Your search keyword '"Irwin Chaiken"' showing total 165 results

1. Adenosine deaminase augments SARS-CoV-2 specific cellular and humoral responses in aged mouse models of immunization and challenge

Author

Ebony N. Gary, Nicholas J. Tursi, Bryce M. Warner, Gina Cuismano, Jennifer Connors, Elizabeth M. Parzych, Bryan D. Griffin, Matthew R. Bell, Ali R. Ali, Drew Frase, Casey E. Hojecki, Gabriela A. Canziani, Irwin Chaiken, Toshitha Kannan, Estella Moffat, Carissa Embury-Hyatt, Sarah K. Wooton, Andrew Kossenkov, Ami Patel, Darwyn Kobasa, Michele A. Kutzler, Elias K. Haddad, and David B. Weiner

Subjects

age, SARS, DNA vaccine, adjuvant, adenosine deaminase (ADA), Immunologic diseases. Allergy, RC581-607

Abstract

Despite numerous clinically available vaccines and therapeutics, aged patients remain at increased risk for COVID-19 morbidity. Furthermore, various patient populations, including the aged can have suboptimal responses to SARS-CoV-2 vaccine antigens. Here, we characterized vaccine-induced responses to SARS-CoV-2 synthetic DNA vaccine antigens in aged mice. Aged mice exhibited altered cellular responses, including decreased IFNγ secretion and increased TNFα and IL-4 secretion suggestive of TH2-skewed responses. Aged mice exhibited decreased total binding and neutralizing antibodies in their serum but significantly increased TH2-type antigen-specific IgG1 antibody compared to their young counterparts. Strategies to enhance vaccine-induced immune responses are important, especially in aged patient populations. We observed that co-immunization with plasmid-encoded adenosine deaminase (pADA)enhanced immune responses in young animals. Ageing is associated with decreases in ADA function and expression. Here, we report that co-immunization with pADA enhanced IFNγ secretion while decreasing TNFα and IL-4 secretion. pADA expanded the breadth and affinity SARS-CoV-2 spike-specific antibodies while supporting TH1-type humoral responses in aged mice. scRNAseq analysis of aged lymph nodes revealed that pADA co-immunization supported a TH1 gene profile and decreased FoxP3 gene expression. Upon challenge, pADA co-immunization decreased viral loads in aged mice. These data support the use of mice as a model for age-associated decreased vaccine immunogenicity and infection-mediated morbidity and mortality in the context of SARS-CoV-2 vaccines and provide support for the use of adenosine deaminase as a molecular adjuvant in immune-challenged populations.

Published

2023

2. The Case for S2: The Potential Benefits of the S2 Subunit of the SARS-CoV-2 Spike Protein as an Immunogen in Fighting the COVID-19 Pandemic

Author

Priyanka Shah, Gabriela A. Canziani, Erik P. Carter, and Irwin Chaiken

Subjects

SARS-CoV-2, S2 subunit, COVID-19, coronavirus, spike protein, antibodies, Immunologic diseases. Allergy, RC581-607

Abstract

As COVID-19 cases continue to rise, it is imperative to learn more about antibodies and T-cells produced against the causative virus, SARS-CoV-2, in order to guide the rapid development of therapies and vaccines. While much of the current antibody and vaccine research focuses on the receptor-binding domain of S1, a less-recognized opportunity is to harness the potential benefits of the more conserved S2 subunit. Similarities between the spike proteins of both SARS-CoV-2 and HIV-1 warrant exploring S2. Possible benefits of employing S2 in therapies and vaccines include the structural conservation of S2, extant cross-reactive neutralizing antibodies in populations (due to prior exposure to common cold coronaviruses), the steric neutralization potential of antibodies against S2, and the stronger memory B-cell and T-cell responses. More research is necessary on the effect of glycans on the accessibility and stability of S2, SARS-CoV-2 mutants that may affect infectivity, the neutralization potential of antibodies produced by memory B-cells, cross-reactive T-cell responses, antibody-dependent enhancement, and antigen competition. This perspective aims to highlight the evidence for the potential advantages of using S2 as a target of therapy or vaccine design.

Published

2021

3. The HIV-1 Env gp120 Inner Domain Shapes the Phe43 Cavity and the CD4 Binding Site

Author

Jérémie Prévost, William D. Tolbert, Halima Medjahed, Rebekah T. Sherburn, Navid Madani, Daria Zoubchenok, Gabrielle Gendron-Lepage, Althea E. Gaffney, Melissa C. Grenier, Sharon Kirk, Natasha Vergara, Changze Han, Brendan T. Mann, Agnès L. Chénine, Adel Ahmed, Irwin Chaiken, Frank Kirchhoff, Beatrice H. Hahn, Hillel Haim, Cameron F. Abrams, Amos B. Smith, Joseph Sodroski, Marzena Pazgier, and Andrés Finzi

Subjects

Env, gp120, CD4, CD4mc, CRF01_AE, ADCC, Microbiology, QR1-502

Abstract

ABSTRACT The HIV-1 envelope glycoproteins (Env) undergo conformational changes upon interaction of the gp120 exterior glycoprotein with the CD4 receptor. The gp120 inner domain topological layers facilitate the transition of Env to the CD4-bound conformation. CD4 engages gp120 by introducing its phenylalanine 43 (Phe43) in a cavity (“the Phe43 cavity”) located at the interface between the inner and outer gp120 domains. Small CD4-mimetic compounds (CD4mc) can bind within the Phe43 cavity and trigger conformational changes similar to those induced by CD4. Crystal structures of CD4mc in complex with a modified CRF01_AE gp120 core revealed the importance of these gp120 inner domain layers in stabilizing the Phe43 cavity and shaping the CD4 binding site. Our studies reveal a complex interplay between the gp120 inner domain and the Phe43 cavity and generate useful information for the development of more-potent CD4mc. IMPORTANCE The Phe43 cavity of HIV-1 envelope glycoproteins (Env) is an attractive druggable target. New promising compounds, including small CD4 mimetics (CD4mc), were shown to insert deeply into this cavity. Here, we identify a new network of residues that helps to shape this highly conserved CD4 binding pocket and characterize the structural determinants responsible for Env sensitivity to small CD4 mimetics.

Published

2020

4. Click Chemistry in Peptide-Based Drug Design

Author

Irwin Chaiken, Rachna Aneja, and Huiyuan Li

Subjects

click chemistry, triazoles, application, peptides, drug discovery, Organic chemistry, QD241-441

Abstract

Click chemistry is an efficient and chemoselective synthetic method for coupling molecular fragments under mild reaction conditions. Since the advent in 2001 of methods to improve stereochemical conservation, the click chemistry approach has been broadly used to construct diverse chemotypes in both chemical and biological fields. In this review, we discuss the application of click chemistry in peptide-based drug design. We highlight how triazoles formed by click reactions have been used for mimicking peptide and disulfide bonds, building secondary structural components of peptides, linking functional groups together, and bioconjugation. The progress made in this field opens the way for synthetic approaches to convert peptides with promising functional leads into structure-minimized and more stable forms.

Published

2013

5. Pharmacophore Variants of the Macrocyclic Peptide Triazole Inactivator of HIV-1 Env

Author

Monisha Gupta, Gabriela Canziani, Charles Gotuaco Ang, Mohammadjavad Mohammadi, Cameron F. Abrams, Derek Yang, III Amos B. Smith, and Irwin Chaiken

Abstract

Previously we established a family of macrocyclic peptide triazoles (cPTs) that inactivate the Env protein complex of HIV-1, and identified the pharmacophore that engages Env’s receptor binding pocket. Here, we examined the hypothesis that the side chains of both components of the triazole Pro - Trp segment of cPT pharmacophore work in tandem to make intimate contacts with two proximal subsites of the overall CD4 binding site of gp120 to stabilize binding and function. Variations of the triazole Pro R group, which previously had been significantly optimized, led to identification of a variant MG-II-20 that contains a pyrazole substitution. MG-II-20 has improved functional properties over previously examined variants, with Kd for gp120 in the nM range. In contrast, new variants of the Trp indole side chain, with either methyl- or bromo- components appended, had disruptive effects on gp120 binding, reflecting the sensitivity of function to changes in this component of the encounter complex. Plausible in silico models of cPT:gp120 complex structures were obtained that are consistent with the overall hypothesisof occupancy by the triazole Pro and Trp side chains, respectively, into the β20/21 and Phe43 sub-cavities. The overall results strengthen the definition of the cPT-Env inactivator binding site and provide a new lead composition (MG-II-20) as well as structure-function findings to guide future HIV-1 Env inactivator design.

Published

2023

6. Irreversible Inactivation of SARS-CoV-2 by Lectin Engagement with Two Glycan Clusters on the Spike Protein

Author

Aakansha Nangarlia, Farah Fazloon Hassen, Gabriela Canziani, Praneeta Bandi, Choya Talukder, Fengwen Zhang, Douglas Krauth, Ebony Gary, David Weiner, Paul Bieniasz, Sonia Navas-Martin, Barry O'Keefe, Charles Ang, and Irwin Chaiken

Abstract

Host cell infection by SARS-CoV-2, similar to that by HIV-1, is driven by a conformationally metastable and highly glycosylated surface entry protein complex, and infection by these viruses has been shown to be inhibited by the mannose-specific lectins Cyanovirin-N (CV-N) and Griffithsin (GRFT). We discovered in this study that CV-N and His6-tagged GRFT not only inhibit SARS-CoV-2 infection but also lead to irreversibly inactivated pseudovirus particles. The irreversibility effect was revealed by the observation that pseudoviruses first treated with either CV-N or GRFT and then washed to remove all soluble lectin did not recover infectivity. Infection inhibition of SARS-CoV-2 pseudovirus mutants with single-site glycan mutations in Spike suggested that two glycan clusters in S1 are important for both CV-N and GRFT inhibition, one cluster associated with the RBD (receptor binding domain) and the second with the S1/S2 cleavage site. We observed lectin antiviral effects with several SARS-CoV-2 pseudovirus variants, including the recently emerged omicron, as well as a fully infectious coronavirus, therein reflecting the breadth of lectin antiviral function and the potential for pan-coronavirus inactivation. Mechanistically, observations made in this work indicate that multivalent lectin interaction with S1 glycans is likely a driver of the lectin infection inhibition and irreversible inactivation effect and suggest the possibility that lectin inactivation is caused by an irreversible conformational effect on Spike. Overall, lectins' irreversible inactivation of SARS-CoV-2, taken with their breadth of function, reflects the therapeutic potential of multivalent lectins targeting the vulnerable metastable Spike before host cell encounter.

Published

2023

7. Anti‐S2 Protection in COVID‐19 Infection and SARS‐CoV‐2 Spike Vaccination

Author

Gabriela A. Canziani, Jackie Tang, Aakansha Nangarlia, Shiyu Zhang, Farah Fazloon‐Hassen, Choya Taludker, Jennifer Connors, Gina Cusimano, Mariana Bernui, Matt Bell, Michele Kutzler, Elias Haddad, Charles Cairns, and Irwin Chaiken

Subjects

Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2022

8. Identification of a glycan cluster in gp120 essential for irreversible HIV-1 lytic inactivation by a lectin-based recombinantly engineered protein conjugate

Author

Alexej Dick, Brendon Ngo, Aakansha Nangarlia, Bijay Parajuli, Irwin Chaiken, Shiyu Zhang, Kriti Acharya, Bibek Parajuli, and Cameron F. Abrams

Subjects

Glycan, Glycosylation, viruses, Calorimetry, HIV Envelope Protein gp120, Gp41, Biochemistry, Epitope, law.invention, Protein–protein interaction, Epitopes, 03 medical and health sciences, law, Lectins, Protein trimer, Humans, Binding site, Molecular Biology, 030304 developmental biology, 0303 health sciences, biology, Chemistry, 030302 biochemistry & molecular biology, Gene Products, env, virus diseases, Cell Biology, Surface Plasmon Resonance, Cell biology, Lytic cycle, HIV-1, biology.protein, Recombinant DNA, Protein Binding

Abstract

We previously discovered a class of recombinant lectin conjugates, denoted lectin DLIs (‘dual-acting lytic inhibitors’) that bind to the HIV-1 envelope (Env) protein trimer and cause both lytic inactivation of HIV-1 virions and cytotoxicity of Env-expressing cells. To facilitate mechanistic investigation of DLI function, we derived the simplified prototype microvirin (MVN)-DLI, containing an MVN domain that binds high-mannose glycans in Env, connected to a DKWASLWNW sequence (denoted ‘Trp3’) derived from the membrane-associated region of gp41. The relatively much stronger affinity of the lectin component than Trp3 argues that the lectin functions to capture Env to enable Trp3 engagement and consequent Env membrane disruption and virolysis. The relatively simplified engagement pattern of MVN with Env opened up the opportunity, pursued here, to use recombinant glycan knockout gp120 variants to identify the precise Env binding site for MVN that drives DLI engagement and lysis. Using mutagenesis combined with a series of biophysical and virological experiments, we identified a restricted set of residues, N262, N332 and N448, all localized in a cluster on the outer domain of gp120, as the essential epitope for MVN binding. By generating these mutations in the corresponding HIV-1 virus, we established that the engagement of this glycan cluster with the lectin domain of MVN*-DLI is the trigger for DLI-derived virus and cell inactivation. Beyond defining the initial encounter step for lytic inactivation, this study provides a guide to further elucidate DLI mechanism, including the stoichiometry of Env trimer required for function, and downstream DLI optimization.

