Your search keyword '"Hubert François Gaertner"' showing total 32 results

1. Prognostic and therapeutic considerations of antibodies against c‐ter apolipoprotein A‐1 in the general population

Author

Peter Vollenweider, Nicolas Vuilleumier, Gérard Waeber, François Mach, Fabrizio Montecucco, Nathalie Satta, Karim J. Brandt, Fabienne Burger, Julien Virzi, Oliver Hartley, Pedro Marques-Vidal, Hubert François Gaertner, Panagiotis Antiochos, and Sabrina Pagano

Subjects

lcsh:Immunologic diseases. Allergy, Anti‐apoA‐1 IgG, Apolipoprotein B, CoLaus study, C‐terminal A1 peptide, Immunology, Population, ddc:616.07, 030204 cardiovascular system & hematology, anti‐apoA‐1 IgG, 03 medical and health sciences, 0302 clinical medicine, In vivo, Immunology and Allergy, Medicine, Passive immunisation, education, General Nursing, 030304 developmental biology, ddc:616, passive immunisation, 0303 health sciences, education.field_of_study, biology, business.industry, Mortality rate, Autoantibody, Original Articles, ApoE−/− mice, 3. Good health, biology.protein, Biomarker (medicine), Original Article, Apolipoprotein A1, lipids (amino acids, peptides, and proteins), Antibody, business, lcsh:RC581-607

Abstract

Objectives Autoantibodies against apolipoprotein A1 (anti‐apoA1 IgGs) and its C‐terminal region (cter apoA1) have emerged as an independent biomarker for cardiovascular disease. Cter apoA1 mimetic peptides were shown to reverse the deleterious anti‐apoA1 IgG effects in vitro. We evaluated the association of anti‐cter apoA1 IgGs with overall mortality in the general population and tested the ability of a cter apoA1 mimetic peptide to reverse the anti‐apoA1 IgG‐induced inflammatory response and mortality in vitro and in vivo, respectively. Methods Anti‐cter apoA1 IgGs were measured in serum samples of 6386 participants of the CoLaus study of which 5220 were followed for a median duration of 5.6 years. The primary outcome was overall mortality. The peptide inhibitory concentration 50% (IC50) was determined in vitro on HEK‐Blue‐4 and RAW cells. ApoE−/− mice were exposed to 16 weeks of anti‐apoA1IgG passive immunisation with and without peptide co‐incubation. Results Anti‐cter apoA1 IgGs were associated with higher interleukin 6 levels and independently predicted overall mortality; an increase of one standard deviation of anti‐cter apoA1 IgG level was associated with an 18% increase in mortality risk (hazard ratio: 1.18, 95% confidence interval: 1.04–1.33; P = 0.009). The cterApoA1 analogue reversed the antibody‐mediated inflammatory response with an IC50 of 1 µm in vitro but did not rescue the significant anti‐apoA1 IgG‐induced mortality rate in vivo (69% vs. 23%, LogRank P = 0.02). Conclusion Anti‐cter apoA1 IgG independently predicts overall mortality in the general population. Despite being effective in vitro, our cter apoA1 analogue did not reverse the anti‐apoA1 IgG‐induced mortality in mice. Our data suggest that these autoantibodies are not readily treatable through cognate peptide immunomodulation., Autoantibodies against apolipoprotein A1 (anti‐apoA1 IgGs) have emerged as an independent cardiovascular risk factor in different settings including in the general population and seem to be preferentially oriented against the its C‐terminal region (cterA1) in humans. In this translational work, we extend previous knowledge in the field by demonstrating for the first time that anti‐cterA1 IgGs are independently predictive of premature mortality in a large general population sample of 5220 individuals. Furthermore, we also report that, despite being effective in vitro, our cterA1 analogue did not reverse the significant anti‐apoA1 IgG‐induced mortality in mice.

Published

2020

2. High-Affinity Binding of Chemokine Analogs that Display Ligand Bias at the HIV-1 Co-receptor CCR5

Author

He Tian, Jennifer C. Peeler, Manija A. Kazmi, Thomas Huber, Mizuho Horioka, Alexandre Fürstenberg, Oliver Hartley, Thomas P. Sakmar, Emily Lorenzen, Yamina A. Berchiche, Carlos A. Rico, and Hubert François Gaertner

Subjects

0303 health sciences, Chemokine, Co-receptor, biology, Chemistry, Chemokine receptor CCR5, 030302 biochemistry & molecular biology, Native chemical ligation, Ligand (biochemistry), CCL5, 3. Good health, 03 medical and health sciences, Biochemistry, biology.protein, Binding site, Bioorthogonal chemistry, 030304 developmental biology

Abstract

The chemokine receptor CCR5 is a drug target to prevent transmission of HIV/AIDS. We studied four analogs of the native chemokine RANTES (CCL5) that have anti-HIV potencies of around 25 pM, which is more than four orders-of-magnitude higher than that of RANTES itself. It has been hypothesized that the ultra-high potency of the analogs is due to their ability to bind populations of receptors not accessible to native chemokines. To test this hypothesis, we developed a homogeneous dual-color fluorescence cross-correlation spectroscopy (FCCS) assay for saturation and competition binding experiments. The FCCS assay has the advantage that it does not rely on competition with radioactively labeled native chemokines used in conventional assays. We prepared site-specifically labeled fluorescent analogs using native chemical ligation of synthetic peptides, followed by bioorthogonal fluorescent labeling. We engineered a mammalian cell expression construct to provide fluorescently labeled CCR5, which was purified using a tandem immunoaffinity and size-exclusion chromatography approach to obtain monomeric fluorescent CCR5 in detergent solution. We found subnanomolar binding affinities for the two analogs 5P12-RANTES and 5P14-RANTES, and about twenty-fold reduced affinities for PSC-RANTES and 6P4-RANTES. Using homologous and heterologous competition experiments with unlabeled chemokine analogs, we conclude that the analogs all bind at the same binding site; whereas, the native chemokines (RANTES and MIP1α) fail to displace bound fluorescent analogs even at tens of micromolar concentrations. Our results can be rationalized with de novo structural models of the N-terminal tails of the synthetic chemokines that adopt a different binding mode as compared to the parent compound.

Published

2019

3. High-Affinity Binding of Chemokine Analogs that Display Ligand Bias at the HIV-1 Coreceptor CCR5

Author

Manija A. Kazmi, Mizuho Horioka, Thomas Huber, Jennifer C. Peeler, He Tian, Thomas P. Sakmar, Alexandre Fürstenberg, Oliver Hartley, Yamina A. Berchiche, Carlos A. Rico, Hubert François Gaertner, and Emily Lorenzen

Subjects

Chemokine, Receptors, CCR5, Chemokine receptor CCR5, Biophysics, ddc:616.07, Ligands, Binding, Competitive, Models, Biological, CCL5, 03 medical and health sciences, 0302 clinical medicine, Competitive, Chemokine CCL5/metabolism, Models, Receptors, Humans, Binding site, Receptor, Chemokine CCL5, 030304 developmental biology, HIV-1/metabolism, 0303 health sciences, biology, Chemistry, Articles, Binding, Ligand (biochemistry), Native chemical ligation, Biological, 3. Good health, Chemokines/metabolism, HEK293 Cells, Biochemistry, CCR5/metabolism, ddc:540, biology.protein, HIV-1, Bioorthogonal chemistry, Chemokines, 030217 neurology & neurosurgery, Protein Binding

Abstract

The chemokine receptor CCR5 is a drug target to prevent transmission of HIV/AIDS. We studied four analogs of the native chemokine regulated, on activation, normal T-cell-expressed, and secreted (RANTES) (CCL5) that have anti-HIV potencies of around 25 pM, which is more than four orders of magnitude higher than that of RANTES itself. It has been hypothesized that the ultrahigh potency of the analogs is due to their ability to bind populations of receptors not accessible to native chemokines. To test this hypothesis, we developed a homogeneous dual-color fluorescence cross-correlation spectroscopy assay for saturation- and competition-binding experiments. The fluorescence cross-correlation spectroscopy assay has the advantage that it does not rely on competition with radioactively labeled native chemokines used in conventional assays. We prepared site-specifically labeled fluorescent analogs using native chemical ligation of synthetic peptides, followed by bioorthogonal fluorescent labeling. We engineered a mammalian cell expression construct to provide fluorescently labeled CCR5, which was purified using a tandem immunoaffinity and size-exclusion chromatography approach to obtain monomeric fluorescent CCR5 in detergent solution. We found subnanomolar binding affinities for the two analogs 5P12-RANTES and 5P14-RANTES and about 20-fold reduced affinities for PSC-RANTES and 6P4-RANTES. Using homologous and heterologous competition experiments with unlabeled chemokine analogs, we conclude that the analogs all bind at the same binding site, whereas the native chemokines (RANTES and MIP-1α) fail to displace bound fluorescent analogs even at tens of micromolar concentrations. Our results can be rationalized with de novo structural models of the N-terminal tails of the synthetic chemokines that adopt a different binding mode as compared to the parent compound.

