Your search keyword '"Gabriela Canziani"' showing total 11 results

1. Llama nanoantibodies with therapeutic potential against human norovirus diarrhea.

Author

Lorena Garaicoechea, Andrea Aguilar, Gabriel I Parra, Marina Bok, Stanislav V Sosnovtsev, Gabriela Canziani, Kim Y Green, Karin Bok, and Viviana Parreño

Subjects

Medicine, Science

Abstract

Noroviruses are a major cause of acute gastroenteritis, but no vaccines or therapeutic drugs are available. Llama-derived single chain antibody fragments (also called VHH) are small, recombinant monoclonal antibodies of 15 kDa with several advantages over conventional antibodies. The aim of this study was to generate recombinant monoclonal VHH specific for the two major norovirus (NoV) genogroups (GI and GII) in order to investigate their potential as immunotherapy for the treatment of NoV diarrhea. To accomplish this objective, two llamas were immunized with either GI.1 (Norwalk-1968) or GII.4 (MD2004) VLPs. After immunization, peripheral blood lymphocytes were collected and used to generate two VHH libraries. Using phage display technology, 10 VHH clones specific for GI.1, and 8 specific for GII.4 were selected for further characterization. All VHH recognized conformational epitopes in the P domain of the immunizing VP1 capsid protein, with the exception of one GII.4 VHH that recognized a linear P domain epitope. The GI.1 VHHs were highly specific for the immunizing GI.1 genotype, with only one VHH cross-reacting with GI.3 genotype. The GII.4 VHHs reacted with the immunizing GII.4 strain and showed a varying reactivity profile among different GII genotypes. One VHH specific for GI.1 and three specific for GII.4 could block the binding of homologous VLPs to synthetic HBGA carbohydrates, saliva, and pig gastric mucin, and in addition, could inhibit the hemagglutination of red blood cells by homologous VLPs. The ability of Nov-specific VHHs to perform well in these surrogate neutralization assays supports their further development as immunotherapy for NoV treatment and immunoprophylaxis.

Published

2015

2. Characterization of neutralizing affinity-matured human respiratory syncytial virus F binding antibodies in the sub-picomolar affinity range

Author

José A. Melero, Eilyn R. Lacy, and Gabriela Canziani

Subjects

Phage display, biology, medicine.drug_class, Chemistry, Monoclonal antibody, Molecular biology, Immunoglobulin G, Epitope, Motavizumab, Structural Biology, Biotinylation, biology.protein, medicine, Virus-neutralizing Antibody, Avidity, Molecular Biology, medicine.drug

Abstract

In the human adaptation and optimization of a mouse anti-human respiratory syncytial virus neutralizing antibody, affinity assessment was crucial to distinguish among potential candidates and to evaluate whether this correlated with function in vitro and in vivo. This affinity assessment was complicated by the trimeric nature of the antigen target, respiratory syncytial virus F (RSV-F) glycoprotein. In the initial affinity screen, surface plasmon resonance was used to determine the intrinsic binding affinities of anti-RSV-F Fab and immunoglobulin G (IgG) to the extracellular domain of RSV-F. This assessment required minimal biotinylation of the RSV-F protein and design of a capture strategy to minimize avidity effects. Approximately 30 Fabs were selected from three optimization phage display libraries on the basis of an initial ELISA screen. Surface plasmon resonance analysis demonstrated the success of optimization with some candidates from the screened libraries having low picomolar dissociation constants, more than 700-fold tighter than the parental monoclonal antibody (B21M). The affinities of these antibodies were further evaluated by a kinetic exclusion assay, a solution binding technology. One IgG (monoclonal antibody 029) displayed a low picomolar K(D) comparable with that of motavizumab, an RSV antibody in clinical study. Kinetic exclusion assay showed that two other of the matured IgGs (011 and 019) had sub-picomolar dissociation constants that could not be resolved further. We discuss the relevance of these interaction analysis results in the light of recently published data on the mechanism of F-driven viral fusion during paramyxoviral infection and 101F epitope conservation revealed from the recent crystal structure of RSV-F in the post-fusion state.

