Your search keyword '"HIV Envelope Protein gp120 metabolism"' showing total 106 results

1. Investigating the Effect of GLU283 Protonation State on the Conformational Heterogeneity of CCR5 by Molecular Dynamics Simulations.

Author

Dogan B and Durdağı S

Subjects

Glutamic Acid chemistry, Glutamic Acid metabolism, Humans, Binding Sites, Molecular Dynamics Simulation, Receptors, CCR5 chemistry, Receptors, CCR5 metabolism, Maraviroc chemistry, Maraviroc pharmacology, Maraviroc metabolism, Protein Conformation, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, Protons

Abstract

CCR5 is a class A GPCR and serves as one of the coreceptors facilitating HIV-1 entry into host cells. This receptor has vital roles in the immune system and is involved in the pathogenesis of different diseases. Various studies were conducted to understand its activation mechanism, including structural studies in which inactive and active states of the receptor were determined in complex with various binding partners. These determined structures provided opportunities to perform molecular dynamics (MD) simulations and to analyze conformational changes observed in the protein structures. The atomic-level dynamic studies allow us to explore the effects of ionizable residues on the receptor. Here, our aim was to investigate the conformational changes in CCR5 when it forms a complex with either the inhibitor maraviroc (MRV), an approved anti-HIV drug, or HIV-1 envelope protein GP120, and compare these changes to the receptor's apo form. In our simulations, we considered both ionized and protonated states of ionizable binding site residue GLU283 7.39 in CCR5 as the protonation state of this residue was considered ambiguously in previous studies. Our molecular simulations results suggested that in fact, the change in the protonation state of GLU283 7.39 caused interaction profiles to be different between CCR5 and its binding partners, GP120 or MRV. We observed that when the protonated state of GLU283 7.39 was considered in complex with the envelope protein GP120, there were substantial structural changes in CCR5, indicating that it adopts a more active-like conformation. On the other hand, CCR5 in complex with MRV always adopted an inactive conformation regardless of the protonation state. Hence, the CCR5 coreceptor displays conformational heterogeneity not only depending on its binding partner but also influenced by the protonation state of the binding site binding site residue GLU283 7.39 . This outcome is also in accordance with some studies showing that GP120 binding could activate signaling pathways. This outcome could also have significant implications for discovering novel CCR5 inhibitors as anti-HIV drugs using in silico methods such as molecular docking, as it may be necessary to consider the protonated state of GLU283 7.39 .

Published

2024

2. Glycan-Modified Peptides for Dual Inhibition of Human Immunodeficiency Virus Entry into Dendritic Cells and T Cells.

Author

Cheng S, Li M, Feng Y, Liu T, He L, Xu M, Ma L, and Li X

Subjects

Humans, Animals, Rats, Cell Line, Lectins, C-Type metabolism, Dendritic Cells metabolism, Polysaccharides pharmacology, HIV Envelope Protein gp120 metabolism, HIV-1 metabolism, HIV Infections

Abstract

Dendritic cells (DCs) play a crucial role in HIV-1 infection of CD4+ T cells. DC-SIGN, a lectin expressed on the surface of DCs, binds to the highly mannosylated viral membrane protein gp120 to capture HIV-1 virions and then transport them to target T cells. In this study, we modified peptide C34, an HIV-1 fusion inhibitor, at different sites using different sizes of the DC-SIGN-specific carbohydrates to provide dual-targeted HIV inhibition. The dual-target binding was confirmed by mechanistic studies. Pentamannose-modified C34 inhibited virus entry into both DC-SIGN+ 293T cells (52%-71% inhibition at 500 μM) and CD4+ TZM-b1 cells (EC 50 = 0.7-1.7 nM). One conjugate, NC-M5, showed an extended half-life relative to C34 in rats ( T 1/2 : 7.8 vs 1.02 h). These improvements in antiviral activity and pharmacokinetics have potential for HIV treatment and the development of dual-target inhibitors for pathogens that require the involvement of DC-SIGN for infection.

Published

2024

3. Synthesis and Immunological Evaluation of Pentamannose-Based HIV-1 Vaccine Candidates.

Author

Liu CC, Huo CX, Zhai C, Zheng XJ, Xiong DC, and Ye XS

Subjects

Animals, Antibodies, Neutralizing, Epitopes chemistry, Glycoconjugates metabolism, HIV Antibodies chemistry, HIV Envelope Protein gp120 metabolism, Humans, Mice, Polysaccharides chemistry, HIV-1 metabolism, Vaccines

Abstract

Dense glycosylation and the trimeric conformation of the human immunodeficiency virus-1 (HIV-1) envelope protein limit the accessibility of some cellular glycan processing enzymes and end up with high-mannose-type N -linked glycans on the envelope spike, among which the Man 5 GlcNAc 2 structure occupies a certain proportion. The Man 5 GlcNAc 2 glycan composes the binding sites of some potent broadly neutralizing antibodies, and some lectins that can bind Man 5 GlcNAc 2 show HIV-neutralizing activity. Therefore, Man 5 GlcNAc 2 is a potential target for HIV-1 vaccine development. Herein, a highly convergent and effective strategy was developed for the synthesis of Man 5 and its monofluoro-modified, trifluoro-modified, and S -linked analogues. We coupled these haptens to carrier protein CRM197 and evaluated the immunogenicity of the glycoconjugates in mice. The serological assays showed that the native Man 5 conjugates failed to induce Man 5 -specific antibodies in vivo , while the modified analogue conjugates induced stronger antibody responses. However, these antibodies could not bind the native gp120 antigen. These results demonstrated that the immune tolerance mechanism suppressed the immune responses to Man 5 -related structures and the conformation of glycan epitopes on the synthesized glycoconjugates was distinct from that of native glycan epitopes on gp120.

Published

2022

4. HIV-1 Env-Dependent Cell Killing by Bifunctional Small-Molecule/Peptide Conjugates.

Author

Gaffney A, Nangarlia A, Ang CG, Gossert S, Rashad Ahmed AA, Hossain MA, Abrams CF, Smith AB 3rd, and Chaiken I

Subjects

Peptides chemistry, Small Molecule Libraries chemistry, Cell Death drug effects, HIV Envelope Protein gp120 metabolism, HIV Envelope Protein gp41 metabolism, HIV-1 metabolism, Peptides pharmacology, Small Molecule Libraries pharmacology

Abstract

A strategy has been established for the synthesis of a family of bifunctional HIV-1 inhibitor covalent conjugates with the potential to bind simultaneously to both the gp120 and gp41 subunits of the HIV-1 envelope glycoprotein trimeric complex (Env). One component of the conjugates is derived from BNM-III-170, a small-molecule CD4 mimic that binds to gp120. The second component, comprised of the peptide DKWASLWNW ("Trp3"), was derived from the N-terminus of the HIV-1 gp41 Membrane Proximal External Region (MPER) and found previously to bind to the gp41 subunit of Env. The resulting bifunctional conjugates were shown to inhibit virus cell infection with low micromolar potency and to induce lysis of the HIV-1 virion. Crucially, virolysis was found to be dependent on the covalent linkage of the BNM-III-170 and Trp3 domains, as coadministration of a mixture of the un-cross-linked components proved to be nonlytic. However, a significant magnitude of lytic activity was observed in Env-negative and other control pseudoviruses, suggesting parallel mechanisms of action of the conjugates involving Env interaction and direct membrane disruption. Computational modeling suggested strong membrane-binding activity of BNM-III-170, which may underly the nonspecific virolytic effects of the conjugates. To investigate the scope of the membrane effect, cell-based cytotoxicity and membrane permeability assays were performed employing flow cytometry. Here, we observed a dose-dependent and specific cytotoxic effect on HIV-1 Env-expressing cells by the small-molecule bifunctional inhibitor. Most importantly, Env-negative cells were not susceptible to the cytotoxic effect upon exposure to this construct at concentrations where cell-killing effects were observed for Env-positive cells. Computational structural modeling supports a mechanism in which the bifunctional inhibitors bind to the gp120 and gp41 subunits in tandem in open-state Env trimers and induce relative motion of the gp120 subunits consistent with models of Env inactivation. This observation supports the idea that the cell-killing effect of the small-molecule bifunctional inhibitor is due to specific Env conformational triggering. This work lays important groundwork to advance a small-molecule bifunctional inhibitor approach for eliminating Env-expressing infected cells and the eradication of HIV-1.

Published

2021

5. The Impact of Sustained Immunization Regimens on the Antibody Response to Oligomannose Glycans.

Author

Nguyen DN, Redman RL, Horiya S, Bailey JK, Xu B, Stanfield RL, Temme JS, LaBranche CC, Wang S, Rodal AA, Montefiori DC, Wilson IA, and Krauss IJ

Subjects

Animals, Antibodies, Neutralizing, Antibody Formation, Binding Sites, Glycosylation, HIV Envelope Protein gp120 metabolism, HIV Envelope Protein gp120 urine, HIV Infections prevention & control, Humans, Immunization, Mannosidases metabolism, Oligosaccharides urine, Protein Binding, Protein Conformation, Rabbits, Small Molecule Libraries chemistry, Vaccination, AIDS Vaccines metabolism, Glycopeptides chemistry, HIV Antibodies metabolism, HIV Envelope Protein gp120 chemistry, Oligosaccharides chemistry, Vaccines, Conjugate metabolism

Abstract

The high mannose patch (HMP) of the HIV envelope protein (Env) is the structure most frequently targeted by broadly neutralizing antibodies; therefore, many researchers have attempted to use mimics of this region as a vaccine immunogen. In our previous efforts, vaccinating rabbits with evolved HMP mimic glycopeptides containing Man 9 resulted in an overall antibody response targeting the glycan core and linker rather than the full glycan or Manα1→2Man tips of Man 9 glycans. A possible reason could be processing of our immunogen by host serum mannosidases. We sought to test whether more prolonged dosing could increase the antibody response to intact glycans, possibly by increasing the availability of intact Man 9 to germinal centers. Here, we describe a study investigating the impact of immunization regimen on antibody response by testing immunogen delivery through bolus, an exponential series of mini doses, or a continuously infusing mini-osmotic pump. Our results indicate that, with our glycopeptide immunogens, standard bolus immunization elicited the strongest HIV Env-binding antibody response, even though higher overall titers to the glycopeptide were elicited by the exponential and pump regimens. Antibody selectivity for intact glycan was, if anything, slightly better in the bolus-immunized animals.

Published

2020

6. Preclinical Optimization of gp120 Entry Antagonists as anti-HIV-1 Agents with Improved Cytotoxicity and ADME Properties through Rational Design, Synthesis, and Antiviral Evaluation.

Author

Curreli F, Ahmed S, Benedict Victor SM, Iusupov IR, Belov DS, Markov PO, Kurkin AV, Altieri A, and Debnath AK

Subjects

Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacokinetics, Caco-2 Cells, HEK293 Cells, HIV Envelope Protein gp120 metabolism, Humans, Microbial Sensitivity Tests, Molecular Structure, Pyridines chemical synthesis, Pyridines pharmacokinetics, Pyrroles chemical synthesis, Pyrroles pharmacokinetics, Structure-Activity Relationship, Thiazoles chemical synthesis, Thiazoles pharmacokinetics, Anti-HIV Agents pharmacology, HIV Envelope Protein gp120 antagonists & inhibitors, Pyridines pharmacology, Pyrroles pharmacology, Thiazoles pharmacology

Abstract

We previously reported a milestone in the optimization of NBD-11021, an HIV-1 gp120 antagonist, by developing a new and novel analogue, NBD-14189 ( Ref1 ), which showed antiviral activity against HIV-1 HXB2 , with a half maximal inhibitory concentration of 89 nM. However, cytotoxicity remained high, and the absorption, distribution, metabolism, and excretion (ADME) data showed relatively poor aqueous solubility. To optimize these properties, we replaced the phenyl ring in the compound with a pyridine ring and synthesized a set of 48 novel compounds. One of the new analogues, NBD-14270 ( 8 ), showed a marked improvement in cytotoxicity, with 3-fold and 58-fold improvements in selectivity index value compared with that of Ref1 and NBD-11021, respectively. Furthermore, the in vitro ADME data clearly showed improvements in aqueous solubility and other properties compared with those for Ref1 . The data for 8 indicated that the pyridine scaffold is a good bioisostere for phenyl, allowing the further optimization of this molecule.