Published

2019

4. Enhancing Antitumor Immune Responses by Optimized Combinations of Cell-penetrating Peptide-based Vaccines and Adjuvants

Author

Madiha Derouazi, Else-Marit Suso-Inderberg, Hubert François Gaertner, Pierre-Yves Dietrich, Paul R. Walker, Wilma Di Berardino-Besson, Sébastien Wälchli, Oliver Hartley, Elodie Belnoue, Fabrice Cerini, Andres M. Salazar, Stéphane König, Susanna Carboni, and Isabelle Dunand-Sauthier

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, medicine.medical_treatment, Epitopes, T-Lymphocyte, Cell-Penetrating Peptides, CD8-Positive T-Lymphocytes, ddc:616.07, Biology, Cancer Vaccines, Epitope, Mice, 03 medical and health sciences, Transduction (genetics), Cross-Priming, Immune system, Adjuvants, Immunologic, Antigen, In vivo, Cell Line, Tumor, Neoplasms, Drug Discovery, Genetics, medicine, Animals, Humans, Cytotoxic T cell, Molecular Biology, ddc:616, Pharmacology, Circular Dichroism, Histocompatibility Antigens Class I, Vaccination, Histocompatibility Antigens Class II, Dendritic Cells, ddc:616.8, Disease Models, Animal, Treatment Outcome, 030104 developmental biology, Immunology, Trans-Activators, Cell-penetrating peptide, Cancer research, Molecular Medicine, Female, Original Article, Adjuvant

Abstract

Cell penetrating peptides (CPPs) from the protein ZEBRA are promising candidates to exploit in therapeutic cancer vaccines, since they can transport antigenic cargos into dendritic cells and induce tumor-specific T cells. Employing CPPs for a given cancer indication will require engineering to include relevant tumor-associated epitopes, administration with an appropriate adjuvant, and testing for antitumor immunity. We assessed the importance of structural characteristics, efficiency of in vitro transduction of target cells, and choice of adjuvant in inducing the two key elements in antitumor immunity, CD4 and CD8 T cells, as well as control of tumor growth in vivo. Structural characteristics associated with CPP function varied according to CPP truncations and cargo epitope composition, and correlated with in vitro transduction efficiency. However, subsequent in vivo capacity to induce CD4 and CD8 T cells was not always predicted by in vitro results. We determined that the critical parameter for in vivo efficacy using aggressive mouse tumor models was the choice of adjuvant. Optimal pairing of a particular ZEBRA-CPP sequence and antigenic cargo together with adjuvant induced potent antitumor immunity. Our results highlight the irreplaceable role of in vivo testing of novel vaccine constructs together with adjuvants to select combinations for further development.Molecular Therapy (2016); doi:10.1038/mt.2016.134.

Published

2016

5. Characterisation of preproendothelin-1 derived peptides identifies Endothelin-Like Domain Peptide as a modulator of Endothelin-1

Author

Amrita Ahluwalia, Irène Rossitto-Borlat, Elizabeth G. Wood, Pedro R. Cutillas, Jale Yuzugulen, Nimesh S. A. Patel, Hubert François Gaertner, Inmaculada C Villar, Roger Corder, Keith Rose, Oliver Hartley, James Jegard, and Julie A. Douthwaite

Subjects

0301 basic medicine, medicine.medical_specialty, Science, Peptide, ddc:616.07, 030204 cardiovascular system & hematology, Article, Cell Line, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Tandem Mass Spectrometry, Internal medicine, medicine, Humans, Protein Precursors, ddc:616, Heart Failure, chemistry.chemical_classification, A549 cell, Multidisciplinary, Endothelin-1, business.industry, Endothelial Cells, Biological activity, Endothelin 1, Peptide Fragments, 3. Good health, 030104 developmental biology, Endocrinology, chemistry, A549 Cells, Cell culture, Culture Media, Conditioned, Injections, Intravenous, Medicine, medicine.symptom, Endothelin receptor, business, Biomarkers, Vasoconstriction, Chromatography, Liquid

Abstract

Endothelin-1 (ET-1) is involved in the pathogenesis of cardiac and renal diseases, and in the progression of tumour growth in cancer, but current diagnosis and treatment remain inadequate. Peptides derived from the 212 amino acid precursor preproendothelin-1 (ppET-1) may have utility as biomarkers, or cause biological effects that are unaffected by endothelin receptor antagonists. Here, we used specific immunoassays and LC-MS/MS to identify NT-proET-1 (ppET-1[18–50]), Endothelin-Like Domain Peptide (ELDP, ppET-1[93–166]) and CT-proET-1 (ppET-1[169–212]) in conditioned media from cultured endothelial cells. Synthesis of these peptides correlated with ET-1, and plasma ELDP and CT-proET-1 were elevated in patients with chronic heart failure. Clearance rates of NT-proET-1, ELDP and CT-proET-1 were determined after i.v. injection in anaesthetised rats. CT-proET-1 had the slowest systemic clearance, hence providing a biological basis for it being a better biomarker of ET-1 synthesis. ELDP contains the evolutionary conserved endothelin-like domain sequence, which potentially confers biological activity. On isolated arteries ELDP lacked direct vasoconstrictor effects. However, it enhanced ET-1 vasoconstriction and prolonged the increase in blood pressure in anaesthetised rats. ELDP may therefore contribute to disease pathogenesis by augmenting ET-1 responses.

Published

2017

6. Definition of Human Apolipoprotein A-I Epitopes Recognized by Autoantibodies Present in Patients with Cardiovascular Diseases

Author

Hanno Langen, Michelle Butterfield, Oliver Hartley, Nicolas Vuilleumier, Paul Cutler, Priscila Camillo Teixeira, Sabrina Pagano, Axel Ducret, Philippe Ferber, and Hubert François Gaertner

Subjects

Apolipoprotein B, Myocardial Infarction, Gene Expression, ddc:616.07, 030204 cardiovascular system & hematology, Biochemistry, Chromatography, Affinity, Immunoglobulin G, Epitope, Epitopes, 0302 clinical medicine, Sequence Analysis, Protein, Cardiovascular Disease, polycyclic compounds, Epitopes/chemistry/immunology, 0303 health sciences, Plaque, Atherosclerotic, 3. Good health, Titer, Immunoglobulin G/biosynthesis/blood, lipids (amino acids, peptides, and proteins), Atherosclerosis/immunology, Autoantibodies/biosynthesis/blood, Protein Purification, Immunoreactive Peptides, Immunology, Molecular Sequence Data, Enzyme-Linked Immunosorbent Assay, Biology, Autoimmune Disease, 03 medical and health sciences, Mass Spectrometry (MS), medicine, Humans, Peptides/chemistry/immunology, Amino Acid Sequence, ddc:576, Molecular Biology, Autoantibodies, 030304 developmental biology, Anti-apolipoprotein A-I, Autoimmune disease, Apolipoprotein A-I/chemistry/immunology, Apolipoprotein A-I, Autoantibody, nutritional and metabolic diseases, Cell Biology, Atherosclerosis, medicine.disease, Epitope mapping, Polyclonal antibodies, biology.protein, Biological Markers/analysis, Plaque, Atherosclerotic/blood/diagnosis/immunology/pathology, Peptides, Biomarkers, Epitope Mapping, Myocardial Infarction/blood/diagnosis/immunology/pathology

Abstract

Background: Autoantibodies to apoA-I can be considered markers and mediators of cardiovascular disease. Results: Methodologies for identification of human apoA-I epitopes are described. Two novel immunoreactive peptides were recognized by autoantibodies from cardiac patients. Conclusion: We developed a new procedure to isolate, purify, and identify apoA-I epitopes. Significance: Developing new epitope mapping approaches opens new avenues for biomarkers and therapy., Autoantibodies to apolipoprotein A-I (anti-apoA-I IgG) have been shown to be both markers and mediators of cardiovascular disease, promoting atherogenesis and unstable atherosclerotic plaque. Previous studies have shown that high levels of anti-apoA-I IgGs are independently associated with major adverse cardiovascular events in patients with myocardial infarction. Autoantibody responses to apoA-I can be polyclonal and it is likely that more than one epitope may exist. To identify the specific immunoreactive peptides in apoA-I, we have developed a set of methodologies and procedures to isolate, purify, and identify novel apoA-I endogenous epitopes. First, we generated high purity apoA-I from human plasma, using thiophilic interaction chromatography followed by enzymatic digestion specifically at lysine or arginine residues. Immunoreactivity to the different peptides generated was tested by ELISA using serum obtained from patients with acute myocardial infarction and high titers of autoantibodies to native apoA-I. The immunoreactive peptides were further sequenced by mass spectrometry. Our approach successfully identified two novel immunoreactive peptides, recognized by autoantibodies from patients suffering from myocardial infarction, who contain a high titer of anti-apoA-I IgG. The discovery of these epitopes may open innovative prognostic and therapeutic opportunities potentially suitable to improve current cardiovascular risk stratification.