Published

2012

3. His-tag binding by antibody C706 mimics β-amyloid recognition

Author

Galina Obmolova, Sonia S. Jung, Gary L. Gilliland, Yonghong Zhao, Lester L. Gutshall, Alexey Teplyakov, and Gabriela Canziani

Subjects

chemistry.chemical_classification, Amyloid beta-Peptides, biology, medicine.drug_class, P3 peptide, Antibodies, Monoclonal, Peptide, Plasma protein binding, Monoclonal antibody, Protein Structure, Secondary, Epitope, Protein Structure, Tertiary, Protein structure, Biochemistry, chemistry, Alzheimer Disease, Structural Biology, Extracellular, biology.protein, medicine, Humans, Antibody, Molecular Biology, Protein Binding

Abstract

Alzheimer's disease is a progressive neurodegenerative disease characterized by extracellular deposits of β-amyloid (Aβ) plaques. Aggregation of the Aβ42 peptide leading to plaque formation is believed to play a central role in Alzheimer's disease pathogenesis. Anti-Aβ monoclonal antibodies can reduce amyloid plaques and could possibly be used for immunotherapy. We have developed a monoclonal antibody C706, which recognizes the human Aβ peptide. Here we report the crystal structure of the antibody Fab fragment at 1.7 A resolution. The structure was determined in two crystal forms, P21 and C2. Although the Fab was crystallized in the presence of Aβ16, no peptide was observed in the crystals. The antigen-binding site is blocked by the hexahistidine tag of another Fab molecule in both crystal forms. The poly-His peptide in an extended conformation occupies a crevice between the light and heavy chains of the variable domain. Two consecutive histidines (His4–His5) stack against tryptophan residues in the central pocket of the antigen-binding surface. In addition, they form hydrogen bonds to the acidic residues at the bottom of the pocket. The mode of his-tag binding by C706 resembles the Aβ recognition by antibodies PFA1 and WO2. All three antibodies recognize the same immunodominant B-cell epitope of Aβ. By similarity, residues Phe–Arg–His of Aβ would be a major portion of the C706 epitope. Copyright © 2010 John Wiley & Sons, Ltd.

Published

2010

4. Down modulation of human TLR3 function by a monoclonal antibody

Author

Jeremy Korteweg, Jill Carton, Mark Cunningham, Michael Brigham-Burke, Heena Beck, M. Lamine Mbow, Jill Giles-Komar, Roberta J. Lamb, Robert T. Sarisky, Jarrat Jordan, Lani San Mateo, Karen E. Duffy, Cynthia Duchala, and Gabriela Canziani

Subjects

medicine.drug_class, viruses, Immunology, Pilot Projects, chemical and pharmacologic phenomena, Endogeny, Biology, Monoclonal antibody, Cell Line, Mice, medicine, Animals, Humans, Antibodies, Blocking, Receptor, Cell Line, Transformed, Mice, Inbred BALB C, Messenger RNA, Innate immune system, Antibodies, Monoclonal, virus diseases, hemic and immune systems, Molecular biology, Toll-Like Receptor 3, RNA silencing, TLR3, Female, Binding Sites, Antibody, Signal transduction

Abstract

Toll-like receptors are a family of pattern-recognition receptors that contribute to the innate immune response. Toll-like receptor 3 (TLR3) signals in response to foreign, endogenous and synthetic ligands including viral dsRNA, bacterial RNA, mitochondrial RNA, endogenous necrotic cell mRNA and the synthetic dsRNA analog, poly(I:C). We have generated a monoclonal antibody (mAb CNTO2424) that recognizes the extracellular domain (ECD) of human TLR3 in a conformation-dependent manner. CNTO2424 down-regulates poly(I:C)-induced production of IL-6, IL-8, MCP-1, RANTES, and IP-10 in human lung epithelial cells. In addition, mAb CNTO2424 was able to interfere with the known TLR3-dependent signaling pathways, namely NF-κB, IRF-3/ISRE, and p38 MAPK. The generation of this neutralizing anti-TLR3 mAb provides a unique tool to better understand TLR3 signaling and potential cross-talk between TLR3 and other molecules.

Published

2007

5. Structure-based Design of Mimetics for Granulocyte-macrophage Colony Stimulating Factor (GM-CSF)

Author

Irwin Chaiken, Joanna Bajgier, Carmela Plugariu, William V. Williams, A. Paul Godillot, Gabriela Canziani, Cristina Monfardini, Joann Kwah, and Thomas Kieber-Emmons

Subjects

Stereochemistry, Molecular Sequence Data, Anti-Inflammatory Agents, Peptide, Biology, medicine.disease_cause, Drug Discovery, medicine, Animals, Humans, Amino Acid Sequence, Binding site, Peptide sequence, Pharmacology, chemistry.chemical_classification, Binding Sites, Molecular Mimicry, Granulocyte-Macrophage Colony-Stimulating Factor, Receptor–ligand kinetics, Cyclic peptide, Molecular mimicry, chemistry, Biochemistry, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, Drug Design, Rab, Peptides, Alpha chain