Published

2020

7. Multivalent Cluster Nanomolecules for Inhibiting Protein-Protein Interactions.

Author

Qian EA, Han Y, Messina MS, Maynard HD, Král P, and Spokoyny AM

Subjects

Cell Adhesion drug effects, Cell Adhesion Molecules chemistry, Cell Adhesion Molecules metabolism, Engineering, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, Lectins, C-Type chemistry, Lectins, C-Type metabolism, Molecular Dynamics Simulation, Protein Binding drug effects, Protein Conformation, Receptors, Cell Surface chemistry, Receptors, Cell Surface metabolism, Signal Transduction drug effects, Nanostructures chemistry

Abstract

Multivalent protein-protein interactions serve central roles in many essential biological processes, ranging from cell signaling and adhesion to pathogen recognition. Uncovering the rules that govern these intricate interactions is important not only to basic biology and chemistry but also to the applied sciences where researchers are interested in developing molecules to promote or inhibit these interactions. Here we report the synthesis and application of atomically precise inorganic cluster nanomolecules consisting of an inorganic core and a covalently linked densely packed layer of saccharides. These hybrid agents are stable under biologically relevant conditions and exhibit multivalent binding capabilities, which enable us to study the complex interactions between glycosylated structures and a dendritic cell lectin receptor. Importantly, we find that subtle changes in the molecular structure lead to significant differences in the nanomolecule's protein-binding properties. Furthermore, we demonstrate an example of using these hybrid nanomolecules to effectively inhibit protein-protein interactions in a human cell line. Ultimately, this work reveals an intricate interplay between the structural design of multivalent agents and their biological activities toward protein surfaces.

Published

2019

8. Preclinical Safety Evaluation of HIV-1 gp120 Responsive Microbicide Delivery System in C57BL/6 Female Mice.

Author

Coulibaly FS, Ezoulin MJM, Dim DC, Molteni A, and Youan BC

Subjects

Administration, Intravaginal, Animals, Calcium Carbonate metabolism, Chemokines metabolism, Dynamic Light Scattering, Female, HIV Infections drug therapy, Immunohistochemistry, Interleukin-1alpha metabolism, Interleukin-1beta metabolism, Interleukin-7 metabolism, Mice, Mice, Inbred C57BL, Microscopy, Electron, Scanning, Osmolar Concentration, Tenofovir therapeutic use, Tumor Necrosis Factor-alpha metabolism, Vagina virology, Anti-Infective Agents therapeutic use, HIV Envelope Protein gp120 metabolism, HIV-1 drug effects, HIV-1 pathogenicity

Abstract

Many novel vaginal/rectal microbicide formulations failed clinically due to safety concerns, indicating the need for the early investigation of lead microbicide formulations. In this study, the preclinical safety of an HIV-1 gp120 and mannose responsive microbicide delivery system (MRP) is evaluated in C57BL/6 mice. MRP was engineered through the layer-by-layer coating of calcium carbonate (CaCO 3 ) with Canavalia ensiformis lectin (Con A) and glycogen. MRP mean particle diameter and zeta potential were 857.8 ± 93.1 nm and 2.37 ± 4.12 mV, respectively. Tenofovir (TFV) encapsulation and loading efficiencies in MRP were 70.1% and 16.3% w/w, respectively. When exposed to HIV-1 rgp120 (25 μg/mL), MRP released a significant amount of TFV (∼5-fold higher) in vaginal and seminal fluid mixture compared to the control (pre-exposure) level (∼59 μg/mL) in vaginal fluid alone. Unlike the positive control treated groups (e.g., nonoxynol-9), no significant histological damages and CD45+ cells infiltration were observed in the vaginal and major reproductive organ epithelial layers. This was probably due to MRP biocompatibility and its isosmolality (304.33 ± 0.58 mOsm/kg). Furthermore, compared to negative controls, there was no statistically significant increase in pro-inflammatory cytokines such as IL1α, Ilβ, IL7, IP10, and TNFα. Collectively, these data suggest that MRP is a relatively safe nanotemplate for HIV-1 gp120 stimuli responsive vaginal microbicide delivery system.

Published

2019

9. Discovery of the Human Immunodeficiency Virus Type 1 (HIV-1) Attachment Inhibitor Temsavir and Its Phosphonooxymethyl Prodrug Fostemsavir.

Author

Wang T, Ueda Y, Zhang Z, Yin Z, Matiskella J, Pearce BC, Yang Z, Zheng M, Parker DD, Yamanaka GA, Gong YF, Ho HT, Colonno RJ, Langley DR, Lin PF, Meanwell NA, and Kadow JF

Subjects

Animals, Anti-HIV Agents metabolism, Anti-HIV Agents pharmacology, Caco-2 Cells, Cell Membrane metabolism, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, Humans, Molecular Docking Simulation, Organophosphates pharmacology, Permeability, Prodrugs pharmacology, Protein Conformation, Rats, Triazoles metabolism, Drug Discovery, HIV-1 drug effects, HIV-1 physiology, Organophosphates metabolism, Piperazines metabolism, Piperazines pharmacology, Prodrugs metabolism, Triazoles pharmacology, Virus Attachment drug effects

Abstract

The optimization of the 4-methoxy-6-azaindole series of HIV-1 attachment inhibitors (AIs) that originated with 1 to deliver temsavir (3, BMS-626529) is described. The most beneficial increases in potency and pharmacokinetic (PK) properties were attained by incorporating N-linked, sp 2 -hybridized heteroaryl rings at the 7-position of the heterocyclic nucleus. Compounds that adhered to a coplanarity model afforded targeted antiviral potency, leading to the identification of 3 with characteristics that provided for targeted exposure and PK properties in three preclinical species. However, the physical properties of 3 limited plasma exposure at higher doses, both in preclinical studies and in clinical trials as the result of dissolution- and/or solubility-limited absorption, a deficiency addressed by the preparation of the phosphonooxymethyl prodrug 4 (BMS-663068, fostemsavir). An extended-release formulation of 4 is currently in phase III clinical trials where it has shown promise as part of a drug combination therapy in highly treatment-experienced HIV-1 infected patients.

Published

2018

10. Bifunctional Chimera That Coordinately Targets Human Immunodeficiency Virus 1 Envelope gp120 and the Host-Cell CCR5 Coreceptor at the Virus-Cell Interface.

Author

Rashad AA, Song LR, Holmes AP, Acharya K, Zhang S, Wang ZL, Gary E, Xie X, Pirrone V, Kutzler MA, Long YQ, and Chaiken I

Subjects

Anti-HIV Agents metabolism, Drug Design, HIV Envelope Protein gp120 chemistry, Models, Molecular, Molecular Targeted Therapy, Protein Conformation, Small Molecule Libraries chemistry, Triazoles chemistry, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, HIV Envelope Protein gp120 metabolism, HIV-1 drug effects, HIV-1 metabolism, Receptors, CCR5 metabolism

Abstract

To address the urgent need for new agents to reduce the global occurrence and spread of AIDS, we investigated the underlying hypothesis that antagonists of the HIV-1 envelope (Env) gp120 protein and the host-cell coreceptor (CoR) protein can be covalently joined into bifunctional synergistic combinations with improved antiviral capabilities. A synthetic protocol was established to covalently combine a CCR5 small-molecule antagonist and a gp120 peptide triazole antagonist to form the bifunctional chimera. Importantly, the chimeric inhibitor preserved the specific targeting properties of the two separate chimera components and, at the same time, exhibited low to subnanomolar potencies in inhibiting cell infection by different pseudoviruses, which were substantially greater than those of a noncovalent mixture of the individual components. The results demonstrate that targeting the virus-cell interface with a single molecule can result in improved potencies and also the introduction of new phenotypes to the chimeric inhibitor, such as the irreversible inactivation of HIV-1.

Published

2018

11. Anionic Carbosilane Dendrimers Destabilize the GP120-CD4 Complex Blocking HIV-1 Entry and Cell to Cell Fusion.

Author

Guerrero-Beltran C, Rodriguez-Izquierdo I, Serramia MJ, Araya-Durán I, Márquez-Miranda V, Gomez R, de la Mata FJ, Leal M, González-Nilo F, and Muñoz-Fernández MA

Subjects

Anions chemistry, Anions pharmacology, Anti-HIV Agents chemistry, CD4 Antigens metabolism, Cell Line, Dendrimers chemistry, HIV Infections metabolism, HIV-1 physiology, Humans, Models, Molecular, Silanes chemistry, Anti-HIV Agents pharmacology, Dendrimers pharmacology, HIV Envelope Protein gp120 metabolism, HIV Infections drug therapy, HIV-1 drug effects, Silanes pharmacology, Virus Internalization drug effects

Abstract

Cell-to-cell transmission is the most effective pathway for the spread of human immunodeficiency virus (HIV-1). Infected cells expose virus-encoded fusion proteins on their surface as a consequence of HIV-1 replicative cycle that interacts with noninfected cells through CD4 receptor and CXCR4 coreceptor leading to the formation of giant multinucleated cells known as syncytia. Our group previously described the potent activity of dendrimers against CCR5-tropic viruses. Nevertheless, the study of G1-S4, G2-S16, and G3-S16 dendrimers in the context of X4-HIV-1 tropic cell-cell fusion referred to syncytium formation remains still unknown. These dendrimers showed a suitable biocompatibility in all cell lines studied and our results demonstrated that anionic carbosilane dendrimers G1-S4, G2-S16, and G3-S16 significantly inhibit the X4-HIV-1 infection, as well as syncytia formation, in a dose dependent manner. We also demonstrated that G2-S16 and G1-S4 significantly reduced syncytia formation in HIV-1 Env-mediated cell-to-cell fusion model. Molecular modeling and in silico models showed that G2-S16 dendrimer interfered with gp120-CD4 complex and demonstrated its potential use for a treatment.

Published

2018

12. Layer-by-Layer Engineered Microbicide Drug Delivery System Targeting HIV-1 gp120: Physicochemical and Biological Properties.

Author

Coulibaly FS, Ezoulin MJM, Purohit SS, Ayon NJ, Oyler NA, and Youan BC

Subjects

Administration, Intravaginal, Animals, Biological Assay, Calcium Carbonate chemistry, Chemistry, Pharmaceutical methods, Concanavalin A chemistry, Cross-Linking Reagents chemistry, Drug Liberation, Female, Glycogen chemistry, HIV Infections virology, HIV-1 metabolism, Humans, Keratinocytes, Lactobacillus crispatus drug effects, Methylmannosides chemistry, Mice, Nanoparticles chemistry, RAW 264.7 Cells, Swine, Tenofovir pharmacology, Vagina cytology, Vagina microbiology, Anti-HIV Agents pharmacology, Anti-Infective Agents, Local pharmacology, Chemical Engineering methods, Drug Delivery Systems methods, HIV Envelope Protein gp120 metabolism, HIV Infections prevention & control, HIV-1 drug effects

Abstract

The purpose of this study was to engineer a model anti-HIV microbicide (tenofovir) drug delivery system targeting HIV-1 envelope glycoprotein gp120 (HIV-1 g120) for the prevention of HIV sexual transmission. HIV-1 g120 and mannose responsive particles (MRP) were prepared through the layer-by-layer coating of calcium carbonate (CaCO 3 ) with concanavalin A (Con A) and glycogen. MRP average particle size ranged from 881.7 ± 15.45 nm to 1130 ± 15.72 nm, depending on the number of Con A layers. Tenofovir encapsulation efficiency in CaCO 3 was 74.4% with drug loading of 16.3% (w/w). MRP was non-cytotoxic to Lactobacillus crispatus, human vaginal keratinocytes (VK2), and murine macrophage RAW 264.7 cells and did not induce any significant proinflammatory nitric oxide release. Overall, compared to control, no statistically significant increase in proinflammatory cytokine IL-1α, IL-1β, IL-6, MKC, IL-7, and interferon-γ-inducible protein 10 (IP10) levels was observed. Drug release profiles in the presence of methyl α-d-mannopyranoside and recombinant HIV-1 envelope glycoprotein gp120 followed Hixson-Crowell and Hopfenberg kinetic models, indicative of a surface-eroding system. The one Con A layer containing system was found to be the most sensitive (∼2-fold increase in drug release vs control SFS:VFS) at the lowest HIV gp120 concentration tested (25 μg/mL). Percent mucoadhesion, tested ex vivo on porcine vaginal tissue, ranged from 10% to 21%, depending on the number of Con A layers in the formulation. Collectively, these data suggested that the proposed HIV-1 g120 targeting, using MRP, potentially represent a safe and effective template for vaginal microbicide drug delivery, if future preclinical studies are conclusive.

Published

2017

13. Design of HIV Coreceptor Derived Peptides That Inhibit Viral Entry at Submicromolar Concentrations.

Author

Bobyk KD, Mandadapu SR, Lohith K, Guzzo C, Bhargava A, Lusso P, and Bewley CA

Subjects

Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, HIV Envelope Protein gp120 metabolism, HIV Infections metabolism, HIV-1 drug effects, Humans, Peptides chemistry, Receptors, CCR5 metabolism, Receptors, CXCR4 metabolism, Viral Proteins chemistry, Viral Proteins pharmacology, Virion chemistry, Peptides pharmacology

Abstract

HIV/AIDS continues to pose an enormous burden on global health. Current HIV therapeutics include inhibitors that target the enzymes HIV protease, reverse transcriptase, and integrase, along with viral entry inhibitors that block the initial steps of HIV infection by preventing membrane fusion or virus-coreceptor interactions. With regard to the latter, peptides derived from the HIV coreceptor CCR5 were previously shown to modestly inhibit entry of CCR5-tropic HIV strains, with a peptide containing residues 178-191 of the second extracellular loop (peptide 2C) showing the strongest inhibition. Here we use an iterative approach of amino acid scanning at positions shown to be important for binding the HIV envelope, and recombining favorable substitutions to greatly improve the potency of 2C. The most potent candidate peptides gain neutralization breadth and inhibit CXCR4 and CXCR4/CCR5-using viruses, rather than CCR5-tropic strains only. We found that gains in potency in the absence of toxicity were highly dependent on amino acid position and residue type. Using virion capture assays we show that 2C and the new peptides inhibit capture of CD4-bound HIV-1 particles by antibodies whose epitopes are located in or around variable loop 3 (V3) on gp120. Analysis of antibody binding data indicates that interactions between CCR5 ECL2-derived peptides and gp120 are localized around the base and stem of V3 more than the tip. In the absence of a high-resolution structure of gp120 bound to coreceptor CCR5, these findings may facilitate structural studies of CCR5 surrogates, design of peptidomimetics with increased potency, or use as functional probes for further study of HIV-1 gp120-coreceptor interactions.