Published

2014

7. A novel µ-conopeptide, CnIIIC, exerts potent and preferential inhibition of NaV1.2/1.4 channels and blocks neuronal nicotinic acetylcholine receptors

Author

Philippe Favreau, Rolf Boelens, Jordi Molgó, Hubert François Gaertner, Daniel Bertrand, Jan Tytgat, Enrico Leipold, Henry G. Hocking, Ludovic Carlier, Dieter D' hoedt, Reto Stöcklin, Marco Cordova, Sébastien Schlumberger, René Markgraf, Oliver Hartley, Evelyne Benoit, Marianne Paolini-Bertrand, and Stefan H. Heinemann

Subjects

Pharmacology, 0303 health sciences, Sodium channel, 030302 biochemistry & molecular biology, Biology, Potassium channel, 3. Good health, 03 medical and health sciences, Nicotinic acetylcholine receptor, Nicotinic agonist, medicine, Biophysics, Conotoxin, Nicotinic Antagonist, medicine.symptom, Neuroscience, 030304 developmental biology, Acetylcholine receptor, Muscle contraction

Abstract

BACKGROUND AND PURPOSE The µ-conopeptide family is defined by its ability to block voltage-gated sodium channels (VGSCs), a property that can be used for the development of myorelaxants and analgesics. We characterized the pharmacology of a new µ-conopeptide (µ-CnIIIC) on a range of preparations and molecular targets to assess its potential as a myorelaxant. EXPERIMENTAL APPROACH µ-CnIIIC was sequenced, synthesized and characterized by its direct block of elicited twitch tension in mouse skeletal muscle and action potentials in mouse sciatic and pike olfactory nerves. µ-CnIIIC was also studied on HEK-293 cells expressing various rodent VGSCs and also on voltage-gated potassium channels and nicotinic acetylcholine receptors (nAChRs) to assess cross-interactions. Nuclear magnetic resonance (NMR) experiments were carried out for structural data. KEY RESULTS Synthetic µ-CnIIIC decreased twitch tension in mouse hemidiaphragms (IC50= 150 nM), and displayed a higher blocking effect in mouse extensor digitorum longus muscles (IC = 46 nM), compared with µ-SIIIA, µ-SmIIIA and µ-PIIIA. µ-CnIIIC blocked NaV1.4 (IC50= 1.3 nM) and NaV1.2 channels in a long-lasting manner. Cardiac NaV1.5 and DRG-specific NaV1.8 channels were not blocked at 1 µM. µ-CnIIIC also blocked the α3β2 nAChR subtype (IC50= 450 nM) and, to a lesser extent, on the α7 and α4β2 subtypes. Structure determination of µ-CnIIIC revealed some similarities to α-conotoxins acting on nAChRs. CONCLUSION AND IMPLICATIONS µ-CnIIIC potently blocked VGSCs in skeletal muscle and nerve, and hence is applicable to myorelaxation. Its atypical pharmacological profile suggests some common structural features between VGSCs and nAChR channels.

Published

2012

8. CC Chemokine Receptor 5 (CCR5) Desensitization

Author

Oliver Hartley, Gabriel Kuenzi, Michelangelo Foti, Jean-Michel Escola, and Hubert François Gaertner

Subjects

Receptor recycling, CCR1, 0303 health sciences, viruses, virus diseases, Cell Biology, Biology, CXCR3, Biochemistry, CCL5, 3. Good health, Cell biology, 03 medical and health sciences, Chemokine receptor, 0302 clinical medicine, Homologous desensitization, CC chemokine receptors, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology, G protein-coupled receptor

Abstract

CC chemokine receptor 5 (CCR5), the major HIV coreceptor, is a G protein-coupled receptor (GPCR) involved in cell activation and migration in response to chemokines. Blockade of CCR5 is an effective anti-HIV strategy, and potent anti-HIV chemokine analogs such as PSC-RANTES have been developed. These inhibitors act by interfering with receptor trafficking, thereby inducing prolonged intracellular sequestration of CCR5. Like many GPCRs, CCR5 is desensitized following agonist activation. The initial steps in this process are well understood, but later stages, including where CCR5 is sequestered during desensitization, and how anti-HIV chemokine analogs intervene to achieve prolonged sequestration, have yet to be elucidated in detail. In this study we demonstrate that CCR5 cycles to and from the cell surface via the endosome recycling compartment and the trans-Golgi network during desensitization, accumulating in the trans-Golgi network following internalization by both PSC-RANTES and CCL5, the native ligand from which it was derived. In addition, we show that unlike CCR5 sequestered by CCL5, CCR5 sequestered by PSC-RANTES cannot be induced to return to the cell surface by addition of the small molecule CCR5 inhibitor, TAK-779, and that association of PSC-RANTES with CCR5 is more durable than that of native CCL5 during desensitization. Our findings reconcile the previously conflicting descriptions of the location of sequestered CCR5 during desensitization, as well as providing more general insights into potential trafficking routes for endocytosed GPCRs and further elucidation of the unusual inhibitory mechanism of chemokine analogs with potent anti-HIV activity.

Published

2010

9. Highly potent HIV inhibition: engineering a key anti-HIV structure from PSC-RANTES into MIP-1 /CCL4

Author

Irene Borlat, Brigitte Dufour, Robin E. Offord, Richard J. Fish, Olivier Lebeau, Fabrice Cerini, Marc Parmentier, Gabriel Kuenzi, Astrid Melotti, Jean-Yves Springael, Hubert François Gaertner, and Oliver Hartley

Subjects

Chemokine, Anti-HIV Agents, Molecular Sequence Data, Human immunodeficiency virus (HIV), Bioengineering, CCL4, HIV/drug effects, medicine.disease_cause, digestive system, Biochemistry, CCL5, Structure-Activity Relationship, Chemokine CCL4/genetics/therapeutic use, medicine, Humans, Potency, ddc:610, Amino Acid Sequence, Chemokine CCL4, Chemokine CCL5, Molecular Biology, Cells, Cultured, biology, Anti hiv, digestive, oral, and skin physiology, HIV, virus diseases, hemic and immune systems, Ligand (biochemistry), Chemokine CCL5/genetics/therapeutic use, Virology, digestive system diseases, Anti-HIV Agents/chemical synthesis, Drug Design, biology.protein, Cells Cultured, Pharmacophore, Biotechnology

Abstract

The HIV coreceptor CCR5 is a validated target for both the prevention and therapy of HIV infection. PSC-RANTES, an N-terminally modified analogue of one of the natural chemokine ligands of CCR5 (RANTES/CCL5), is a potent inhibitor of HIV entry into target cells. Here, we set out to engineer the anti-HIV activity of PSC-RANTES into another natural CCR5 ligand (MIP-1beta/CCL4), by grafting into it the key N-terminal pharmacophore region from PSC-RANTES. We were able to identify MIP-1beta/CCL4 analogues that retain the receptor binding profile of MIP-1beta/CCL4, but acquire the very high anti-HIV potency and characteristic inhibitory mechanism of PSC-RANTES. Unexpectedly, we discovered that in addition to N-terminal structures from PSC-RANTES, the side chain of Lys33 is also necessary for full anti-HIV potency.

Published

2008

10. Generating Chemokine Analogs with Enhanced Pharmacological Properties Using Phage Display

Author

Fabrice Cerini, Guy Gorochov, Karim Dorgham, Irène Rossitto-Borlat, Hubert François Gaertner, Oliver Hartley, Astrid Melotti, Centre d'Immunologie et de Maladies Infectieuses (CIMI), Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Department of Structural Biology and Bioinformatics, Structural Biology and Bioinformatics, Department of Pathology and Immunology, and University of Geneva [Switzerland]

Subjects

0301 basic medicine, Library design, Chemokine, Phage display, [SDV.BIO]Life Sciences [q-bio]/Biotechnology, biology, [SDV]Life Sciences [q-bio], Receptor signaling, Computational biology, Bioinformatics, 03 medical and health sciences, 030104 developmental biology, CX3CR1, biology.protein, [SDV.IB]Life Sciences [q-bio]/Bioengineering, Peptide library, ComputingMilieux_MISCELLANEOUS

Abstract

Phage display technology, which allows extremely rare ligands to be selected from libraries of variants according to user-defined selection criteria, has made a huge impact on the life sciences. In this chapter, we describe phage display methods for the discovery of chemokine analogs with enhanced pharmacological properties. We discuss strategies for chemokine library design and provide a recommended technique for library construction. We also describe cell-based library selection approaches that we have used to discover chemokine analogs, not only receptor antagonists but also variants with unusual effects on receptor signaling and trafficking. By providing a survey of the different phage chemokine projects that we have undertaken, we comment on the parameters most likely to affect success. Finally, we discuss how phage display-derived chemokine analogs with altered pharmacological activity represent valuable tools to better understand chemokine biology, and why certain among them have the potential to be developed as new medicines.

