唾液酸酶
病毒
合理设计
病毒学
病毒复制
酶
神经氨酸酶
甲型流感病毒
生物
复制(统计)
H5N1亚型流感病毒
药品
抗病毒药物
微生物学
化学
药理学
生物化学
遗传学
作者
Mark von Itzstein,Wen‐Yang Wu,Gaik B. Kok,Michael S. Pegg,Jeffrey C. Dyason,Betty Jin,Tho van Phan,Mark L. Smythe,Hume F. White,Stuart W. Oliver,Peter M. Colman,Joseph Varghese,David Ryan,Jacqueline M. Woods,Richard C. Bethell,Vanessa J. Hotham,J. M. Cameron,Charles R. Penn
出处
期刊:Nature
[Nature Portfolio]
日期:1993-06-01
卷期号:363 (6428): 418-423
被引量:1842
摘要
Two potent inhibitors based on the crystal structure of influenza virus sialidase have been designed. These compounds are effective inhibitors not only of the enzyme, but also of the virus in cell culture and in animal models. The results provide an example of the power of rational, computer-assisted drug design, as well as indicating significant progress in the development of a new therapeutic or prophylactic treatment for influenza infection.
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