Abstract

Granulocyte-macrophage colony stimulating factor (GM-CSF) activity has been linked to pro-inflammatory effects in autoimmune syndromes, such as rheumatoid arthritis. Thus GM-CSF mimetics with antagonist activity might play a therapeutic role in these diseases. The human GM-CSF core structure consists of a four alpha-helix bundle, and GM-CSF activity is controlled by its binding to a two-subunit receptor. A number of residues located on the B and C helices of GM-CSF are postulated to interact with the alpha chain of the GM-CSF receptor (GM-CSFR). Several approaches have been successfully utilized to develop peptide mimetics of this site, including peptides from the native sequence, a peptide derived from a recombinant antibody (rAb) light chain which mimicked GM-CSF receptor binding activity, and structurally guided de novo design. Analysis of the rAb light chain had suggested mimicry of GM-CSF with residues mostly contributed by the CDR I region. Key residues involved in CDR I peptide/GM-CSFR binding were identified by truncation and alteration of individual residues, while the structural elements required to antagonize the biological action of GM-CSF were separately tested in binding and inhibitory activity assays of multiple cyclic analogues. A peptide designed to retain the loop conformation of the CDR I region of the rAb light chain competed with GM-CSF for both antibody and receptor binding, but the role of specific residues in antibody versus receptor binding differed markedly. These studies suggest that structural analysis of peptide mimetics can reveal differences in receptor and antibody binding, perhaps including key interactions that impact binding kinetics. Peptide mimetics of other four-helix bundle cytokines are reviewed, including helical and reverse turn mimetics of helical structures. Use of peptide mimetics coupled with structural and kinetic analysis provides a powerful approach to identifying important receptor-ligand interactions, which implications for rational design of novel therapeutics.

Published

2002

6. Biosensor analysis of dynamics of interleukin 5 receptor subunit βc interaction with IL5:IL5Rα complexes

Author

Stefan Zahn, Emma Evergren, Gabriela Canziani, Jeffery J. Scibek, Irwin Chaiken, and Donald Van Ryk

Subjects

Time Factors, Macromolecular Substances, medicine.drug_class, Protein subunit, Biophysics, Biosensing Techniques, Plasma protein binding, Spodoptera, Biology, Monoclonal antibody, Biochemistry, Cell Line, medicine, Animals, Receptor, Molecular Biology, Interleukin-5 receptor, Ligand binding assay, Receptors, Interleukin, Cell Biology, Receptors, Interleukin-5, Receptor–ligand kinetics, Kinetics, Protein Subunits, Ectodomain, Chromatography, Gel, Interleukin-5, Protein Binding

Abstract

To gain insight into IL5 receptor subunit recruitment mechanism, and in particular the experimentally elusive pathway for assembly of signaling subunit beta(c), we constructed a soluble beta(c) ectodomain (s(beta)(c)) and developed an optical biosensor assay to measure its binding kinetics. Functionally active s(beta)(c) was anchored via a C-terminal His tag to immobilized anti-His monoclonal antibodies on the sensor surface. Using this surface, we quantitated for the first time direct binding of s(beta)(c) to IL5R(alpha) complexed to either wild-type or single-chain IL5. Binding was much weaker if at all with either R(alpha) or IL5 alone. Kinetic evaluation revealed a moderate affinity (0.2-1 microM) and relatively fast off rate for the s(beta)(c) interaction with IL5:R(alpha) complexes. The data support a model in which beta(c) recruitment occurs with preformed IL5:R(alpha) complex. Dissociation kinetics analysis suggests that the IL5-alpha-beta(c) complex is relatively short-lived. Overall, this study solidifies a model of sequential recruitment of receptor subunits by IL5, provides a novel biosensor binding assay of beta(c) recruitment dynamics, and sets the stage for more advanced characterization of the roles of structural elements within R(alpha), beta(c), and cytokines of the IL5/IL3/GM-CSF family in receptor recruitment and activation.

Published

2002

7. Rapid Progression to Simian AIDS Can Be Accompanied by Selection of CD4-Independent gp120 Variants with Impaired Ability To Bind CD4

Author

Gabriela Canziani, Susan V. Westmoreland, J. Charles Whitbeck, Roselyn J. Eisenberg, Gary H. Cohen, Elena V. Ryzhova, Francisco Gonzalez-Scarano, and Andrew A. Lackner

Subjects

viruses, Dissociation rate, Immunology, Simian Acquired Immunodeficiency Syndrome, Mutagenesis (molecular biology technique), medicine.disease_cause, Microbiology, Viral Envelope Proteins, Virology, medicine, Animals, Asparagine, Membrane Glycoproteins, biology, Genetic Variation, Surface Plasmon Resonance, Simian immunodeficiency virus, Macaca mulatta, Phenotype, Membrane glycoproteins, Binding ability, Simian AIDS, Insect Science, CD4 Antigens, Disease Progression, biology.protein, Pathogenesis and Immunity, Simian Immunodeficiency Virus