Published

2016

11. A scalable low-cost cGMP process for clinical grade production of the HIV inhibitor 5P12-RANTES in Pichia pastoris

Author

Stephan B Abramson, Nico Callewaert, Ilya I. Tolstorukov, Michael M. Meagher, Jay C. Harner, Hubert François Gaertner, Anthony R Sump, Dustin J Peterson, Scott Brown, Robin E. Offord, Bram Laukens, Robert C Sealock, Knut Madden, Fabrice Cerini, Scott K. Johnson, John T Harms, Oliver Hartley, and Anna M. Oommen

Subjects

0106 biological sciences, 0301 basic medicine, Chemokine, PROTEIN, HIV Infections, Pilot Projects, ddc:616.07, Bioinformatics, 01 natural sciences, Pichia, Bioreactors, VAGINAL TRANSMISSION, PROTECTION, Chromatography, High Pressure Liquid, biology, virus diseases, ENTRY INHIBITORS, Chromatography, Ion Exchange, 3. Good health, Biopharmaceutical, CHEMOKINES, Chemokines, CC, 5P12-RANTES, Biotechnology, medicine.drug, EXPRESSION, Process development, Anti-HIV Agents, Microbicide, CCL5, Article, Pichia pastoris, RANTES, 03 medical and health sciences, Inhibitory Concentration 50, MICROBICIDES, 010608 biotechnology, medicine, Humans, HIGHLY POTENT, Biology and Life Sciences, HIV, Virus Internalization, biology.organism_classification, Yeast, Entry inhibitor, Microbicides for sexually transmitted diseases, cGMP, 030104 developmental biology, RHESUS MACAQUES, Immunology, Fermentation, biology.protein, CCR5

Abstract

In the continued absence of an effective anti-HIV vaccine, approximately 2 million new HIV infections occur every year, with over 95% of these in developing countries. Calls have been made for the development of anti-HIV drugs that can be formulated for topical use to prevent HIV transmission during sexual intercourse. Because these drugs are principally destined for use in low-resource regions, achieving production costs that are as low as possible is an absolute requirement. 5P12-RANTES, an analog of the human chemokine protein RANTES/CCL5, is a highly potent HIV entry inhibitor which acts by achieving potent blockade of the principal HIV coreceptor, CCR5. Here we describe the development and optimization of a scalable low-cost production process for 5P12-RANTES based on expression in Pichia pastoris. At pilot (150 L) scale, this cGMP compliant process yielded 30 g of clinical grade 5P12-RANTES. As well as providing sufficient material for the first stage of clinical development, this process represents an important step towards achieving production of 5P12-RANTES at a cost and scale appropriate to meet needs for topical HIV prevention worldwide., Highlights • New medicines are required to prevent the spread of HIV/AIDS in low-resource regions. • 5P12-RANTES, a chemokine analog, is a promising new candidate drug. • We describe a process for producing clinical grade cGMP 5P12-RANTES in Pichia pastoris. • This is a key step to achieving production at cost and scale appropriate for use worldwide.

Published

2016

12. Native Chemical Ligation through in Situ O to S Acyl Shift

Author

Matteo Villain, Sonia Manganiello, Paolo Botti, and Hubert François Gaertner

Subjects

In situ, Time Factors, Stereochemistry, Sulfuric Acid Esters, Ligands, Thioester, Sensitivity and Specificity, Biochemistry, Peptide bond, Molecule, Cysteine, Physical and Theoretical Chemistry, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Molecular Structure, Chemistry, Organic Chemistry, Hydrogen-Ion Concentration, Native chemical ligation, Amides, Combinatorial chemistry, Oxygen, lipids (amino acids, peptides, and proteins), Chemical ligation, Peptides, Ligation, Sulfur

Abstract

[reaction: see text] A novel strategy to generate thioester peptides compatible with Fmoc chemistry is presented. Peptide-C(alpha)oxy-(2-mercapto-1-carboxyamide)ethyl ester undergoes an O to S acyl shift during ligation and the newly formed thioester intermediate reacts with an N-terminal cysteine fragment generating a product with native amide bond at the ligation site.

Published

2004

13. Medicinal chemistry applied to a synthetic protein: Development of highly potent HIV entry inhibitors

Author

Jill Wilken, Robin E. Offord, Marc Alizon, Laurent Picard, Donald E. Mosier, Alejandra Ramos, Fabrice Cerini, Darren A. Thompson, Cristina Pastore, Nikolaus Heveker, Astrid Melotti, Brigitte Dufour, Oliver Hartley, Stephen J. Kent, Richard J. Fish, and Hubert François Gaertner

Subjects

CD4-Positive T-Lymphocytes, Receptors, CCR5, Anti-HIV Agents, Mononuclear/transplantation, HIV Infections, Anti-HIV Agents/chemical synthesis/chemistry/pharmacology, CHO Cells, Mice, SCID, ddc:616.07, Biology, Chemokine CCL5/analogs & derivatives/chemical synthesis/chemistry/pharmacology, SCID, Viral/blood, Chemical synthesis, Medicinal chemistry, HIV-1/drug effects/isolation & purification, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Cricetinae, Receptors, Leukocytes, Animals, Humans, Structure–activity relationship, Potency, ddc:576.5, CD4-Positive T-Lymphocytes/drug effects/immunology, ddc:576, Receptor, Chemokine CCL5, Multidisciplinary, Chinese hamster ovary cell, Biological Sciences, Small molecule, chemistry, CCR5/metabolism, HIV Infections/drug therapy/prevention & control/virology, Drug Design, HIV-1, Leukocytes, Mononuclear, RNA, RNA, Viral, Pharmacophore, Derivative (chemistry)

Abstract

We have used total chemical synthesis to perform high-resolution dissection of the pharmacophore of a potent anti-HIV protein, the aminooxypentane oxime of [glyoxylyl 1 ]RANTES(2-68), known as AOP–RANTES, of which we designed and made 37 analogs. All involved incorporation of one or more rationally chosen nonnatural noncoded structures, for which we found a clear comparative advantage over coded ones. We investigated structure–activity relationships in the pharmacophore by screening the analogs for their ability to block the HIV entry process and produced a derivative, PSC-RANTES { N -nonanoyl, des-Ser 1 [ l -thioproline 2 , l -cyclohexylglycine 3 ]-RANTES(2–68)}, which is 50 times more potent than AOP–RANTES. This promising group of compounds might be optimized yet further as potential prophylactic and therapeutic anti-HIV agents. The remarkable potency of our RANTES analogs probably involves the unusual mechanism of intracellular sequestration of CC-chemokine receptor 5 (CCR5), and it has been suggested that this arises from enhanced affinity for the receptor. We found that inhibitory potency and capacity to induce CCR5 down-modulation do appear to be correlated, but that unexpectedly, inhibitory potency and affinity for CCR5 do not. We believe this study represents the proof of principle for the use of a medicinal chemistry approach, above all one showing the advantage of noncoded structures, to the optimization of the pharmacological properties of a protein. Medicinal chemistry of small molecules is the foundation of modern pharmaceutical practice, and we believe we have shown that techniques have now reached the point at which the approach could also be applied to the many macromolecular drugs now in common use.

Published

2004

14. Industrial-scale proteomics: From liters of plasma to chemically synthesized proteins

Author

Jacques Colinge, Andrew Johnson, Keith Rose, Cedric Saudrais, Matteo Villain, Denise Hochstrasser, Frederic Ranno, Isabelle Cusin, Manfred Heller, Günter Böhm, Anne Gleizes, Paolo Botti, Thierry Baussant, Silvia Jimenez, Laure Menin, Lydie Bougueleret, Christoph Menzel, Hubert François Gaertner, Amos Marc Bairoch, John Rogers, Martin Kussmann, Diana Wetmore, and Patricia Rodriguez-Tomé

Subjects

Proteomics, Time Factors, Electrophoresis, Gel, Two-Dimensional/methods, Proteome, Molecular Sequence Data, Blood Proteins/metabolism, Blood Chemical Analysis/methods, Peptide, Peptides/chemistry, Biochemistry, Mass Spectrometry, Plasma, Humans, Electrophoresis, Gel, Two-Dimensional, Trypsin, Amino Acid Sequence, ddc:576, Molecular Biology, Peptide sequence, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Chromatography, Albumin, Computational Biology, Blood Proteins, Chromatography, Ion Exchange, Plasma/metabolism, Matrix-assisted laser desorption/ionization, Databases as Topic, chemistry, Immunoglobulin G/chemistry, Immunoglobulin G, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Trypsin/pharmacology, Chromatography, Gel, Bottom-up proteomics, Proteomics/methods, Peptides, Digestion, Blood Chemical Analysis, Subcellular Fractions

Abstract

Human blood plasma is a useful source of proteins associated with both health and disease. Analysis of human blood plasma is a challenge due to the large number of peptides and proteins present and the very wide range of concentrations. In order to identify as many proteins as possible for subsequent comparative studies, we developed an industrial-scale (2.5 liter) approach involving sample pooling for the analysis of smaller proteins (M(r) generally < ca. 40 000 and some fragments of very large proteins). Plasma from healthy males was depleted of abundant proteins (albumin and IgG), then smaller proteins and polypeptides were separated into 12 960 fractions by chromatographic techniques. Analysis of proteins and polypeptides was performed by mass spectrometry prior to and after enzymatic digestion. Thousands of peptide identifications were made, permitting the identification of 502 different proteins and polypeptides from a single pool, 405 of which are listed here. The numbers refer to chromatographically separable polypeptide entities present prior to digestion. Combining results from studies with other plasma pools we have identified over 700 different proteins and polypeptides in plasma. Relatively low abundance proteins such as leptin and ghrelin and peptides such as bradykinin, all invisible to two-dimensional gel technology, were clearly identified. Proteins of interest were synthesized by chemical methods for bioassays. We believe that this is the first time that the small proteins in human blood plasma have been separated and analyzed so extensively.