Published

2020

9. The Case for S2: The Potential Benefits of the S2 Subunit of the SARS-CoV-2 Spike Protein as an Immunogen in Fighting the COVID-19 Pandemic

Author

Gabriela A. Canziani, Erik P Carter, Priyanka Shah, and Irwin Chaiken

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, COVID-19 Vaccines, Immunogen, T-Lymphocytes, Protein subunit, Immunology, coronavirus, Cross Reactions, Antibodies, Viral, medicine.disease_cause, spike protein, Virus, Neutralization, Epitope, Epitopes, 03 medical and health sciences, S2 subunit, Immunogenicity, Vaccine, 0302 clinical medicine, Antibody Specificity, Immunity, SARS-CoV-2 vaccine, medicine, Animals, Humans, Immunology and Allergy, antibodies, Coronavirus, biology, SARS-CoV-2, COVID-19, immunity, Antibodies, Neutralizing, Virology, Protein Subunits, 030104 developmental biology, Perspective, Host-Pathogen Interactions, Spike Glycoprotein, Coronavirus, Vaccines, Subunit, biology.protein, Antibody, lcsh:RC581-607, 030217 neurology & neurosurgery

Abstract

As COVID-19 cases continue to rise, it is imperative to learn more about antibodies and T-cells produced against the causative virus, SARS-CoV-2, in order to guide the rapid development of therapies and vaccines. While much of the current antibody and vaccine research focuses on the receptor-binding domain of S1, a less-recognized opportunity is to harness the potential benefits of the more conserved S2 subunit. Similarities between the spike proteins of both SARS-CoV-2 and HIV-1 warrant exploring S2. Possible benefits of employing S2 in therapies and vaccines include the structural conservation of S2, extant cross-reactive neutralizing antibodies in populations (due to prior exposure to common cold coronaviruses), the steric neutralization potential of antibodies against S2, and the stronger memory B-cell and T-cell responses. More research is necessary on the effect of glycans on the accessibility and stability of S2, SARS-CoV-2 mutants that may affect infectivity, the neutralization potential of antibodies produced by memory B-cells, cross-reactive T-cell responses, antibody-dependent enhancement, and antigen competition. This perspective aims to highlight the evidence for the potential advantages of using S2 as a target of therapy or vaccine design.

Published

2021

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

Author

Althea Gaffney, Aakansha Nangarlia, Adel Ahmed Rashad Ahmed, Cameron F. Abrams, Steven T. Gossert, Alamgir Hossain, Amos B. Smith, Irwin Chaiken, and Charles G. Ang

Subjects

0301 basic medicine, Membrane permeability, Protein subunit, viruses, Peptide, HIV Envelope Protein gp120, Gp41, 01 natural sciences, Biochemistry, Article, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, Cytotoxic T cell, Bifunctional, Cytotoxicity, chemistry.chemical_classification, Cell Death, 010405 organic chemistry, Chemistry, virus diseases, General Medicine, HIV Envelope Protein gp41, 0104 chemical sciences, 030104 developmental biology, Cell killing, Biophysics, HIV-1, Molecular Medicine, Peptides

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

11. Altered Env conformational dynamics as a mechanism of resistance to peptide‑triazole HIV‑1 inactivators

Author

Gabriela A. Canziani, Irwin Chaiken, Lucía Enríquez Rodríguez, Michael J. Root, Adel A. Rashad, Shiyu Zhang, Alexej Dick, and Andrew P. Holmes

Subjects

Anti-HIV Agents, Protein Conformation, viruses, Mutant, HIV Infections, Peptide, Gp120 shedding, HIV Envelope Protein gp120, Recombinant virus, medicine.disease_cause, Conformational dynamics, Protein structure, Resistance mechanism, Viral entry, Virology, Drug Resistance, Viral, medicine, Humans, Binding site, Envelope glycoproteins, chemistry.chemical_classification, Mutation, Binding Sites, Chemistry, Research, Triazoles, Virus Internalization, RC581-607, Isothermal titration calorimetry (ITC), Entry inhibitor, gp120 shedding, Macrocyclic peptide, Molecular Docking Simulation, Infectious Diseases, Surface plasmon resonance (SPR), Biophysics, HIV-1, Immunologic diseases. Allergy, Peptides, Virus escape, medicine.drug

Abstract

Background We previously developed drug-like peptide triazoles (PTs) that target HIV-1 Envelope (Env) gp120, potently inhibit viral entry, and irreversibly inactivate virions. Here, we investigated potential mechanisms of viral escape from this promising class of HIV-1 entry inhibitors. Results HIV-1 resistance to cyclic (AAR029b) and linear (KR13) PTs was obtained by dose escalation in viral passaging experiments. High-level resistance for both inhibitors developed slowly (relative to escape from gp41-targeted C-peptide inhibitor C37) by acquiring mutations in gp120 both within (Val255) and distant to (Ser143) the putative PT binding site. The similarity in the resistance profiles for AAR029b and KR13 suggests that the shared IXW pharmacophore provided the primary pressure for HIV-1 escape. In single-round infectivity studies employing recombinant virus, V255I/S143N double escape mutants reduced PT antiviral potency by 150- to 3900-fold. Curiously, the combined mutations had a much smaller impact on PT binding affinity for monomeric gp120 (four to ninefold). This binding disruption was entirely due to the V255I mutation, which generated few steric clashes with PT in molecular docking. However, this minor effect on PT affinity belied large, offsetting changes to association enthalpy and entropy. The escape mutations had negligible effect on CD4 binding and utilization during entry, but significantly altered both binding thermodynamics and inhibitory potency of the conformationally-specific, anti-CD4i antibody 17b. Moreover, the escape mutations substantially decreased gp120 shedding induced by either soluble CD4 or AAR029b. Conclusions Together, the data suggest that the escape mutations significantly modified the energetic landscape of Env’s prefusogenic state, altering conformational dynamics to hinder PT-induced irreversible inactivation of Env. This work therein reveals a unique mode of virus escape for HIV-1, namely, resistance by altering the intrinsic conformational dynamics of the Env trimer.

Published

2021

12. Roles of variable linker length in dual acting virucidal entry inhibitors on HIV-1 potency via on-the-fly free energy molecular simulations

Author

Irwin Chaiken, Cameron F. Abrams, Bibek Parajuli, and Steven T. Gossert

Subjects

Glycan, Recombinant Fusion Proteins, Molecular Dynamics Simulation, Gp41, Biochemistry, law.invention, 03 medical and health sciences, Structure-Activity Relationship, Glycoprotein complex, law, Lectins, Molecular Biology, 030304 developmental biology, 0303 health sciences, biology, Chemistry, 030302 biochemistry & molecular biology, Lectin, Fusion protein, HIV Envelope Protein gp41, Docking (molecular), For the Record, Biophysics, biology.protein, Recombinant DNA, HIV-1, Linker

Abstract

The Dual‐Acting Virolytic Entry Inhibitors, or DAVEI's, are a class of recombinant chimera fusion proteins consisting of a lectin, a flexible polypeptide linker, and a fragment of the membrane‐proximal external region (MPER) of HIV‐1 gp41. DAVEIs trigger virolysis of HIV‐1 virions through interactions with the trimeric envelope glycoprotein complex (Env), though the details of these interactions are not fully determined as yet. The purpose of this work was to use structural modeling to rationalize a dependence of DAVEI potency on the molecular length of the linker connecting the two components. We used temperature accelerated molecular dynamics and on‐the‐fly parameterization to compute free energy versus end‐to‐end distance for two different linker lengths, DAVEI L0 (His(6)) and DAVEI L2 ([Gly(4)Ser](2)His(6)). Additionally, an envelope model was created based on a cryo‐electron microscopy‐derived structure of a cleaved, soluble Env construct, with high‐mannose glycans added which served as putative docking locations for the lectin, along with MPER added that served as a putative docking location for the MPER region of DAVEI (MPER(DAVEI)). Using MD simulation, distances between the lectin C‐terminus and Env gp41 MPER were measured. We determined that none of the glycans were close enough to gp41 MPER to allow DAVEI L0 to function, while one, N448, will allow DAVEI L2 to function. These findings are consistent with the previously determined dependence of lytic function on DAVEI linker lengths. This supports the hypothesis that DAVEI's engage Env at both glycans and the Env MPER in causing membrane poration and lysis.

Published

2020

13. The HIV-1 Env gp120 Inner Domain Shapes the Phe43 Cavity and the CD4 Binding Site

Author

Changze Han, Agnès L. Chenine, Sharon Kirk, Rebekah Sherburn, Adel Ahmed Rashad Ahmed, Marzena Pazgier, Cameron F. Abrams, Amos B. Smith, Jérémie Prévost, William D. Tolbert, Navid Madani, Natasha Gupta Vergara, Brendan Mann, Irwin Chaiken, Gabrielle Gendron-Lepage, Andrés Finzi, Frank Kirchhoff, Halima Medjahed, Hillel Haim, Daria Zoubchenok, Melissa C. Grenier, Althea Gaffney, Beatrice H. Hahn, and Joseph Sodroski

Subjects

CD4-Positive T-Lymphocytes, viruses, Human immunodeficiency virus (HIV), Druggability, CD4 mimetic, HIV Envelope Protein gp120, medicine.disease_cause, Insert (molecular biology), Biomimetics, CRF01_AE, CD4mc, chemistry.chemical_classification, 0303 health sciences, Thymocytes, Chemistry, virus diseases, QR1-502, 3. Good health, Phe43 cavity, Domain (ring theory), CD4 Antigens, ADCC, Crystallization, Research Article, Protein Binding, Env, Phenylalanine, Binding pocket, Microbiology, CD4 binding site, Host-Microbe Biology, Cell Line, 03 medical and health sciences, Dogs, Protein Domains, Virology, medicine, Animals, Humans, Binding site, 030304 developmental biology, Binding Sites, 030306 microbiology, neutralization, CD4, gp120, HEK293 Cells, Biophysics, HIV-1, Glycoprotein

Abstract

The Phe43 cavity of HIV-1 envelope glycoproteins (Env) is an attractive druggable target. New promising compounds, including small CD4 mimetics (CD4mc), were shown to insert deeply into this cavity. Here, we identify a new network of residues that helps to shape this highly conserved CD4 binding pocket and characterize the structural determinants responsible for Env sensitivity to small CD4 mimetics., The HIV-1 envelope glycoproteins (Env) undergo conformational changes upon interaction of the gp120 exterior glycoprotein with the CD4 receptor. The gp120 inner domain topological layers facilitate the transition of Env to the CD4-bound conformation. CD4 engages gp120 by introducing its phenylalanine 43 (Phe43) in a cavity (“the Phe43 cavity”) located at the interface between the inner and outer gp120 domains. Small CD4-mimetic compounds (CD4mc) can bind within the Phe43 cavity and trigger conformational changes similar to those induced by CD4. Crystal structures of CD4mc in complex with a modified CRF01_AE gp120 core revealed the importance of these gp120 inner domain layers in stabilizing the Phe43 cavity and shaping the CD4 binding site. Our studies reveal a complex interplay between the gp120 inner domain and the Phe43 cavity and generate useful information for the development of more-potent CD4mc.

