Crystal structure of an antiviral ankyrin targeting the HIV-1 capsid and molecular modeling of the ankyrin-capsid complex

被引:10
|
作者
Praditwongwan, Warachai [1 ,2 ]
Chuankhayan, Phimonphan [3 ]
Saoin, Somphot [1 ,2 ]
Wisitponchai, Tanchanok [4 ]
Lee, Vannajan Sanghiran [5 ,6 ,7 ,8 ]
Nangola, Sawitree [9 ]
Hong, Saw See [10 ,11 ,12 ]
Minard, Philippe [13 ,14 ]
Boulanger, Pierre [10 ,11 ]
Chen, Chun-Jung [3 ,15 ,16 ]
Tayapiwatana, Chatchai [1 ,2 ]
机构
[1] Chiang Mai Univ, Div Clin Immunol, Dept Med Technol, Fac Associated Med Sci, Chiang Mai 50200, Thailand
[2] Chiang Mai Univ, Natl Ctr Genet Engn & Biotechnol, Biomed Technol Res Unit, Natl Sci & Technol Dev Agcy,Fac Associated Med Sc, Chiang Mai 50200, Thailand
[3] Natl Synchrotron Radiat Res Ctr, Sci Res Div, Life Sci Grp, Hsinchu 30076, Taiwan
[4] Chiang Mai Univ, Ctr Biomed Engn, Fac Engn, Chiang Mai 50200, Thailand
[5] Chiang Mai Univ, CSML, Dept Chem, Fac Sci, Chiang Mai 50200, Thailand
[6] Chiang Mai Univ, Fac Sci, Ctr Excellence Innovat Chem, Chiang Mai 50200, Thailand
[7] Chiang Mai Univ, Fac Sci, Mat Sci Res Ctr, Chiang Mai 50200, Thailand
[8] Univ Malaya, Dept Chem, Fac Sci, Kuala Lumpur 50603, Malaysia
[9] Univ Phayao, Div Clin Immunol & Transfus Sci, Dept Med Technol, Sch Allied Hlth Sci, Phayao 56000, Thailand
[10] Univ Lyon 1, Lab Retrovirus & Comparat Pathol, UMR 754, F-69366 Lyon 07, France
[11] INRA, UMR 754, F-69366 Lyon 07, France
[12] INSERM, F-75013 Paris, France
[13] Univ Paris 11, IBBMC, UMR 8619, F-91405 Orsay, France
[14] CNRS, F-91405 Orsay, France
[15] Natl Tsing Hua Univ, Dept Phys, Hsinchu 30013, Taiwan
[16] Natl Cheng Kung Univ, Inst Biotechnol, Tainan 701, Taiwan
关键词
HIV-1; CA protein; Ankyrins; Molecular docking; Modeling; Viral assembly; Antivirals; VIRUS-LIKE PARTICLES; BETULINIC ACID DSB; REPEAT PROTEIN; COMBINATORIAL LIBRARIES; BINDING-SITE; GAG PROTEINS; INHIBITOR; DOMAIN; ZDOCK; CRYSTALLOGRAPHY;
D O I
10.1007/s10822-014-9772-9
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
Ankyrins are cellular repeat proteins, which can be genetically modified to randomize amino-acid residues located at defined positions in each repeat unit, and thus create a potential binding surface adaptable to macromolecular ligands. From a phage-display library of artificial ankyrins, we have isolated Ank(GAG)1D4, a trimodular ankyrin which binds to the HIV-1 capsid protein N-terminal domain (NTDCA) and has an antiviral effect at the late steps of the virus life cycle. In this study, the determinants of the Ank(GAG)1D4-NTDCA interaction were analyzed using peptide scanning in competition ELISA, capsid mutagenesis, ankyrin crystallography and molecular modeling. We determined the Ank(GAG)1D4 structure at 2.2 resolution, and used the crystal structure in molecular docking with a homology model of HIV-1 capsid. Our results indicated that NTDCA alpha-helices H1 and H7 could mediate the formation of the capsid-Ank(GAG)1D4 binary complex, but the interaction involving H7 was predicted to be more stable than with H1. Arginine-18 (R18) in H1, and R132 and R143 in H7 were found to be the key players of the Ank(GAG)1D4-NTDCA interaction. This was confirmed by R-to-A mutagenesis of NTDCA, and by sequence analysis of trimodular ankyrins negative for capsid binding. In Ank(GAG)1D4, major interactors common to H1 and H7 were found to be S45, Y56, R89, K122 and K123. Collectively, our ankyrin-capsid binding analysis implied a significant degree of flexibility within the NTDCA domain of the HIV-1 capsid protein, and provided some clues for the design of new antivirals targeting the capsid protein and viral assembly.
引用
收藏
页码:869 / 884
页数:16
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