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Anti‐Dengue‐Virus Activity and Structure–Activity Relationship Studies of Lycorine Derivatives
Authors:Peng Wang  Lin‐Feng Li  Dr Qing‐Yin Wang  Dr Lu‐Qing Shang  Dr Pei‐Yong Shi  Prof?Dr Zheng Yin
Affiliation:1. Department of Chemistry, Nankai University, Tianjin 300071 (P.R. China);2. State Key Laboratory of Elemento‐Organic Chemistry, Nankai University, Tianjin 300071 (P.R. China);3. College of Pharmacy, Nankai University, Tianjin 300071 (P.R. China);4. Novartis Institute for Tropical Diseases, 10 Biopolis Road, #05‐01 Chromos, Singapore 138670 (Singapore)
Abstract:Dengue is a systemic viral infection that is transmitted to humans by Aedes mosquitoes. No vaccines or specific therapeutics are currently available for dengue. Lycorine, which is a natural plant alkaloid, has been shown to possess antiviral activities against flaviviruses. In this study, a series of novel lycorine derivatives were synthesized and assayed for their inhibition of dengue virus (DENV) in cell cultures. Among the lycorine analogues, 1‐acetyllycorine exhibited the most potent anti‐DENV activity (EC50=0.4 μM ) with a reduced cytotoxicity (CC50>300 μM ), which resulted in a selectivity index (CC50/EC50) of more than 750. The ketones 1‐acetyl‐2‐oxolycorine (EC50=1.8 μM ) and 2‐oxolycorine (EC50=0.5 μM ) also exhibited excellent antiviral activities with low cytotoxicity. Structure–activity relationships for the lycorine derivatives against DENV are discussed. A three‐dimensional quantitative structure–activity relationship model was established by using a comparative molecular‐field analysis protocol in order to rationalize the experimental results. Further modifications of the hydroxy group at the C1 position with retention of a ketone at the C2 position could potentially lead to inhibitors with improved overall properties.
Keywords:alkaloids  antiviral agents  dengue virus  lycorine  structure–  activity relationships
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