Identification of Adjacent NNRTI Binding Pocket in Multi-mutated HIV1- RT Enzyme Model: An in silico Study

R.F.       Kamil; U.       Debnath; S.       Verma; Y.S.       Prabhakar

Abstract

Introduction: A possible strategy to combat mutant strains is to have a thorough structural evaluation before and after mutations to identify the diversity in the non-nucleoside inhibitor binding pocket and their effects on enzyme-ligand interactions to generate novel NNRTI’s accordingly.

Objective: The primary objective of this study was to find effects of multiple point mutations on NNRTI binding pocket. This study included the contribution of each individual mutation in NNIBP that propose an adjacent binding pocket which can be used to discover novel NNRTI derivatives.

Methods: An in Silico model of HIV-1 RT enzyme with multiple mutations K103N, Y181C and Y188L was developed and evaluated. Two designed NNRTI pyridinone derivatives were selected as ligands for docking studies with the homology model through alignment based docking and residue based docking approaches. Binding pockets of wild type HIV-1 RT and multi-mutated homology model were compared thoroughly.

Result and Discussion: K103N mutation narrowed the entrance of NNRTI binding pocket and forbade electrostatic interaction with α amino group of LYS103. Mutations Y181C and Y188L prevented NNRTI binding by eliminating aromatic π interactions offered by tyrosine rings. Docking study against new homology model suggested an adjacent binding pocket with combination of residues in palm and connection domains. This pocket is approximately 14.46Å away from conventional NNRTI binding site.

Conclusion: Increased rigidity, steric hindrance and losses of important interactions cumulatively prompt ligands to adapt adjacent NNRTI binding pocket. The proposed new and adjacent binding pocket is identified by this study which can further be evaluated to generate novel derivatives.

Keywords: AIDS, HIV1-RT, NNRTIs, Non nucleoside inhibitor binding pocket, Docking, MD simulation.

« Previous Next »

