Author: Wang, Peng; Li, Linâ€Feng; Wang, Qingâ€Yin; Shang, Luâ€Qing; Shi, Peiâ€Yong; Yin, Zheng
Title: Antiâ€Dengueâ€Virus Activity and Structure–Activity Relationship Studies of Lycorine Derivatives Cord-id: uhbr50ol Document date: 2014_2_26
ID: uhbr50ol
Snippet: 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, 1â€acetyllycorine exhibited the most potent antiâ
Document: 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, 1â€acetyllycorine exhibited the most potent antiâ€DENV activity (EC(50)=0.4 μm) with a reduced cytotoxicity (CC(50)>300 μm), which resulted in a selectivity index (CC(50)/EC(50)) of more than 750. The ketones 1â€acetylâ€2â€oxolycorine (EC(50)=1.8 μm) and 2â€oxolycorine (EC(50)=0.5 μm) also exhibited excellent antiviral activities with low cytotoxicity. Structure–activity relationships for the lycorine derivatives against DENV are discussed. A threeâ€dimensional quantitative structure–activity relationship model was established by using a comparative molecularâ€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.
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