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| Title | Structural basis of second-generation HIV integrase inhibitor action and viral resistance. |
|---|---|
| Journal, issue, pages | Science, Vol. 367, Issue 6479, Page 806-810, Year 2020 |
| Publish date | Feb 14, 2020 |
Authors | Nicola J Cook / Wen Li / Dénes Berta / Magd Badaoui / Allison Ballandras-Colas / Andrea Nans / Abhay Kotecha / Edina Rosta / Alan N Engelman / Peter Cherepanov / ![]() |
| PubMed Abstract | Although second-generation HIV integrase strand-transfer inhibitors (INSTIs) are prescribed throughout the world, the mechanistic basis for the superiority of these drugs is poorly understood. We ...Although second-generation HIV integrase strand-transfer inhibitors (INSTIs) are prescribed throughout the world, the mechanistic basis for the superiority of these drugs is poorly understood. We used single-particle cryo-electron microscopy to visualize the mode of action of the advanced INSTIs dolutegravir and bictegravir at near-atomic resolution. Glutamine-148→histidine (Q148H) and glycine-140→serine (G140S) amino acid substitutions in integrase that result in clinical INSTI failure perturb optimal magnesium ion coordination in the enzyme active site. The expanded chemical scaffolds of second-generation compounds mediate interactions with the protein backbone that are critical for antagonizing viruses containing the Q148H and G140S mutations. Our results reveal that binding to magnesium ions underpins a fundamental weakness of the INSTI pharmacophore that is exploited by the virus to engender resistance and provide a structural framework for the development of this class of anti-HIV/AIDS therapeutics. |
External links | Science / PubMed:32001525 / PubMed Central |
| Methods | EM (single particle) |
| Resolution | 2.81 - 3.36 Å |
| Structure data | EMDB-10041, PDB-6rwl: EMDB-10042, PDB-6rwm: EMDB-10043, PDB-6rwn: EMDB-10044, PDB-6rwo: |
| Chemicals | ![]() ChemComp-ZN: ![]() ChemComp-MG: ![]() ChemComp-KLQ: ![]() ChemComp-CL: ![]() ChemComp-HOH: ![]() ChemComp-DLU: |
| Source |
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Keywords | RECOMBINATION / retroviral integrase / lentivirus / strand transfer inhibior / protein-DNA complex |
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simian immunodeficiency virus
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