Your search keyword '"Humbert, Michael"' showing total 9 results

1. A LiTat 1.5 variant surface glycoprotein-derived peptide with diagnostic potential for Trypanosoma brucei gambiense.

Author

Van Nieuwenhove L, Büscher P, Balharbi F, Humbert M, Guisez Y, and Lejon V

Subjects

Area Under Curve, Enzyme-Linked Immunosorbent Assay, Humans, Sensitivity and Specificity, Antibodies, Protozoan blood, Epitopes, Peptides, Trypanosoma brucei gambiense immunology, Trypanosomiasis, African diagnosis, Variant Surface Glycoproteins, Trypanosoma

Abstract

Objective: To evaluate the accuracy of a peptide, corresponding to the variant surface glycoprotein (VSG) LiTat 1.5 amino acid (AA) sequence 268-281 and identified through alignment of monoclonal antibody selected mimotopes, for diagnosis of Trypanosoma brucei gambiense sleeping sickness., Methods: A synthetic biotinylated peptide (peptide 1.5/268-281), native VSG LiTat 1.3 and VSG LiTat 1.5 were tested in an indirect ELISA with 102 sera from patients with HAT and 102 endemic HAT-negative controls., Results: The area under the curve (AUC) of peptide 1.5/268-281 was 0.954 (95% confidence interval 0.918-0.980), indicating diagnostic potential. The areas under the curve of VSG LiTat 1.3 and LiTat 1.5 were 1.000 (0.982-1.000) and 0.997 (0.973-1.000), respectively, and significantly higher than the AUC of peptide 1.5/268-281. On a model of VSG LiTat 1.5, peptide 1.5/268-281 was mapped near the top of the VSG., Conclusions: A biotinylated peptide corresponding to AA 268-281 of VSG LiTat 1.5 may replace the native VSG in serodiagnostic tests, but the diagnostic accuracy is lower than for the full-length native VSG LiTat 1.3 and VSG LiTat 1.5., (© 2013 Blackwell Publishing Ltd.)

Published

2013

2. Identification of mimotopes with diagnostic potential for Trypanosoma brucei gambiense variant surface glycoproteins using human antibody fractions.

Author

Van Nieuwenhove L, Büscher P, Balharbi F, Humbert M, Dieltjens T, Guisez Y, and Lejon V

Subjects

Clinical Laboratory Techniques methods, Humans, Parasitology methods, Antibodies, Protozoan blood, Epitopes, Peptides, Trypanosoma brucei gambiense immunology, Trypanosomiasis, African diagnosis, Variant Surface Glycoproteins, Trypanosoma immunology

Abstract

Background: At present, screening of the population at risk for gambiense human African trypanosomiasis (HAT) is based on detection of antibodies against native variant surface glycoproteins (VSGs) of Trypanosoma brucei (T.b.) gambiense. Drawbacks of these native VSGs include culture of infective T.b. gambiense trypanosomes in laboratory rodents, necessary for production, and the exposure of non-specific epitopes that may cause cross-reactions. We therefore aimed at identifying peptides that mimic epitopes, hence called "mimotopes," specific to T.b. gambiense VSGs and that may replace the native proteins in antibody detection tests., Methodology/principal Findings: A Ph.D.-12 peptide phage display library was screened with polyclonal antibodies from patient sera, previously affinity purified on VSG LiTat 1.3 or LiTat 1.5. The peptide sequences were derived from the DNA sequence of the selected phages and synthesised as biotinylated peptides. Respectively, eighteen and twenty different mimotopes were identified for VSG LiTat 1.3 and LiTat 1.5, of which six and five were retained for assessment of their diagnostic performance. Based on alignment of the peptide sequences on the original protein sequence of VSG LiTat 1.3 and 1.5, three additional peptides were synthesised. We evaluated the diagnostic performance of the synthetic peptides in indirect ELISA with 102 sera from HAT patients and 102 endemic negative controls. All mimotopes had areas under the curve (AUCs) of ≥0.85, indicating their diagnostic potential. One peptide corresponding to the VSG LiTat 1.3 protein sequence also had an AUC of ≥0.85, while the peptide based on the sequence of VSG LiTat 1.5 had an AUC of only 0.79., Conclusions/significance: We delivered the proof of principle that mimotopes for T.b. gambiense VSGs, with diagnostic potential, can be selected by phage display using polyclonal human antibodies.

