Your search keyword '"Antibodies, Monoclonal"' showing total 1,704 results

1. Development of betabodies: The next generation of phosphatidylserine targeting agents.

Author

Phinney NZ, Huang X, Toombs JE, and Brekken RA

Subjects

Humans, Animals, Mice, Tumor Microenvironment, Antibodies, Monoclonal, Recombinant Fusion Proteins metabolism, Recombinant Fusion Proteins genetics, Cell Line, Tumor, Neoplasms metabolism, Neoplasms drug therapy, Neoplasms immunology, Neoplasms pathology, Phosphatidylserines metabolism

Abstract

Externalized phosphatidylserine (PS) is a phospholipid and a selective marker of the tumor microenvironment (TME). It is exposed on the outer leaflet of the plasma membrane of tumor-associated endothelial cells, apoptotic tumor cells, and some viable tumor cells, where it functions in part to suppress immune responses by binding to PS receptors expressed on tumor-infiltrating myeloid cells. PS has been targeted with antibodies, such as bavituximab, that bind the phospholipid via a cofactor, β2-glycoprotein 1 (β2GP1); these antibodies showed excellent specificity for tumor vasculature and induce an immune stimulatory environment. We have advanced this concept by developing the next generation of PS targeting agent, a fusion protein (betabody) constructed by linking PS-binding domain V of β2GP1 to the Fc of an IgG2a. Betabodies bind to externalized PS with high affinity (∼1 nM), without the requirement of a co-factor and localize robustly to the TME. We demonstrate that betabodies are a direct PS-targeting agent that has the potential to be used as anti-tumor therapy, drug delivery vehicles, and tools for imaging the TME., Competing Interests: Conflict of interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: The authors declare that they have no conflicts of interest. A patent (US 8,956,616 B2) on betabodies has been issued to the University of Texas System, the authors of this manuscript are not associated with the patent., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

2. Generation of antibodies to an extracellular region of the transporters Glut1/Glut4 by immunization with a designed antigen.

Author

Sumikawa T, Nakakido M, Matsunaga R, Kuroda D, Nagatoishi S, and Tsumoto K

Subjects

Antibodies, Monoclonal, Glucose Transporter Type 1 genetics, Glucose Transporter Type 1 immunology, Immunization, Recombinant Proteins chemistry, Glucose Transporter Type 4 genetics, Glucose Transporter Type 4 immunology, Membrane Transport Proteins, Peptides

Abstract

Monoclonal antibodies are one of the fastest growing class of drugs. Nevertheless, relatively few biologics target multispanning membrane proteins because of technical challenges. To target relatively small extracellular regions of multiple membrane-spanning proteins, synthetic peptides, which are composed of amino acids corresponding to an extracellular region of a membrane protein, are often utilized in antibody discovery. However, antibodies to these peptides often do not recognize parental membrane proteins. In this study, we designed fusion proteins in which an extracellular helix of the membrane protein glucose transporter 1 (Glut1) was grafted onto the scaffold protein Adhiron. In the initial design, the grafted fragment did not form a helical conformation. Molecular dynamics simulations of full-length Glut1 suggested the importance of intramolecular interactions formed by surrounding residues in the formation of the helical conformation. A fusion protein designed to maintain such intramolecular interactions did form the desired helical conformation in the grafted region. We then immunized an alpaca with the designed fusion protein and obtained VHH (variable region of heavy-chain antibodies) using the phage display method. The binding of these VHH antibodies to the recombinant Glut1 protein was evaluated by surface plasmon resonance, and their binding to Glut1 on the cell membrane was further validated by flow cytometry. Furthermore, we also succeeded in the generation of a VHH against another integral membrane protein, glucose transporter 4 (Glut4) with the same strategy. These illustrates that our combined biochemical and computational approach can be applied to designing other novel fusion proteins for generating site-specific antibodies., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

3. Matrixed CDR grafting: A neoclassical framework for antibody humanization and developability.

Author

Gupta P, Horspool AM, Trivedi G, Moretti G, Datar A, Huang ZF, Chiecko J, Kenny CH, and Marlow MS

Subjects

Animals, Humans, Mice, Antibody Affinity, Complementarity Determining Regions chemistry, Antibodies, Monoclonal, Antibodies, Monoclonal, Humanized chemistry