Published

2004

15. Native Chemical Ligation with Aspartic and Glutamic Acids asC-Terminal Residues: Scope and Limitations

Author

Paolo Botti, Hubert François Gaertner, and Matteo Villain

Subjects

chemistry.chemical_classification, Stereochemistry, Organic Chemistry, Side reaction, Thioester, Phenacyl, Native chemical ligation, Residue (chemistry), chemistry.chemical_compound, chemistry, Peptide synthesis, Chemical ligation, Physical and Theoretical Chemistry, Protecting group

Abstract

A new side reaction during Native Chemical Ligation (NCL) at aspartic and glutamic acid/cysteine ligation sites is reported. To exploit NCL at these sites, test peptides having either a C-terminal unprotected aspartyl or glutamyl thioester were ligated with a peptide containing an N-terminal free cysteine generating, in each case, two major compounds having equal masses but different retention times by HPLC analysis. Comparison of these ligation products with reference peptides of identical sequence synthesized by total SPPS (solid phase peptide synthesis) with both natural and unnatural backbones at the cysteinyl residue is in agreement with the hypothesis of migration of the thioester moiety on the side chain carboxyl group of both C-terminal Asp and Glu residues. Enzymatic digestion of the purified ligation products with a V8-protease further confirmed the nature of the side reaction, with a total resistance of the non-natural backbone peptide to the protease. To overcome this problem the use of a protecting group stable to both HF cleavage and ligation conditions, but removable after ligation, became a necessity. A series of side-chain protected derivatives were selected, specifically 9-fluorenylmethyl ester (OFm), (phenylsulfonyl)ethyl ester (OPse), 2,2,2-trichloroethyl ester (OTce), and phenacyl esters (OPac). For the glutamic acid, OPse gave the best results, generating the correct peptide and avoiding the isomerization at the γ-carboxyl group. In the case of the aspartic residue, all the protecting groups were removed under basic conditions, worsening the problem and generating, for example, 70% yield of the β-isomer after OFm deprotection. This prompted us to propose a protecting group derived from the phenacyl ester 1-methyl-2-oxo-2-phenylethyl ester (OMop). This protecting group showed greater stability during the ligation reaction than OPac and OTce, and was easily removed by Zn/acetic acid reduction after the ligation step. (© Wiley-VCH Verlag GmbH & Co. KGaA, 69451 Weinheim, Germany, 2003)

Published

2003

16. Human Immunodeficiency Virus Type 1 Entry Inhibitors Selected on Living Cells from a Library of Phage Chemokines

Author

Robin E. Offord, Oliver Hartley, Anouk Heimann, Karim Dorgham, Danielle Perez-Bercoff, Fabrice Cerini, Guy Gorochov, Hubert François Gaertner, Gianfranco Pancino, and Patrice Debré

Subjects

CCR1, Chemokine, Receptors, CCR5, Anti-HIV Agents, Chemokine receptor CCR5, Immunology, CCR3, CHO Cells, C-C chemokine receptor type 6, ddc:616.07, Membrane Fusion/drug effects, Chemokine CCL5/analogs & derivatives/genetics/pharmacology, Binding, Competitive, Membrane Fusion, Microbiology, CXCR4, CCL5, Cell Line, Chemokine receptor, Competitive, Peptide Library, Cricetinae, Virology, Anti-HIV Agents/pharmacology, Receptors, Vaccines and Antiviral Agents, Animals, Humans, ddc:576, Chemokines/genetics/pharmacology, Chemokine CCL5, biology, Binding, Molecular biology, CCR5/metabolism, Insect Science, Mutation, HIV-1, biology.protein, Chemokines, HIV-1/drug effects/pathogenicity

Abstract

The chemokine receptors CCR5 and CXCR4 are promising non-virus-encoded targets for human immunodeficiency virus (HIV) therapy. We describe a selection procedure to isolate mutant forms of RANTES (CCL5) with antiviral activity considerably in excess of that of the native chemokine. The phage-displayed library of randomly mutated and N-terminally extended variants was screened by using live CCR5-expressing cells, and two of the selected mutants, P1 and P2, were further characterized. Both were significantly more potent HIV inhibitors than RANTES, with P2 being the most active (50% inhibitory concentration of 600 pM in a viral coat-mediated cell fusion assay, complete protection of target cells against primary HIV type 1 strains at a concentration of 10 nM). P2 resembles AOP-RANTES in that it is a superagonist of CCR5 and potently induces receptor sequestration. P1, while less potent than P2, has the advantage of significantly reduced signaling activity via CCR5 (30% of that of RANTES). Additionally, both P1 and P2 exhibit not only significantly increased affinity for CCR5 but also enhanced receptor selectivity, retaining only trace levels of signaling activity via CCR1 and CCR3. The phage chemokine approach that was successfully applied here could be adapted to other chemokine-chemokine receptor systems and used to further improve the first-generation mutants reported in this paper.

Published

2003

17. The Human Autoantibody Response to Apolipoprotein A-I Is Focused on the C-Terminal Helix: A New Rationale for Diagnosis and Treatment of Cardiovascular Disease?

Author

Sabrina Pagano, Nicolas Vuilleumier, Tiphaine Mannic, Paul Cutler, Priscila Camillo Teixeira, Nathalie Satta, François Mach, Hubert François Gaertner, Fabrice Cerini, and Oliver Hartley

Subjects

Apolipoprotein B, Molecular Sequence Data, lcsh:Medicine, Disease, ddc:616.07, 030204 cardiovascular system & hematology, Protein Engineering, Bioinformatics, Protein Structure, Secondary, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, polycyclic compounds, Medicine, Humans, Amino Acid Sequence, ddc:576, Interleukin 6, lcsh:Science, 030304 developmental biology, Autoantibodies, Cause of death, 0303 health sciences, Multidisciplinary, Apolipoprotein A-I, biology, business.industry, Interleukin-6, Tumor Necrosis Factor-alpha, Circular Dichroism, lcsh:R, Autoantibody, 3. Good health, Immobilized Proteins, Terminal (electronics), Cardiovascular Diseases, Immunoglobulin G, Helix, Risk stratification, Immunology, biology.protein, AUTOANTIBODY RESPONSE, lipids (amino acids, peptides, and proteins), lcsh:Q, Inflammation Mediators, Cardiology and Cardiovascular Medicine, business, Peptides, Research Article

Abstract

Background Cardiovascular disease (CVD) is the leading cause of death worldwide and new approaches for both diagnosis and treatment are required. Autoantibodies directed against apolipoprotein A-I (ApoA-I) represent promising biomarkers for use in risk stratification of CVD and may also play a direct role in pathogenesis. Methodology To characterize the anti-ApoA-I autoantibody response, we measured the immunoreactivity to engineered peptides corresponding to the different alpha-helical regions of ApoA-I, using plasma from acute chest pain cohort patients known to be positive for anti-ApoA-I autoantibodies. Principal Findings Our results indicate that the anti-ApoA-I autoantibody response is strongly biased towards the C-terminal alpha-helix of the protein, with an optimized mimetic peptide corresponding to this part of the protein recapitulating the diagnostic accuracy for an acute ischemic coronary etiology (non-ST segment elevation myocardial infarction and unstable angina) obtainable using intact endogenous ApoA-I in immunoassay. Furthermore, the optimized mimetic peptide strongly inhibits the pathology-associated capacity of anti-ApoA-I antibodies to elicit proinflammatory cytokine release from cultured human macrophages. Conclusions In addition to providing a rationale for the development of new approaches for the diagnosis and therapy of CVD, our observations may contribute to the elucidation of how anti-ApoA-I autoantibodies are elicited in individuals without autoimmune disease.

Published

2015

18. δ-Conotoxins synthesized using an acid-cleavable solubility tag approach reveal key structural determinants for NaV subtype selectivity

Author

Hubert François Gaertner, Philippe Favreau, Marianne Paolini-Bertrand, Daniel Biass, Steve Peigneur, Aude Violette, Oliver Hartley, Jan Tytgat, and Reto Stöcklin

Subjects

Voltage-Gated Sodium Channels, ddc:616.07, Biochemistry, Chemical synthesis, Xenopus laevis, Protein Isoforms, Conotoxin, Disulfides, Peptide sequence, Chromatography, High Pressure Liquid, biology, Chemistry, Peptide chemical synthesis, Molecular Pharmacology, musculoskeletal system, 3. Good health, Protein Structure and Folding, Female, Ion Channel Gating, Conotoxins/chemical synthesis/chemistry/pharmacology, Conus Snail/chemistry, Spectrometry, Mass, Electrospray Ionization, Stereochemistry, Oocytes/drug effects/metabolism/physiology, Molecular Sequence Data, complex mixtures, Protein Isoforms/genetics/physiology, Structure-Activity Relationship, Ion Channel Gating/drug effects/genetics/physiology, Peptide Fragments/chemical synthesis/chemistry/pharmacology, parasitic diseases, Structure–activity relationship, Animals, Amino Acid Sequence, ddc:576, Molecular Biology, Ion channel, Voltage-Gated Sodium Channels/genetics/physiology, Dose-Response Relationship, Drug, fungi, Conus Snail, Cell Biology, Acids/chemistry, biology.organism_classification, Peptide Fragments, nervous system, Solubility, Conus consors, Oocytes, Conotoxins, Acids, Disulfides/chemistry

Abstract

Conotoxins are venom peptides from cone snails with multiple disulfide bridges that provide a rigid structural scaffold. Typically acting on ion channels implicated in neurotransmission, conotoxins are of interest both as tools for pharmacological studies and as potential new medicines. δ-Conotoxins act by inhibiting inactivation of voltage-gated sodium channels (Nav). Their pharmacology has not been extensively studied because their highly hydrophobic character makes them difficult targets for chemical synthesis. Here we adopted an acid-cleavable solubility tag strategy that facilitated synthesis, purification, and directed disulfide bridge formation. Using this approach we readily produced three native δ-conotoxins from Conus consors plus two rationally designed hybrid peptides. We observed striking differences in Nav subtype selectivity across this group of compounds, which differ in primary structure at only three positions: 12, 23, and 25. Our results provide new insights into the structure-activity relationships underlying the Nav subtype selectivity of δ-conotoxins. Use of the acid-cleavable solubility tag strategy should facilitate synthesis of other hydrophobic peptides with complex disulfide bridge patterns.

