Structural basis of second-generation HIV integrase inhibitor action and viral resistance

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Cook, Nicola | Li, Wen | Berta, Dénes | Badaoui, Magd | Ballandras-Colas, Allison | Nans, Andrea | Kotecha, Abhay | Rosta, Edina | Engelman, Alan | Cherepanov, Peter

Edité par CCSD ; American Association for the Advancement of Science (AAAS) -

International audience. Strengths and weaknesses of an HIV drug Retroviruses replicate by inserting a copy of their RNA, which has been reverse transcribed into DNA, into the host genome. This process involves the intasome, a nucleoprotein complex comprising copies of the viral integrase bound at the ends of the viral DNA. HIV integrase strand-transfer inhibitors (INSTIs) stop HIV from replicating by blocking the viral integrase and are widely used in HIV treatment. Cook et al. describe structures of second-generation inhibitors bound to the simian immunodeficiency virus (SIV) intasome and to an intasome with integrase mutations known to cause drug resistance. Passos et al. describe the structures of the HIV intasome bound to a second-generation inhibitor and to developmental compounds that are promising drug leads. These structures show how mutations can cause subtle changes in the active site that affect drug binding, show the basis for the higher activity of later-generation inhibitors, and may guide development of better drugs. Science , this issue p. 806 , p. 810

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