Abstract

Discovery and optimization of a biotherapeutic monoclonal antibody requires a careful balance of target engagement and physicochemical developability properties. To take full advantage of the sequence diversity provided by different antibody discovery platforms, a rapid and reliable process for humanization of antibodies from nonhuman sources is required. Canonically, maximizing homology of the human variable region (V-region) to the original germline was believed to result in preservation of binding, often without much consideration for inherent molecular properties. We expand on this approach by grafting the complementary determining regions (CDRs) of a mouse anti-LAG3 antibody into an extensive matrix of human variable heavy chain (VH) and variable light chain (VL) framework regions with substantially broader sequence homology to assess the impact on complementary determining region-framework compatibility through progressive evaluation of expression, affinity, biophysical developability, and function. Specific VH and VL framework sequences were associated with major expression and purification phenotypes. Greater VL sequence conservation was correlated with retained or improved affinity. Analysis of grafts that bound the target demonstrated that initial developability criteria were significantly impacted by VH, but not VL. In contrast, cell binding and functional characteristics were significantly impacted by VL, but not VH. Principal component analysis of all factors identified multiple grafts that exhibited more favorable antibody properties, notably with nonoptimal sequence conservation. Overall, this study demonstrates that modern throughput systems enable a more thorough, customizable, and systematic analysis of graft-framework combinations, resulting in humanized antibodies with improved global properties that may progress through development more quickly and with a greater probability of success., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

4. Inhibition of cleavage of human complement component C5 and the R885H C5 variant by two distinct high affinity anti-C5 nanobodies.

Author

Struijf EM, De la O Becerra KI, Ruyken M, de Haas CJC, van Oosterom F, Siere DY, van Keulen JE, Heesterbeek DAC, Dolk E, Heukers R, Bardoel BW, Gros P, and Rooijakkers SHM

Subjects

Humans, Complement Activation, Complement Membrane Attack Complex, Complement System Proteins metabolism, Antibodies, Monoclonal, Complement C5 antagonists & inhibitors, Complement C5 genetics, Single-Domain Antibodies

Abstract

The human complement system plays a crucial role in immune defense. However, its erroneous activation contributes to many serious inflammatory diseases. Since most unwanted complement effector functions result from C5 cleavage into C5a and C5b, development of C5 inhibitors, such as clinically approved monoclonal antibody eculizumab, are of great interest. Here, we developed and characterized two anti-C5 nanobodies, UNbC5-1 and UNbC5-2. Using surface plasmon resonance, we determined a binding affinity of 119.9 pM for UNbC5-1 and 7.7 pM for UNbC5-2. Competition experiments determined that the two nanobodies recognize distinct epitopes on C5. Both nanobodies efficiently interfered with C5 cleavage in a human serum environment, as they prevented red blood cell lysis via membrane attack complexes (C5b-9) and the formation of chemoattractant C5a. The cryo-EM structure of UNbC5-1 and UNbC5-2 in complex with C5 (3.6 Å resolution) revealed that the binding interfaces of UNbC5-1 and UNbC5-2 overlap with known complement inhibitors eculizumab and RaCI3, respectively. UNbC5-1 binds to the MG7 domain of C5, facilitated by a hydrophobic core and polar interactions, and UNbC5-2 interacts with the C5d domain mostly by salt bridges and hydrogen bonds. Interestingly, UNbC5-1 potently binds and inhibits C5 R885H, a genetic variant of C5 that is not recognized by eculizumab. Altogether, we identified and characterized two different, high affinity nanobodies against human C5. Both nanobodies could serve as diagnostic and/or research tools to detect C5 or inhibit C5 cleavage. Furthermore, the residues targeted by UNbC5-1 hold important information for therapeutic inhibition of different polymorphic variants of C5., Competing Interests: Conflict of interest E. D. and R. H. are employees of QVQ Holding BV. Other authors declare no conflict of interest with the contents of this article., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

5. Exploring cellular biochemistry with nanobodies

Author

Ross W. Cheloha, Charlotte Wijne, Thomas U. Schwartz, Thibault J. Harmand, and Hidde L. Ploegh

Subjects

0301 basic medicine, 030102 biochemistry & molecular biology, medicine.drug_class, JBC Reviews, Cytological Techniques, Antibodies, Monoclonal, Context (language use), Cell Biology, Single-Domain Antibodies, Protein chemistry, Monoclonal antibody, Biochemistry, Antibody fragments, 03 medical and health sciences, Synthetic biology, 030104 developmental biology, Membrane protein, Chemical functionalization, medicine, Animals, Humans, Molecular Biology

Abstract

Reagents that bind tightly and specifically to biomolecules of interest remain essential in the exploration of biology and in their ultimate application to medicine. Besides ligands for receptors of known specificity, agents commonly used for this purpose are monoclonal antibodies derived from mice, rabbits, and other animals. However, such antibodies can be expensive to produce, challenging to engineer, and are not necessarily stable in the context of the cellular cytoplasm, a reducing environment. Heavy chain–only antibodies, discovered in camelids, have been truncated to yield single-domain antibody fragments (VHHs or nanobodies) that overcome many of these shortcomings. Whereas they are known as crystallization chaperones for membrane proteins or as simple alternatives to conventional antibodies, nanobodies have been applied in settings where the use of standard antibodies or their derivatives would be impractical or impossible. We review recent examples in which the unique properties of nanobodies have been combined with complementary methods, such as chemical functionalization, to provide tools with unique and useful properties.