Abstract

Aspartate 368 on human immunodeficiency virus type 1 (HIV-1) gp120 forms multiple contacts with CD4; in mutagenesis studies, its replacement by asparagine and corresponding changes in simian immunodeficiency virus SIVmac (D385N) reduced binding with CD4. Nevertheless, simian immunodeficiency virus envelopes with D385N were prevalent in several studies. Extending these observations, we also found D385N to be dominant among env clones from two rhesus macaques that progressed rapidly to simian AIDS. These envelopes showed a CD4-independent phenotype as well as reduced affinity to CD4. Moreover, an adjacent change, G383R, which was frequently coselected with D385N, further decreased binding. An optical biosensor study demonstrated that the SIVmac239 gp120 bound to CD4 with kinetics similar to those of HIV-1. However, the gp120s with D385N and G383R showed a 40-fold reduction in affinity, with a drastic increase in dissociation rate, indicating an inherently unstable complex. This finding showed that rapid progression to simian AIDS may be accompanied by the selection of CD4-independent gp120 variants with impaired CD4 binding ability.

Published

2002

8. Conformational Changes of gp120 in Epitopes near the CCR5 Binding Site Are Induced by CD4 and a CD4 Miniprotein Mimetic

Author

Raymond W. Sweet, Richard T. Wyatt, Irwin Chaiken, Wayne A. Hendrickson, Wentao Zhang, Peter D. Kwong, Carmela Plugariu, Gabriela Canziani, and Joseph Sodroski

Subjects

Charybdotoxin, Receptors, CCR5, Protein Conformation, viruses, Molecular Sequence Data, Epitopes, T-Lymphocyte, Biosensing Techniques, HIV Envelope Protein gp120, medicine.disease_cause, Binding, Competitive, Biochemistry, Epitope, Immunoglobulin Fab Fragments, Protein structure, Antigen, medicine, Humans, Amino Acid Sequence, Binding site, Peptide sequence, Sequence Deletion, biology, Chemistry, Molecular Mimicry, virus diseases, Envelope glycoprotein GP120, Peptide Fragments, Molecular mimicry, Solubility, CD4 Antigens, HIV-1, biology.protein, Biophysics, Binding Sites, Antibody, Protein Binding, Binding domain

Abstract

Binding of the T-cell antigen CD4 to human immunodeficiency virus type 1 (HIV-1) envelope glycoprotein gp120 has been reported to induce conformational rearrangements in the envelope complex that facilitate recognition of the CCR5 coreceptor and consequent viral entry into cells. To better understand the mechanism of virus docking and cell fusion, we developed a three-component gp120-CD4-17b optical biosensor assay to visualize the CD4-induced conformational change of gp120 as seen through envelope binding to a neutralizing human antibody, 17b, which binds to epitopes overlapping the CCR5 binding site. The 17b Fab fragment was immobilized on a dextran sensor surface, and kinetics of gp120 binding were evaluated by both global and linear transformation analyses. Adding soluble CD4 (sCD4) increased the association rate of full-length JR-FL gp120 by 25-fold. This change is consistent with greater exposure of the 17b binding epitope on gp120 when CD4 is bound and correlates with CD4-induced conformational changes in gp120 leading to higher affinity binding to coreceptor. A smaller enhancement of 17b binding by sCD4 was observed with a mutant of gp120, DeltaJR-FL protein, which lacks V1 and V2 variable loops and N- and C-termini. Biosensor results for JR-FL and DeltaJR-FL argue that CD4-induced conformational changes in the equilibrium state of gp120 lead both to movement of V1/V2 loops and to conformational rearrangement in the gp120 core structure and that both of these lead to greater exposure of the coreceptor-binding epitope in gp120. A 17b binding enhancement effect on JR-FL also was observed with a 32-amino acid charybdotoxin miniprotein construct that contains an epitope predicted to mimic the Phe 43/Arg 59 region of CD4 and that competes with CD4 for gp120 binding. Results with this construct argue that CD4-mimicking molecules with surrogate structural elements for the Phe 43/Arg 59 components of CD4 are sufficient to elicit a similar gp120 conformational isomerization as expressed by CD4 itself.