Published

2014

19. Multi-Color, Single-Molecule Fluorescence Imaging of GPCR Signalosomes

Author

Thomas Huber, Alexandre Fürstenberg, He Tian, Oliver Hartley, Thomas P. Sakmar, and Hubert François Gaertner

Subjects

0303 health sciences, Chemokine, biology, Kinase, Chemokine receptor CCR5, media_common.quotation_subject, Biophysics, 010402 general chemistry, 01 natural sciences, CCL5, 0104 chemical sciences, 3. Good health, 03 medical and health sciences, Biochemistry, Cell surface receptor, biology.protein, Receptor, Internalization, 030304 developmental biology, G protein-coupled receptor, media_common

Abstract

G protein-coupled receptors (GPCRs) are the largest superfamily of membrane receptors in the human genome and they are targets for a quarter of all prescription drugs. Activation of a GPCR by an agonist ligand results in G protein-mediated downstream signaling, followed by kinase action and arrestin-mediated desensitization, internalization/sequestration, and recycling. Selective manipulation of these individual steps of the GPCR activation cycle is often desired when creating drugs targeting a given receptor. We are interested in the C-C chemokine receptor CCR5 that is the major HIV coreceptor used in person-to-person transmission. Globally, the HIV/AIDS pandemic has caused nearly 30 million deaths and a similar number of people are currently infected. Certain analogues of the chemokine RANTES/CCL5 are highly potent entry inhibitors against R5-tropic HIV-1 strains, in vitro and in vivo. Three such analogues, 5P12-, 5P14-, and 6P4-RANTES, are particularly interesting because while they differ only slightly in structure they show strikingly different pharmacological profiles (G protein-linked signaling activity, stimulation of receptor internalization). We have recently developed a general, simple, and robust method for stoichiometric, site-specific fluorescence labeling of expressed GPCRs. The method is based on bioorthogonal conjugation of a fluorescent reporter group to a genetically encoded azido group introduced into expressed GPCRs using amber codon suppression.[1] We have adopted a similar strategy for fluorescent labeling of chemokines with azido groups introduced by chemical synthesis. Here we present our progress towards automated, multi-color, single-molecule fluorescence studies of the compositional and conformational dynamics of GPCR signaling complexes ("signalosomes") using fluorescently labeled chemokines and receptors in biochemically defined systems.[1] H Tian, TP Sakmar, & T Huber (2013) Site-specific labeling of genetically encoded azido groups for multi-color, single-molecule fluorescence imaging of GPCRs. Methods in Cell Biology, 117, in press.

Published

2014

20. Synthesis of a thioester linker precursor for a general preparation of peptide C-terminal thioacids

Author

Matteo Villain, Paolo Botti, Lynne Canne, and Hubert François Gaertner

Subjects

chemistry.chemical_classification, Organic Chemistry, Peptide, Thioester, Biochemistry, Combinatorial chemistry, Phenoxyacetic acid, chemistry.chemical_compound, chemistry, Reagent, Drug Discovery, Thiol, Peptide synthesis, Linker

Abstract

A general procedure to prepare peptide thioacids by solid-phase peptide synthesis is presented. The method involves the synthesis of 4-[α-( S -acetyl)mercaptobenzyl]phenoxyacetic acid as general precursor. This reagent once attached to a solid support is derivatized with the Boc-amino acid of choice after deprotection of the thiol.

Published

2004

21. Alteration of Synaptic Network Dynamics by the Intellectual Disability Protein PAK3

Author

Yann Bernardinelli, Bernadett Boda, Gaëlle Combeau, Hubert François Gaertner, Aline Dubos, Jean-Vianney Barnier, Oliver Hartley, Dominique Muller, Department of Basic Neurosciences, Faculty of Medicine, University of Geneva, Centre de Neurosciences Paris-Sud (CNPS), Université Paris-Sud - Paris 11 (UP11)-Centre National de la Recherche Scientifique (CNRS), Department of Pathology and Immunology, University of Geneva [Switzerland], and Centre National de la Recherche Scientifique (CNRS)-Université Paris-Sud - Paris 11 (UP11)

Subjects

[SDV.NEU.NB]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Neurobiology, CDC42, ddc:616.07, Gene mutation, Biology, medicine.disease_cause, Synaptic Transmission, 03 medical and health sciences, Mice, 0302 clinical medicine, Organ Culture Techniques, Intellectual Disability, Intellectual disability, medicine, Animals, Humans, Learning, Small GTPase, Intellectual Disability/genetics/metabolism/physiopathology, 030304 developmental biology, P21-Activated Kinases/deficiency/genetics, 0303 health sciences, Mutation, [SDV.NEU.PC]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Psychology and behavior, Kinase, Effector, General Neuroscience, [SDV.NEU.SC]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Cognitive Sciences, Learning/physiology, Articles, medicine.disease, ddc:616.8, Rats, Spine (zoology), Nerve Net/abnormalities/metabolism/physiopathology, p21-Activated Kinases, Synaptic Transmission/genetics, Nerve Net, Neuroscience, 030217 neurology & neurosurgery, HeLa Cells

Abstract

International audience; Several gene mutations linked to intellectual disability in humans code for synaptic molecules implicated in small GTPase signaling. This is the case of the Rac/Cdc42 effector p21-activated kinase 3 (PAK3). The mechanisms responsible for the intellectual defects and the consequences of the mutation on the development and wiring of brain networks remain unknown. Here we show that expression of PAK3 mutants, suppression of PAK3, or inhibition of PAK3 function in rat hippocampal slice cultures interfere with activity-mediated spine dynamics. Inhibition of PAK3 resulted in two main alterations: (1) an increased growth of new, unstable spines, occurring in clusters, and mediated by activity; and (2) an impairment of plasticity-mediated spine stabilization interfering with the formation of persistent spines. Additionally, we find that PAK3 is specifically recruited by activity from dendrites into spines, providing a new mechanism through which PAK3 could participate in the control of both spine stabilization and local spine growth. Together, these data identify a novel function of PAK3 in regulating activity-mediated rearrangement of synaptic connectivity associated with learning and suggest that defects in spine formation and refinement during development could account for intellectual disability.

Published

2012

22. Chemo-enzymic backbone engineering of proteins. Site-specific incorporation of synthetic peptides that mimic the 64-74 disulfide loop of granulocyte colony-stimulating factor

Author

D Timms, R Camble, R Cotton, Hubert François Gaertner, Keith Rose, and Robin E. Offord

Subjects

Stereochemistry, Chemistry, C-terminus, Chemical modification, Biological activity, Cell Biology, Hydrazide, Biochemistry, Chemical synthesis, law.invention, Serine, chemistry.chemical_compound, law, Recombinant DNA, Molecular Biology, Function (biology)

Abstract

We present the concept of chemo-enzymic backbone engineering of proteins. Recombinant DNA techniques are used to produce appropriate proteins that are enzymically fragmented to give the starting materials. These fragments are modified specifically at their chain termini either enzymically (coupling of a hydrazide to the C terminus) or chemically (periodate oxidation of N-terminal serine to a glyoxylyl function). The modified fragments, which need no side protection whatever, are mixed together and religate themselves spontaneously under mild conditions. The hydrazone bond thus formed can be reduced if desired, which stabilizes the linkage and enhances the flexibility of the local conformation. In this way biologically or chemically derived structures can be incorporated into the protein, and the choice of the chemical ones is free of all of the constraints of the genetic code. We believe that this combined approach gives access to constructions that could not be derived by either recombinant or chemical methods alone. We illustrate the particularity of this concept by the engineered modifications of the 64-74 disulfide loop region of human granulocyte colony-stimulating factor. Analogs constructed include one which, in spite of having a nonpeptide link in its backbone, has full biological activity.