Published

2017

14. Synthesis, Antiviral Potency, in Vitro ADMET, and X-ray Structure of Potent CD4 Mimics as Entry Inhibitors That Target the Phe43 Cavity of HIV-1 gp120.

Author

Curreli F, Kwon YD, Belov DS, Ramesh RR, Kurkin AV, Altieri A, Kwong PD, and Debnath AK

Subjects

Biomimetic Materials chemistry, Biomimetic Materials pharmacology, CD4 Antigens chemistry, CD4 Antigens pharmacology, Cell Line, Crystallography, X-Ray, HIV Envelope Protein gp120 chemistry, HIV Infections metabolism, HIV Infections virology, HIV-1 metabolism, HIV-1 physiology, Humans, Molecular Docking Simulation, Molecular Targeted Therapy, Structure-Activity Relationship, Virus Internalization drug effects, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, HIV Envelope Protein gp120 metabolism, HIV Infections drug therapy, HIV-1 drug effects, Pyrroles chemistry, Pyrroles pharmacology, Thiazoles chemistry, Thiazoles pharmacology

Abstract

In our attempt to optimize the lead HIV-1 entry antagonist, NBD-11021, we present in this study the rational design and synthesis of 60 new analogues and determination of their antiviral activity in a single-cycle and a multicycle infection assay to derive a comprehensive structure-activity relationship (SAR). Two of these compounds, NBD-14088 and NBD-14107, showed significant improvement in antiviral activity compared to the lead entry antagonist in a single-cycle assay against a large panel of Env-pseudotyped viruses. The X-ray structure of a similar compound, NBD-14010, confirmed the binding mode of the newly designed compounds. The in vitro ADMET profiles of these compounds are comparable to that of the most potent attachment inhibitor BMS-626529, a prodrug of which is currently undergoing phase III clinical trials. The systematic study presented here is expected to pave the way for improving the potency, toxicity, and ADMET profile of this series of compounds with the potential to be moved to the early preclinical development.

Published

2017

15. Structural Analysis of the Glycosylated Intact HIV-1 gp120-b12 Antibody Complex Using Hydroxyl Radical Protein Footprinting.

Author

Li X, Grant OC, Ito K, Wallace A, Wang S, Zhao P, Wells L, Lu S, Woods RJ, and Sharp JS

Subjects

Antibodies, Monoclonal chemistry, Antibodies, Monoclonal metabolism, Glycosylation, HIV Antibodies chemistry, HIV Antibodies metabolism, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 immunology, Humans, Hydroxyl Radical, Models, Molecular, Molecular Dynamics Simulation, Protein Conformation, Protein Domains, Antibodies, Neutralizing chemistry, Antibodies, Neutralizing metabolism, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, Protein Footprinting methods

Abstract

Glycoprotein gp120 is a surface antigen and virulence factor of human immunodeficiency virus 1. Broadly neutralizing antibodies (bNAbs) that react to gp120 from a variety of HIV isolates offer hope for the development of broadly effective immunogens for vaccination purposes, if the interactions between gp120 and bNAbs can be understood. From a structural perspective, gp120 is a particularly difficult system because of its size, the presence of multiple flexible regions, and the large amount of glycosylation, all of which are important in gp120-bNAb interactions. Here, the interaction of full-length, glycosylated gp120 with bNAb b12 is probed using high-resolution hydroxyl radical protein footprinting (HR-HRPF) by fast photochemical oxidation of proteins. HR-HRPF allows for the measurement of changes in the average solvent accessible surface area of multiple amino acids without the need for measures that might alter the protein conformation, such as mutagenesis. HR-HRPF of the gp120-b12 complex coupled with computational modeling shows a novel extensive interaction of the V1/V2 domain, probably with the light chain of b12. Our data also reveal HR-HRPF protection in the C3 domain caused by interaction of the N330 glycan with the b12 light chain. In addition to providing information about the interactions of full-length, glycosylated gp120 with b12, this work serves as a template for the structural interrogation of full-length glycosylated gp120 with other bNAbs to better characterize the interactions that drive the broad specificity of the bNAb.

Published

2017

16. Global N-Glycan Site Occupancy of HIV-1 gp120 by Metabolic Engineering and High-Resolution Intact Mass Spectrometry.

Author

Struwe WB, Stuckmann A, Behrens AJ, Pagel K, and Crispin M

Subjects

Binding Sites, HIV Envelope Protein gp120 metabolism, HIV-1 metabolism, Mass Spectrometry methods, Metabolic Engineering, Polysaccharides metabolism

Abstract

A vital step in HIV vaccine development strategies has been the observation that some infected individuals generate broadly neutralizing antibodies that target the glycans on the surface of HIV-1 gp120. These antibodies target glycan epitopes on viral envelope spikes, and yet the positions and degree of occupancy of glycosylation sites is diverse. Therefore, there is a need to understand glycosylation occupancy on recombinant immunogens. The sheer number of potential glycosylation sites and degree of chemical heterogeneity impedes assessing the global sequon occupancy of gp120 glycoforms. Here, we trap the glycan processing of recombinant gp120 to generate homogeneous glycoforms, facilitating occupancy assessment by intact mass spectrometry. We show that gp120 monomers of the BG505 strain contain either fully occupied sequons or missing the equivalent of one and sometimes two glycans across the molecule. This biosynthetic engineering approach enables the analysis of therapeutically important glycoproteins otherwise recalcitrant to analysis by native mass spectrometry.

Published

2017

17. Computational Evaluation of HIV-1 gp120 Conformations of Soluble Trimeric gp140 Structures as Targets for de Novo Docking of First- and Second-Generation Small-Molecule CD4 Mimics.

Author

Moraca F, Acharya K, Melillo B, Smith AB 3rd, Chaiken I, and Abrams CF

Subjects

Drug Discovery, HIV Envelope Protein gp120 chemistry, HIV Infections drug therapy, HIV Infections virology, HIV-1 drug effects, HIV-1 metabolism, Humans, Ligands, Molecular Docking Simulation, Molecular Dynamics Simulation, env Gene Products, Human Immunodeficiency Virus chemistry, CD4 Antigens chemistry, CD4 Antigens pharmacology, HIV Envelope Protein gp120 metabolism, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology, env Gene Products, Human Immunodeficiency Virus metabolism

Abstract

Small-molecule CD4 mimics (SMCM's) bind to the gp120 subunit of the HIV-1 envelope glycoprotein (Env) and have been optimized to block cell infection in vitro. The lack of the V1/2 and V3 loops and the presence of the β2/3 and β20/21 strands (bridging sheet) in the available structures of the monomeric gp120 core may limit its applicability as a target for further synthetic optimization of SMCM potency and/or breadth. Here, we employ a combination of binding-site search, docking, estimation of protein-ligand interaction energy, all-atom molecular dynamics, and ELISA-based CD4-binding competition assays to create, characterize, and rationalize models of first- and second-generation of SMCM's bound to the distinct, trimeric BG505 SOSIP.664 structures 4NCO and 4TVP containing V1/2 and V3 loops with no bridging sheet. We demonstrate that the in silico neutralization of the highly conserved D368 is necessary to obtain the correct orientation of SMCM in their binding site when docking against the monomeric gp120 core. The computational results correlate with IC 50 's measured in CD4 binding competition ELISA and with K D 's measured on gp120 core monomer. This supports the hypothesis that the 4NCO trimeric structure represents a viable target for further SMCM's optimization with advantages over both the 4TVP trimer and gp120 core monomer. Finally, the docking protocol has been optimized to screen compounds that can clearly interact with the highly conserved residue D368, increasing the likelihood of future optimizations to arrive at SMCM's with a broader spectrum of activity.

Published

2016

18. Human CD4 Metastability Is a Function of the Allosteric Disulfide Bond in Domain 2.

Author

Owen GR, Channell JA, Forsyth VT, Haertlein M, Mitchell EP, Capovilla A, Papathanasopoulos M, and Cerutti NM

Subjects

HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, Humans, Major Histocompatibility Complex, Models, Molecular, Oxidation-Reduction, Protein Binding, Protein Folding, Protein Stability, Protein Structure, Secondary, Protein Structure, Tertiary, Temperature, Allosteric Site, CD4 Antigens chemistry, CD4 Antigens metabolism, Disulfides chemistry, Protein Interaction Domains and Motifs

Abstract

CD4 is expressed on the surface of specific leukocytes where it plays a key role in the activation of immunostimulatory T-cells and acts as a primary receptor for HIV-1 entry. CD4 has four ecto-domains (D1-D4) of which D1, D2, and D4 contain disulfide bonds. Although disulfide bonds commonly serve structural or catalytic functions, a rare class of disulfide bonds possessing unusually high dihedral strain energy and a relative ease of reduction can impact protein function by shuffling their redox state. D2 of CD4 possesses one such "allosteric" disulfide. While it is becoming accepted that redox exchange of the D2 allosteric disulfide plays an essential role in regulating CD4 activity, the biophysical consequences of its reduction remain incompletely understood. By analyzing the hydrodynamic volume, secondary structure, and thermal stability of the reduced and nonreduced forms of the single D1 and D2 domains, as well as the various redox isomers of two domain CD4, we have shown that ablation of the allosteric disulfide bond in domain 2 results in both a favorable structural collapse and an increase in the stability of CD4. Conversely, ablating the structural disulfide of D1 results in destabilizing structural rearrangements in CD4. These findings expand our understanding of the mechanisms by which oxidoreduction of the D2 allosteric disulfide regulates CD4 function; they reveal the intrinsic disulfide-dependent metastability of D2 and illustrate that redox shuffling of the allosteric disulfide results in previously undescribed conformational changes in CD4 that are likely important for its interaction with its protein partners.

Published

2016

19. Screening Platform toward New Anti-HIV Aptamers Set on Molecular Docking and Fluorescence Quenching Techniques.

Author

Oliviero G, Stornaiuolo M, D'Atri V, Nici F, Yousif AM, D'Errico S, Piccialli G, Mayol L, Novellino E, Marinelli L, Grieco P, Carotenuto A, Noppen S, Liekens S, Balzarini J, and Borbone N

Subjects

Anti-HIV Agents chemical synthesis, Aptamers, Nucleotide chemical synthesis, Cell Line, Tumor, Fluorescent Dyes chemical synthesis, Fluorescent Dyes chemistry, HIV drug effects, HIV metabolism, HIV Envelope Protein gp120 antagonists & inhibitors, HIV Envelope Protein gp120 metabolism, Humans, Reproducibility of Results, Spectrometry, Fluorescence, Thermodynamics, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Aptamers, Nucleotide chemistry, Aptamers, Nucleotide pharmacology, Drug Evaluation, Preclinical methods, Fluorescence, Molecular Docking Simulation

Abstract

By using a new rapid screening platform set on molecular docking simulations and fluorescence quenching techniques, three new anti-HIV aptamers targeting the viral surface glycoprotein 120 (gp120) were selected, synthesized, and assayed. The use of the short synthetic fluorescent peptide V35-Fluo mimicking the V3 loop of gp120, as the molecular target for fluorescence-quenching binding affinity studies, allowed one to measure the binding affinities of the new aptamers for the HIV-1 gp120 without the need to obtain and purify the full recombinant gp120 protein. The almost perfect correspondence between the calculated Kd and the experimental EC50 on HIV-infected cells confirmed the reliability of the platform as an alternative to the existing methods for aptamer selection and measuring of aptamer-protein equilibria.