Published

2012

3. A peptide inhibitor of HIV-1 assembly in vitro.

Author

Sticht J, Humbert M, Findlow S, Bodem J, Müller B, Dietrich U, Werner J, and Kräusslich HG

Subjects

Amino Acid Sequence, Antiviral Agents genetics, Binding Sites, Capsid ultrastructure, Capsid Proteins genetics, Enzyme-Linked Immunosorbent Assay, Gene Products, gag genetics, Microscopy, Electron, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Peptide Library, Peptides genetics, Antiviral Agents metabolism, Capsid physiology, Capsid Proteins metabolism, Gene Products, gag metabolism, HIV-1 physiology, Peptides metabolism, Virus Assembly physiology

Abstract

Formation of infectious HIV-1 involves assembly of Gag polyproteins into immature particles and subsequent assembly of mature capsids after proteolytic disassembly of the Gag shell. We report a 12-mer peptide, capsid assembly inhibitor (CAI), that binds the capsid (CA) domain of Gag and inhibits assembly of immature- and mature-like capsid particles in vitro. CAI was identified by phage display screening among a group of peptides with similar sequences that bind to a single reactive site in CA. Its binding site was mapped to CA residues 169-191, with an additional contribution from the last helix of CA. This result was confirmed by a separate X-ray structure analysis showing that CAI inserts into a conserved hydrophobic groove and alters the CA dimer interface. The CAI binding site is a new target for antiviral development, and CAI is the first known inhibitor directed against assembly of immature HIV-1.

Published

2005

4. 3D-Epitope-Explorer (3DEX): localization of conformational epitopes within three-dimensional structures of proteins.

Author

Schreiber A, Humbert M, Benz A, and Dietrich U

Subjects

Algorithms, Amino Acid Sequence, Amino Acids chemistry, Antibodies, Humans, Models, Molecular, Molecular Mimicry, Software, Epitope Mapping, HIV Envelope Protein gp120 chemistry, Peptide Library, Peptides chemistry, Peptides immunology, Protein Conformation

Abstract

Neutralizing antibodies often recognize conformational, discontinuous epitopes. Linear peptides mimicking such conformational epitopes can be selected from phage display peptide libraries by screening with the respective antibodies. However, it is difficult to localize these "mimotopes" within the three-dimensional (3D) structures of the target proteins. Knowledge of conformational epitopes of neutralizing antibodies would help to design antigens able to elicit protective immune responses. Therefore, we provide here a software that allows to localize linear peptide sequences within 3D structures of proteins. The 3D-Epitope-Explorer (3DEX) software allows to map conformational epitopes in 3D protein structures based on an algorithm that takes into account the physicochemical neighborhood of C(alpha)- or C(beta)-atoms of individual amino acids. A given amino acid of a peptide sequence is localized within the protein and the software searches within predefined distances for the amino acids neighboring that amino acid in the peptide. Surface exposure of the amino acids can also be taken into consideration. The procedure is then repeated for the remaining amino acids of the peptide. The introduction of a joker function allows to map peptide mimotopes, which do not necessarily have 100% sequence homology to the protein. Using this software we were able to localize mimotopes selected from phage displayed peptide libraries with polyclonal antibodies from HIV-positive patient plasma within the 3D structure of gp120, the exterior glycoprotein of HIV-1. We also analyzed two recently published peptide sequences corresponding to known conformational epitopes to further confirm the integrity of 3DEX., ((c) 2005 Wiley Periodicals, Inc.)

Published

2005

5. Novel Biopanning Strategy To Identify Epitopes Associated with Vaccine Protection.

Author

Bachler, Barbara C., Humbert, Michael, Palikuqi, Brisa, Siddappa, Nagadenahalli B., Lakhashe, Samir K., Rasmussen, Robert A., and Ruprecht, Ruth M.