Published

1994

23. Highly potent, fully recombinant anti-HIV chemokines: Reengineering a low-cost microbicide

Author

Gabriel Kuenzi, Irène Rossitto-Borlat, Astrid Melotti, Jean-Michel Escola, Donald E. Mosier, Guy Gorochov, Oliver Hartley, Hubert François Gaertner, Robin E. Offord, Fabrice Cerini, Rebecca Nedellec, and Janelle R. Salkowitz

Subjects

Agonist, Chemokine, Receptors, CCR5, medicine.drug_class, media_common.quotation_subject, Leukocytes, Mononuclear/drug effects/virology, Antiviral Agents/pharmacology, Biology, Pharmacology, HIV/drug effects, Protein Engineering, Endocytosis/drug effects, Antiviral Agents, law.invention, Anti-Infective Agents, law, Microbicide, Signal Transduction/drug effects, Receptors, Virus/metabolism, medicine, Potency, Humans, ddc:576, Recombinant Proteins/pharmacology, Internalization, Chemokine CCL5, Anti-Infective Agents/economics/pharmacology, media_common, Multidisciplinary, Chemokine CCL5/chemistry, Receptors, CCR5/metabolism, virus diseases, HIV, Reproducibility of Results, Biological Sciences, Endocytosis, Recombinant Proteins, Entry inhibitor, Hela Cells, Recombinant DNA, biology.protein, Leukocytes, Mononuclear, Receptors, Virus, Chemokines/pharmacology, Signal transduction, Chemokines, medicine.drug, HeLa Cells, Signal Transduction

Abstract

New prevention strategies for use in developing countries are urgently needed to curb the worldwide HIV/AIDS epidemic. The N-terminally modified chemokine PSC-RANTES is a highly potent entry inhibitor against R5-tropic HIV-1 strains, with an inhibitory mechanism involving long-term intracellular sequestration of the HIV coreceptor, CCR5. PSC-RANTES is fully protective when applied topically in a macaque model of vaginal HIV transmission, but it has 2 potential disadvantages related to further development: the requirement for chemical synthesis adds to production costs, and its strong CCR5 agonist activity might induce local inflammation. It would thus be preferable to find a recombinant analogue that retained the high potency of PSC-RANTES but lacked its agonist activity. Using a strategy based on phage display, we set out to discover PSC-RANTES analogs that contain only natural amino acids. We sought molecules that retain the potency and inhibitory mechanism of PSC-RANTES, while trying to reduce CCR5 signaling to as low a level as possible. We identified 3 analogues, all of which exhibit in vitro potency against HIV-1 comparable to that of PSC-RANTES. The first, 6P4-RANTES, resembles PSC-RANTES in that it is a strong agonist that induces prolonged intracellular sequestration of CCR5. The second, 5P12-RANTES, has no detectable G protein-linked signaling activity and does not bring about receptor sequestration. The third, 5P14-RANTES, induces significant levels of CCR5 internalization without detectable G protein-linked signaling activity. These 3 molecules represent promising candidates for further development as topical HIV prevention strategies.

Published

2008

24. Semisynthetic analogues of PSC-RANTES, a potent anti-HIV protein

Author

Robin E. Offord, Oliver Hartley, Hubert François Gaertner, Gabriel Kuenzi, and Paolo Botti

Subjects

Spectrometry, Mass, Electrospray Ionization, Stereochemistry, HIV Fusion Inhibitors/pharmacology, Thiazolidine, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Hydrazide, Chemical synthesis, chemistry.chemical_compound, HIV Fusion Inhibitors, Microbicide, medicine, Peptide bond, Humans, Chromatography High Pressure Liquid, ddc:610, ddc:576, Chemokine CCL5, Chromatography, High Pressure Liquid, Pharmacology, Chemistry, Organic Chemistry, Combinatorial chemistry, Semisynthesis, Entry inhibitor, Hela Cells, Chemokine CCL5/chemistry/pharmacology, Spectrometry Mass Electrospray Ionization, Linker, Biotechnology, medicine.drug, HeLa Cells

Abstract

New HIV prevention methods are needed, and among those currently being explored are "microbicides", substances applied topically to prevent HIV acquisition during sexual intercourse. The chemokine analogue PSC-RANTES (N(alpha)(n-nonanoyl)-des-Ser(1)-[ L-thioprolyl(2), L-cyclohexylglycyl(3)]-RANTES(4-68)) is a highly potent HIV entry inhibitor which has shown promising efficacy in its initial evaluation as a candidate microbicide. However, a way must be found to produce the molecule by cheaper means than total chemical synthesis. Since the only noncoded structures are located at the N-terminus, a possible solution would be to produce a protein fragment representing all but the N-terminal region using low-cost recombinant production methods and then to attach, site specifically, a short synthetic fragment containing the noncoded N-terminal structures. Here, we describe the evaluation of a range of different conjugation chemistries in order to identify those with potential for development as economical routes to production of a PSC-RANTES analogue with antiviral activity as close as possible to that of the parent protein. The strategies tested involved linkage through oxime, hydrazone/hydrazide, and Psi[CH2-NH] bonds, as well as through a peptide bond obtained either by a thiazolidine rearrangement or by direct alpha-amino acylation of a protein fragment in which 4 of the 5 lysine residues of the native sequence were replaced by arginine (the fifth lysine is essential for activity). Where conjugation involved replacement of one or more residues with a linker moiety, the point in the main chain at which the linker was introduced was varied. The resulting panel of 22 PSC-RANTES analogues was evaluated for anti-HIV activity in an entry inhibition assay. The [Arg (25,45,56,57)] PSC-RANTES analogue has comparable potency to PSC-RANTES, and one of the oxime linked analogues, 4L-57, has potency only 5-fold lower, with scope for improvement. Both represent promising leads for development as microbicide compounds that could be produced at low cost via semisynthesis.

Published

2008

25. The venom of the snake genus Atheris contains a new class of peptides with clusters of histidine and glycine residues

Author

Philippe Favreau, Philippe Bulet, Olivier Cheneval, André Ménez, Laure Menin, Franck Principaud, Hubert François Gaertner, Robert Thai, Reto Stöcklin, Sophie Michalet, Atheris Laboratories, Département d'Ingénierie et d'Etudes des Protéines, Commissariat à l'énergie atomique et aux énergies alternatives (CEA), and CEN/Saclay

Subjects

Spectrometry, Mass, Electrospray Ionization, Atheris, MESH: Sequence Analysis, Protein, Molecular Sequence Data, MESH: Viperidae, Glycine, Venom, MESH: Amino Acid Sequence, Viper Venoms, Tandem mass spectrometry, MESH: Peptide Mapping, MESH: Spectrometry, Mass, Electrospray Ionization, Peptide Mapping, Analytical Chemistry, MESH: Histidine, Protein sequencing, Viperidae, Sequence Analysis, Protein, biology.animal, Consensus sequence, Animals, MESH: Animals, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Histidine, Amino Acid Sequence, Spectroscopy, MESH: Molecular Sequence Data, biology, Edman degradation, MESH: Peptides, Chemistry, Organic Chemistry, De novo peptide sequencing, biology.organism_classification, MESH: Glycine, MESH: Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Biochemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, MESH: Viper Venoms, Peptides

Abstract

We investigated venoms from members of the genus Atheris (Serpentes, Viperidae), namely the rough scale bush viper (Atheris squamigera), the green bush viper (A. chlorechis) and the great lakes bush viper (A. nitschei), using mass spectrometry-based strategies, relying on matrix-assisted laser desorption/ionisation time-of-flight mass spectrometry (MALDI-TOF-MS) and electrospray ionisation tandem mass spectrometry (ESI-MS/MS) with de novo peptide sequencing. We discovered a set of novel peptides with masses in the 2-3 kDa range and containing poly-His and poly-Gly segments (pHpG). Complete primary structural elucidation and confirmation of two sequences by Edman degradation indicated the consensus sequence EDDH(9)GVG(10). Bioinformatic investigations in protein sequence databanks did not show relevant homology with known peptides or proteins. However, a more extensive investigation of data in nucleic acid databases revealed some similarities to the precursor sequences of bradykinin potentiating peptides (BPP) and C-type natriuretic peptides (CNP), agents that are known to affect the cardiovascular system by acting on specific metalloproteases and receptors. The novel pHpG peptides found in Atheris venoms might also act on the cardiovascular system by inhibiting particular metalloproteases, which however remain to be identified.

Published

2007

26. In vitro and in silico processes to identify differentially expressed proteins

Author

Stéphanie Carraud, Anne Niknejad, Patricia Rodriguez-Tomé, Nicolas Budin, Irène Fasso, Matteo Villain, Sophie Lagache, Abderrahim Karmime, Nicolas Pinaud, Marianne Paolini, Hassan Mattou, Nicolas Christmann, Eve Mahe, Nicolas Barrillat, Nadia Allet, Sylvain Raimondi, Lydie Bougueleret, Thierry Baussant, Paolo Botti, Camille Schmidt, Frederic Ranno, Cedric Saudrais, Denis Canet, Gerald Rossellat, Anne Gleizes, Nicolas Dafflon, Frédéric Perret, Benoît Depresle, Catherine Jeandenans, Pierre-Olivier Regamey, Samia Reffas, Celia Boiteau, Keith Rose, Hubert François Gaertner, Pascal Frauchiger, Isabelle Cusin, Jacques Colinge, Eduardo Gonzalez-Couto, Marc Moniatte, Alexandre Masselot, Diego Chiappe, Thomas Kowall, Pierre-Antoine Rey, and Catherine Zwahlen

Subjects

Proteomics, Databases, Factual, Information Management, In silico, Sample (statistics), Biology, computer.software_genre, Biochemistry, Plot (graphics), Mass Spectrometry, Set (abstract data type), User-Computer Interface, Humans, Molecular Biology, Expressed sequence tag, Data processing, Chromatography, Gene Expression Profiling, Computational Biology, Proteins, Reproducibility of Results, Body Fluids, Identification (information), Data mining, Peptides, computer

Abstract

We present an integrated proteomics platform designed for performing differential analyses. Since reproducible results are essential for comparative studies, we explain how we improved reproducibility at every step of our laboratory processes, e.g. by taking advantage of the powerful laboratory information management system we developed. The differential capacity of our platform is validated by detecting known markers in a real sample and by a spiking experiment. We introduce an innovative two-dimensional (2-D) plot for displaying identification results combined with chromatographic data. This 2-D plot is very convenient for detecting differential proteins. We also adapt standard multivariate statistical techniques to show that peptide identification scores can be used for reliable and sensitive differential studies. The interest of the protein separation approach we generally apply is justified by numerous statistics, complemented by a comparison with a simple shotgun analysis performed on a small volume sample. By introducing an automatic integration step after mass spectrometry data identification, we are able to search numerous databases systematically, including the human genome and expressed sequence tags. Finally, we explain how rigorous data processing can be combined with the work of human experts to set high quality standards, and hence obtain reliable (false positive < 0.35%) and nonredundant protein identifications.