Published

2020

14. Metastable HIV-1 Surface Protein Env Sensitizes Cell Membranes to Transformation and Poration by Dual-Acting Virucidal Entry Inhibitors

Author

Adel A. Rashad, Cameron F. Abrams, Marg Rajpara, Michele A. Kutzler, Md. Alamgir Hossain, Kriti Acharya, Charles G. Ang, Irwin Chaiken, Harry Bach, and Alexej Dick

Subjects

viruses, Cell, Biochemistry, Mannose-Binding Lectin, Protein Structure, Secondary, Article, Flow cytometry, chemistry.chemical_compound, Bacterial Proteins, HIV Fusion Inhibitors, medicine, Humans, Viability assay, Amino Acid Sequence, Cytotoxicity, medicine.diagnostic_test, Protein Stability, HEK 293 cells, Cell Membrane, env Gene Products, Human Immunodeficiency Virus, virus diseases, Transfection, Virus Internalization, Transmembrane protein, Cell biology, Calcein, medicine.anatomical_structure, HEK293 Cells, chemistry

Abstract

Dual-acting virucidal entry inhibitors (DAVEIs) have previously been shown to cause irreversible inactivation of HIV-1 Env-presenting pseudovirus by lytic membrane transformation. This study examined whether this transformation could be generalized to include membranes of Env-presenting cells. Flow cytometry was used to analyze HEK293T cells transiently transfected with increasing amounts of DNA encoding JRFL Env, loaded with calcein dye, and treated with serial dilutions of microvirin (Q831K/M83R)-DAVEI. Comparing calcein retention against intact Env expression (via Ab 35O22) on individual cells revealed effects proportional to Env expression. "Low-Env" cells experienced transient poration and calcein leakage, while "high-Env" cells were killed. The cell-killing effect was confirmed with an independent mitochondrial activity-based cell viability assay, showing dose-dependent cytotoxicity in response to DAVEI treatment. Transfection with increasing quantities of Env DNA showed further shifts toward "High-Env" expression and cytotoxicity, further reinforcing the Env dependence of the observed effect. Controls with unlinked DAVEI components showed no effect on calcein leakage or cell viability, confirming a requirement for covalently linked DAVEI compounds to achieve Env transformation. These data demonstrate that the metastability of Env is an intrinsic property of the transmembrane protein complex and can be perturbed to cause membrane disruption in both virus and cell contexts.

Published

2020

15. Peptide Triazole Thiol Irreversibly Inactivates Metastable HIV-1 Env by Accessing Conformational Triggers Intrinsic to Virus–Cell Entry

Author

Ann Haftl, Irwin Chaiken, Cameron F. Abrams, Shiyu Zhang, Charles G. Ang, Michele A. Kutzler, Erik P Carter, and Adel A. Rashad

Subjects

Env, entry inhibition, 0301 basic medicine, Microbiology (medical), membrane poration, Lysis, QH301-705.5, 030106 microbiology, Mutant, Peptide, Microbiology, Article, Flow cytometry, metastability, Turn (biochemistry), 03 medical and health sciences, chemistry.chemical_compound, Virology, medicine, peptide triazole, Biology (General), chemistry.chemical_classification, medicine.diagnostic_test, flow cytometry, HEK 293 cells, Transfection, 6-helix bundle, MPER, Calcein, 030104 developmental biology, chemistry, HIV-1, Biophysics

Abstract

KR13, a peptide triazole thiol previously established to inhibit HIV-1 infection and cause virus lysis, was evaluated by flow cytometry against JRFL Env-presenting cells to characterize induced Env and membrane transformations leading to irreversible inactivation. Transiently transfected HEK293T cells were preloaded with calcein dye, treated with KR13 or its thiol-blocked analogue KR13b, fixed, and stained for gp120 (35O22), MPER (10E8), 6-helix-bundle (NC-1), immunodominant loop (50-69), and fusion peptide (VRC34.01). KR13 induced dose-dependent transformations of Env and membrane characterized by transient poration, MPER exposure, and 6-helix-bundle formation (analogous to native fusion events), but also reduced immunodominant loop and fusion peptide exposure. Using a fusion peptide mutant (V504E), we found that KR13 transformation does not require functional fusion peptide for poration. In contrast, simultaneous treatment with fusion inhibitor T20 alongside KR13 prevented membrane poration and MPER exposure, showing that these events require 6-helix-bundle formation. Based on these results, we formulated a model for PTT-induced Env transformation portraying how, in the absence of CD4/co-receptor signaling, PTT may provide alternate means of perturbing the metastable Env-membrane complex, and inducing fusion-like transformation. In turn, the results show that such transformations are intrinsic to Env and can be diverted for irreversible inactivation of the protein complex.

Published

2021

16. Recognition of HIV-inactivating peptide triazoles by the recombinant soluble Env trimer, BG505 SOSIP.664

Author

Kriti Acharya, Francesca Moraca, Adel A. Rashad, Per Johan Klasse, Irwin Chaiken, Cameron F. Abrams, and John P. Moore

Subjects

0301 basic medicine, chemistry.chemical_classification, 010405 organic chemistry, viruses, Protein subunit, virus diseases, Peptide, Trimer, 01 natural sciences, Biochemistry, Virus, 0104 chemical sciences, law.invention, 03 medical and health sciences, 030104 developmental biology, chemistry, Structural Biology, law, Recombinant DNA, Biophysics, Pharmacophore, Receptor, Molecular Biology, Binding selectivity

Abstract

Peptide triazole (PT) antagonists interact with gp120 subunits of HIV-1 Env trimers to block host cell receptor interactions, trigger gp120 shedding, irreversibly inactivate virus and inhibit infection. Despite these enticing functions, understanding the structural mechanism of PT-Env trimer encounter has been limited. In this work, we combined competition interaction analysis and computational simulation to demonstrate PT binding to the recombinant soluble trimer, BG505 SOSIP.664, a stable variant that resembles native virus spikes in binding to CD4 receptor as well as known conformationally-dependent Env antibodies. Binding specificity and computational modeling fit with encounter through complementary PT pharmacophore Ile-triazolePro-Trp interaction with a 2-subsite cavity in the Env gp120 subunit of SOSIP trimer similar to that in monomeric gp120. These findings argue that PTs are able to recognize and bind a closed prefusion state of Env trimer upon HIV-1 encounter. The results provide a structural model of how PTs exert their function on virion trimeric spike protein and a platform to inform future antagonist design. Proteins 2017; 85:843-851. © 2016 Wiley Periodicals, Inc.

Published

2017

17. Chemical optimization of macrocyclic HIV-1 inactivators for improving potency and increasing the structural diversity at the triazole ring

Author

Alexej Dick, Ann Haftl, Kriti Acharya, Irwin Chaiken, Adel A. Rashad, Andrew P. Holmes, and Rachna Aneja

Subjects

0301 basic medicine, Macrocyclic Compounds, Anti-HIV Agents, Stereochemistry, Triazole, Microbial Sensitivity Tests, HIV Envelope Protein gp120, Ring (chemistry), Biochemistry, Article, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Moiety, Physical and Theoretical Chemistry, Methylene, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, Drug discovery, Organic Chemistry, Aromaticity, Triazoles, Cyclic peptide, 030104 developmental biology, chemistry, HIV-1, Pharmacophore

Abstract

HIV-1 entry inhibition remains an urgent need for AIDS drug discovery and development. We previously reported the discovery of cyclic peptide triazoles (cPTs) that retain the HIV-1 irreversible inactivation functions of the parent linear peptides (PTs) and have massively increased proteolytic resistance. Here, in an initial structure-activity relationship investigation, we evaluated the effects of variations in key structural and functional components of the cPT scaffold in order to produce a platform for developing next-generation cPTs. Some structural elements, including stereochemistry around the cyclization residues and Ile and Trp side chains in the gp120-binding pharmacophore, exhibited relatively low tolerance for change, reflecting the importance of these components for function. In contrast, in the pharmacophore-central triazole position, the ferrocene moiety could be successfully replaced with smaller aromatic rings, where a p-methyl-phenyl methylene moiety gave cPT 24 with an IC50 value of 180 nM. Based on the observed activity of the biphenyl moiety when installed on the triazole ring (cPT 23, IC50 ∼ 269 nM), we further developed a new on-resin synthetic method to easily access the bi-aryl system during cPT synthesis, in good yields. A thiophene-containing cPT AAR029N2 (36) showed enhanced entropically favored binding to Env gp120 and improved antiviral activity (IC50 ∼ 100 nM) compared to the ferrocene-containing analogue. This study thus provides a crucial expansion of chemical space in the pharmacophore to use as a starting point, along with other allowable structural changes, to guide future optimization and minimization for this important class of HIV-1 killing agents.

Published

2017

18. Irreversible HIV-1 Inactivation Employing a Small Molecule Dual-Action Virolytic Entry Inhibitor Strategy

Author

Aakansha Nangarlia, Cameron F. Abrams, Adel A. Rashad, Irwin Chaiken, Amos B. Smith, Steven T. Gossert, Alamgir Hossain, and Althea Gaffney

Subjects

chemistry.chemical_classification, Lysis, viruses, virus diseases, Peptide, Gp41, Small molecule, Entry inhibitor, chemistry, Lytic cycle, Covalent bond, Biophysics, medicine, Glycoprotein, medicine.drug

Abstract

The design, synthesis and validation of a family of small molecule “Dual-Action Virucidal EntryInhibitors” (DAVEIs) has been achieved that result in irreversible lytic inactivation of HIV-1 virions. These constructs contained two functional components that endow the capacity to bindsimultaneously to both the gp120 and gp41 subunits of the HIV-1 Envelope glycoprotein (Env). One component is derived from BNM-III-170, a small molecule CD4 mimic warhead that binds togp120. The second component, a Trp3 peptide, is a 9-amino acid segment based on the gp41 Membrane Proximal External Region (MPER) that has been proposed to bind to the gp41 MPERdomain of the Env. The resulting smDAVEIs both inhibit infection with low micromolar potency and induce lysis of the HIV-1 virion. The lytic activity was selective for functional HIV-1 virions. Crucially, virolysis was found to be dependent on covalent tethering of the BNM-III-170 and Trp3 domains with various spacers, as coadministration of the un-crosslinked components proved not to be lytic. Computational modeling supports a mechanism in which DAVEIs bind to open-state Env trimers and induce relative motion of gp120 subunits that further opens the trimers. Overall, this work represents a promising new step toward the use of small-molecule DAVEIs for eradication of HIV.