Published

2020

6. The serum protein transthyretin as a platform for dimerization and tetramerization of antibodies and Fab fragments to enable target clustering

Author

Kenneth W. Walker, Ian Foltz, Hossein Salimi-Moosavi, Richele Bruno, Fei Lee, Zhulun Wang, Julie M. Bailis, Stephen Smith, Tina Wang, and Phillip An

Subjects

0301 basic medicine, endocrine system, Recombinant Fusion Proteins, Biochemistry, Conatumumab, Immunoglobulin Fab Fragments, Mice, 03 medical and health sciences, chemistry.chemical_compound, Antineoplastic Agents, Immunological, Tetramer, Cell Line, Tumor, Animals, Humans, Prealbumin, Receptor, Molecular Biology, 030102 biochemistry & molecular biology, biology, Chemistry, C-terminus, Antibodies, Monoclonal, nutritional and metabolic diseases, Neoplasms, Experimental, Cell Biology, Protein engineering, Ligand (biochemistry), Xenograft Model Antitumor Assays, Transthyretin, 030104 developmental biology, Protein Structure and Folding, biology.protein, Protein Multimerization, Antibody

Abstract

Transthyretin (TTR) is an abundant homotetrameric serum protein and was selected here for engineering higher-valency molecules because of its compact size, simple structure, and natural propensity to tetramerize. To demonstrate this utility, we fused TTR to the C terminus of conatumumab, an antibody that targets tumor necrosis factor–related apoptosis-inducing ligand receptor 2, as heavy chains to form antibody dimers and Fab heavy chains to form Fab tetramers. Moreover, we used constant heavy domain 3 heterodimerization substitutions to create TTR-mediated conatumumab tetramers. The conatumumab–TTR fusions displayed substantially enhanced potency in cell-based assays, as well as in murine tumor xenograft models. We conclude that antibody–TTR fusions may provide a powerful platform for multimerizing antibody and Fab fragments to enhance the capabilities of human therapeutics that benefit from target clustering and higher-order antigen-binding valency.

Published

2020

7. Antibody-guided proteases enable selective and catalytic degradation of challenging therapeutic targets.

Author

Romei MG, Leonard B, Kim I, Kim HS, and Lazar GA

Subjects

Immunoglobulin G, Antibodies, Monoclonal, Endopeptidases, Peptide Hydrolases metabolism, Biological Therapy methods

Abstract

The exquisite specificity, natural biological functions, and favorable development properties of antibodies make them highly effective agents as drugs. Monoclonal antibodies are particularly strong as inhibitors of systemically accessible targets where trough-level concentrations can sustain full target occupancy. Yet beyond this pharmacologic wheelhouse, antibodies perform suboptimally for targets of high abundance and those not easily accessible from circulation. Fundamentally, this restraint on broader application is due largely to the stoichiometric nature of their activity-one drug molecule is generally able to inhibit a maximum of two target molecules at a time. Enzymes in contrast are able to catalytically turnover multiple substrates, making them a natural sub-stoichiometric solution for targets of high abundance or in poorly accessible sites of action. However, enzymes have their own limitations as drugs, including, in particular, the polypharmacology and broad specificity often seen with native enzymes. In this study, we introduce antibody-guided proteolytic enzymes to enable selective sub-stoichiometric turnover of therapeutic targets. We demonstrate that antibody-mediated substrate targeting can enhance enzyme activity and specificity, with proof of concept for two challenging target proteins, amyloid-β and immunoglobulin G. This work advances a new biotherapeutic platform that combines the favorable properties of antibodies and proteolytic enzymes to more effectively suppress high-bar therapeutic targets., Competing Interests: Conflict of interest All authors are current or former employees of Genentech, a member of the Roche Group, and are shareholders in Roche., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

8. A novel epitope-presenting thermostable scaffold for the development of highly specific insulin-like growth factor-1/2 antibodies

Author

Michael Schräml, Marco Bocola, Sabine Goller, David Casagolda, Hartmut Düfel, Heidi Klöppel-Swarlik, Christian Scholz, Leopold Von Proff, Carmen Peeß, Alessandra Hoppe, Michael Gerg, and Frank Kowalewsky

