Your search keyword '"Verrips, Theo"' showing total 2 results

1. Llama antibody fragments recognizing various epitopes of the CD4bs neutralize a broad range of HIV-1 subtypes A, B and C.

Author

Strokappe, Nika, Szynol, Agnieszka, Aasa-Chapman, Marlèn, Gorlani, Andrea, Forsman Quigley, Anna, Hulsik, David Lutje, Chen, Lei, Weiss, Robin, de Haard, Hans, and Verrips, Theo

Subjects

Animals, Camelids, New World, Humans, HIV-1, Immunoglobulin Variable Region, Complementarity Determining Regions, Antigens, CD4, HIV Envelope Protein gp120, HIV Antibodies, Epitopes, Neutralization Tests, Immunization, Amino Acid Substitution, Mutagenesis, Site-Directed, Cross Reactions, Binding, Competitive, Amino Acid Sequence, Sequence Homology, Amino Acid, Molecular Sequence Data, Immunoglobulin Heavy Chains, env Gene Products, Human Immunodeficiency Virus, Antibodies, Neutralizing, In Vitro Techniques, CD4 Antigens, Antibodies, Neutralizing, Binding, Competitive, Camelids, New World, Mutagenesis, Site-Directed, Sequence Homology, Amino Acid, env Gene Products, Human Immunodeficiency Virus, General Science & Technology

Abstract

Many of the neutralising antibodies, isolated to date, display limited activities against the globally most prevalent HIV-1 subtypes A and C. Therefore, those subtypes are considered to be an important target for antibody-based therapy. Variable domains of llama heavy chain antibodies (VHH) have some superior properties compared with classical antibodies. Therefore we describe the application of trimeric forms of envelope proteins (Env), derived from HIV-1 of subtype A and B/C, for a prolonged immunization of two llamas. A panel of VHH, which interfere with CD4 binding to HIV-1 Env were selected with use of panning. The results of binding and competition assays to various Env, including a variant with a stabilized CD4-binding state (gp120(Ds2)), cross-competition experiments, maturation analysis and neutralisation assays, enabled us to classify the selected VHH into three groups. The VHH of group I were efficient mainly against viruses of subtype A, C and B'/C. The VHH of group II resemble the broadly neutralising antibody (bnmAb) b12, neutralizing mainly subtype B and C viruses, however some had a broader neutralisation profile. A representative of the third group, 2E7, had an even higher neutralization breadth, neutralizing 21 out of the 26 tested strains belonging to the A, A/G, B, B/C and C subtypes. To evaluate the contribution of certain amino acids to the potency of the VHH a small set of the mutants were constructed. Surprisingly this yielded one mutant with slightly improved neutralisation potency against 92UG37.A9 (subtype A) and 96ZM651.02 (subtype C). These findings and the well-known stability of VHH indicate the potential application of these VHH as anti-HIV-1 microbicides.

Published

2012

2. Crystal structure of the neutralizing Llama V(HH) D7 and its mode of HIV-1 gp120 interaction.

Author

Hinz, Andreas, Lutje Hulsik, David, Forsman, Anna, Koh, Willie Wee-Lee, Belrhali, Hassan, Gorlani, Andrea, de Haard, Hans, Weiss, Robin A, Verrips, Theo, and Weissenhorn, Winfried

Subjects

HIV-1, Immunoglobulin Fragments, Complementarity Determining Regions, HIV Envelope Protein gp120, Solvents, Neutralization Tests, Sequence Alignment, DNA Mutational Analysis, Inhibitory Concentration 50, Binding Sites, Amino Acid Sequence, Protein Structure, Secondary, Structural Homology, Protein, Protein Binding, Surface Properties, Models, Molecular, Molecular Sequence Data, Immunoglobulin Heavy Chains, Mutant Proteins, CD4 Antigens, Models, Molecular, Protein Structure, Secondary, Structural Homology, Protein, General Science & Technology

Abstract

HIV-1 entry into host cells is mediated by the sequential binding of the envelope glycoprotein gp120 to CD4 and a chemokine receptor. Antibodies binding to epitopes overlapping the CD4-binding site on gp120 are potent inhibitors of HIV entry, such as the llama heavy chain antibody fragment V(HH) D7, which has cross-clade neutralizing properties and competes with CD4 and mAb b12 for high affinity binding to gp120. We report the crystal structure of the D7 V(HH) at 1.5 A resolution, which reveals the molecular details of the complementarity determining regions (CDR) and substantial flexibility of CDR3 that could facilitate an induced fit interaction with gp120. Structural comparison of CDRs from other CD4 binding site antibodies suggests diverse modes of interaction. Mutational analysis identified CDR3 as a key component of gp120 interaction as determined by surface plasmon resonance. A decrease in affinity is directly coupled to the neutralization efficiency since mutations that decrease gp120 interaction increase the IC50 required for HIV-1 IIIB neutralization. Thus the structural study identifies the long CDR3 of D7 as the key determinant of interaction and HIV-1 neutralization. Furthermore, our data confirm that the structural plasticity of gp120 can accommodate multiple modes of antibody binding within the CD4 binding site.

Published

2010