Published

2019

19. Back Cover: Mechanical characterization of HIV-1 with a solid-state nanopore sensor

Author

Prashanta Dutta, Y. M. Nuwan D. Y. Bandara, Irwin Chaiken, Armin Darvish, Jungsuk Kim, Gaurav Goyal, Ramalingam Venkat Kalyana Sundaram, Bin Peng, Jung Soo Lee, Jugal Saharia, Min Jun Kim, and Chi Won Ahn

Subjects

Nanopore, Materials science, Clinical Biochemistry, Human immunodeficiency virus (HIV), medicine, Solid-state, Nanotechnology, Cover (algebra), medicine.disease_cause, Biochemistry, Analytical Chemistry, Characterization (materials science)

Published

2019

20. Pharmacokinetic Stability of Macrocyclic Peptide Triazole HIV-1 Inactivators Alone and in Liposomes

Author

Aakansha Nangarlia, Gianfranco Pasut, Rachna Aneja, Adel A. Rashad, Steven P. Wrenn, Antonella Grigoletto, Irwin Chaiken, and Jeffrey M. Jacobson

Subjects

Macrocyclic Compounds, Anti-HIV Agents, medicine.medical_treatment, Cell, Triazole, HIV-1, liposomes, macrocyclic peptide triazole, pharmacokinetic stability, Microbial Sensitivity Tests, Pharmacology, 010402 general chemistry, Cleavage (embryo), 01 natural sciences, Biochemistry, Article, chemistry.chemical_compound, Pharmacokinetics, Structural Biology, In vivo, Drug Discovery, medicine, Molecular Biology, Liposome, Protease, 010405 organic chemistry, Chemistry, Organic Chemistry, General Medicine, Triazoles, In vitro, 0104 chemical sciences, medicine.anatomical_structure, Liposomes, Molecular Medicine, Peptides

Abstract

Previously, we reported the discovery of macrocyclic peptide triazoles (cPTs) that bind to HIV-1 Env gp120, inhibit virus cell infection with nanomolar potencies, and cause irreversible virion inactivation. Given the appealing virus-killing activity of cPTs and resistance to protease cleavage observed in vitro, we here investigated in vivo pharmacokinetics of the cPT AAR029b. AAR029b was investigated both alone and encapsulated in a PEGylated liposome formulation that was designed to slowly release inhibitor. Pharmacokinetic analysis in rats showed that the half-life of FITC-AAR029b was substantial both alone and liposome-encapsulated, 2.92 and 8.87 hours, respectively. Importantly, liposome-encapsulated FITC-AAR029b exhibited a 15-fold reduced clearance rate from serum compared with the free FITC-cPT. This work thus demonstrated both the in vivo stability of cPT alone and the extent of pharmacokinetic enhancement via liposome encapsulation. The results obtained open the way to further develop cPTs as long-acting HIV-1 inactivators against HIV-1 infection.

Published

2019

21. 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

Bruno Melillo, Francesca Moraca, Amos B. Smith, Kriti Acharya, Cameron F. Abrams, and Irwin Chaiken

Subjects

0301 basic medicine, Stereochemistry, General Chemical Engineering, Protein subunit, In silico, HIV Infections, HIV Envelope Protein gp120, Molecular Dynamics Simulation, Library and Information Sciences, Biology, Ligands, 01 natural sciences, Article, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, Molecular dynamics, Drug Discovery, Humans, Binding site, env Gene Products, Human Immunodeficiency Virus, General Chemistry, Interaction energy, Small molecule, 0104 chemical sciences, Computer Science Applications, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, 030104 developmental biology, Monomer, chemistry, Docking (molecular), CD4 Antigens, HIV-1

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 IC50’s measured in CD4 binding competition ELISA and with KD’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

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

Author

Huiyuan Li, Irwin Chaiken, Lauren D. Bailey, Ramalingam Venkat Kalyana Sundaram, Adel A. Rashad, Arangassery Rosemary Bastian, Karl Weiss, James Huynh, Steven P. Wrenn, Rachna Aneja, Elisabeth S. Papazoglou, and Cameron F. Abrams

Subjects

0301 basic medicine, Lysis, Membrane Fluidity, viruses, Membrane lipids, Cell, HIV Core Protein p24, Beta-Cyclodextrins, HIV Envelope Protein gp120, Biology, Biochemistry, Article, Membrane Lipids, 03 medical and health sciences, chemistry.chemical_compound, Cell Line, Tumor, medicine, Membrane fluidity, Humans, Sulfhydryl Compounds, 030102 biochemistry & molecular biology, Cholesterol, beta-Cyclodextrins, Triazoles, Cell biology, Thiazoles, 030104 developmental biology, Membrane, medicine.anatomical_structure, Lytic cycle, chemistry, HIV-1, lipids (amino acids, peptides, and proteins), Peptides

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

23. Mechanical characterization of HIV-1 with a solid-state nanopore sensor

Author

Gaurav Goyal, Irwin Chaiken, Jung Soo Lee, Y. M. Nuwan D. Y. Bandara, Ramalingam Venkat Kalyana Sundaram, Min Jun Kim, Jugal Saharia, Armin Darvish, Prashanta Dutta, Chi Won Ahn, Jungsuk Kim, and Bin Peng

Subjects

viruses, Clinical Biochemistry, 02 engineering and technology, 01 natural sciences, Biochemistry, Virus, Article, Analytical Chemistry, Membrane Lipids, Nanopores, Viral envelope, Infectivity, Fusion, Chemistry, 010401 analytical chemistry, Virion, Electrochemical Techniques, Viral membrane, 021001 nanoscience & nanotechnology, 0104 chemical sciences, Biomechanical Phenomena, Nanopore, Membrane, Cholesterol, Membrane protein, Biophysics, HIV-1, 0210 nano-technology

Abstract

Enveloped viruses fuse with cells to transfer their genetic materials and infect the host cell. Fusion requires deformation of both viral and cellular membranes. Since the rigidity of viral membrane is a key factor in their infectivity, studying the rigidity of viral particles is of great significance in understating viral infection. In this paper, a nanopore is used as a single molecule sensor to characterize the deformation of pseudo-type human immunodeficiency virus type 1 at sub-micron scale. Non-infective immature viruses were found to be more rigid than infective mature viruses. In addition, the effects of cholesterol and membrane proteins on the mechanical properties of mature viruses were investigated by chemically modifying the membranes. Furthermore, the deformability of single virus particles was analyzed through a recapturing technique, where the same virus was analyzed twice. The findings demonstrate the ability of nanopore resistive pulse sensing to characterize the deformation of a single virus as opposed to average ensemble measurements.

Published

2018

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

Author

Andrew P. Holmes, Li-Rui Song, Irwin Chaiken, Michele A. Kutzler, Xin Xie, Ebony N. Gary, Adel A. Rashad, Vanessa Pirrone, Kriti Acharya, Shiyu Zhang, Ya-Qiu Long, and Zhi-Long Wang

Subjects

0301 basic medicine, Models, Molecular, Receptors, CCR5, Anti-HIV Agents, Protein Conformation, Cell, Peptide, HIV Envelope Protein gp120, 01 natural sciences, Virus, Article, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, Chimera (genetics), Protein structure, Drug Discovery, medicine, Molecular Targeted Therapy, Receptor, Bifunctional, chemistry.chemical_classification, 010405 organic chemistry, Triazoles, Phenotype, 0104 chemical sciences, Cell biology, 030104 developmental biology, medicine.anatomical_structure, chemistry, Drug Design, HIV-1, Molecular Medicine

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

25. Roles of Conserved Tryptophans in Trimerization of HIV-1 Membrane-Proximal External Regions: Implications for Virucidal Design via Alchemical Free-Energy Molecular Simulations

Author

Steven T. Gossert, Bibek Parajuli, Irwin Chaiken, and Cameron F. Abrams

Subjects

0301 basic medicine, Models, Molecular, Mutant, Trimer, Protomer, 010402 general chemistry, Gp41, 01 natural sciences, Biochemistry, Article, Protein–protein interaction, 03 medical and health sciences, Molecular dynamics, Structural Biology, Molecular Biology, chemistry.chemical_classification, Tryptophan, virus diseases, Virus Internalization, HIV Envelope Protein gp41, 0104 chemical sciences, 030104 developmental biology, chemistry, Biophysics, HIV-1, Thermodynamics, Protein Multimerization, Glycoprotein, Linker

Abstract

The Dual-Action Virolytic Entry Inhibitors, or “DAVEI’s,” are a class of recombinant fusions of a lectin, a linker polypeptide, and a 15-residue fragment from the membrane-proximal external region (MPER) of HIV-1 gp41. DAVEI’s trigger rupture of HIV-1 virions, and the interaction site between DAVEI MPER and HIV-1 lies in the gp41 component of the envelope glycoprotein Env. Here we explore the hypothesis that DAVEI MPER engages Env gp41 in a mode structurally similar to a crystallographic MPER trimer. We used alchemical free-energy perturbation to assess the thermodynamic roles of each of the four conserved tryptophan residues on each protomer of MPER(3). We found that a W666A mutation had a large positive ΔΔG for all three protomers, while W672A had a large positive ΔΔG for only two of the three protomers, with the other tryptophans remaining unimportant contributors to MPER(3) stability. The protomer for which W672 is not important is unique in the placement of its W666 sidechain between the other two protomers. We show that the unique orientation of this W666 sidechain azimuthally rotates its protomer away from the orientation it would have if the trimer were symmetric, resulting in the diminished interaction of this W672 with the rest of MPER(3). Our findings are consistent with our previous experimental study of W-to-A mutants of DAVEI. This suggests that DAVEI MPER may engage HIV-1 Env to form a mixed trimer state in which one DAVEI MPER forms a trimer by displacing a more weakly interacting protomer of the endogenous Env MPER trimer.

Published

2018

26. Peptide triazole inactivators of HIV-1: how do they work and what is their potential?

Author

Irwin Chaiken and Adel A. Rashad

Subjects

Virus inactivation, Anti-HIV Agents, Stereochemistry, Peptidomimetic, Triazole, Human immunodeficiency virus (HIV), Peptide, HIV Envelope Protein gp120, Biology, medicine.disease_cause, Catalysis, Article, chemistry.chemical_compound, Drug Discovery, medicine, Humans, Pharmacology, Cell entry, chemistry.chemical_classification, Cycloaddition Reaction, Triazoles, Virus Internalization, chemistry, HIV-1, Molecular Medicine, Peptides, Copper

Published

2015

27. Macrocyclic Envelope Glycoprotein Antagonists that Irreversibly Inactivate HIV-1 before Host Cell Encounter

Author

Ramalingam Venkat Kalyana Sundaram, Adel A. Rashad, Caitlin Duffy, Rachna Aneja, and Irwin Chaiken

Subjects

Models, Molecular, Anti-HIV Agents, Protein Conformation, Peptidomimetic, viruses, Cell, HIV Envelope Protein gp120, Peptides, Cyclic, Article, Cell Line, Drug Discovery, medicine, Chymotrypsin, Humans, Trypsin, chemistry.chemical_classification, Oligopeptide, biology, Virion, Triazoles, Virus Internalization, Cyclic peptide, medicine.anatomical_structure, Biochemistry, chemistry, Cell culture, HIV-1, biology.protein, Molecular Medicine, Glycoprotein, Oligopeptides, medicine.drug

Abstract

We derived macrocyclic HIV-1 antagonists as a new class of peptidomimetic drug leads. Cyclic peptide triazoles (cPTs) retained the gp120 inhibitory and virus-inactivating signature of parent PTs, arguing that cyclization locked an active conformation. The 6-residue cPT 9 (AAR029b) exhibited sub-micromolar antiviral potencies in inhibiting cell infection and triggering gp120 shedding that causes irreversible virion inactivation. Importantly, cPTs were stable to trypsin and chymotrypsin, compared to substantial susceptibility of corresponding linear PTs.

Published

2015

28. Abasic Phosphorothioate Oligomers Inhibit HIV-1 Reverse Transcription and Block Virus Transmission across Polarized Ectocervical Organ Cultures

Author

Isaac Zentner, Sharon H. Anderson, Carol Lackman-Smith, Beth A. Snyder, Suhman Chung, Yvonne M. Mueller, Karissa Lozenski, Aidan S Hancock, Irwin Chaiken, Stuart F. J. LeGrice, Deena Ratner, Alina C. Boesteanu, Phalguni Gupta, Marie K. Mankowski, Jennifer L. Hope, Natalie M. Jones, Joseph A. Fraietta, Brian Wigdahl, and Peter D. Katsikis

Subjects

Male, Receptors, CXCR4, Receptors, CCR5, Protein Data Bank (RCSB PDB), Gene Expression, Phosphorothioate Oligonucleotides, Cervix Uteri, Biology, Antiviral Agents, Virus, Mice, Structure-Activity Relationship, Organ Culture Techniques, Immune system, In vivo, Viral entry, Animals, Humans, Structure–activity relationship, Pharmacology (medical), Pharmacology, Mucous Membrane, Deoxyribose, Epithelial Cells, Reverse Transcription, Virus Internalization, Virology, Reverse transcriptase, Mice, Inbred C57BL, Microbicides for sexually transmitted diseases, Infectious Diseases, Vagina, HIV-1, Sperm Motility, Reverse Transcriptase Inhibitors, Female

Abstract

In the absence of universally available antiretroviral (ARV) drugs or a vaccine against HIV-1, microbicides may offer the most immediate hope for controlling the AIDS pandemic. The most advanced and clinically effective microbicides are based on ARV agents that interfere with the earliest stages of HIV-1 replication. Our objective was to identify and characterize novel ARV-like inhibitors, as well as demonstrate their efficacy at blocking HIV-1 transmission. Abasic phosphorothioate 2′ deoxyribose backbone (PDB) oligomers were evaluated in a variety of mechanistic assays and for their ability to inhibit HIV-1 infection and virus transmission through primary human cervical mucosa. Cellular and biochemical assays were used to elucidate the antiviral mechanisms of action of PDB oligomers against both lab-adapted and primary CCR5- and CXCR4-utilizing HIV-1 strains, including a multidrug-resistant isolate. A polarized cervical organ culture was used to test the ability of PDB compounds to block HIV-1 transmission to primary immune cell populations across ectocervical tissue. The antiviral activity and mechanisms of action of PDB-based compounds were dependent on oligomer size, with smaller molecules preventing reverse transcription and larger oligomers blocking viral entry. Importantly, irrespective of molecular size, PDBs potently inhibited virus infection and transmission within genital tissue samples. Furthermore, the PDB inhibitors exhibited excellent toxicity and stability profiles and were found to be safe for vaginal application in vivo . These results, coupled with the previously reported intrinsic anti-inflammatory properties of PDBs, support further investigations in the development of PDB-based topical microbicides for preventing the global spread of HIV-1.

