude, Kraus, Jean-Louis
Format: Article
Language:English
Subjects:
Anti-HIV Agents - chemical synthesis
Anti-HIV Agents - chemistry
Anti-HIV Agents - pharmacology
Antibiotics. Antiinfectious agents. Antiparasitic agents
Antiviral agents
azidothymidine
bicyclam
Bicyclam-AZT Conjugates
Biological and medical sciences
Cell Line
CXCR4 protein
Drug Design
Heterocyclic Compounds - chemistry
Heterocyclic Compounds - pharmacology
HIV-1 - drug effects
HIV-1 - physiology
Human immunodeficiency virus 1
Humans
Magnetic Resonance Spectroscopy
Medical sciences
Molecular Structure
MT-4 cells
MT4 cells
Pharmacology. Drug treatments
Receptors, CXCR4 - drug effects
Spectrometry, Mass, Fast Atom Bombardment
Virus Replication - drug effects
Zidovudine - chemistry
Zidovudine - pharmacology
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Summary: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 μg/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.
ISSN:0022-2623
1520-4804
DOI:10.1021/jm980358u