Published

2016

20. Impact of HIV-1 Membrane Cholesterol on Cell-Independent Lytic Inactivation and Cellular Infectivity.

Author

Kalyana Sundaram RV, Li H, Bailey L, Rashad AA, Aneja R, Weiss K, Huynh J, Bastian AR, Papazoglou E, Abrams C, Wrenn S, and Chaiken I

Subjects

Cell Line, Tumor, HIV Core Protein p24 metabolism, HIV Envelope Protein gp120 metabolism, HIV-1 drug effects, HIV-1 pathogenicity, Humans, Membrane Fluidity, Peptides chemistry, Peptides pharmacology, Sulfhydryl Compounds chemistry, Sulfhydryl Compounds pharmacology, Thiazoles chemistry, Thiazoles pharmacology, Triazoles chemistry, Triazoles pharmacology, beta-Cyclodextrins pharmacology, Cholesterol metabolism, HIV-1 physiology, Membrane Lipids metabolism

Abstract

Peptide triazole thiols (PTTs) have been found previously to bind to HIV-1 Env spike gp120 and cause irreversible virus inactivation by shedding gp120 and lytically releasing luminal capsid protein p24. Since the virions remain visually intact, lysis appears to occur via limited membrane destabilization. To better understand the PTT-triggered membrane transformation involved, we investigated the role of envelope cholesterol on p24 release by measuring the effect of cholesterol depletion using methyl beta-cyclodextrin (MβCD). An unexpected bell-shaped response of PTT-induced lysis to [MβCD] was observed, involving lysis enhancement at low [MβCD] vs loss of function at high [MβCD]. The impact of cholesterol depletion on PTT-induced lysis was reversed by adding exogenous cholesterol and other sterols that support membrane rafts, while sterols that do not support rafts induced only limited reversal. Cholesterol depletion appears to cause a reduced energy barrier to lysis as judged by decreased temperature dependence with MβCD. Enhancement/replenishment responses to [MβCD] also were observed for HIV-1 infectivity, consistent with a similar energy barrier effect in the membrane transformation of virus cell fusion. Overall, the results argue that cholesterol in the HIV-1 envelope is important for balancing virus stability and membrane transformation, and that partial depletion, while increasing infectivity, also makes the virus more fragile. The results also reinforce the argument that the lytic inactivation and infectivity processes are mechanistically related and that membrane transformations occurring during lysis can provide an experimental window to investigate membrane and protein factors important for HIV-1 cell entry.

Published

2016

21. Structure-Based Design of a Small Molecule CD4-Antagonist with Broad Spectrum Anti-HIV-1 Activity.

Author

Curreli F, Kwon YD, Zhang H, Scacalossi D, Belov DS, Tikhonov AA, Andreev IA, Altieri A, Kurkin AV, Kwong PD, and Debnath AK

Subjects

Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, Cell Fusion, Cell Line, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, HIV Reverse Transcriptase metabolism, HIV-1 isolation & purification, HIV-1 physiology, Humans, Hydrogen Bonding, Models, Molecular, Molecular Conformation, Oxalates chemical synthesis, Oxalates pharmacology, Piperidines chemical synthesis, Piperidines pharmacology, Protein Conformation, Pyrroles chemical synthesis, Pyrroles pharmacology, Receptors, CCR5 metabolism, Receptors, CXCR4 metabolism, Reverse Transcriptase Inhibitors chemical synthesis, Reverse Transcriptase Inhibitors chemistry, Reverse Transcriptase Inhibitors pharmacology, Stereoisomerism, Structure-Activity Relationship, Thiazoles chemical synthesis, Thiazoles pharmacology, Virus Internalization drug effects, Anti-HIV Agents chemistry, CD4 Antigens metabolism, HIV-1 drug effects, Oxalates chemistry, Piperidines chemistry, Pyrroles chemistry, Thiazoles chemistry

Abstract

Earlier we reported the discovery and design of NBD-556 and their analogs which demonstrated their potential as HIV-1 entry inhibitors. However, progress in developing these inhibitors has been stymied by their CD4-agonist properties, an unfavorable trait for use as drug. Here, we demonstrate the successful conversion of a full CD4-agonist (NBD-556) through a partial CD4-agonist (NBD-09027), to a full CD4-antagonist (NBD-11021) by structure-based modification of the critical oxalamide midregion, previously thought to be intolerant of modification. NBD-11021 showed unprecedented neutralization breath for this class of inhibitors, with pan-neutralization against a panel of 56 Env-pseudotyped HIV-1 representing diverse subtypes of clinical isolates (IC50 as low as 270 nM). The cocrystal structure of NBD-11021 complexed to a monomeric HIV-1 gp120 core revealed its detail binding characteristics. The study is expected to provide a framework for further development of NBD series as HIV-1 entry inhibitors for clinical application against AIDS.

Published

2015

22. Mass spectrometry approach and ELISA reveal the effect of codon optimization on N-linked glycosylation of HIV-1 gp120.

Author

Honarmand Ebrahimi K, West GM, and Flefil R

Subjects

Amino Acid Sequence, Binding Sites genetics, Codon genetics, Electrophoresis, Polyacrylamide Gel, Glycoproteins genetics, Glycoproteins metabolism, Glycosylation, HEK293 Cells, HIV Envelope Protein gp120 genetics, Humans, Molecular Sequence Data, Mutation, Peptides analysis, Peptides metabolism, Proteomics methods, Enzyme-Linked Immunosorbent Assay methods, HIV Envelope Protein gp120 metabolism, Oligosaccharides metabolism, Tandem Mass Spectrometry methods

Abstract

The genes encoding many viral proteins such as HIV-1 envelope glycoprotein gp120 have a tendency for codons that are poorly used by the human genome. Why these codons are frequently present in the HIV genome is not known. The presence of these codons limits expression of HIV-1 gp120 for biochemical studies. The poor codons are replaced by synonymous codons that are frequently present in the highly expressed human genes to overexpress this protein. Whether this codon optimization affects functional properties of gp120 such as its N-linked glycosylation is unknown. We applied a bottom-up mass-spectrometry-based workflow for the direct measurement of deglycosylated and unglycosylated peptides with putative N-linked glycosylation sites, that is, NxS/T motifs. Using this mass-spectrometry approach in combination with ELISA, it is found that codon optimization significantly reduces the frequency with which the dolichol pyrophosphate-linked oligosaccharide is added by the catalytic subunits of oligosaccharide transferase complex to the glycosylation sites. This reduction affects binding of glycan-dependent broadly neutralizing antibodies. These data are essential for biochemical studies of gp120 and successful development of a vaccine against HIV-1. Furthermore, they demonstrate a mass-spectrometry approach for studying the site-specific N-linked glycosylation efficiency of glycoproteins.

Published

2014

23. Kinetics study on the HIV-1 ectodomain protein quaternary structure formation reveals coupling of chain folding and self-assembly in the refolding cascade.

Author

Cheng SF, Sung TC, Chang CC, Chou MJ, Chiang YW, and Chang DK

Subjects

Amino Acid Substitution, Electron Spin Resonance Spectroscopy, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 metabolism, HIV Envelope Protein gp41 genetics, HIV Envelope Protein gp41 metabolism, Kinetics, Light, Protein Refolding, Protein Structure, Quaternary, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Rhodamines chemistry, Scattering, Radiation, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp41 chemistry, HIV-1 metabolism

Abstract

Entry of HIV-1 into the target cell is mediated by the envelope glycoprotein consisting of noncovalently associated surface subunit gp120 and transmembrane subunit gp41. To form a functional gp41 complex, the protein undergoes hairpin formation and self-assembly. The fusion event can be inhibited by gp41-derived peptides at nanomolar concentration and is highly dependent on the time of addition, implying a role of folding kinetics on the inhibitory action. Oligomerization of the gp41 ectodomain was demonstrated by light scattering measurements. Kinetic study by stopped-flow fluorescence and absorption measurements (i) revealed a multistate folding pathway and stable intermediates; (ii) showed a dissection of fast and slow components for early and late stages of folding, respectively, with 3 orders of magnitude difference in the time scale; (iii) showed the slow process was attributed to misfolding and unzipping of the hairpin; and (iv) showed retardation of the native hairpin formation is assumed to lead to coupling of the correctly registered hairpin and self-assembly. This coupling allows the deduction on the time scale of intrachain folding (0.1-1 s) for the protein. The folding reaction was illustrated by a free energy profile to explain the temporal dichotomy of fast and slow steps of folding as well as effective inhibition by gp41-derived peptide.

Published

2014

24. Site-selective solid-phase synthesis of a CCR5 sulfopeptide library to interrogate HIV binding and entry.

Author

Liu X, Malins LR, Roche M, Sterjovski J, Duncan R, Garcia ML, Barnes NC, Anderson DA, Stone MJ, Gorry PR, and Payne RJ

Subjects

Base Sequence, Cell Line virology, HIV Envelope Protein gp120 metabolism, Host-Pathogen Interactions, Humans, Molecular Sequence Data, Peptide Fragments chemical synthesis, Peptide Fragments chemistry, Peptide Fragments metabolism, Tyrosine chemistry, HIV-1 pathogenicity, Peptide Library, Receptors, CCR5 chemistry, Receptors, CCR5 metabolism, Solid-Phase Synthesis Techniques methods

Abstract

Tyrosine (Tyr) sulfation is a common post-translational modification that is implicated in a variety of important biological processes, including the fusion and entry of human immunodeficiency virus type-1 (HIV-1). A number of sulfated Tyr (sTyr) residues on the N-terminus of the CCR5 chemokine receptor are involved in a crucial binding interaction with the gp120 HIV-1 envelope glycoprotein. Despite the established importance of these sTyr residues, the exact structural and functional role of this post-translational modification in HIV-1 infection is not fully understood. Detailed biological studies are hindered in part by the difficulty in accessing homogeneous sulfopeptides and sulfoproteins through biological expression and established synthetic techniques. Herein we describe an efficient approach to the synthesis of sulfopeptides bearing discrete sulfation patterns through the divergent, site-selective incorporation of sTyr residues on solid support. By employing three orthogonally protected Tyr building blocks and a solid-phase sulfation protocol, we demonstrate the synthesis of a library of target N-terminal CCR5(2-22) sulfoforms bearing discrete and differential sulfation at Tyr10, Tyr14, and Tyr15, from a single resin-bound intermediate. We demonstrate the importance of distinct sites of Tyr sulfation in binding gp120 through a competitive binding assay between the synthetic CCR5 sulfopeptides and an anti-gp120 monoclonal antibody. These studies revealed a critical role of sulfation at Tyr14 for binding and a possible additional role for sulfation at Tyr10. N-terminal CCR5 variants bearing a sTyr residue at position 14 were also found to complement viral entry into cells expressing an N-terminally truncated CCR5 receptor.

Published

2014

25. Glycoform analysis of recombinant and human immunodeficiency virus envelope protein gp120 via higher energy collisional dissociation and spectral-aligning strategy.

Author

Yang W, Shah P, Toghi Eshghi S, Yang S, Sun S, Ao M, Rubin A, Jackson JB, and Zhang H

Subjects

Amino Acid Sequence, Carbohydrate Conformation, Glycopeptides chemistry, Glycosylation, HEK293 Cells, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 metabolism, Humans, Ions, Molecular Sequence Data, Recombinant Proteins analysis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Virion chemistry, Glycopeptides analysis, HIV Envelope Protein gp120 analysis, HIV Envelope Protein gp120 chemistry, Tandem Mass Spectrometry methods

Abstract

Envelope protein gp120 of human immunodeficiency virus (HIV) is armored with a dense glycan shield, which plays critical roles in envelope folding, immune-evasion, infectivity, and immunogenicity. Site-specific glycosylation profiling of recombinant gp120 is very challenging. Therefore, glycoproteomic analysis of native viral gp120 is still formidable to date. This challenge promoted us to employ a Q-Exactive mass spectrometer to identify low abundant glycopeptides from virion-associated gp120. To search the HCD-MS data for glycopeptides, a novel spectral-aligning strategy was developed. This strategy depends on the observation that glycopeptides and the corresponding deglycosylated peptides share very similar MS/MS pattern in terms of b- and y-ions that do not contain the site of glycosylation. Moreover, glycopeptides with an identical peptide backbone show nearly resembling spectra regardless of the attached glycan structures. For the recombinant gp120, this "copy-paste" spectral pattern of glycopeptides facilitated identification of 2224 spectra using only 18 spectral templates, and after precursor mass correction, 1268 (57%) spectra were assigned to 460 unique glycopeptides accommodating 19 N-linked and one O-linked glycosylation sites (glycosites). Strikingly, we were able to observe five N- and one O-linked glycosites in native gp120. We further revealed that except for Asn276 in the C2 region, glycans were processed to contain both high mannose and hybrid/complex glycans; an additional four N-linked glycosites were decorated with high mannose type. Core 1 O-linked glycan Gal1GalNAc1 was seen for the O-linked glycosite at Thr499. This direct observation of site-specific glycosylation of virion-derived gp120 has implications in HIV glycobiology and vaccine design.

Published

2014

26. Structure-based design, synthesis and validation of CD4-mimetic small molecule inhibitors of HIV-1 entry: conversion of a viral entry agonist to an antagonist.