Published

2014

29. Targeting cell surface HIV-1 Env protein to suppress infectious virus formation

Author

Kantharaju Kamanna, Irwin Chaiken, Ramalingam Venkat Kalyana Sundaram, Charles G. Ang, Caitlin Duffy, Yu-Hung Huang, Karyn McFadden, Arangassery Rosemary Bastian, Farida Shaheen, and Lauren D. Bailey

Subjects

0301 basic medicine, Cancer Research, P24 capsid protein, viruses, CHO Cells, Biology, Gp41, Antiviral Agents, Virus, Article, 03 medical and health sciences, Cricetulus, Virology, Cytotoxic T cell, Animals, Humans, Viral shedding, Virus Assembly, HEK 293 cells, env Gene Products, Human Immunodeficiency Virus, virus diseases, Transfection, Triazoles, 030104 developmental biology, Infectious Diseases, HEK293 Cells, Capsid, biology.protein, HIV-1, Virus Inactivation, Peptides

Abstract

HIV-1 Env protein is essential for host cell entry, and targeting Env remains an important antiretroviral strategy. We previously found that a peptide triazole thiol KR13 and its gold nanoparticle conjugate AuNP-KR13 directly and irreversibly inactivate the virus by targeting the Env protein, leading to virus gp120 shedding, membrane disruption and p24 capsid protein release. Here, we examined the consequences of targeting cell-surface Env with the virus inactivators. We found that both agents led to formation of non-infectious virus from transiently transfected HEK293T cells. The budded non-infectious viruses lacked Env gp120 but contained gp41. Importantly, budded virions also retained the capsid protein p24, in stark contrast to p24 leakage from viruses directly treated by these agents and arguing that the agents led to deformed viruses by transforming the cells at a stage before virus budding. We found that the Env inactivators caused gp120 shedding from the transiently transfected HEK293T cells as well as non-producer CHO-K1-gp160 cells. Additionally, AuNP-KR13 was cytotoxic against the virus-producing HEK293T and CHO-K1-gp160 cells, but not untransfected HEK293T or unmodified CHO-K1 cells. The results obtained reinforce the argument that cell-surface HIV-1 Env is metastable, as on virus particles, and provides a conformationally vulnerable target for virus suppression and infectious cell inactivation.

Published

2017

30. Covalent Conjugation of a Peptide Triazole to HIV-1 gp120 Enables Intramolecular Binding Site Occupancy

Author

Andrew P. Holmes, Srivats Rajagopal, Caitlin Duffy, Cameron F. Abrams, Rachna Aneja, Ali Emileh, Irwin Chaiken, Arangassery Rosemary Bastian, Huiyuan Li, and Ferit Tuzer

Subjects

viruses, Mutant, Peptide, HIV Envelope Protein gp120, Molecular Dynamics Simulation, Biochemistry, Article, law.invention, Polyethylene Glycols, law, Viral entry, Biotinylation, Binding site, Receptor, chemistry.chemical_classification, Binding Sites, Chemistry, virus diseases, Antibodies, Monoclonal, Triazoles, 3. Good health, CD4 Antigens, Mutation, Recombinant DNA, Biophysics, HIV-1, Glycoprotein, Peptides

Abstract

The HIV-1 gp120 glycoprotein is the main viral surface protein responsible for initiation of the entry process and, as such, can be targeted for the development of entry inhibitors. We previously identified a class of broadly active peptide triazole (PT) dual antagonists that inhibit gp120 interactions at both its target receptor and coreceptor binding sites, induce shedding of gp120 from virus particles prior to host-cell encounter, and consequently can prevent viral entry and infection. However, our understanding of the conformational alterations in gp120 by which PT elicits its dual receptor antagonism and virus inactivation functions is limited. Here, we used a recently developed computational model of the PT-gp120 complex as a blueprint to design a covalently conjugated PT-gp120 recombinant protein. Initially, a single-cysteine gp120 mutant, E275CYU-2, was expressed and characterized. This variant retains excellent binding affinity for peptide triazoles, for sCD4 and other CD4 binding site (CD4bs) ligands, and for a CD4-induced (CD4i) ligand that binds the coreceptor recognition site. In parallel, we synthesized a PEGylated and biotinylated peptide triazole variant that retained gp120 binding activity. An N-terminally maleimido variant of this PEGylated PT, denoted AE21, was conjugated to E275C gp120 to produce the AE21-E275C covalent conjugate. Surface plasmon resonance interaction analysis revealed that the PT-gp120 conjugate exhibited suppressed binding of sCD4 and 17b to gp120, signatures of a PT-bound state of envelope protein. Similar to the noncovalent PT-gp120 complex, the covalent conjugate was able to bind the conformationally dependent mAb 2G12. The results argue that the PT-gp120 conjugate is structurally organized, with an intramolecular interaction between the PT and gp120 domains, and that this structured state embodies a conformationally entrapped gp120 with an altered bridging sheet but intact 2G12 epitope. The similarities of the PT-gp120 conjugate to the noncovalent PT-gp120 complex support the orientation of binding of PT to gp120 predicted in the molecular dynamics simulation model of the PT-gp120 noncovalent complex. The conformationally stabilized covalent conjugate can be used to expand the structural definition of the PT-induced "off" state of gp120, for example, by high-resolution structural analysis. Such structures could provide a guide for improving the subsequent structure-based design of inhibitors with the peptide triazole mode of action.

Published

2014

31. 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

Joseph Sodroski, Wayne A. Hendrickson, Amos B. Smith, Ernesto Freire, Joel R. Courter, Irwin Chaiken, Peter D. Kwong, Judith M. LaLonde, Navid Madani, and Arne Schön

Subjects

Anti-HIV Agents, Protein Conformation, Allosteric regulation, HIV Envelope Protein gp120, Gp41, Crystallography, X-Ray, Article, Small Molecule Libraries, Structure-Activity Relationship, Protein structure, Viral envelope, Viral entry, Structure–activity relationship, Humans, Chemistry, Molecular Mimicry, General Medicine, General Chemistry, Small molecule, 3. Good health, Cell biology, Crystallography, Drug Design, CD4 Antigens, Host-Pathogen Interactions, HIV-1

Abstract

Conspectus 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

32. A Model of Peptide Triazole Entry Inhibitor Binding to HIV-1 gp120 and the Mechanism of Bridging Sheet Disruption

Author

Carole A. Bewley, Cameron F. Abrams, Judith M. LaLonde, Ferit Tuzer, Diogo Rodrigo Magalhães Moreira, Ali Emileh, Irwin Chaiken, Herman Yeh, and M. Umashankara

Subjects

Anti-HIV Agents, Protein Conformation, Stereochemistry, viruses, Triazole, HIV Infections, Peptide, HIV Envelope Protein gp120, Molecular Dynamics Simulation, Biochemistry, Molecular Docking Simulation, Article, chemistry.chemical_compound, Molecular dynamics, Protein structure, medicine, Humans, Receptor, Nuclear Magnetic Resonance, Biomolecular, chemistry.chemical_classification, virus diseases, Triazoles, Entry inhibitor, chemistry, Docking (molecular), HIV-1, Mutagenesis, Site-Directed, Peptides, medicine.drug

Abstract

Peptide triazole (PT) entry inhibitors prevent HIV-1 infection by blocking the binding of viral gp120 to both the HIV-1 receptor and the coreceptor on target cells. Here, we used all-atom explicit solvent molecular dynamics (MD) to propose a model for the encounter complex of the peptide triazoles with gp120. Saturation transfer difference nuclear magnetic resonance (STD NMR) and single-site mutagenesis experiments were performed to test the simulation results. We found that docking of the peptide to a conserved patch of residues lining the "F43 pocket" of gp120 in a bridging sheet naïve gp120 conformation of the glycoprotein led to a stable complex. This pose prevents formation of the bridging sheet minidomain, which is required for receptor-coreceptor binding, providing a mechanistic basis for dual-site antagonism of this class of inhibitors. Burial of the peptide triazole at the gp120 inner domain-outer domain interface significantly contributed to complex stability and rationalizes the significant contribution of hydrophobic triazole groups to peptide potency. Both the simulation model and STD NMR experiments suggest that the I-X-W [where X is (2S,4S)-4-(4-phenyl-1H-1,2,3-triazol-1-yl)pyrrolidine] tripartite hydrophobic motif in the peptide is the major contributor of contacts at the gp120-PT interface. Because the model predicts that the peptide Trp side chain hydrogen bonding with gp120 S375 contributes to the stability of the PT-gp120 complex, we tested this prediction through analysis of peptide binding to gp120 mutant S375A. The results showed that a peptide triazole KR21 inhibits S375A with 20-fold less potency than WT, consistent with predictions of the model. Overall, the PT-gp120 model provides a starting point for both the rational design of higher-affinity peptide triazoles and the development of structure-minimized entry inhibitors that can trap gp120 into an inactive conformation and prevent infection.

Published

2013

33. Recognition of HIV-inactivating peptide triazoles by the recombinant soluble Env trimer, BG505 SOSIP.664

Author

Kriti, Acharya, Adel A, Rashad, Francesca, Moraca, Per Johan, Klasse, John P, Moore, Cameron, Abrams, and Irwin, Chaiken

Subjects

Protein Conformation, alpha-Helical, viruses, Gene Expression, Enzyme-Linked Immunosorbent Assay, CHO Cells, HIV Envelope Protein gp120, Molecular Dynamics Simulation, Antibodies, Viral, Antiviral Agents, Binding, Competitive, Article, Cricetulus, Animals, Humans, Protein Interaction Domains and Motifs, Binding Sites, virus diseases, Triazoles, Recombinant Proteins, Protein Structure, Tertiary, Molecular Docking Simulation, Kinetics, Solubility, HIV-1, Protein Conformation, beta-Strand, Protein Multimerization, Peptides, Protein Binding

Abstract

Peptide triazole (PT) antagonists interact with gp120 subunits of HIV-1 Env trimers to block host cell receptor interactions, trigger gp120 shedding, irreversibly inactivate virus and inhibit infection. Despite these enticing functions, understanding the structural mechanism of PT-Env trimer encounter has been limited. In this work, we combined competition interaction analysis and computational simulation to demonstrate PT binding to the recombinant soluble trimer, BG505 SOSIP.664, a stable variant that resembles native virus spikes in binding to CD4 receptor as well as known conformationally-dependent Env antibodies. Binding specificity and computational modeling fit with encounter through complementary PT pharmacophore Ile-triazolePro-Trp interaction with a 2-subsite cavity in the Env gp120 subunit of SOSIP trimer similar to that in monomeric gp120. These findings argue that PTs are able to recognize and bind a closed prefusion state of Env trimer upon HIV-1 encounter. The results provide a structural model of how PTs exert their function on virion trimeric spike protein and a platform to inform future antagonist design. Proteins 2017; 85:843-851. © 2016 Wiley Periodicals, Inc.