Graphical Abstract

[1] 
Kent A, Sepkowitz MD. AIDS-the first 20 years. N Engl J Med  2001; 344(23): 1764-72.
[2] 
Douek DC, Roederer M, Koup RA. Emerging Concepts in the Immunopathogenesis of AIDS. Annu Rev Med  2009; 60(1): 471-84.
[3] 
Leitner T, Keuken C, Hahn B, et al. HIV sequence compendium 2008 los alamos HIV sequence database. HIV Seq Compend  2008; 1-7.
[4] 
Hu WS, Hughes SH. HIV-1 reverse transcription. Cold Spring Harb Perspect Med  2012; 2(10): 1-22.
[5] 
Kohlstaedt LA, Wang J, Friedman JM, Rice PA, Steitz TA. Crystal structure at 3.5 A resolution of HIV-1 reverse transcriptase complexed with an inhibitor. Science  1992; 256(5065): 1783-90.
[6] 
Jacobo-Molina A, Ding J, Nanni RG, et al. Crystal structure of human immunodeficiency virus type 1 reverse transcriptase complexed with double-stranded DNA at 3.0 A resolution shows bent DNA. Proc Natl Acad Sci  1993; 90(13): 6320-4.
[7] 
Castro HC, Loureiro NIV, Pujol-Luz M, et al. HIV-1 reverse transcriptase: a therapeutical target in the spotlight. Curr Med Chem  2006; 13(3): 313-24.
[8] 
Alcaro S, Artese A, Ceccherini-Silberstein F, et al. Computational analysis of human immunodeficiency virus (HIV) Type-1 reverse transcriptase crystallographic models based on significant conserved residues found in Highly Active Antiretroviral Therapy (HAART)-treated patients. Curr Med Chem  2010; 17(4): 290-308.
[9] 
Sluis-Cremer N, Arion D, Parniak MA. Molecular mechanisms of HIV-1 resistance to nucleoside reverse transcriptase inhibitors (NRTIs). C Cell Mol Life Sci  2000; 57(January): 1408-22.
[10] 
Cihlar T, Ray AS. Nucleoside and nucleotide HIV reverse transcriptase inhibitors: 25 years after zidovudine. Antiviral Res  2010; 85: 39-58.
[11] 
Rittinger K, Divita G, Goody RS. Human immunodeficiency virus reverse transcriptase substrate-induced conformational changes and the mechanism of inhibition by nonnucleoside inhibitors. Proc Natl Acad Sci USA  1995; 92: 8046-9.
[12] 
Huang H. Structure of a covalently trapped catalytic complex of HIV-1 reverse transcriptase: implications for drug resistance. Science  1998; 282(5394): 1669-75.
[13] 
Beyer A, Lawtrakul L, Hannongbua S, Wolschann P.  Systematic investigation of non-nucleoside inhibitors of HIV-1 reverse transcriptase (NNRTIs). Monatshefte for Chemie/Chemical Mon 2004; 135(8): 1047-59.
[14] 
Rodgers DW, Gamblin SJ. The structure of unliganded reverse transcriptase from the human immunodeficiency virus type 1. Proc Natl Acad Sci USA  1995; 92(4): 1222-6.
[15] 
Sluis-Cremer N, Temiz NA, Bahar I. Conformational changes in HIV-1 reverse transcriptase induced by nonnucleoside reverse transcriptase inhibitor binding. Curr HIV Res  2004; 2(4): 323-32.
[16] 
Ren J, Esnouf R, Garman E, et al. High resolution structures of HIV-1 RT from four RT-inhibitor complexes. Nat Struct Biol  1995; 2(4): 293-302.
[17] 
Hsiou Y, Ding J, Das K, Clark AD, Hughes SH, Arnold E. Structure of unliganded HIV-1 reverse transcriptase at 2.7 Å resolution: Implications of conformational changes for polymerization and inhibition mechanisms. Structure  1996; 4(7): 853-60.
[18] 
Shen LL, Jiang HL.  Steered molecular dynamics simulation on the binding of NNRTIs to HIV-1 RT. In: Biophysical Journal 2003; 3547-63.
[19] 
Sluis-Cremer N, Arion D, Parniak MA. Destabilization of the HIV-1 reverse transcriptase dimer upon interaction with N-acyl hydrazone inhibitors. Mol Pharmacol  2002; 62(2): 398-405.
[20] 
Mark A. Wainberg. HIV resistance to nevirapine and other non-nucleoside reverse transcriptase inhibitors.pdf. J of Acquir Immune Defic Syndr  2003; 34: S2-7.
[21] 
Conway B, Wainberg MA, Hall D, et al. Development of drug resistance in patients receiving combinations of zidovudine, didanosine and nevirapine. AIDS  2001; 15(10): 1269-74.
[22] 