Subjects

*VACCINE research, *EPITOPES, *ANTIGENS, *PEPTIDES, *PATHOGENIC microorganisms

Abstract

Identifying immune correlates of protection is important to develop vaccines against infectious diseases. We designed a novel, universally applicable strategy to profile the antibody (Ab) repertoire of protected vaccine recipients, using recombinant phages encoding random peptide libraries. The new approach, termed "protection-linked (PL) biopanning," probes the Ab paratopes of protected vaccinees versus those with vaccine failure. As proof of concept, we screened plasma samples from vaccinated rhesus macaques (RMs) that had completely resisted multiple mucosal challenges with R5-tropic simian-human immunodeficiency viruses (SHIVs). The animals had been immunized with a m ulticomponent vaccine (multimeric HIV-1 gp 160, HIV-1 Tat, and SIV Gag-Pol particles). After PL biopanning, we analyzed the phagotopes selected for amino acid homologies; in addition to the expected Env mimotopes, one recurring motif reflected the neutralizing Ab epitope at the N terminus (NT) of HIV- 1 Tat. Subsequent binding and functional assays indicated that anti-Tat NT Abs were present only in completely or partially protected RMs; peak viremia of the latter was inversely correlated with anti-Tat NT Ab titers. In contrast, highly viremic, unvaccinated controls did not develop detectable Abs against the same epitope. Based upon the protective effect observed in vivo, we suggest that Tat should be included in multicomponent HIV-1 vaccines. Our data highlight the power of the new PL-biopanning strategy to identify Ab responses with significant association to vaccine protection, regardless of the mechanism(s) or targets of the protective Abs. PL biopanning is also unbiased with regard to pathogens or disease model, making it a universal tool. [ABSTRACT FROM AUTHOR]

Published

2013

6. A Li Tat 1.5 variant surface glycoprotein-derived peptide with diagnostic potential for Trypanosoma brucei gambiense.

Author

Nieuwenhove, Liesbeth, Büscher, Philippe, Balharbi, Fatima, Humbert, Michael, Guisez, Yves, and Lejon, Veerle

Subjects

MEMBRANE glycoproteins, TRYPANOSOMA brucei, EPIDEMIC encephalitis, MONOCLONAL antibodies, PEPTIDES, SENSITIVITY & specificity (Statistics), CONFIDENCE intervals

Abstract

Copyright of Tropical Medicine & International Health is the property of Wiley-Blackwell and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2013

7. Identification of Mimotopes with Diagnostic Potential for Trypanosoma brucei gambiense Variant Surface Glycoproteins Using Human Antibody Fractions.

Author

Nieuwenhove, Liesbeth Van, Buscher, Philippe, Balharbi, Fatima, Humbert, Michael, Dieltjens, Tessa, Guisez, Yves, and Lejon, Veerle

Subjects

TRYPANOSOMA brucei, TRYPANOSOMIASIS, GLYCOPROTEINS, LABORATORY rodents, PEPTIDES, NUCLEOTIDE sequence, AMINO acid sequence

Abstract

Background: At present, screening of the population at risk for gambiense human African trypanosomiasis (HAT) is based on detection of antibodies against native variant surface glycoproteins (VSGs) of Trypanosoma brucei (T.b.) gambiense. Drawbacks of these native VSGs include culture of infective T.b. gambiense trypanosomes in laboratory rodents, necessary for production, and the exposure of non-specific epitopes that may cause cross-reactions. We therefore aimed at identifying peptides that mimic epitopes, hence called "mimotopes," specific to T.b. gambiense VSGs and that may replace the native proteins in antibody detection tests. Methodology/Principal Findings: A Ph.D.-12 peptide phage display library was screened with polyclonal antibodies from patient sera, previously affinity purified on VSG LiTat 1.3 or LiTat 1.5. The peptide sequences were derived from the DNA sequence of the selected phages and synthesised as biotinylated peptides. Respectively, eighteen and twenty different mimotopes were identified for VSG LiTat 1.3 and LiTat 1.5, of which six and five were retained for assessment of their diagnostic performance. Based on alignment of the peptide sequences on the original protein sequence of VSG LiTat 1.3 and 1.5, three additional peptides were synthesised. We evaluated the diagnostic performance of the synthetic peptides in indirect ELISA with 102 sera from HAT patients and 102 endemic negative controls. All mimotopes had areas under the curve (AUCs) of ≥0.85, indicating their diagnostic potential. One peptide corresponding to the VSG LiTat 1.3 protein sequence also had an AUC of ≥0.85, while the peptide based on the sequence of VSG LiTat 1.5 had an AUC of only 0.79. Conclusions/Significance: We delivered the proof of principle that mimotopes for T.b. gambiense VSGs, with diagnostic potential, can be selected by phage display using polyclonal human antibodies. [ABSTRACT FROM AUTHOR]