Published

2004

27. Synthesis and evaluation of fluorescent chemokines labeled at the amino terminal

Author

Timothy N. C. Wells, Robin E. Offord, Amanda E. I. Proudfoot, and Hubert François Gaertner

Subjects

Chemokine, Fluorophore, biology, Chemistry, Fluorescence, law.invention, Proinflammatory cytokine, chemistry.chemical_compound, Biochemistry, Confocal microscopy, law, biology.protein, Side chain, Moiety, Conjugate

Abstract

Publisher Summary Chemokines are a rapidly growing family of proinflammatory cytokines that are involved in cell recruitment and activation. This chapter observes the direct binding of chemokines by techniques such as fluorescence activated cell sorting (FACS) analysis and confocal microscopy. Binding with fluorescent ligands has been limited to the commercially available phycoerythrin-IL-8 conjugate, which consists of the addition of a relatively large fluorescent moiety of 240 kDa attached to the 8-kDa protein through its side chains. Such a conjugate is many times larger than the chemokine itself, and because there are so many side chains available for conjugation, the product is likely to be a mixture of structural isomers. Therefore a highly controlled, site-specific reaction is sought to attach fluorophores to the polypeptide chain to ensure that each chain had one fluorophore, always at the same, chosen position in the chain. The chemical reactions involved had to be efficient and, so as not to compromise the biological behavior of the products, had to take place under mild, aqueous conditions.

Published

1997

28. Characterisation of the 'Endothelin-Like Domain Peptide' (ELDP) co-synthesised with Endothelin-1 from the EDN1 gene

Author

S A Nimesh, Irène Rossitto-Borlat, Roger Corder, Jale Yuzugulen, Oliver Hartley, Patel, Inmaculada C Villar, Keith Rose, Amrita Ahluwalia, James Jegard, Pedro R. Cutillas, Hubert François Gaertner, Elizabeth G. Wood, Julie A. Douthwaite, and Alexander Montoya

Subjects

chemistry.chemical_classification, Pharmacology, Toxicology and Pharmaceutics(all), Biochemistry, Genetics and Molecular Biology(all), Chemistry, Peptide, General Medicine, General Pharmacology, Toxicology and Pharmaceutics, Endothelin receptor, Endothelin 1, Gene, General Biochemistry, Genetics and Molecular Biology, Domain (software engineering), Cell biology

Published

2013

29. Site-specific attachment of functionalized poly(ethylene glycol) to the amino terminus of proteins

Author

Robin E. Offord and Hubert François Gaertner

Subjects

Threonine, Transamination, Stereochemistry, Neutrophils, Sialoglycoproteins, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Dinoprostone, Polyethylene Glycols, Serine, chemistry.chemical_compound, Residue (chemistry), Structure-Activity Relationship, Polymer chemistry, Granulocyte Colony-Stimulating Factor, Animals, Humans, Cells, Cultured, Skin, Pharmacology, chemistry.chemical_classification, Binding Sites, Organic Chemistry, Interleukin-8, Periodate, Proteins, Polymer, Fibroblasts, Oxime, Hematopoietic Stem Cells, Peptide Fragments, Rats, Chemotaxis, Leukocyte, Interleukin 1 Receptor Antagonist Protein, chemistry, Indicators and Reagents, Ethylene glycol, Biotechnology, Protein Binding

Abstract

A convenient method for the construction of site-specifically modified poly(ethylene glycol)-protein conjugates is described. This method relies on the ability to generate a reactive carbonyl group in place of the terminal amino group. If the protein has N-terminal serine or threonine, this can be done by very mild periodate oxidation and generates a glyoxylyl group. A method less restricted by the nature of the N-terminal residue, but which requires somewhat harsher conditions, is metal-catalyzed transamination, which gives a keto group. The N-terminal-introduced reactive carbonyl group specifically reacts, under mild acidic conditions, with an aminooxy-functionalized poly(ethylene glycol) to form a stable oxime bond. Using polymers of different size and shape (linear or multibranched), various conjugates of IL-8, G-CSF, and IL-1ra were constructed and further characterized with respect to their biological activity and pharmacokinetic behavior in rats. Unlike most previous methods, this approach places a single PEG chain at a defined site on the protein. It should therefore be more likely to conserve biological activity when the latter depends on interaction with another macromolecule (unlike enzymic activity which often survives multiple PEGylation).

Published

1996

30. Site-specific religation of G-CSF fragments through a thioether bond

Author

David Timms, Hubert François Gaertner, Roger Camble, Robin E. Offord, Keith Rose, and Ronald Cotton

Subjects

Stereochemistry, Proteolysis, Recombinant Fusion Proteins, Molecular Sequence Data, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Alkylation, Sulfides, Mass Spectrometry, law.invention, chemistry.chemical_compound, Hydroxylamine, Thioether, law, Granulocyte Colony-Stimulating Factor, medicine, Amino Acid Sequence, Pharmacology, medicine.diagnostic_test, Enzymatic digestion, Organic Chemistry, Acetylation, Peptide Fragments, Recombinant Proteins, Molecular Weight, chemistry, Iodoacetic anhydride, Recombinant DNA, Electrophoresis, Polyacrylamide Gel, Derivative (chemistry), Biotechnology

Abstract

A new approach is described for linking, through a thioether bond, the C-terminus of one unprotected polypeptide with the N-terminus of another. Homocysteine thiolactone is attached to the C-terminus of one polypeptide by reverse proteolysis and provides through hydroxylamine treatment a free sulfhydryl group. The alpha-amino group of a second polypeptide is selectively iodoacetylated by reaction with iodoacetic anhydride at pH 6.0 or the N-hydroxysuccinimide ester derivative at pH 7.0. Coupling of the two modified fragments occurs in a spontaneous alkylation reaction under mild conditions. After preliminary experiments with small peptides, this approach was extended to large protein fragments derived from recombinant analogs of G-CSF by enzymatic digestion. This approach provides a means of making head-to-tail protein chimeras or introducing noncoded structural elements into a protein.

Published

1994

31. Reverse proteolysis as a means of introducing non-coded changes into proteins

Author

I. Fisch, K. Rose, Hubert François Gaertner, and R. E. Offord

Subjects

medicine.diagnostic_test, Chemistry, Proteolysis, medicine, Cell biology

Published

1993

32. Efficient Orthogonal Bioconjugation of Dendrimers for Synthesis of Bioactive Nanoparticles

Author

Laure Menin, Fabrice Cerini, Oliver Hartley, Arun T. Kamath, Hubert François Gaertner, Claire-Anne Siegrist, and Anne-Françoise Rochat

Subjects

Dendrimers, Native Chemical Ligation, Biomedical Engineering, Pharmaceutical Science, Nanoparticle, Mannose, Bioengineering, Nanotechnology, ddc:616.07, Protein Dendrimers, Mice, chemistry.chemical_compound, Polyamines/chemical synthesis/chemistry/pharmacokinetics, Macrophages/drug effects/metabolism, Dendrimer, Oximes, Polyamines, Multivalent Peptide, Animals, Moiety, Responses, ddc:576, Pharmacology, Mice, Inbred BALB C, Bioconjugation, Molecular Structure, Chemistry, Macrophages, Organic Chemistry, Fluorescein/chemistry, Dendritic Cells, Nucleophilic Catalysis, Native chemical ligation, Combinatorial chemistry, Hydrazone, Dendritic Cells/drug effects/metabolism, Dendrimers/chemical synthesis/chemistry/pharmacokinetics, Click chemistry, Nanoparticles, Fluorescein, Click Chemistry, Nanoparticles/chemistry, In-Vivo, Linker, Delivery, Oximes/chemistry, Biotechnology

Abstract

Nanoparticles carrying biologically active functional sets (e.g., targeting moiety, payload, tracer) have potential use in a wide range of clinical applications. Though complex, such constructions should, as far as possible, have a defined molecular architecture and be monodisperse. However, the existing methods to achieve this goal are unsuitable for the incorporation of peptides and proteins, and those that provide for orthogonal introduction of two different types of functional element are incompatible with the use of commercially available materials. In this study, we have developed approaches for the production of nanoparticles based on commercially available polyamidoamine (PAMAM) dendrimers. First, we identified an optimized oxime conjugation strategy under which complex dendrimers can be fully decorated not only with model peptides, but also with recombinant proteins (insulin was taken as an example). Second, we developed a strategy based on a two-chain covalent heterodendrimer (a "diblock") based on cystamine core PAMAM dendrimers and used it to generate heterodendrimers, into which a peptide array and a mannose array were orthogonally introduced. Finally, by incorporating a functionalized linker into the diblock architecture we were able to site-specifically introduce a third functional element into the nanoparticle. We exemplified this approach using fluorescein, a mannose array, and a peptide array as the three functionalities. We showed that incorporation of a mannose array into a nanoparticle strongly and specifically enhances uptake by sentinel cells of the immune system, an important property for vaccine delivery applications. These PAMAM dendrimer-based approaches represent a robust and versatile platform for the development of bioactive nanoparticles.