Shulman N, Zolopa AR, Passaro D, et al. Phenotypic hypersusceptibility to non-nucleoside reverse transcriptase inhibitors in treatment-experienced HIV-infected patients: Impact on virological response to efavirenz-based therapy. AIDS  2001; 15(9): 1125-32.
[23] 
Jackson JB, Becker-Pergola G, Guay LA, et al. Identification of the K103N resistance mutationin Ugandan women receiving nevirapine to prevent HIV-1 vertical transmission. AIDS  2000; 14(11): 111-5.
[24] 
Kuiken C, Korber B, Shafer RW. HIV sequence databases. AIDS Rev  2003; 5: 52-61.
[25] 
Ren J, Stammers DK. Structural basis for drug resistance mechanisms for non-nucleoside inhibitors of HIV reverse transcriptase. Virus Res  2008; 134(1-2): 157-70.
[26] 
Das K, Lewi PJ, Hughes SH, Arnold E. Crystallography and the design of anti-AIDS drugs: Conformational flexibility and positional adaptability are important in the design of non-nucleoside HIV-1 reverse transcriptase inhibitors. Progress in Biophysics and Molecular Biology  2005; 88: 209-31.
[27] 
Lansdon EB, Brendza KM, Hung M, et al. Crystal structures of HIV-1 reverse transcriptase with etravirine (TMC125) and rilpivirine (TMC278): Implications for drug design. J Med Chem  2010; 53(10): 4295-9.
[28] 
Ren J, Nichols C, Bird L, et al. Structural mechanisms of drug resistance for mutations at codons 181 and 188 in HIV-1 reverse transcriptase and the improved resilience of second generation non-nucleoside inhibitors. J Mol Biol  2001; 312(4): 795-805.
[29] 
Chong P, Sebahar P, Youngman M, et al. Rational design of potent non-nucleoside inhibitors of HIV-1 reverse transcriptase. J Med Chem  2012; 55(23): 10601-9.
[30] 
Himmel DM, Das K, Clark AD, et al. Crystal structures for HIV-1 reverse transcriptase in complexes with three pyridinone derivatives: A new class of non-nucleoside inhibitors effective against a broad range of drug-resistant strains. J Med Chem  2005; 48(24): 7582-91.
[31] 
Sahlberg C, Zhou X. Development of non-nucleoside reverse transcriptase inhibitors for Anti- HIV therapy. Antiinfect Agents Med Chem  2008; 7(2): 101-17.
[32] 
Berman HM, Kleywegt GJ, Nakamura H, Markley JL. The Protein Data Bank archive as an open data resource. J Comput Aided Mol Des  2014; 28(10): 1009-14.
[33] 
Hall TA. BioEdit: a user-friendly biological sequence alignment editor and analysis program for Windows 95/98/NT. Nucleic Acids Symp Ser  1999; 41: 95-8.
[34] 
Hall T, Biosciences I, Carlsbad C. BioEdit: An important software for molecular biology. GERF Bull Biosci  2011; 2: 60-1.
[35] 
McWilliam H, Li W, Uludag M, et al. Analysis tool web services from the EMBL-EBI. Nucleic Acids Res  2013; 41: 597-600.
[36] 
Larkin MA, Blackshields G, Brown NP, et al. Clustal W and Clustal X version 2.0. Bioinformatics  2007; 23(21): 2947-8.
[37] 
Goujon M, McWilliam H, Li W, et al. A new bioinformatics analysis tools framework at EMBL-EBI. Nucleic Acids Res  2010; 38(Suppl. 2): 695-9.
[38] 
Webb B, Sali A. Comparative protein structure modeling using MODELLER  Curr Protoc Bioinform 2014; 47: 5.6.1-32.
[39] 
Guex N, Peitsch MC. SWISS-MODEL and the Swiss-PdbViewer: An environment for comparative protein modeling. Electrophoresis  1997; 18(15): 2714-23.
[40] 
ChemicalComputingGroupInc. Molecular Operating Environment (MOE). Sci Comput Instrum  2004; 22(1): 32.
[41] 
Humphrey W, Dalke A, Schulten K. Visual molecular dynamics. J Mol Graph  1996; 14(1): 33-8.
[42] 
Ribeiro J V, Bernardi RC, Rudack T, et al.  QwikMD — Integrative
molecular dynamics toolkit for novices and experts. Nat Publ Gr
2016; (May): 1-14.
[43] 
Phillips JC, Braun R, Wang W, et al. Scalable molecular dynamics with NAMD. J Comput Chem  2005; 26: 1781-802.
[44] 
Debnath U, Verma S, Jain S, Katti SB, Prabhakar YS. Pyridones as NNRTIs against HIV-1 mutants: 3D-QSAR and protein informatics. J Comput Aided Mol Des  2013; 27(7): 637-54.
[45] 