Author

Courter JR, Madani N, Sodroski J, Schön A, Freire E, Kwong PD, Hendrickson WA, Chaiken IM, LaLonde JM, and Smith AB 3rd

Subjects

CD4 Antigens chemistry, Crystallography, X-Ray, Drug Design, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, HIV-1 pathogenicity, Host-Pathogen Interactions, Humans, Molecular Mimicry, Protein Conformation, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology, Structure-Activity Relationship, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, CD4 Antigens metabolism, HIV-1 drug effects

Abstract

This Account provides an overview of a multidisciplinary consortium focused on structure-based strategies to devise small molecule antagonists of HIV-1 entry into human T-cells, which if successful would hold considerable promise for the development of prophylactic modalities to prevent HIV transmission and thereby alter the course of the AIDS pandemic. Entry of the human immunodeficiency virus (HIV) into target T-cells entails an interaction between CD4 on the host T-cell and gp120, a component of the trimeric envelope glycoprotein spike on the virion surface. The resultant interaction initiates a series of conformational changes within the envelope spike that permits binding to a chemokine receptor, formation of the gp41 fusion complex, and cell entry. A hydrophobic cavity at the CD4-gp120 interface, defined by X-ray crystallography, provided an initial site for small molecule antagonist design. This site however has evolved to facilitate viral entry. As such, the binding of prospective small molecule inhibitors within this gp120 cavity can inadvertently trigger an allosteric entry signal. Structural characterization of the CD4-gp120 interface, which provided the foundation for small molecule structure-based inhibitor design, will be presented first. An integrated approach combining biochemical, virological, structural, computational, and synthetic studies, along with a detailed analysis of ligand binding energetics, revealed that modestly active small molecule inhibitors of HIV entry can also promote viral entry into cells lacking the CD4 receptor protein; these competitive inhibitors were termed small molecule CD4 mimetics. Related congeners were subsequently identified with both improved binding affinity and more potent viral entry inhibition. Further assessment of the affinity-enhanced small molecule CD4 mimetics demonstrated that premature initiation of conformational change within the viral envelope spike, prior to cell encounter, can lead to irreversible deactivation of viral entry machinery. Related congeners, which bind the same gp120 site, possess different propensities to elicit the allosteric response that underlies the undesired enhancement of CD4-independent viral entry. Subsequently, key hotspots in the CD4-gp120 interface were categorized using mutagenesis and isothermal titration calorimetry according to the capacity to increase binding affinity without triggering the allosteric signal. This analysis, combined with cocrystal structures of small molecule viral entry agonists with gp120, led to the development of fully functional antagonists of HIV-1 entry. Additional structure-based design exploiting two hotspots followed by synthesis has now yielded low micromolar inhibitors of viral entry.

Published

2014

27. Interfacial cavity filling to optimize CD4-mimetic miniprotein interactions with HIV-1 surface glycoprotein.

Author

Morellato-Castillo L, Acharya P, Combes O, Michiels J, Descours A, Ramos OH, Yang Y, Vanham G, Ariën KK, Kwong PD, Martin L, and Kessler P

Subjects

Amino Acid Sequence, Anti-HIV Agents chemistry, Anti-HIV Agents toxicity, Binding, Competitive, Cell Line, HIV Envelope Protein gp120 chemistry, HIV-1 metabolism, HIV-1 physiology, Models, Molecular, Molecular Sequence Data, Peptide Fragments chemistry, Peptide Fragments toxicity, Protein Binding, Protein Structure, Tertiary, Virus Internalization drug effects, Anti-HIV Agents metabolism, Anti-HIV Agents pharmacology, CD4 Antigens chemistry, HIV Envelope Protein gp120 metabolism, HIV-1 drug effects, Peptide Fragments metabolism, Peptide Fragments pharmacology

Abstract

Ligand affinities can be optimized by interfacial cavity filling. A hollow (Phe43 cavity) between HIV-1 surface glycoprotein (gp120) and cluster of differentiation 4 (CD4) receptor extends beyond residue phenylalanine 43 of CD4 and cannot be fully accessed by natural amino acids. To increase HIV-1 gp120 affinity for a family of CD4-mimetic miniproteins (miniCD4s), we targeted the gp120 Phe43 cavity with 11 non-natural phenylalanine derivatives, introduced into a miniCD4 named M48 (1). The best derivative, named M48U12 (13), bound HIV-1 YU2 gp120 with 8 pM affinity and showed potent HIV-1 neutralization. It contained a methylcyclohexyl derivative of 4-aminophenylalanine, and its cocrystal structure with gp120 revealed the cyclohexane ring buried within the gp120 hydrophobic core but able to assume multiple orientations in the binding pocket, and the aniline nitrogen potentially providing a focus for further improvement. Altogether, the results provide a framework for filling the interfacial Phe43 cavity to enhance miniCD4 affinity.

Published

2013

28. Significant differences in cell-cell fusion and viral entry between strains revealed by scanning mutagenesis of the C-heptad repeat of HIV gp41.

Author

Diaz-Aguilar B, Dewispelaere K, Yi HA, and Jacobs A

Subjects

Cell Fusion, HEK293 Cells, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 metabolism, HIV Envelope Protein gp41 chemistry, HIV-1 genetics, Humans, Membrane Fusion, Mutation, Receptors, CXCR4 genetics, Virus Internalization, HIV Envelope Protein gp41 genetics, HIV Envelope Protein gp41 metabolism, HIV-1 physiology

Abstract

The transmembrane subunit, gp41, of the HIV envelope mediates the viral fusion step of entry into the host cell. The protein consists of an extracellular domain, a transmembrane domain, and a cytoplasmic tail. The extracellular domain contains a fusion peptide, an N-terminal heptad repeat, a loop region, a C-terminal heptad repeat (CHR), and a membrane-proximal external region. For this study, we examined each amino acid in the CHR (residues 623-659) by alanine scanning mutagenesis in two HIV strains: one CCR5-utilizing strain (JRFL) and one CXCR4-utilizing strain (HXB2). We studied the functional importance of each amino acid residue by measuring mutational effects in both cell-cell fusion and viral entry and assessing envelope expression and gp120-gp41 proteolytic processing. The transmembrane subunit of the HIV envelope, gp41, is very sensitive to subtle changes, like alanine substitution, which severely affect envelope function at multiple sites. Two important general findings are apparent when the entire data set from this study is taken into account. (1) Strain HXB2 is much more stable to mutagenesis than strain JRFL, and (2) viral entry is much more stable to mutagenesis than cell-cell fusion. These findings strengthen our notion that gp41 is a vulnerable target for therapeutic and prophylactic intervention. Further structural studies aimed at gaining a full understanding of the intermediate states that drive HIV membrane fusion are imperative.

Published

2013

29. Characterization of host-cell line specific glycosylation profiles of early transmitted/founder HIV-1 gp120 envelope proteins.

Author

Go EP, Liao HX, Alam SM, Hua D, Haynes BF, and Desaire H

Subjects

Amino Acid Sequence, Animals, CHO Cells, Chromatography, Liquid, Cricetinae, Cricetulus, Glycosylation, HEK293 Cells, HIV Envelope Protein gp120 chemistry, Humans, Mass Spectrometry, Molecular Sequence Data, Sequence Homology, Amino Acid, Surface Plasmon Resonance, HIV Envelope Protein gp120 metabolism

Abstract

Glycosylation plays an essential role in regulating protein function by modulating biological, structural, and therapeutic properties. However, due to its inherent heterogeneity and diversity, the comprehensive analysis of protein glycosylation remains a challenge. As part of our continuing effort in the analysis of glycosylation profiles of recombinant HIV-1 envelope-based immunogens, we evaluated and compared the host-cell specific glycosylation pattern of recombinant HIV-1 surface glycoprotein, gp120, derived from clade C transmitted/founder virus 1086.C expressed in Chinese hamster ovary (CHO) and human embryonic kidney containing T antigen (293T) cell lines. We used an integrated glycopeptide-based mass mapping workflow that includes a partial deglycosylation step described in our previous study with the inclusion of a fragmentation technique, electron transfer dissociation (ETD), to complement collision-induced dissociation. The inclusion of ETD facilitated the analysis by providing additional validation for glycopeptide identification and expanding the identified glycopeptides to include coverage of O-linked glycosylation. The site-specific glycosylation analysis shows that the transmitted/founder 1086.C gp120 expressed in CHO and 293T displayed distinct similarities and differences. For N-linked glycosylation, two sites (N386 and N392) in the V4 region were populated with high mannose glycans in the CHO cell-derived 1086.C gp120, while these sites had a mixture of high mannose and processed glycans in the 293T cell-derived 1086.C gp120. Compositional analysis of O-linked glycans revealed that 293T cell-derived 1086.C gp120 consisted of core 1, 2, and 4 type O-linked glycans, while CHO cell-derived 1086.C exclusively consisted of core 1 type O-linked glycans. Overall, glycosylation site occupancy of the CHO and 293T cell-derived 1086.C gp120 showed a high degree of similarity except for one site at N88 in the C1 region. This site was partially occupied in 293T-gp120 but fully occupied in CHO-gp120. Site-specific glycopeptide analysis of transmitted/founder 1086.C gp120 expressed in CHO cells revealed the presence of phosphorylated glycans, while 293T cell-produced 1086.C gp120 glycans were not phosphorylated. While the influence of phosphorylated glycans on immunogenicity is unclear, distinguishing host-cell specific variations in glycosylation profiles provide insights into the similarity (or difference) in recombinant vaccine products. While these differences had minimal effect on envelope antigenicity, they may be important in considering immunogenicity and functional capacities of recombinant envelope proteins produced in different expression systems.

Published

2013

30. A novel synthetic bivalent ligand to probe chemokine receptor CXCR4 dimerization and inhibit HIV-1 entry.

Author

Choi WT, Kumar S, Madani N, Han X, Tian S, Dong CZ, Liu D, Duggineni S, Yuan J, Sodroski JG, Huang Z, and An J

Subjects

HIV Envelope Protein gp120 metabolism, Ligands, Models, Molecular, Peptide Fragments chemical synthesis, Peptide Fragments chemistry, Protein Structure, Quaternary, Receptors, CXCR4 metabolism, Signal Transduction drug effects, Drug Design, HIV-1 drug effects, HIV-1 physiology, Peptide Fragments pharmacology, Protein Multimerization drug effects, Receptors, CXCR4 chemistry, Virus Internalization drug effects

Abstract

Chemokine receptor CXCR4 is one of two principal coreceptors for the entry of HIV-1 into target cells. CXCR4 is known to form homodimers. We previously demonstrated that the amino terminus of viral macrophage protein II (vMIP-II) is the major determinant for CXCR4 recognition, and that V1 peptide derived from the N-terminus of vMIP-II (1-21 residues) showed significant CXCR4 binding. Interestingly, an all-d-amino acid analogue of V1 peptide, DV1 peptide, displayed an even higher binding affinity and strong antiviral activity in inhibiting the replication of CXCR4-dependent HIV-1 strains. In this study, we synthetically linked two DV1 peptides with the formation of a disulfide bond between the two cysteine residues present in the peptide sequence to generate a dimeric molecule potentially capable of interacting with two CXCR4 receptors. DV1 dimer exhibited enhanced binding affinity and antiviral activity compared with those of DV1 monomer. Ligand binding site mapping experiments showed that DV1 dimer overlaps with HIV-1 gp120 on CXCR4 binding sites, including several transmembrane (TM) residues located close to the extracellular side and the N-terminus of CXCR4. This finding was supported by the molecular modeling of CXCR4 dimer-DV1 dimer interaction based on the crystal structure of CXCR4, which showed that DV1 dimer is capable of interacting with the CXCR4 dimeric structure by allowing the N-terminus of each DV1 monomer to reach into the binding pocket of CXCR4 monomer. The development of this bivalent ligand provides a tool for further probing the functions of CXCR4 dimerization and studying CXCR4 heterodimerization with other receptors.

Published

2012

31. The role of individual carbohydrate-binding sites in the function of the potent anti-HIV lectin griffithsin.

Author

Xue J, Gao Y, Hoorelbeke B, Kagiampakis I, Zhao B, Demeler B, Balzarini J, and Liwang PJ

Subjects

Binding Sites, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 metabolism, HIV Infections drug therapy, HIV Infections genetics, HIV Infections metabolism, HIV-1 genetics, HIV-1 metabolism, Magnetic Resonance Spectroscopy methods, Mannose genetics, Mannose metabolism, Models, Molecular, Mutation, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Carbohydrates chemistry, HIV-1 drug effects, Plant Lectins chemistry, Plant Lectins pharmacology

Abstract

Griffithsin (GRFT) is a lectin that has been shown to inhibit HIV infection by binding to high mannose glycan structures on the surface of gp120, and it is among the most potent HIV entry inhibitors reported so far. However, important biochemical details on the antiviral mechanism of GRFT action remain unexplored. In order to understand the role of the three individual carbohydrate-binding sites (CBS) in GRFT, mutations were made at each site (D30A, D70A, and D112A), and the resulting mutants were investigated. NMR studies revealed that each GRFT variant was folded but showed significant peak movement on the carbohydrate-binding face of the protein. The wild-type and each point mutant protein appeared as tight dimers with a K(d) below 4.2 μM. Mutation of any individual CBS on GRFT reduced binding of the protein to mannose, and ELISA assays revealed a partial loss of ability of each GRFT point mutant to bind gp120, with a near-complete loss of binding by the triple mutant D30A/D70A/D112A GRFT. A more quantitative surface plasmon resonance (SPR) examination showed a rather small loss of binding to gp120 for the individual GRFT point mutants (K(D): 123 to 245 pM range versus 73 pM for wild-type GRFT), but dramatic loss of the triple mutant to bind gp120 derived from R5 and X4 strains (K(D) > 12 nM). In contrast to the 2- to 3-fold loss of binding to gp120, the single CBS point mutants of GRFT were significantly less able to inhibit viral infection, exhibiting a 26- to 1900-fold loss of potency, while the triple mutant was at least 875-fold less effective against HIV-1 infection. The disparity between HIV-1 gp120 binding ability and HIV inhibitory potency for these GRFT variants indicates that gp120 binding and virus neutralization do not necessarily correlate, and suggests a mechanism that is not based on simple gp120 binding.