Published

2016

34. Lytic Inactivation of Human Immunodeficiency Virus by Dual Engagement of gp120 and gp41 Domains in the Virus Env Protein Trimer

Author

Reina Yu, Adel A. Rashad, Cameron F. Abrams, Irwin Chaiken, Bibek Parajuli, Brendon Ngo, and Kriti Acharya

Subjects

0301 basic medicine, viruses, Peptide, Enzyme-Linked Immunosorbent Assay, Biology, HIV Envelope Protein gp120, Gp41, Biochemistry, Virus, Article, law.invention, 03 medical and health sciences, Chimera (genetics), Biopolymers, law, Cell Line, Tumor, medicine, Humans, chemistry.chemical_classification, 030102 biochemistry & molecular biology, Virulence, HEK 293 cells, HIV, Virology, HIV Envelope Protein gp41, Entry inhibitor, 030104 developmental biology, HEK293 Cells, Lytic cycle, chemistry, Recombinant DNA, Virus Inactivation, medicine.drug

Abstract

We recently reported the discovery of a recombinant chimera, denoted DAVEI (dual-acting virucidal entry inhibitor), which is able to selectively cause specific and potent lytic inactivation of both pseudotyped and fully infectious human immunodeficiency virus (HIV-1) virions. The chimera is composed of the lectin cyanovirin-N (CVN) fused to the 20-residue membrane-proximal external region (MPER) of HIV-1 gp41. Because the Env gp120-binding CVN domain on its own is not lytic, we sought here to determine how the MPER(DAVEI) domain is able to endow the chimera with virolytic activity. We used a protein engineering strategy to identify molecular determinants of MPER(DAVEI) that are important for function. Recombinant mutagenesis and truncation demonstrated that the MPER(DAVEI) domain could be significantly minimized without loss of function. The dependence of lysis on specific MPER sequences of DAVEI, determination of minimal linker length, and competition by a simplified MPER surrogate peptide suggested that the MPER domain of DAVEI interacts with the Env spike trimer, likely with the gp41 region. This conclusion was further supported by observations from binding of the biotinylated MPER surrogate peptide to Env protein expressed on cells, monoclonal antibody competition, a direct binding enzyme-linked immunosorbent assay on viruses with varying numbers of trimeric spikes on their surfaces, and comparison of maximal interdomain spacing in DAVEI to that in high-resolution structures of Env. The finding that MPER(DAVEI) in CVN–MPER linker sequences can be minimized without loss of virolytic function provides an improved experimental path for constructing size-minimized DAVEI chimeras and molecular tools for determining how simultaneous engagement of gp120 and gp41 by these chimeras can disrupt the metastable virus Env spike.

Published

2016

35. HIV-1 ENV gp120 structural determinants for peptide triazole dual receptor site antagonism

Author

Elizabeth C. Upton, Karyn McFadden, Navid Madani, Andrew P. Holmes, Isaac Zentner, Ferit Tuzer, Srivats Rajagopal, Kantharaju Kamanna, Judith M. LaLonde, Joseph Sodroski, Mark Contarino, and Irwin Chaiken

Subjects

chemistry.chemical_classification, Allosteric regulation, Mutant, Peptide, Plasma protein binding, Biology, Biochemistry, Molecular biology, Epitope, Entry inhibitor, chemistry, Structural Biology, Viral entry, medicine, Binding site, Molecular Biology, medicine.drug

Abstract

Despite advances in HIV therapy, viral resistance and side-effects with current drug regimens require targeting new components of the virus. Dual antagonist peptide triazoles (PT) are a novel class of HIV-1 inhibitors that specifically target the gp120 component of the viral spike and inhibit its interaction with both of its cell surface protein ligands, namely the initial receptor CD4 and the co-receptor (CCR5/CXCR4), thus preventing viral entry. Following an initial survey of 19 gp120 alanine mutants by ELISA, we screened 11 mutants for their importance in binding to, and inhibition by the PT KR21 using surface plasmon resonance. Key mutants were purified and tested for their effects on the peptide's affinity and its ability to inhibit binding of CD4 and the co-receptor surrogate mAb 17b. Effects of the mutations on KR21 viral neutralization were measured by single-round cell infection assays. Two mutations, D474A and T257A, caused large-scale loss of KR21 binding, as well as losses in both CD4/17b and viral inhibition by KR21. A set of other Ala mutants revealed more moderate losses in direct binding affinity and inhibition sensitivity to KR21. The cluster of sensitive residues defines a PT functional epitope. This site is in a conserved region of gp120 that overlaps the CD4 binding site and is distant from the co-receptor/17b binding site, suggesting an allosteric mode of inhibition for the latter. The arrangement and sequence conservation of the residues in the functional epitope explain the breadth of antiviral activity, and improve the potential for rational inhibitor development.

Published

2012

36. Solid-State Nanopore Detection of Protein Complexes: Applications in Healthcare and Protein Kinetics

Author

Arangassery Rosemary Bastian, Kevin J. Freedman, Min Jun Kim, and Irwin Chaiken

Subjects

Imagination, Chemical substance, media_common.quotation_subject, Kinetics, Solid-state, Proteins, Nanotechnology, General Chemistry, Biomaterials, Nanopores, chemistry.chemical_compound, Search engine, Nanopore, Monomer, Molecular recognition, chemistry, General Materials Science, Biotechnology, media_common

Abstract

Protein conjugation provides a unique look into many biological phenomena and has been used for decades for molecular recognition purposes. In this study, the use of solid-state nanopores for the detection of gp120-associated complexes are investigated. They exhibit monovalent and multivalent binding to anti-gp120 antibody monomer and dimers. In order to investigate the feasibility of many practical applications related to nanopores, detection of specific protein complexes is attempted within a heterogeneous protein sample, and the role of voltage on complexed proteins is researched. It is found that the electric field within the pore can result in unbinding of a freely translocating protein complex within the transient event durations measured experimentally. The strong dependence of the unbinding time with voltage can be used to improve the detection capability of the nanopore system by adding an additional level of specificity that can be probed. These data provide a strong framework for future protein-specific detection schemes, which are shown to be feasible in the realm of a 'real-world' sample and an automated multidimensional method of detecting events.

Published

2012

37. Multivalent and Flexible PEG-Nitrilotriacetic Acid Derivatives for Non-covalent Protein Pegylation

Author

Anna Mero, Irwin Chaiken, Gianfranco Pasut, Francesco M. Veronese, and Tetsuya Ishino

Subjects

Male, Nitrilotriacetic Acid, Pharmaceutical Science, PEGylation, Protein delivery, Chromatography, Affinity, Protein Structure, Secondary, Polyethylene Glycols, Rats, Sprague-Dawley, chemistry.chemical_compound, Drug Delivery Systems, Protein structure, Affinity chromatography, Coordination Complexes, Granulocyte Colony-Stimulating Factor, PEG ratio, Animals, Organic chemistry, Histidine, Pharmacology (medical), Chelation, Protein secondary structure, Chelating Agents, Pharmacology, Bioconjugation, Organic Chemistry, Nitrilotriacetic acid, Proteins, Surface Plasmon Resonance, Combinatorial chemistry, Rats, chemistry, Molecular Medicine, Protein Binding, Biotechnology

Abstract

A new approach for non-covalent protein PEGylation is translated from immobilized metal ion affinity chromatography, and based on metal coordination bonds between a chelating agent linked to PEG, nitrilotriacetic acid (NTA), and the ring nitrogen of histidines in a protein. PEG-NTA conjugates were synthesized differing in the number of NTA units and in the polymer structure. Three derivatives were investigated in association experiments with five model proteins. The most promising complex, PEG8-(NTA)8–Cu2+–G-CSF (granulocyte colony stimulating factor), was thoroughly characterized and the pharmacokinetic profile was evaluated in rats. The experiments demonstrated that only PEG8-(NTA)8, bearing eight NTA molecules on flexible PEG arms, associated strongly with those proteins having several histidines. The protein secondary structure was not affected in the complex. PEG8-(NTA)8–Cu2+–G-CSF showed a K D of 4.7 nM, as determined by surface plasmon resonance, but the association was not stable in vivo. PEG8-(NTA)8 is the first derivative able to associate with native proteins and form soluble complexes with a nanomolar K D. The study highlights the need of a multivalent and flexible coordination and encourages further investigations to increase the stability of PEG8-(NTA)8 complexes in vivo either through the use of protein mutants or His-tag proteins.

Published

2011

38. Monoclonal Antibody m18 Paratope Leading to Dual Receptor Antagonism of HIV-1 gp120

Author

Srivats Rajagopal, Dimiter S. Dimitrov, Syna Kuriakose Gift, Karyn McFadden, Isaac Zentner, Irwin Chaiken, and Mei-Yun Zhang

Subjects

Models, Molecular, Protein Conformation, medicine.drug_class, Mutant, Complementarity determining region, HIV Antibodies, HIV Envelope Protein gp120, Biology, Monoclonal antibody, Binding, Competitive, Biochemistry, Article, Epitopes, Immunoglobulin Fab Fragments, medicine, Humans, Surface plasmon resonance, Neutralizing antibody, Receptor, Binding Sites, Antibodies, Monoclonal, Antibodies, Neutralizing, Complementarity Determining Regions, Molecular biology, Cell biology, CD4 Antigens, Mutation, HIV-1, biology.protein, Paratope, Antibody, Protein Binding

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

39. HIV Envelope Binding by Macrophage-Expressed gp340 Promotes HIV-1 Infection

Author

Irwin Chaiken, Earl Stoddard, Yanjie Yi, Donald Van Ryk, Georgetta Cannon, Drew Weissman, David Scales, Houping Ni, and Daniel Malamud

Subjects

Innate immune system, Sexual transmission, biology, Immunology, Heparan sulfate, Cell biology, chemistry.chemical_compound, chemistry, Cell culture, biology.protein, Immunology and Allergy, Macrophage, Scavenger receptor, Antibody, Epithelial cell differentiation

Abstract

The scavenger receptor cysteine-rich protein gp340 functions as part of the host innate immune defense system at mucosal surfaces. In the genital tract, its expression by cervical and vaginal epithelial cells promotes HIV trans-infection and may play a role in sexual transmission. Gp340 is an alternatively spliced product of the deleted in malignant brain tumors 1 (DMBT1) gene. In addition to its innate immune system activity, DMBT1 demonstrates instability in multiple types of cancer and plays a role in epithelial cell differentiation. We demonstrate that monocyte-derived macrophages express gp340 and that HIV-1 infection is decreased when envelope cannot bind it. Inhibition of infection occurred at the level of fusion of M-, T-, and dual-tropic envelopes. Additional HIV-1 envelope binding molecules, such as dendritic cell-specific ICAM-3-grabbing nonintegrin (DC-SIGN), mannose-binding lectin, and heparan sulfate, enhance the efficiency of infection of the cells that express them by increasing the local concentration of infectious virus. Our data suggest that gp340, which is expressed by macrophages in vivo, may function to enhance infection in much the same manner. Its expression on tissue macrophages and epithelial cells suggests important new opportunities for HIV-1 pathogenesis investigation and therapy.