Guillemont J, Benjahad A, Oumouch S, et al. Synthesis and biological evaluation of C-5 methyl substituted 4-arylthio and 4-aryloxy-3-iodopyridin-2(1H)-one type anti-HIV agents. J Med Chem  2009; 52(23): 7473-87.
[46] 
Mills N. ChemDraw Ultra 10.0. J Am Chem Soc  2006; 128(41): 13649-50.
[47] 
Barakat MT, Dean PM. Molecular structure matching by simulated annealing. I. A comparison between different cooling schedules. J Comput Aided Mol Des  1990; 4(3): 295-316.
[48] 
Murugesan V, Sethi N, Prabhakar YS, Katti SB. CoMFA and CoMSIA of diverse pyrrolidine analogues as dipeptidyl peptidase IV inhibitors: active site requirements. Mol Divers  2011; 15(2): 457-66.
[49] 
Morris GM, Goodsell DS, Halliday RS, Huey R, Olson A. Automated docking using a lamarckian genetic algotithm and an empirical binding free energy function. J Comput Chem  1998; 19(14): 1639-62.
[50] 
Morris GM, Huey R, Lindstrom W, et al. Software news and updates autodock4 and autodocktools4: automated docking with selective receptor flexibility. J Comput Chem  2009; 30: 2785-91.
[51] 
Wiederstein M, Sippl MJ. ProSA-web: Interactive web service for the recognition of errors in three-dimensional structures of proteins. Nucleic Acids Res  2007; 35(Suppl. 2): 407-10.
[52] 
Benkert P, Tosatto SCE, Schomburg D. QMEAN: A comprehensive scoring function for model quality assessment. Proteins-Structure Function and Bioinformatics  2008; 71(1): 261-77.
[53] 
Willard L, Ranjan A, Zhang H, et al. VADAR: A web server for quantitative evaluation of protein structure quality. Nucleic Acids Res  2003; 31(13): 3316-9.
[54] 
Colovos C, Yeates TO. Verification of protein structures: Patterns of nonbonded atomic interactions. Protein Sci  1993; 2(9): 1511-9.
[55] 
Ramachandran GN, Sasisekharan V. Conformation of polypeptides and proteins. Adv Protein Chem  1968; 23(C): 283-437.
[56] 
Ramachandran GN, Ramakrishnan C, Sasisekharan V. Stereochemistry of polypeptide chain configurations. J of Mol Biol  1963; 7(1): 95-9.
[57] 
Oberholser K. Proteopedia entry: ramachandran plots. Biochem Mol Biol Educ  2010; 38(6): 430.
[58] 
Hollingsworth SA, Karplus PA. A fresh look at the Ramachandran plot and the occurrence of standard structures in proteins. Biomol Concepts  2010; 1(3-4): 271-83.
[59] 
Hsiou Y, Ding J, Das K, et al. The Lys103Asn mutation of HIV-1 RT: a novel mechanism of drug resistance. J Mol Biol  2001; 309(2): 437-45.
[60] 
Das K, Sarafianos SG, Clark AD, Boyer PL, Hughes SH, Arnold E. Crystal structures of clinically relevant lys103Asn/Tyr181Cys double mutant HIV-1 reverse transcriptase in complexes with ATP and non-nucleoside Inhibitor HBY 097. J Mol Biol  2007; 365(1): 77-89.
[61] 
Esnouf R, Ren J, Ross C, Jones Y, Stammers D, Stuart D. Mechanism of inhibition of HIV-1 reverse transcriptase by non-nucleoside inhibitors. Nat Struct Biol  1995; 2(4): 303-8.
[62] 
Bauman JD, Patel D, Dharia C, et al. Detecting allosteric sites of HIV-1 reverse transcriptase by X-ray crystallographic fragment screening. J Med Chem  2013; 56(7): 2738-46.

Rights & Permissions Print Cite

Article Metrics

46

5

Journal Information

For Authors

For Editors

For Reviewers

Explore Articles

Open Access

Open Access Articles

For Visitors

DOI https://dx.doi.org/10.2174/1570162X16666180412165004	Print ISSN 1570-162X
Publisher Name Bentham Science Publisher	Online ISSN 1873-4251

Current HIV Research

Identification of Adjacent NNRTI Binding Pocket in Multi-mutated HIV1- RT Enzyme Model: An in silico Study

Abstract

Graphical Abstract

Management of HIV: Management of HIV: old challenges and new needs

Current HIV Research

Identification of Adjacent NNRTI Binding Pocket in Multi-mutated HIV1- RT Enzyme Model: An in silico Study

Abstract

Graphical Abstract

Call for Papers in Thematic Issues

Management of HIV: Management of HIV: old challenges and new needs

Related Journals

Related Books