Published

2012

32. Characterization and carbohydrate specificity of pradimicin S.

Author

Shahzad-ul-Hussan S, Ghirlando R, Dogo-Isonagie CI, Igarashi Y, Balzarini J, and Bewley CA

Subjects

Anthracyclines metabolism, Anti-HIV Agents metabolism, Anti-Infective Agents metabolism, Anti-Infective Agents pharmacology, HIV Infections drug therapy, HIV-1 metabolism, Humans, Mannans metabolism, Mannose metabolism, Trisaccharides chemistry, Virus Internalization drug effects, Anthracyclines pharmacology, Anti-HIV Agents pharmacology, Calcium metabolism, HIV Envelope Protein gp120 metabolism, HIV-1 drug effects, Trisaccharides metabolism

Abstract

The pradimicin family of antibiotics is attracting attention due to its anti-infective properties and as a model for understanding the requirements for carbohydrate recognition by small molecules. Members of the pradimicin family are unique among natural products in their ability to bind sugars in a Ca(2+)-dependent manner, but the oligomerization to insoluble aggregates that occurs upon Ca(2+) binding has prevented detailed characterization of their carbohydrate specificity and biologically relevant form. Here we take advantage of the water solubility of pradimicin S (PRM-S), a sulfated glucose-containing analogue of pradimicin A (PRM-A), to show by NMR spectroscopy and analytical ultracentrifugation that at biologically relevant concentrations, PRM-S binds Ca(2+) to form a tetrameric species that selectively binds and engulfs the trisaccharide Manα1-3(Manα1-6)Man over mannose or mannobiose. In functional HIV-1 entry assays, IC(50) values of 2-4 μM for PRM-S corrrelate with the concentrations at which oligomerization occurs as well as the affinities with which PRM-S binds the HIV surface envelope glycoprotein gp120. Together these data reveal the biologically active form of PRM-S, provide an explanation for previous speculations that PRM-A may contain a second mannose binding site, and expand our understanding of the characteristics that can engender a small molecule with the ability to function as a carbohydrate receptor.

Published

2012

33. Design, synthesis, and antiviral activity of entry inhibitors that target the CD4-binding site of HIV-1.

Author

Curreli F, Choudhury S, Pyatkin I, Zagorodnikov VP, Bulay AK, Altieri A, Kwon YD, Kwong PD, and Debnath AK

Subjects

Amides chemistry, Amides pharmacology, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Cell Line, Tumor, Crystallography, X-Ray, Databases, Factual, Drug Design, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, HIV-1 physiology, Humans, Models, Molecular, Oxalates chemistry, Oxalates pharmacology, Piperidines chemistry, Piperidines pharmacology, Stereoisomerism, Structure-Activity Relationship, Thiazoles chemical synthesis, Thiazoles chemistry, Thiazoles pharmacology, Virus Internalization drug effects, Amides chemical synthesis, Anti-HIV Agents chemical synthesis, CD4 Antigens metabolism, HIV-1 drug effects, Oxalates chemical synthesis, Piperidines chemical synthesis

Abstract

The CD4 binding site on HIV-1 gp120 has been validated as a drug target to prevent HIV-1 entry to cells. Previously, we identified two small molecule inhibitors consisting of a 2,2,6,6-tetramethylpiperidine ring linked by an oxalamide to a p-halide-substituted phenyl group, which target this site, specifically, a cavity termed "Phe43 cavity". Here we use synthetic chemistry, functional assessment, and structure-based analysis to explore variants of each region of these inhibitors for improved antiviral properties. Alterations of the phenyl group and of the oxalamide linker indicated that these regions were close to optimal in the original lead compounds. Design of a series of compounds, where the tetramethylpiperidine ring was replaced with new scaffolds, led to improved antiviral activity. These new scaffolds provide insight into the surface chemistry at the entrance of the cavity and offer additional opportunities by which to optimize further these potential-next-generation therapeutics and microbicides against HIV-1.

Published

2012

34. Structure-based design, synthesis, and characterization of dual hotspot small-molecule HIV-1 entry inhibitors.

Author

LaLonde JM, Kwon YD, Jones DM, Sun AW, Courter JR, Soeta T, Kobayashi T, Princiotto AM, Wu X, Schön A, Freire E, Kwong PD, Mascola JR, Sodroski J, Madani N, and Smith AB 3rd

Subjects

CD4 Antigens metabolism, Calorimetry methods, Crystallography, X-Ray, HIV Envelope Protein gp120 metabolism, HIV Fusion Inhibitors chemical synthesis, HIV Infections metabolism, HIV Infections virology, Humans, Indans chemical synthesis, Inhibitory Concentration 50, Magnetic Resonance Spectroscopy, Mass Spectrometry, Models, Molecular, Molecular Dynamics Simulation, Neutralization Tests methods, Structure-Activity Relationship, Thermodynamics, Virus Internalization drug effects, HIV Fusion Inhibitors chemistry, HIV Fusion Inhibitors pharmacology, HIV Infections drug therapy, HIV-1 physiology, Indans chemistry, Indans pharmacology

Abstract

Cellular infection by HIV-1 is initiated with a binding event between the viral envelope glycoprotein gp120 and the cellular receptor protein CD4. The CD4-gp120 interface is dominated by two hotspots: a hydrophobic gp120 cavity capped by Phe43(CD4) and an electrostatic interaction between residues Arg59(CD4) and Asp368(gp120). The CD4 mimetic small-molecule NBD-556 (1) binds within the gp120 cavity; however, 1 and related congeners demonstrate limited viral neutralization breadth. Herein, we report the design, synthesis, characterization, and X-ray structures of gp120 in complex with small molecules that simultaneously engage both binding hotspots. The compounds specifically inhibit viral infection of 42 tier 2 clades B and C viruses and are shown to be antagonists of entry into CD4-negative cells. Dual hotspot design thus provides both a means to enhance neutralization potency of HIV-1 entry inhibitors and a novel structural paradigm for inhibiting the CD4-gp120 protein-protein interaction.

Published

2012

35. Designed cyclic permutants of HIV-1 gp120: implications for envelope trimer structure and immunogen design.

Author

Saha P, Bhattacharyya S, Kesavardhana S, Miranda ER, Ali PS, Sharma D, and Varadarajan R

Subjects

Antibodies, Monoclonal chemistry, Antibodies, Monoclonal immunology, Antibodies, Neutralizing chemistry, Antibodies, Neutralizing immunology, Binding Sites, CD4 Antigens chemistry, CD4 Antigens immunology, Epitopes, HEK293 Cells, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, HIV-1 immunology, Humans, Peptides, Cyclic immunology, Protein Multimerization, Transfection, Vaccines, Synthetic immunology, HIV Envelope Protein gp120 genetics, Peptides, Cyclic chemistry, Vaccines, Synthetic chemistry

Abstract

Most HIV-1 broadly neutralizing antibodies are directed against the gp120 subunit of the env surface protein. Native env consists of a trimer of gp120-gp41 heterodimers, and in contrast to monomeric gp120, preferentially binds CD4 binding site (CD4bs)-directed neutralizing antibodies over non-neutralizing ones. Some cryo-electron tomography studies have suggested that the V1V2 loop regions of gp120 are located close to the trimer interface. We have therefore designed cyclically permuted variants of gp120 with and without the h-CMP and SUMO2a trimerization domains inserted into the V1V2 loop. h-CMP-V1cyc is one such variant in which residues 153 and 142 are the N- and C-terminal residues, respectively, of cyclically permuted gp120 and h-CMP is fused to the N-terminus. This molecule forms a trimer under native conditions and binds CD4 and the neutralizing CD4bs antibodies b12 with significantly higher affinity than wild-type gp120. It binds non-neutralizing CD4bs antibody F105 with lower affinity than gp120. A similar derivative, h-CMP-V1cyc1, bound the V1V2 loop-directed broadly neutralizing antibodies PG9 and PG16 with ∼20-fold higher affinity than wild-type JRCSF gp120. These cyclic permutants of gp120 are properly folded and are potential immunogens. The data also support env models in which the V1V2 loops are proximal to the trimer interface.

Published

2012

36. Binding of HIV-1 gp120 glycoprotein to silica nanoparticles modified with CD4 glycoprotein and CD4 peptide fragments.

Author

Cheng K, El-Boubbou K, and Landry CC

Subjects

CD4 Antigens metabolism, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 metabolism, HIV Infections metabolism, HIV-1 chemistry, HIV-1 genetics, HIV-1 metabolism, Humans, Protein Binding, Recombinant Proteins chemistry, Recombinant Proteins metabolism, CD4 Antigens chemistry, HIV Envelope Protein gp120 chemistry, HIV Infections diagnosis, Nanoparticles chemistry, Peptide Fragments chemistry, Silicon Dioxide chemistry

Abstract

An important step in human immunodeficiency virus infection involves the interaction between the viral envelope glycoprotein gp120 and the human host cell surface receptor CD4. Herein, we describe a CD4-functionalized mesoporous silica-based system to selectively capture HIV-gp120 with high binding efficiency. Using a protection-deprotection strategy developed recently by our group, the external surface of the mesoporous particles was selectively functionalized with soluble CD4 ("sCD4") or an 18-peptide fragment mimicking the gp120 binding region. Confocal microscopy confirmed the CD4 locations and showed that the internal pores can be made accessible after external modification in a controlled manner. An evaluation of the ability of an 18-peptide CD4 fragment versus amide-immobilized sCD4 and sCD4 immobilized through its glycosidic group indicated that while all peptides were selective, the latter method was clearly best, with nearly complete removal of whole gp120 from solution. This study shows, for the first time, that sCD4 bound to mesoporous silica particles actively recognizes and retains high binding affinity for HIV-gp120. It is anticipated that, by proper modification of the accessible internal pores, our methodology can be adopted to develop porous platforms for HIV diagnosis, imaging, drug delivery, and vaccine development., (© 2011 American Chemical Society)

Published

2012

37. Discovery of novel promising targets for anti-AIDS drug developments by computer modeling: application to the HIV-1 gp120 V3 loop.

Author

Andrianov AM, Anishchenko IV, and Tuzikov AV

Subjects

Amino Acid Motifs, Amino Acid Sequence, Computational Biology, Models, Molecular, Molecular Sequence Data, Molecular Targeted Therapy, Protein Conformation, Anti-HIV Agents pharmacology, Computer Simulation, Drug Design, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, HIV-1 drug effects, HIV-1 metabolism

Abstract

The V3 loop on gp120 from HIV-1 is a focus of many research groups involved in anti-AIDS drug studies, because this region of the protein determines the preference of the virus for T-lymphocytes or primary macrophages. Although the V3 loop governs cell tropism and, for this reason, exhibits one of the most attractive targets for anti-HIV-1 drug developments, its high sequence variability is a major complicating factor. Nevertheless, the data on the spatial arrangement of V3 obtained here for different HIV-1 subtypes by computer modeling clearly show that, despite a wide range of 3D folds, this functionally important site of gp120 forms at least three structurally invariant segments, which contain residues critical for cell tropism. It is evident that these conserved V3 segments represent potential HIV-1 vulnerable spots and, therefore, provide a blueprint for the design of novel, potent and broad antiviral agents able to stop the HIV's spread.

Published

2011

38. Structure-based identification and neutralization mechanism of tyrosine sulfate mimetics that inhibit HIV-1 entry.

Author

Acharya P, Dogo-Isonagie C, LaLonde JM, Lam SN, Leslie GJ, Louder MK, Frye LL, Debnath AK, Greenwood JR, Luongo TS, Martin L, Watts KS, Hoxie JA, Mascola JR, Bewley CA, and Kwong PD

Subjects

CD4 Antigens immunology, HIV Envelope Protein gp120 immunology, HIV Envelope Protein gp120 metabolism, HIV Infections drug therapy, HIV-1 physiology, Humans, Models, Molecular, Tyrosine chemistry, Tyrosine pharmacology, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, HIV-1 drug effects, Tyrosine analogs & derivatives, Virus Internalization drug effects

Abstract

Tyrosine sulfate-mediated interactions play an important role in HIV-1 entry. After engaging the CD4 receptor at the cell surface, the HIV-1 gp120 glycoprotein binds to the CCR5 co-receptor via an interaction that requires two tyrosine sulfates, at positions 10 and 14 in the CCR5-N terminus. Building on previous structure determinations of this interaction, here we report the targeting of these tyrosine sulfate binding sites for drug design through in silico screening of small molecule libraries, identification of lead compounds, and characterization of biological activity. A class of tyrosine sulfate-mimicking small molecules containing a "phenyl sulfonate-linker-aromatic" motif was identified that specifically inhibited binding of gp120 to the CCR5-N terminus as well as to sulfated antibodies that recognize the co-receptor binding region on gp120. The most potent of these compounds bound gp120 with low micromolar affinity and its CD4-induced conformation with K(D)'s as tight as ∼50 nM. Neutralization experiments suggested the targeted site to be conformationally inaccessible prior to CD4 engagement. Primary HIV-1 isolates were weakly neutralized, preincubation with soluble CD4 enhanced neutralization, and engineered isolates with increased dependence on the N terminus of CCR5 or with reduced conformational barriers were neutralized with IC(50) values as low as ∼1 μM. These results reveal the potential of targeting the tyrosine sulfate interactions of HIV-1 and provide insight into how mechanistic barriers, evolved by HIV-1 to evade antibody recognition, also restrict small-molecule-mediated neutralization.

