Complex of HIV-1 Integrase with Cellular Ku Protein: Interaction Interface and Search for Inhibitors

被引:5
作者
Ilgova, Ekaterina [1 ]
Galkin, Simon [1 ,2 ]
Khrenova, Maria [1 ,3 ]
Serebryakova, Marina [4 ]
Gottikh, Marina [1 ,4 ]
Anisenko, Andrey [1 ,2 ,4 ]
机构
[1] Lomonosov Moscow State Univ, Chem Dept, Moscow 119992, Russia
[2] Lomonosov Moscow State Univ, Fac Bioengn & Bioinformat, Moscow 119992, Russia
[3] Russian Acad Sci, Res Ctr Biotechnol, Moscow 119071, Russia
[4] Lomonosov Moscow State Univ, Belozersky Inst Phys Chem Biol, Moscow 119992, Russia
基金
俄罗斯基础研究基金会; 俄罗斯科学基金会;
关键词
Ku70; HIV-1; integrase; protein-protein interactions; MOLECULAR-DYNAMICS; DRUG-RESISTANCE; DNA; INFECTION; LEDGF/P75; BINDING; MODEL; ASSAY; RNA; END;
D O I
10.3390/ijms23062908
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The interaction of HIV-1 integrase and the cellular Ku70 protein is necessary for HIV replication due to its positive effect on post-integration DNA repair. We have previously described in detail the Ku70 binding site within integrase. However, the integrase binding site in Ku70 remained poorly characterized. Here, using a peptide fishing assay and site-directed mutagenesis, we have identified residues I72, S73, and I76 of Ku70 as key for integrase binding. The molecular dynamics studies have revealed a possible way for IN to bind to Ku70, which is consistent with experimental data. According to this model, residues I72 and I76 of Ku70 form a "leucine zipper" with integrase residues, and, therefore, their concealment by low-molecular-weight compounds should impede the Ku70 interaction with integrase. We have identified such compounds by molecular docking and have confirmed their capacity to inhibit the formation of the integrase complex with Ku70. Our data demonstrate that the site of IN binding within Ku70 identified in the present work may be used for further search for inhibitors of the integrase binding to Ku70.
引用
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页数:17
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