Published

2008

40. Slow-dissociation effect of common signaling subunit β on IL5 and GM-CSF receptor assembly

Author

Tetsuya Ishino, Meirav Zaks-Zilberman, Jeffery J. Scibek, Adrian E. Harrington, and Irwin Chaiken

Subjects

Protein subunit, Immunology, Interleukin 5 receptor alpha subunit, Biology, Biochemistry, Article, Cell Line, Cytokine Receptor Common beta Subunit, Interleukin-5 Receptor alpha Subunit, Animals, Humans, Immunology and Allergy, Cytokine binding, Receptor, Molecular Biology, GM-CSF Receptor, Granulocyte-Macrophage Colony-Stimulating Factor, Hematology, Receptors, Interleukin-5, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, Biophysics, Drosophila, Interleukin-5, Signal transduction, Cytokine receptor, Signal Transduction

Abstract

Receptor activation by IL5 and GM-CSF is a sequential process that depends on their interaction with a cytokine-specific subunit alpha and recruitment of a common signaling subunit beta (betac). In order to elucidate the assembly dynamics of these receptor subunits, we performed kinetic interaction analysis of the cytokine-receptor complex formation by a surface plasmon resonance biosensor. Using the extracellular domains of receptor fused with C-terminal V5-tag, we developed an assay method to co-anchor alpha and betac subunits on the biosensor surface. We demonstrated that dissociation of the cytokine-receptor complexes was slower when both subunits were co-anchored on the biosensor surface than when alpha subunit alone was anchored. The slow-dissociation effect of betac had a similar impact on GM-CSF receptor stabilization to that of IL5. The effects were abolished by alanine replacement of either Tyr18 or Tyr344 residue in betac, which together constitute key parts of a cytokine binding epitope. The data argue that betac plays an important role in preventing the ligand-receptor complexes from rapidly dissociating. This slow-dissociation effect of betac explains how, when multiple betac cytokine receptor alpha subunits are present on the same cell surface, selective betac usage can be controlled by sequestration in stabilized cytokine-alpha-betac complexes.

Published

2008

41. Interleukin-5 Receptor Subunit Oligomerization and Rearrangement Revealed by Fluorescence Resonance Energy Transfer Imaging

Author

Irwin Chaiken, Meirav Zaks-Zilberman, Adrian E. Harrington, and Tetsuya Ishino

Subjects

Models, Molecular, Yellow fluorescent protein, Time Factors, Protein subunit, Interleukin 5 receptor alpha subunit, Gene Expression, Biology, Crystallography, X-Ray, Biochemistry, Cell Line, Cytokine Receptor Common beta Subunit, Interleukin 10 receptor, alpha subunit, Interleukin-5 Receptor alpha Subunit, Fluorescence Resonance Energy Transfer, Humans, Transgenes, Molecular Biology, Interleukin-5 receptor, Mechanisms of Signal Transduction, Cell Biology, Ligand (biochemistry), Molecular biology, Protein Structure, Tertiary, Förster resonance energy transfer, Mutation, Biophysics, biology.protein, Interleukin-5, Protein Binding

Abstract

Interleukin (IL)-5 exerts hematopoietic functions through binding to the IL-5 receptor subunits, alpha and betac. Specific assembly steps of full-length subunits as they occur in cell membranes, ultimately leading to receptor activation, are not well understood. We tracked the oligomerization of IL-5 receptor subunits using fluorescence resonance energy transfer (FRET) imaging. Full-length IL-5Ralpha and betac were expressed in Phoenix cells as chimeric proteins fused to enhanced cyan or yellow fluorescent protein (CFP or YFP, respectively). A time- and dose-dependent increase in FRET signal between IL-5Ralpha-CFP and betac-YFP was observed in response to IL-5, indicative of heteromeric receptor alpha-betac subunit interaction. This response was inhibited by AF17121, a peptide antagonist of IL-5Ralpha. Substantial FRET signals with betac-CFP and betac-YFP co-expressed in the absence of IL-5Ralpha demonstrated that betac subunits exist as preformed homo-oligomers. IL-5 had no effect on this betac-alone FRET signal. Interestingly, the addition of IL-5 to cells co-expressing betac-CFP, betac-YFP, and nontagged IL-5Ralpha led to further increase in FRET efficiency. Observation of preformed betac oligomers fits with the view that this form can lead to rapid cellular responses upon IL-5 stimulation. The IL-5-induced effects on betac assembly in the presence of nontagged IL-5Ralpha provide direct evidence that IL-5 can cause higher order rearrangements of betac homo-oligomers. These results suggest that IL-5 and perhaps other betac cytokines (IL-3 and granulocyte/macrophage colony-stimulating factor) trigger cellular responses by the sequential binding of cytokine ligand to the specificity receptor (subunit alpha), followed by binding of the ligand-subunit alpha complex to, and consequent rearrangement of, a ground state form of betac oligomers.

Published

2008

42. Structural Determinants for Affinity Enhancement of a Dual Antagonist Peptide Entry Inhibitor of Human Immunodeficiency Virus Type-1

Author

Vanessa Pirrone, Shendra R. Miller, Simon Cocklin, Sabine Baxter, Ferit Tuzer, Irwin Chaiken, Judith M. LaLonde, M. Umashankara, Jeffrey C. Klein, Navneet Jawanda, Fred C. Krebs, Arne Schön, Amos B. Smith, Joseph Sodroski, Ernesto Freire, Navid Madani, Hosahudya N. Gopi, and Isaac Zentner

Subjects

Anti-HIV Agents, Stereochemistry, Stereoisomerism, Peptide, HIV Antibodies, HIV Envelope Protein gp120, Article, Cell Line, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, medicine, Peptide synthesis, Humans, Structure–activity relationship, Binding site, Receptor, chemistry.chemical_classification, Binding Sites, Molecular Mimicry, Antibodies, Monoclonal, Triazoles, Virus Internalization, Entry inhibitor, chemistry, CD4 Antigens, HIV-1, Molecular Medicine, Peptides, Protein Binding, medicine.drug, Conjugate

Abstract

Structure-activity correlations were investigated for substituted peptide conjugates that function as dual receptor site antagonists of HIV-1 gp120. A series of peptide conjugates were constructed via click reaction of both aryl and alkyl acetylenes with an internally incorporated azidoproline 6 derived from the parent peptide 1 (12p1, RINNIPWSEAMM). Compared to 1, many of these conjugates were found to exhibit several orders of magnitude increase in both affinity for HIV-1 gp120 and inhibition potencies at both the CD4 and coreceptor binding sites of gp120. We sought to determine structural factors in the added triazole grouping responsible for the increased binding affinity and antiviral activity of the dual inhibitor conjugates. We measured peptide conjugate potencies in both kinetic and cell infection assays. High affinity was sterically specific, being exhibited by the cis- but not the trans-triazole. The results demonstrate that aromatic, hydrophobic, and steric features in the residue 6 side-chain are important for increased affinity and inhibition. Optimizing these features provides a basis for developing gp120 dual inhibitors into peptidomimetic and increasingly smaller molecular weight entry antagonist leads.

Published

2008

43. Structure-Based Rationale for Interleukin 5 Receptor Antagonism

Author

Hosahudya N. Gopi, Adrian E. Harrington, Tetsuya Ishino, and Irwin Chaiken

Subjects

Pharmacology, Receptor Activation Process, Interleukin-5 receptor, Binding Sites, Protein Conformation, Interleukin 5 receptor alpha subunit, Antibodies, Monoclonal, Biology, Peptides, Cyclic, Eosinophils, Interleukin-5 Receptor alpha Subunit, Interleukin-21 receptor, Eosinophilia, Drug Discovery, Immunology, Interleukin-6 receptor, Cancer research, Animals, Humans, Interleukin-5, Interleukin 5, Interleukin 12 receptor, beta 1 subunit, Common gamma chain

Abstract

Human interleukin 5 (IL5) is the major hematopoietin that stimulates the proliferation, migration and activation of eosinophils and is implicated in the pathogenesis of inflammatory and other myeloproliferative diseases. IL5 functions through the signaling of a common receptor subunit beta (beta c), in a receptor activation process that requires initial recruitment of an IL5 specific receptor subunit alpha (IL5Ralpha), for cytokine presentation to beta c. Important advances have been made to understand molecular mechanisms of cytokine recognition and receptor antagonism. Mutational studies indicate that a pair of charge complementary regions play an essential role in specific interaction between IL5Ralpha and IL5. Moreover, peptide studies with the IL5 system have identified a cyclic peptide inhibitor, AF17121, which binds specifically to IL5Ralpha by mimicking the cytokine. A key receptor-recognition pharmacophore has been identified in this peptide inhibitor, and sites of inhibitor recognition can be proposed in the homology-deduced structural model of IL5Ralpha. These results provide an experimental platform to derive enhanced-potency peptidomimetic inhibitors. Such inhibitors have potential use as tools to evaluate the role of eosinophilia in disease and as potential leads to antagonists to treat hyper-eosinophilic diseases such as eosinophilic esophagitis, asthma and chronic myeloproliferative leukemias.

Published

2008

44. Disulfide Sensitivity in the Env Protein Underlies Lytic Inactivation of HIV-1 by Peptide Triazole Thiols

Author

Lauren D. Bailey, Andrew P. Holmes, Adel A. Rashad, Caitlin Duffy, Arangassery Rosemary Bastian, Rachna Aneja, Irwin Chaiken, Huiyuan Li, Ramalingam Venkat Kalyana Sundaram, and Kantharaju Kamanna

Subjects

Lysis, viruses, Peptide, V3 loop, HIV Envelope Protein gp120, Biochemistry, Antiviral Agents, Models, Biological, Article, Inhibitory Concentration 50, Humans, Disulfides, Sulfhydryl Compounds, Binding site, chemistry.chemical_classification, Binding Sites, Dose-Response Relationship, Drug, General Medicine, Triazoles, Molecular Docking Simulation, chemistry, Lytic cycle, Mutation, Thiol, HIV-1, Molecular Medicine, Virus Inactivation, Pharmacophore, Peptides, Linker, Dimerization

Abstract

We investigated the mode of action underlying lytic inactivation of HIV-1 virions by peptide triazole thiol (PTT), in particular the relationship between gp120 disulfides and the C-terminal cysteine-SH required for virolysis. Obligate PTT dimer obtained by PTT SH cross-linking and PTTs with serially truncated linkers between pharmacophore isoleucine-ferrocenyltriazole-proline-tryptophan and cysteine-SH were synthesized. PTT variants showed loss of lytic activity but not binding and infection inhibition upon SH blockade. A disproportionate loss of lysis activity vs binding and infection inhibition was observed upon linker truncation. Molecular docking of PTT onto gp120 argued that, with sufficient linker length, the peptide SH could approach and disrupt several alternative gp120 disulfides. Inhibition of lysis by gp120 mAb 2G12, which binds at the base of the V3 loop, as well as disulfide mutational effects, argued that PTT-induced disruption of the gp120 disulfide cluster at the base of the V3 loop is an important step in lytic inactivation of HIV-1. Further, PTT-induced lysis was enhanced after treating virus with reducing agents dithiothreitol and tris (2-carboxyethyl)phosphine. Overall, the results are consistent with the view that the binding of PTT positions the peptide SH group to interfere with conserved disulfides clustered proximal to the CD4 binding site in gp120, leading to disulfide exchange in gp120 and possibly gp41, rearrangement of the Env spike, and ultimately disruption of the viral membrane. The dependence of lysis activity on thiol-disulfide interaction may be related to intrinsic disulfide exchange susceptibility in gp120 that has been reported previously to play a role in HIV-1 cell infection.

Published

2015

45. Short Communication: Inhibition of DC-SIGN-Mediated HIV-1 Infection by Complementary Actions of Dendritic Cell Receptor Antagonists and Env-Targeting Virus Inactivators

Author

Irwin Chaiken, Zafar K. Khan, Frank Fieschi, Rajnish S. Dave, Matthew Hutchinson, Sergey Pustylnikov, Vanessa Porkolab, Pooja Jain, and Adel A. Rashad

Subjects

0301 basic medicine, Immunology, Serum albumin, Oligosaccharides, Receptors, Cell Surface, Pharmacology, HIV Envelope Protein gp120, Ligands, gag Gene Products, Human Immunodeficiency Virus, Virus, Cell Line, 03 medical and health sciences, Virology, Humans, Lectins, C-Type, Receptor, Serum Albumin, Binding Sites, biology, Dextrans, Dendritic cell, Dendritic Cells, Triazoles, Viral Load, DC-SIGN, 030104 developmental biology, Infectious Diseases, Gene Expression Regulation, Cell culture, Host-Pathogen Interactions, biology.protein, HIV-1, Signal transduction, Peptides, Viral load, Cell Adhesion Molecules, Mannose, Protein Binding, Signal Transduction

Abstract

The DC-SIGN receptor on human dendritic cells interacts with HIV gp120 to promote both infection of antigen-presenting cells and transinfection of T cells. We hypothesized that in DC-SIGN-expressing cells, both DC-SIGN ligands such as dextrans and gp120 antagonists such as peptide triazoles would inhibit HIV infection with potential complementary antagonist effects. To test this hypothesis, we evaluated the effects of dextran (D66), isomaltooligosaccharides (D06), and several peptide triazoles (HNG156, K13, and UM15) on HIV infection of B-THP-1/DC-SIGN cells. In surface plasmon resonance competition assays, D66 (IC50 = 35.4 μM) and D06 (IC50 = 3.4 mM) prevented binding of soluble DC-SIGN to immobilized mannosylated bovine serum albumin (BSA). An efficacious dose-dependent inhibition of DC-SIGN-mediated HIV infection in both pretreatment and posttreatment settings was observed, as indicated by inhibitory potentials (EC50) [D66 (8 μM), D06 (48 mM), HNG156 (40 μM), UM15 (100 nM), and K13 (25 nM)]. Importantly, both dextrans and peptide triazoles significantly decreased HIV gag RNA levels [D66 (7-fold), D06 (13-fold), HNG156 (7-fold), K-13 (3-fold), and UM15 (6-fold)]. Interestingly, D06 at the highest effective concentration showed a 14-fold decrease of infection, while its combination with 50 μM HNG156 showed a 26-fold decrease. Hence, these compounds can combine to inactivate the viruses and suppress DC-SIGN-mediated virus-cell interaction that as shown earlier leads to dendritic cell HIV infection and transinfection dependent on the DC-SIGN receptor.