Published

2011

39. Evaluation of the synthesis of sialic acid-PAMAM glycodendrimers without the use of sugar protecting groups, and the anti-HIV-1 properties of these compounds.

Author

Clayton R, Hardman J, LaBranche CC, and McReynolds KD

Subjects

HIV Envelope Protein gp120 metabolism, HIV Infections drug therapy, Humans, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Dendrimers chemistry, Dendrimers pharmacology, HIV-1 drug effects, N-Acetylneuraminic Acid chemistry, N-Acetylneuraminic Acid pharmacology

Abstract

A study was undertaken to evaluate the feasibility of synthesizing six sialic acid-PAMAM glycodendrimers using unprotected sialic acid in as few as 1-4 steps using two different reaction pathways, and to assess the sulfated derivatives for anti-HIV activity. The syntheses were accomplished through either the direct attachment of the sialic acid carboxyl group to amine-terminated PAMAM (a divergent-like approach) using BOP coupling, or by first reacting sialic acid with a polar bifunctional spacer molecule, attaching the sugar-linker to carboxy-terminated PAMAM (a convergent-like approach), and again using BOP-mediated coupling reactions. It was hypothesized that the latter approach would be the most successful method, as any steric congestion between the sialic acid and the PAMAM would be minimized using an intervening polar linker. However, the divergent-like synthesis proved to be the superior method, resulting in 11.4%, 14%, and 28% of the fully substituted generations 0, 1, and 2 sialic acid-PAMAM conjugates, respectively, as compared to 6.4% of only the generation -0.5 sialic acid-linker-PAMAM conjugate for the convergent-like method. Upon sulfation of the four glycodendrimers, binding capabilities to the recombinant HIV protein, gp120, were assessed using an ELISA assay. Compounds that showed promising binding characteristics were then further assessed for inhibition of HIV-1 infection using a well-characterized luciferase reporter gene neutralization assay. The generation 2 sulfated sialic acid-PAMAM glycodendrimer, sulfo-6, bearing 16 sialic acids with 11 sulfate groups incorporated at 4.03% sulfur content by weight, was found to inhibit all four HIV-1 strains tested in the low micromolar range.

Published

2011

40. Design and characterization of stabilized derivatives of human CD4D12 and CD4D1.

Author

Saha P, Barua B, Bhattacharyya S, Balamurali MM, Schief WR, Baker D, and Varadarajan R

Subjects

Antiviral Agents chemical synthesis, Antiviral Agents metabolism, Antiviral Agents pharmacology, CD4 Antigens metabolism, HIV Envelope Protein gp120 antagonists & inhibitors, HIV Envelope Protein gp120 metabolism, Humans, Mutation, Protein Binding genetics, Protein Stability, Protein Structure, Secondary, Protein Structure, Tertiary, Virus Internalization, CD4 Antigens chemistry, CD4 Antigens genetics, Protein Folding

Abstract

CD4 is present on the surface of T-lymphocytes and is the primary cellular receptor for HIV-1. CD4 consists of a cytoplasmic tail, one transmembrane region, and four extracellular domains, D1-D4. A construct consisting of the first two domains of CD4 (CD4D12) is folded and binds gp120 with similar affinity as soluble 4-domain CD4 (sCD4). However, the first domain alone (CD4D1) was previously shown to be largely unfolded and had 3-fold weaker affinity for gp120 when compared to sCD4 [Sharma, D.; et al. (2005) Biochemistry 44, 16192-16202]. We now report the design and characterization of three single-site mutants of CD4D12 (G6A, L51I, and V86L) and one multisite mutant of CD4D1 (G6A/L51I/L5K/F98T). G6A, L51I, and V86L are cavity-filling mutations while L5K and F98T are surface mutations which were introduced to minimize the aggregation of CD4D1 upon removal of the second domain. Two mutations, G6A and V86L in CD4D12 increased the stability and yield of the protein relative to the wild-type protein. The mutant CD4D1 (CD4D1a) with the 4 mutations was folded and more stable compared to the original CD4D1, but both bound gp120 with comparable affinity. In in vitro neutralization assays, both CD4D1a and G6A-CD4D12 were able to neutralize diverse HIV-1 viruses with similar IC(50)s as 4-domain CD4. These stabilized derivatives of human CD4 can be useful starting points for the design of other more complex viral entry inhibitors., (© 2011 American Chemical Society)

Published

2011

41. Targeting HIV entry through interaction with envelope glycoprotein 120 (gp120): synthesis and antiviral evaluation of 1,3,5-triazines with aromatic amino acids.

Author

Lozano V, Aguado L, Hoorelbeke B, Renders M, Camarasa MJ, Schols D, Balzarini J, San-Félix A, and Pérez-Pérez MJ

Subjects

Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, Cells, Cultured, HIV Envelope Protein gp120 chemistry, Humans, Lectins metabolism, Receptors, CCR5 metabolism, Receptors, CXCR4 metabolism, Surface Plasmon Resonance, T-Lymphocytes, Triazines chemical synthesis, Anti-HIV Agents metabolism, HIV Envelope Protein gp120 metabolism, HIV-1 drug effects, Triazines metabolism

Abstract

On the basis of the interesting inhibitory properties that lectins show against HIV-replication through their interaction with glycoprotein 120 (gp120), we here describe the design, synthesis, and anti-HIV evaluation of three series of 1,3,5-triazine derivatives (monomers, dimers, and trimers) functionalized with aromatic amino acids meant to mimic interactions that lectins establish with gp120. While monomers were inactive against HIV replication, dimers showed limited anti-HIV activity that is, however, considerably more significant in the trimers series, with EC(50) values in the lower μM range. These findings most likely reflect the requirement of multivalency of the 1,3,5-triazine derivatives to display anti-HIV activity, as lectins do. The pronounced anti-HIV activity (EC(50) ∼ 20 μM) is accompanied by the absence of toxicity in CEM T-cell line (CC(50) > 250 μM). Moreover, SPR experiments revealed that the prototype trimers with a central core of 2,4,6-triethylbenzene and six l-Trp or six l-Tyr residues at the periphery were efficient binders of CXCR4- and CCR5-tropic HIV-1 gp120 (estimated K(D): lower micromolar range). The collected data support the interest of this novel family of anti-HIV agents and qualify them as potential novel microbicide lead compounds.

Published

2011

42. Enhanced dynamics of HIV gp120 glycoprotein by small molecule binding.

Author

Shrivastava I and LaLonde JM

Subjects

Animals, CD4 Antigens chemistry, CD4 Antigens metabolism, Crystallography, X-Ray, HIV Envelope Protein gp120 genetics, Models, Molecular, Mutagenesis, Oxalates chemistry, Oxalates metabolism, Phenylalanine chemistry, Phenylalanine metabolism, Piperidines chemistry, Piperidines metabolism, Protein Binding genetics, Protein Stability, Protein Structure, Secondary genetics, Protein Structure, Tertiary genetics, Protein Unfolding, Scorpion Venoms chemistry, Scorpion Venoms metabolism, Scorpions, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, Molecular Dynamics Simulation

Abstract

HIV cell entry and infection are driven by binding events to the CD4 and chemokine receptors with associated conformational change of the viral glycoprotein, gp120. Scyllatoxin miniprotein CD4 mimetics and a small molecule inhibitor of CD4 binding, NBD-556, also effectively induce gp120 conformational change. In this study we examine the fluctuation profile of gp120 in context of CD4, a miniprotein mimetic, and NBD-556 with the aim of understanding the effect of ligand binding on gp120 conformational dynamics. Analysis of molecular dynamics trajectories indicate that NBD-556 binding in the Phe 43 cavity enhances the overall mobility of gp120, especially in the outer domain in comparison to CD4 or miniprotein bound complex. Interactions with the more flexible bridging sheet strengthen upon NBD-556 binding and may contribute to gp120 restructuring. The enhanced mobility of D368, E370, and I371 with NBD-556 bound in the Phe 43 cavity suggests that interactions with α3-helix in the outer domain are not optimal, providing further insights into gp120--small molecule interactions that may impact small molecule designs.

Published

2011

43. Conformational and structural features of HIV-1 gp120 underlying the dual receptor antagonism by cross-reactive neutralizing antibody m18.

Author

Gift SK, Zentner IJ, Schön A, McFadden K, Umashankara M, Rajagopal S, Contarino M, Duffy C, Courter JR, Zhang MY, Gershoni JM, Cocklin S, Dimitrov DS, Smith AB 3rd, Freire E, and Chaiken IM

Subjects

Antibodies, Monoclonal immunology, Antibodies, Monoclonal metabolism, Antibodies, Neutralizing immunology, Binding Sites genetics, Binding, Competitive, CD4 Antigens immunology, CD4 Antigens metabolism, Calorimetry, Epitopes immunology, Epitopes metabolism, HIV Antibodies immunology, HIV Antibodies metabolism, HIV Envelope Protein gp120 genetics, HIV-1 immunology, HIV-1 metabolism, Humans, Models, Molecular, Mutation, Protein Binding, Protein Structure, Tertiary, Surface Plasmon Resonance, Thermodynamics, Antibodies, Neutralizing metabolism, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 metabolism, Protein Conformation

Abstract

We investigated the interaction between cross-reactive HIV-1 neutralizing human monoclonal antibody m18 and HIV-1YU-2 gp120 in an effort to understand how this antibody inhibits the entry of virus into cells. m18 binds to gp120 with high affinity (KD≈5 nM) as measured by surface plasmon resonance (SPR) and isothermal titration calorimetry (ITC). SPR analysis further showed that m18 inhibits interactions of gp120 with both soluble CD4 and CD4-induced antibodies that have epitopes overlapping the coreceptor binding site. This dual receptor site antagonism, which occurs with equal potency for both inhibition effects, argues that m18 is not functioning as a mimic of CD4, in spite of the presence of a putative CD4-like loop formed by HCDR3 in the antibody. Consistent with this view, m18 was found to interact with gp120 in the presence of saturating concentrations of a CD4-mimicking small molecule gp120 inhibitor, suggesting that m18 does not require unoccupied CD4 Phe43 binding cavity residues of gp120. Thermodynamic analysis of the m18-gp120 interaction suggests that m18 stabilizes a conformation of gp120 that is unique from and less structured than the CD4-stabilized conformation. Conformational mutants of gp120 were studied for their impact on m18 interaction. Mutations known to disrupt the coreceptor binding region and to lead to complete suppression of 17b binding had minimal effects on m18 binding. This argues that energetically important epitopes for m18 binding lie outside the disrupted bridging sheet region used for 17b and coreceptor binding. In contrast, mutations in the CD4 region strongly affected m18 binding. Overall, the results obtained in this work argue that m18, rather than mimicking CD4 directly, suppresses both receptor binding site functions of HIV-1 gp120 by stabilizing a nonproductive conformation of the envelope protein. These results can be related to prior findings about the importance of conformational entrapment as a common mode of action for neutralizing CD4bs antibodies, with differences mainly in epitope utilization and the extent of gp120 structuring.

Published

2011

44. Monoclonal antibody m18 paratope leading to dual receptor antagonism of HIV-1 gp120.

Author

Gift SK, McFadden K, Zentner IJ, Rajagopal S, Zhang MY, Dimitrov DS, and Chaiken IM

Subjects

Antibodies, Monoclonal chemistry, Antibodies, Monoclonal genetics, Antibodies, Neutralizing chemistry, Antibodies, Neutralizing genetics, Antibodies, Neutralizing metabolism, Binding Sites drug effects, Binding, Competitive, CD4 Antigens immunology, Complementarity Determining Regions chemistry, Complementarity Determining Regions genetics, Complementarity Determining Regions metabolism, Epitopes chemistry, Epitopes genetics, HIV Antibodies chemistry, HIV Antibodies genetics, HIV Antibodies metabolism, HIV-1 immunology, HIV-1 metabolism, Humans, Immunoglobulin Fab Fragments chemistry, Immunoglobulin Fab Fragments immunology, Immunoglobulin Fab Fragments metabolism, Models, Molecular, Mutation, Protein Binding, Protein Conformation, Antibodies, Monoclonal metabolism, CD4 Antigens metabolism, Epitopes metabolism, HIV Envelope Protein gp120 metabolism

Abstract

We sought to identify sequences in the monoclonal antibody m18 complementarity determining regions (CDRs) that are responsible for its interaction with HIV-1 gp120 and inhibition of the envelope receptor binding sites. In the accompanying paper (DOI 10.1021/bi101160r), we reported that m18 inhibits CD4 binding through a nonactivating mechanism that, at the same time, induces conformational effects leading to inhibition of the coreceptor site. Here, we sought to define the structural elements in m18 responsible for these actions. Direct binding and competition analyses using surface plasmon resonance showed that YU-2 gp120 binding is stabilized by a broad paratope of residues in the m18 CDRs. Additionally, several m18 residues were identified for which mutants retained high affinity for gp120 but had suppressed CD4 and 17b inhibition activities. A subset of these mutants did, however, neutralize HXBc2 viral infection. The results obtained in this work demonstrate that the combined m18 paratope contains subsets of residues that are differentially important for the binding and inhibition functions of the m18 neutralizing antibody. The data also add to prior observations that high-affinity antibodies that do not inhibit monomeric gp120 receptor site interactions may still exhibit significant antiviral activity.

