KuINins as a New Class of HIV-1 Inhibitors That Block Post-Integration DNA Repair.
Andrey AnisenkoSimon GalkinAndrey A MikhaylovMaria G KhrenovaYulia AgapkinaSergey KorolevLidia GarkulVasilissa ShirokovaViktoria A IkonnikovaAlexander A KorlyukovPavel DorovatovskiiMikhail S BaranovMarina GottikhPublished in: International journal of molecular sciences (2023)
Integration of HIV-1 genomic cDNA results in the formation of single-strand breaks in cellular DNA, which must be repaired for efficient viral replication. Post-integration DNA repair mainly depends on the formation of the HIV-1 integrase complex with the Ku70 protein, which promotes DNA-PK assembly at sites of integration and its activation. Here, we have developed a first-class inhibitor of the integrase-Ku70 complex formation that inhibits HIV-1 replication in cell culture by acting at the stage of post-integration DNA repair. This inhibitor, named s17, does not affect the main cellular function of Ku70, namely its participation in the repair of double-strand DNA breaks through the non-homologous end-joining pathway. Using a molecular dynamics approach, we have constructed a model for the interaction of s17 with Ku70. According to this model, the interaction of two phenyl radicals of s17 with the L76 residue of Ku70 is important for this interaction. The requirement of two phenyl radicals in the structure of s17 for its inhibitory properties was confirmed using a set of s17 derivatives. We propose to stimulate compounds that inhibit post-integration repair by disrupting the integrase binding to Ku70 KuINins.
Keyphrases
- dna repair
- antiretroviral therapy
- dna damage
- hiv positive
- hiv testing
- hiv infected
- human immunodeficiency virus
- molecular dynamics
- hepatitis c virus
- dna damage response
- hiv aids
- men who have sex with men
- circulating tumor
- cell free
- single molecule
- south africa
- physical activity
- density functional theory
- sars cov
- amino acid
- oxidative stress
- wastewater treatment
- small molecule
- copy number