Published

2012

8. Inducing Cross-Clade Neutralizing Antibodies against HIV-1 by Immunofocusing.

Author

Humbert, Michael, Rasmussen, Robert A., Ong, Helena, Kaiser, Fabian M. P., Shiu-Lok Hu, and Ruprecht, Ruth M.

Subjects

*IMMUNOGLOBULINS, *HIV, *VIRAL disease prevention, *VIRAL vaccines, *IMMUNITY, *IMMUNOGENETICS, *PEPTIDES, *EPITOPES, *SIMIAN immunodeficiency virus

Abstract

Background: Although vaccines are important in preventing viral infections by inducing neutralizing antibodies (nAbs), HIV- 1 has proven to be a difficult target and escapes humoral immunity through various mechanisms. We sought to test whether HIV-1 Env mimics may serve as immunogens. Methodology/Principal Findings: Using random peptide phage display libraries, we identified the epitopes recognized by polyclonal antibodies of a rhesus monkey that had developed high-titer, broadly reactive nAbs after infection with a simianhuman immunodeficiency virus (SHIV) encoding env of a recently transmitted HIV-1 clade C (HIV-C). Phage peptide inserts were analyzed for conformational and linear homology using computational analysis; some peptides mimicked various domains of the original HIV-C Env, such as conformational V3 loop epitopes and the conserved linear region of the gp120 Cterminus. Next, we devised a novel prime/boost strategy to test the immunogenicity of such phage-displayed peptides and primed mice only once with HIV-C gp160 DNA followed by boosting with mixtures of recombinant phages. Conclusions/Significance: This strategy, which was designed to focus the immune system on a few Env epitopes (immunofocusing), not only induced HIV-C gp160 binding antibodies and cross-clade nAbs, but also linked a conserved HIV Env region for the first time to the induction of nAbs: the C-terminus of gp120. The identification of conserved antigen mimics may lead to novel immunogens capable of inducing broadly reactive nAbs. [ABSTRACT FROM AUTHOR]

Published

2008

9. Unravelling the antigenic landscape of the HIV-1 subtype A envelope of an individual with broad cross-neutralizing antibodies using phage display peptide libraries

Author

Dieltjens, Tessa, Willems, Betty, Coppens, Sandra, Van Nieuwenhove, Lies, Humbert, Michael, Dietrich, Ursula, Heyndrickx, Leo, Vanham, Guido, and Janssens, Wouter

Subjects

*HIV, *PEPTIDES, *GENE targeting, *EPITOPES, *CONFORMATIONAL analysis, *VIRAL vaccines

Abstract

Abstract: Broad cross-neutralizing antibodies from persons infected with HIV-1 target a variety of epitopes. Identification of these HIV-1 epitopes may result in an optimal panel of antigenic peptides to be included in a prophylactic vaccine. Phage display peptide libraries were used to unravel the antigenic landscape of an individual (ITM1) infected with HIV-1 subtype A with broad cross-neutralizing antibodies. A stringent selection strategy resulted in the identification of 60 unique HIV-1 peptide phage, which were subjected to sequence analysis and mapped onto the ITM1 envelope sequences. Four groups of peptide phages were found: the first group (n =11) were similar with the tip of the V3 loop (KxxHxGPxxxF); the second group (n =11) represented the gp41 principal immunodominant domain (CxGxLxCTxNxP); the third group (n =16) could be localized in the V2 loop (KxxxHxxxY); and the fourth group (n =22) mimicked a conformational epitope (HxxS/TNxK). All but the V2-binding antibodies were conserved over the 11 years of follow-up. A neutralization inhibition assay revealed the contribution of the V3 antibodies to the neutralizing capacity of the ITM1 plasma. Overall, the ITM1 immunogenic landscape was mapped and a part of the origin of this broad cross-neutralizing activity was demonstrated. [ABSTRACT FROM AUTHOR]

Published

2010