Published

2011

45. Discovery of a small molecule PDI inhibitor that inhibits reduction of HIV-1 envelope glycoprotein gp120.

Author

Khan MM, Simizu S, Lai NS, Kawatani M, Shimizu T, and Osada H

Subjects

Diethylstilbestrol chemical synthesis, Diethylstilbestrol chemistry, Diethylstilbestrol pharmacology, Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Estrone chemical synthesis, Estrone chemistry, Estrone pharmacology, HIV Envelope Protein gp120 antagonists & inhibitors, High-Throughput Screening Assays, Humans, Masoprocol chemical synthesis, Masoprocol chemistry, Masoprocol pharmacology, Models, Molecular, Molecular Structure, Molecular Weight, Oxidation-Reduction, Parabens chemical synthesis, Parabens chemistry, Parabens pharmacology, Protein Disulfide-Isomerases metabolism, Protein Folding drug effects, Sesquiterpenes chemical synthesis, Sesquiterpenes chemistry, Sesquiterpenes pharmacology, Small Molecule Libraries, Stereoisomerism, Structure-Activity Relationship, Drug Discovery, Enzyme Inhibitors pharmacology, HIV Envelope Protein gp120 metabolism, Protein Disulfide-Isomerases antagonists & inhibitors

Abstract

Protein disulfide isomerase (PDI) is a promiscuous protein with multifunctional properties. PDI mediates proper protein folding by oxidation or isomerization and disrupts disulfide bonds by reduction. The entry of HIV-1 into cells is facilitated by the PDI-catalyzed reductive cleavage of disulfide bonds in gp120. PDI is regarded as a potential drug target because of its reduction activity. We screened a chemical library of natural products for PDI-specific inhibitors in a high-throughput fashion and identified the natural compound juniferdin as the most potent inhibitor of PDI. Derivatives of juniferdin were synthesized, with compound 13 showing inhibitory activities comparable to those of juniferdin but reduced cytotoxicity. Both juniferdin and compound 13 inhibited PDI reductase activity in a dose-dependent manner, with IC(50) values of 156 and 167 nM, respectively. Our results also indicated that juniferdin and compound 13 exert their inhibitory activities specifically on PDI but do not significantly inhibit homologues of this protein family. Moreover, we found that both compounds can inhibit PDI-mediated reduction of HIV-1 envelope glycoprotein gp120.

Published

2011

46. Theoretical studies on the interactions and interferences of HIV-1 glycoprotein gp120 and its coreceptor CCR5.

Author

Da LT and Wu YD

Subjects

Amino Acid Sequence, Animals, CCR5 Receptor Antagonists, Cattle, Chemokine CCL3 metabolism, Chemokine CCL4 metabolism, Chemokine CCL5 metabolism, HIV Envelope Protein gp120 chemistry, Molecular Sequence Data, Protein Binding, Protein Structure, Tertiary drug effects, Receptors, CCR5 chemistry, HIV Envelope Protein gp120 metabolism, HIV-1, Molecular Dynamics Simulation, Receptors, CCR5 metabolism

Abstract

The interaction between the HIV gp120 protein and coreceptor CCR5 or CXCR4 of the host cell is critical in mediating the HIV entry process. A model for the CCR5-gp120 complex has been developed. In the model, the N-terminus of CCR5 binds to three discontinuous domains of gp120, including the fourth conserved (C4) region, β19/β20 connecting loop, and V3 loop. The second extra-cellular loop (ECL2) of CCR5 also interacts with the crown part of the gp120 V3 loop. The bindings of the three CCR5 antagonists, maraviroc, aplaviroc, and vicriviroc, to the trans-membrane domain of CCR5 have been modeled. The bindings are found to affect the conformation of the ECL2 domain, which in turn drives the N-terminus of CCR5 to an altered state. Aplaviroc is more hydrophilic than maraviroc and vicriviroc, and its binding is more interfered by solvent, resulting in a quite different effect to the structure of CCR5 compared with those of the other two molecules. The above results are in accord with experimental observations and provide a structural basis for further design of CCR5 antagonists.

Published

2011

47. High-affinity glycopolymer binding to human DC-SIGN and disruption of DC-SIGN interactions with HIV envelope glycoprotein.

Author

Becer CR, Gibson MI, Geng J, Ilyas R, Wallis R, Mitchell DA, and Haddleton DM

Subjects

Binding, Competitive, Cell Adhesion Molecules chemistry, HIV Envelope Protein gp120 antagonists & inhibitors, Humans, Lectins, C-Type chemistry, Mannose chemistry, Models, Molecular, Protein Binding drug effects, Protein Conformation, Receptors, Cell Surface chemistry, Surface Plasmon Resonance, Cell Adhesion Molecules antagonists & inhibitors, Cell Adhesion Molecules metabolism, HIV Envelope Protein gp120 metabolism, HIV-1, Lectins, C-Type antagonists & inhibitors, Lectins, C-Type metabolism, Mannose metabolism, Mannose pharmacology, Receptors, Cell Surface antagonists & inhibitors, Receptors, Cell Surface metabolism

Abstract

Noncovalent interactions between complex carbohydrates and proteins drive many fundamental processes within biological systems, including human immunity. In this report we aimed to investigate the potential of mannose-containing glycopolymers to interact with human DC-SIGN and the ability of these glycopolymers to inhibit the interactions between DC-SIGN and the HIV envelope glycoprotein gp120. We used a library of glycopolymers that are prepared via combination of copper-mediated living radical polymerization and azide-alkyne [3+2] Huisgen cycloaddition reaction. We demonstrate that a relatively simple glycopolymer can effectively prevent the interactions between a human dendritic cell associated lectin (DC-SIGN) and the viral envelope glycoprotein gp120. This approach may give rise to novel insights into the mechanisms of HIV infection and provide potential new therapeutics.

Published

2010

48. Structural analysis of a highly glycosylated and unliganded gp120-based antigen using mass spectrometry.

Author

Wang L, Qin Y, Ilchenko S, Bohon J, Shi W, Cho MW, Takamoto K, and Chance MR

Subjects

Amino Acid Sequence, Animals, Binding Sites, Cell Line, Drosophila, Glycosylation, HIV Antibodies metabolism, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 metabolism, HIV-1 genetics, Humans, Immunoglobulin G metabolism, In Vitro Techniques, Ligands, Models, Molecular, Molecular Sequence Data, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Protein Conformation, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Surface Plasmon Resonance, Tandem Mass Spectrometry, HIV Envelope Protein gp120 chemistry, HIV-1 chemistry

Abstract

Structural characterization of the HIV-1 envelope protein gp120 is very important for providing an understanding of the protein's immunogenicity and its binding to cell receptors. So far, the crystallographic structure of gp120 with an intact V3 loop (in the absence of a CD4 coreceptor or antibody) has not been determined. The third variable region (V3) of the gp120 is immunodominant and contains glycosylation signatures that are essential for coreceptor binding and entry of the virus into T-cells. In this study, we characterized the structure of the outer domain of gp120 with an intact V3 loop (gp120-OD8) purified from Drosophila S2 cells utilizing mass spectrometry-based approaches. We mapped the glycosylation sites and calculated the glycosylation occupancy of gp120-OD8; 11 sites from 15 glycosylation motifs were determined as having high-mannose or hybrid glycosylation structures. The specific glycan moieties of nine glycosylation sites from eight unique glycopeptides were determined by a combination of ECD and CID MS approaches. Hydroxyl radical-mediated protein footprinting coupled with mass spectrometry analysis was employed to provide detailed information about protein structure of gp120-OD8 by directly identifying accessible and hydroxyl radical-reactive side chain residues. Comparison of gp120-OD8 experimental footprinting data with a homology model derived from the ligated CD4-gp120-OD8 crystal structure revealed a flexible V3 loop structure in which the V3 tip may provide contacts with the rest of the protein while residues in the V3 base remain solvent accessible. In addition, the data illustrate interactions between specific sugar moieties and amino acid side chains potentially important to the gp120-OD8 structure.

Published

2010

49. A general approach for receptor and antibody-targeted detection of native proteins utilizing split-luciferase reassembly.

Author

Stains CI, Furman JL, Porter JR, Rajagopal S, Li Y, Wyatt RT, and Ghosh I

Subjects

Antibodies genetics, Cell Line, Tumor, Gene Expression, HIV Envelope Protein gp120 immunology, HIV Envelope Protein gp120 metabolism, HIV-1 isolation & purification, Humans, Immunoassay methods, Luciferases, Firefly genetics, Luminescent Agents metabolism, Models, Molecular, RNA, Messenger genetics, Receptor, ErbB-2 immunology, Receptor, ErbB-2 metabolism, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Vascular Endothelial Growth Factor A immunology, Vascular Endothelial Growth Factor A metabolism, Antibodies immunology, Biosensing Techniques methods, HIV Envelope Protein gp120 analysis, Luciferases, Firefly metabolism, Receptor, ErbB-2 analysis, Vascular Endothelial Growth Factor A analysis

Abstract

The direct detection of native proteins in heterogeneous solutions remains a challenging problem. Standard methodologies rely on a separation step to circumvent nonspecific signal generation. We hypothesized that a simple and general method for the detection of native proteins in solution could be achieved through ternary complexation, where the conditional signal generation afforded by split-protein reporters could be married to the specificity afforded by either native receptors or specific antibodies. Toward this goal, we describe a solution phase split-luciferase assay for native protein detection, where we fused fragmented halves of firefly luciferase to separate receptor fragments or single-chain antibodies, allowing for conditional luciferase complementation in the presence of several biologically significant protein targets. To demonstrate the utility of this strategy, we have developed and validated assay platforms for the vascular endothelial growth factor, the gp120 coat protein from HIV-1, and the human epidermal growth factor receptor 2 (HER2), a marker for breast cancer. The specificities of the recognition elements, CD4 and the 17b single-chain antibody, employed in the gp120 sensor allowed us to parse gp120s from different clades. Our rationally designed HER2 sensing platform was capable of discriminating between HER2 expression levels in several tumor cell lines. In addition, luminescence from reassembled luciferase was linear across a panel of cell lines with increasing HER2 expression. We envision that the proof of principle studies presented herein may allow for the potential detection of a broad range of biological analytes utilizing ternary split-protein systems.

Published

2010

50. A modeled structure of an aptamer-gp120 complex provides insight into the mechanism of HIV-1 neutralization.

Author

Joubert MK, Kinsley N, Capovilla A, Sewell BT, Jaffer MA, and Khati M

Subjects

Antibodies, Monoclonal genetics, Antibodies, Monoclonal immunology, Binding Sites genetics, Binding Sites immunology, Epitopes genetics, Epitopes immunology, HIV Envelope Protein gp120 genetics, HIV-1 genetics, Humans, Hydrogen Bonding, Molecular Dynamics Simulation, HIV Envelope Protein gp120 immunology, HIV Envelope Protein gp120 metabolism, HIV-1 immunology, HIV-1 metabolism

Abstract

The HIV-1 envelope glycoprotein, gp120, is a key target for a class of drugs called entry inhibitors. Here we used molecular modeling to construct a three-dimensional model of an anti-gp120 RNA aptamer, B40t77, alone and in complex with gp120. An initial model of B40t77 was built from the predicted secondary structure and then subjected to a combination of energy minimization and molecular dynamics. To model the B40t77-gp120 complex, we docked the B40t77 predicted structure onto the CD4-induced epitope of the gp120 crystal structure. A series of gp120 point mutations in the predicted B40t77-gp120 interface were measured for their binding affinity for B40t77 by surface plasmon resonance. According to the model, of the 10 gp120 amino acids that showed a reduction in the level of binding when mutated to alanine, all of them are modeled as making direct contact with B40t77 as part of a hydrogen bonding network. Comparison by electron microscopy of the B40t77-gp120 complex with gp120 alone revealed that only the longest dimension of the complex significantly increased in length, in a manner consistent with the predicted model. Binding assays revealed that B40t77 can weaken the binding of gp120 to the monoclonal antibodies B6, B12, and 2G12, none of which have binding sites that overlap with B40t77, as well as strengthen the binding to the antibody 19b. Thus, B40t77 may induce distant conformational changes in gp120 that disrupt its association with host cells and may suggest a mechanism for aptamer neutralization of HIV-1.

Published

2010