Published

1999

9. Tissue Factor Regulates Plasminogen Binding and Activation

Author

Zhiqiang Fan, Peter J. Larson, Alice Kuo, Douglas B. Cines, Irwin Chaiken, P.N. Raghunath, John Bognacki, John E. Tomaszewski, Gabriela Canziani, and Abd Al-Roof Higazi

Subjects

Urokinase, Chemistry, Plasmin, medicine.medical_treatment, Chinese hamster ovary cell, Immunology, Cell Biology, Hematology, Molecular biology, Biochemistry, Tissue factor, Cell culture, Fibrinolysis, medicine, Binding site, Plasminogen activator, medicine.drug

Abstract

Tissue factor (TF) has been implicated in several important biologic processes, including fibrin formation, atherogenesis, angiogenesis, and tumor cell migration. In that plasminogen activators have been implicated in the same processes, the potential for interactions between TF and the plasminogen activator system was examined. Plasminogen was found to bind directly to the extracellular domain of TF apoprotein (amino acids 1-219) as determined by optical biosensor interaction analysis. A fragment of plasminogen containing kringles 1 through 3 also bound to TF apoprotein, whereas isolated kringle 4 and miniplasminogen did not. Expression of TF on the surface of a stably transfected Chinese hamster ovary (CHO) cell line stimulated plasminogen binding to the cells by 70% more than to control cells. Plasminogen bound to a site on the TF apoprotein that appears to be distinct from the binding site for factors VII and VIIa as judged by a combination of biosensor and cell assays. TF enhanced two-chain urokinase (tcuPA) activation of Glu-plasminogen, but not of miniplasminogen, in a dose-dependent, saturable manner (half maximal stimulation at 59 pmol/L). TF apoprotein induced an effect similar to that of relipidated TF, but a relatively higher concentration of the apoprotein was required (half maximal stimulation at 3.8 nmol/L). The stimulatory effect of TF on plasminogen activation was confirmed when plasmin formation was examined directly on sodium dodecyl sulfate-polyacrylamide gel electrophoresis. In accord with this, TF inhibited fibrinolysis by approximately 74% at a concentration of 14 nmol/L and almost totally inhibited the binding of equimolar concentrations of plasminogen to human umbilical vein endothelial cells and human trophoblasts. Further, CHO cells expressing TF inhibited uPA-mediated fibrinolysis relative to a wild-type control. TF apoprotein and plasminogen were found to colocalize in atherosclerotic plaque. These data suggest that plasminogen localization and activation may be modulated at extravascular sites through a high-affinity interaction between kringles 1 through 3 of plasminogen and the extracellular domain of TF.

Published

1998

10. P1–088: Immunotherapy using a novel anti–beta–amyloid 11–40/42 antibody in Tg2576 mice

Author

Patricia Rafferty, Marc Mercken, Michael Brigham-Burke, Peter J. Bugelski, Gabriela Canziani, Jacqueline Benson, Mary Birchler, Sonia S. Jung, and Don E. Griswold

Subjects

biology, Amyloid, Epidemiology, Chemistry, Health Policy, medicine.medical_treatment, Immunotherapy, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, biology.protein, medicine, Cancer research, Neurology (clinical), Geriatrics and Gerontology, Antibody, Beta (finance)

Published

2006

11. Targeting carbohydrate antigens in HIV vaccine development

Author

Anastas Pashov, Jason Plaxco, Behjatolah Monzavi-Karbassi, Thomas Kieber-Emmons, Gabriela Canziani, and Stewart L. MacLeod

Subjects

medicine.drug_class, HIV Antigens, Carbohydrates, Cross Reactions, HIV Antibodies, Monoclonal antibody, Mice, Antigen, Peptide Library, medicine, Animals, Humans, HIV vaccine, AIDS Vaccines, Mice, Inbred BALB C, Vaccines, Conjugate, General Veterinary, General Immunology and Microbiology, biology, Mimotope, Molecular Mimicry, Public Health, Environmental and Occupational Health, Lectin, Virology, Infectious Diseases, Concanavalin A, biology.protein, Molecular Medicine, Female, Antibody, Sequence motif

Abstract

Peptide mimotopes provide a strategy to augment human immunodeficiency virus 1 (HIV-1) specific carbohydrate reactive immune responses. Their antigenic and immunological properties will depend on the optimization of motif clustering and multimerization. We observe that structural variants of the same mimetic motif, linear versus cyclic, can be used to tune the properties of the antibodies elicited. The expansion of the database of mimotope sequence motifs can be increased by analyzing structures that bind to HIV directed monoclonal antibody 2G12 and the lectin Concanavalin A (Con A), fostering new mimotope designs. Such analysis indicates that these reagents bind to subsets of mannosyl antigens on the envelope (env) protein.

Published

2005