Published

2015

46. Peptide Triazole Inactivators of HIV-1 Utilize a Conserved Two-Cavity Binding Site at the Junction of the Inner and Outer Domains of Env gp120

Author

Caitlin Duffy, Irwin Chaiken, Ramalingam Venkat Kalyana Sundaram, Rachna Aneja, Lauren D. Bailey, Adel A. Rashad, and Huiyuan Li

Subjects

Peptidomimetic, Anti-HIV Agents, viruses, Peptide, Plasma protein binding, HIV Envelope Protein gp120, Molecular Docking Simulation, Article, Structure-Activity Relationship, Drug Discovery, Structure–activity relationship, Binding site, chemistry.chemical_classification, Binding Sites, Chemistry, virus diseases, Antibodies, Monoclonal, Triazoles, Small molecule, Biochemistry, Docking (molecular), CD4 Antigens, Mutation, Biophysics, HIV-1, Molecular Medicine, Thermodynamics, Virus Inactivation, Peptidomimetics, Peptides, Hydrophobic and Hydrophilic Interactions, Protein Binding

Abstract

We used coordinated mutagenesis, synthetic design, and flexible docking to investigate the structural mechanism of Env gp120 encounter by peptide triazole (PT) inactivators of HIV-1. Prior results demonstrated that the PT class of inhibitors suppresses binding at both CD4 and coreceptor sites on Env and triggers gp120 shedding, leading to cell-independent irreversible virus inactivation. Despite these enticing anti-HIV-1 phenotypes, structural understanding of the PT-gp120 binding mechanism has been incomplete. Here we found that PT engages two inhibitor ring moieties at the junction between the inner and outer domains of the gp120 protein. The results demonstrate how combined occupancy of two gp120 cavities can coordinately suppress both receptor and coreceptor binding and conformationally entrap the protein in a destabilized state. The two-cavity model has common features with small molecule gp120 inhibitor binding sites and provides a guide for further design of peptidomimetic HIV-1 inactivators based on the PT pharmacophore.

Published

2015

47. Click Chemistry on Azidoproline: High-Affinity Dual Antagonist for HIV-1 Envelope Glycoprotein gp120

Author

Sabine Baxter, Kalyan C. Tirupula, Hosahudya N. Gopi, Sandya Ajith, and Irwin Chaiken

Subjects

Pharmacology, chemistry.chemical_classification, Azides, Proline, Anti-HIV Agents, Chemistry, Molecular Sequence Data, Organic Chemistry, Antagonist, HIV Envelope Protein gp120, DUAL (cognitive architecture), Hiv 1 envelope, Biochemistry, Structure-Activity Relationship, CD4 Antigens, Drug Discovery, Click chemistry, Molecular Medicine, Amino Acid Sequence, General Pharmacology, Toxicology and Pharmaceutics, Glycoprotein, Protein Binding

Published

2006

48. Real-time monitoring of the membrane-binding and insertion properties of the cholesterol-dependent cytolysin anthrolysin O fromBacillus anthracis

Author

Richard F. Rest, Simon Cocklin, Emily Young, Monika Jost, Patrick J. Loll, Aleister J. Saunders, Irwin Chaiken, Noreen M. Robertson, Can Zhang, Stephen D. Weeks, Elise M. Mosser, Samar Seal, and Hans Weber

Subjects

Cell Survival, Bacterial Toxins, Cholesterol-dependent cytolysin, Models, Biological, Cell membrane, Hemolysin Proteins, Mice, chemistry.chemical_compound, Bacterial Proteins, Structural Biology, medicine, Animals, Humans, Molecular Biology, POPC, Cells, Cultured, Ergosterol, Membrane Glycoproteins, Cell Death, biology, Cytotoxins, Schneider 2 cells, Cell Membrane, Temperature, biology.organism_classification, Recombinant Proteins, Sterol, Bacillus anthracis, Kinetics, Cytolysis, Cholesterol, Drosophila melanogaster, medicine.anatomical_structure, Biochemistry, chemistry, lipids (amino acids, peptides, and proteins)

Abstract

Bacillus anthracis has recently been shown to secrete a potently hemolytic/cytolytic protein that has been designated anthrolysin O (ALO). In this work, we initiated a study of this potential anthrax virulence factor in an effort to understand the membrane-binding properties of this protein. Recombinant anthrolysin O (rALO35-512) and two N-terminally truncated versions of ALO (rALO390-512 and rALO403-512) from B. anthracis were overproduced in Escherichia coli and purified to homogeneity. The role of cholesterol in the cytolytic activity of ALO was probed in cellular cholesterol depletion assays using mouse and human macrophage-like lines, and also Drosophila Schneider 2 cells. Challenging the macrophage cells with rALO35-512, but not rALO390-512 or rALO403-512, resulted in cell death by lysis, with this cytolysis being abolished by depletion of the membrane cholesterol. Drosophila cells, which contain ergosterol as their major membrane sterol, were resistant to rALO-mediated cytolysis. In order to determine the molecular mechanism of this resistance, the interaction of rALO with model membranes comprised of POPC alone, or with a variety of structurally similar sterols including ergosterol, was probed using Biacore. Both rALO35-512 and rALO403-512 demonstrated robust binding to model membranes composed of POPC and cholesterol, with amount of protein bound proportional to the cholesterol content. Ergosterol supported greatly reduced binding of both rALO35-512 and rALO403-512, whereas other sterols tested did not support binding. The rALO403-512--membrane interaction demonstrated an equilibrium dissociation constant (KD) in the low nanomolar range, whereas rALO35-512 exhibited complex kinetics likely due to the multiple events involved in pore formation. These results establish the pivotal role of cholesterol in the action of rALO. The biosensor method developed to measure ALO recognition of cholesterol in a membrane environment could be extended to provide a platform for the screening of inhibitors of other membrane-binding proteins and peptides.

Published

2006

49. Receptor Epitope Usage by an Interleukin-5 Mimetic Peptide

Author

Tetsuya Ishino, Dominick Panarello, Irwin Chaiken, Madhushree Bhattacharya, and Cecilia Urbina

Subjects

Models, Molecular, Time Factors, Polymers, Interleukin 5 receptor alpha subunit, Peptide, Biosensing Techniques, Biochemistry, Epitope, Epitopes, Thioredoxins, Protein structure, Interleukin-5 Receptor alpha Subunit, 5-HT5A receptor, Receptor, Peptide sequence, chemistry.chemical_classification, Alanine, Recombinant Proteins, Cytokines, Plasmids, Protein Binding, Stereochemistry, Recombinant Fusion Proteins, Genetic Vectors, Molecular Sequence Data, Biology, Arginine, Binding, Competitive, Inhibitory Concentration 50, Cell Line, Tumor, Escherichia coli, Humans, Amino Acid Sequence, Binding site, Molecular Biology, Base Sequence, Sequence Homology, Amino Acid, Granulocyte-Macrophage Colony-Stimulating Factor, DNA, Receptors, Interleukin, Cell Biology, Surface Plasmon Resonance, Fibronectins, Protein Structure, Tertiary, Kinetics, chemistry, Interleukin-3, Interleukin-5, Peptides

Abstract

The cyclic peptide AF17121 is a library-derived antagonist for human interleukin-5 (IL5) receptor alpha (IL5Ralpha) and inhibits IL5 activity. Our previous results have demonstrated that the sixth arginine residue of the peptide is crucial for the inhibitory effect and that several acidic residues in the N- and C-terminal regions also make a contribution, although to a lesser extent (Ruchala, P., Varadi, G., Ishino, T., Scibek, J., Bhattacharya, M., Urbina, C., Van Ryk, D., Uings, I., and Chaiken, I. (2004) Biopolymers 73, 556-568). However, the recognition mechanism of the receptor has remained unresolved. In this study, AF17121 was fused to thioredoxin by recombinant DNA techniques and examined for IL5Ralpha interaction using a surface plasmon resonance biosensor method. Kinetic analysis revealed that the dissociation rate of the peptide.receptor complex is comparable with that of the cytokine.receptor complex. The fusion peptide competed with IL5 for both biological function and interaction with IL5Ralpha, indicating that the binding sites on the receptor are shared by AF17121 and IL5. To define the epitope residues for AF17121, we defined its binding footprint on IL5Ralpha by alanine substitution of Asp(55), Asp(56), Glu(58), Lys(186), Arg(188), and Arg(297) of the receptor. Marked effects on the interaction were observed in all three fibronectin type III domains of IL5Ralpha, in particular Asp(55), Arg(188), and Arg(297) in the D1, D2, and D3 domains, respectively. This footprint represents a significant subset of that for IL5 binding. The fact that AF17121 mimics the receptor binding capability of IL5 but antagonizes biological function evokes several models for how IL5 induces activation of the multisubunit receptor system.

Published

2005

50. Small-molecule inhibitors of HIV-1 entry block receptor-induced conformational changes in the viral envelope glycoproteins

Author

Jason J. Chruma, Arne Schön, Liping Wang, Amos B. Smith, Joseph Sodroski, Jason M. Cox, Ernesto Freire, Navid Madani, Irwin Chaiken, Alyssa C. Biorn, Ngoc Phan, Simon Cocklin, Jeffrey C. Klein, and Zhihai Si

Subjects

Coiled coil, chemistry.chemical_classification, Multidisciplinary, Protein Conformation, viruses, virus diseases, Biological Sciences, Biology, Gp41, HIV Envelope Protein gp41, Piperazines, Transmembrane protein, Cell Line, Heptad repeat, Receptors, HIV, Protein structure, Biochemistry, Viral envelope, chemistry, HIV Fusion Inhibitors, HIV-1, Biophysics, Humans, Receptor, Glycoprotein

Abstract

When interacting with the CD4 receptor, the HIV gp120 envelope glycoprotein undergoes conformational changes that allow binding to the chemokine receptor. Receptor binding is proposed to lead to conformational changes in the gp41 transmembrane envelope glycoprotein involving the creation and/or exposure of a coiled coil consisting of three heptad repeat (HR) sequences. The subsequent interaction of the HR2 region of gp41 with this coiled coil results in the assembly of a six-helix bundle that promotes the fusion of the viral and target cell membranes. Here we show that CD4 binding to gp120 induces the formation and/or exposure of the gp41 HR1 coiled coil in a process that does not involve gp120 shedding and that depends on the proteolytic maturation of the gp160 envelope glycoprotein precursor. Importantly, BMS-806 and related HIV-1 entry inhibitors bind gp120 and block the CD4 induction of HR1 exposure without significantly affecting CD4 binding. Moreover, these compounds do not disrupt gp120-chemokine receptor binding or the HR1-HR2 interaction within gp41. These studies thus define a receptor-induced conformational rearrangement of gp120-gp41 that is important for both CD4-dependent and CD4-independent HIV-1 entry and is susceptible to inhibition by low-molecular-weight compounds.

Published

2004