Subjects

0301 basic medicine, antigen mimic, Immunogen, medicine.drug_class, FKBP domain, Molecular Dynamics Simulation, Monoclonal antibody, medicine.disease_cause, Biochemistry, Epitope, Epitopes, 03 medical and health sciences, Insulin-Like Growth Factor II, antibody, medicine, Humans, chaperone, Insulin-Like Growth Factor I, Molecular Biology, Escherichia coli, 030102 biochemistry & molecular biology, biology, Chemistry, FK-506 binding protein, Temperature, Antibodies, Monoclonal, protein engineering, Cell Biology, Protein engineering, Thermus thermophilus, biology.organism_classification, insulin-like growth factor (IGF), immunogen, antigen presentation, 030104 developmental biology, FKBP, Chaperone (protein), Protein Structure and Folding, biology.protein

Abstract

High sequence and structural homology between mature human insulin-like growth factors IGF-1 and IGF-2 makes serological discrimination by immunodiagnostic IGF tests a challenging task. There is an urgent need for highly specific IGF-1 and IGF-2 antibodies, yet only a short sequence element, i.e. the IGF loop, provides enough difference in sequence to discriminate between the two molecules. We sought to address this unmet demand by investigating novel chimeric immunogens as carriers for recombinant peptide motif grafting. We found Thermus thermophilus sensitive to lysis D (SlyD) and Thermococcus gammatolerans SlyD FK-506–binding protein (FKBP) domains suitable for presentation of the predefined epitopes, namely the IGF-1 and IGF-2 loops. Chimeric SlyD-IGF proteins allowed for the development of exceptionally specific IGF-1 and IGF-2 monoclonal antibodies. The selected antibodies bound with high affinity to the distinct IGF epitopes displayed on the protein scaffolds, as well as on the mature human IGF isoforms. The respective SlyD scaffolds display favorable engineering properties in that they are small, monomeric, and cysteine-free and can be produced in high yields in a prokaryotic host, such as Escherichia coli. In conclusion, FKBP domains from thermostable SlyD proteins are highly suitable as a generic scaffold platform for epitope grafting.

Published

2019

9. Functional genomic characterization of a synthetic anti-HER3 antibody reveals a role for ubiquitination by RNF41 in the anti-proliferative response

Author

Kevin R. Brown, Frederic A. Fellouse, Jacob P. Turowec, Kamaldeep K. Jawanda, Sachdev S. Sidhu, Jason Moffat, James Pan, Xiaowei Wang, and Esther Lau

Subjects

0301 basic medicine, Receptor, ErbB-3, Ubiquitin-Protein Ligases, Sequence Homology, Breast Neoplasms, Mice, SCID, Synthetic lethality, Biochemistry, Receptor tyrosine kinase, Mice, 03 medical and health sciences, Ubiquitin, Tumor Cells, Cultured, Animals, Humans, Amino Acid Sequence, skin and connective tissue diseases, Molecular Biology, Cell Proliferation, 030102 biochemistry & molecular biology, biology, Genome, Human, Ubiquitination, Antibodies, Monoclonal, Cell Biology, Xenograft Model Antitumor Assays, 3. Good health, Synthetic antibody, Ubiquitin ligase, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, body regions, 030104 developmental biology, Proteasome, biology.protein, Cancer research, Female, Antibody, Functional genomics, Signal Transduction

Abstract

Dysregulation of the ErbB family of receptor tyrosine kinases is involved in the progression of many cancers. Antibodies targeting the dimerization domains of family members EGFR and HER2 are approved cancer therapeutics, but efficacy is restricted to a subset of tumors and resistance often develops in response to treatment. A third family member, HER3, heterodimerizes with both EGFR and HER2 and has also been implicated in cancer. Consequently, there is strong interest in developing antibodies that target HER3, but to date, no therapeutics have been approved. To aid the development of anti-HER3 antibodies as cancer therapeutics, we combined antibody engineering and functional genomics screens to identify putative mechanisms of resistance or synthetic lethality with antibody-mediated anti-proliferative effects. We developed a synthetic antibody called IgG 95, which binds to HER3 and promotes ubiquitination, internalization, and receptor down-regulation. Using an shRNA library targeting enzymes in the ubiquitin proteasome system, we screened for genes that effect response to IgG 95 and uncovered the E3 ubiquitin ligase RNF41 as a driver of IgG 95 anti-proliferative activity. RNF41 has been shown previously to regulate HER3 levels under normal conditions and we now show that it is also responsible for down-regulation of HER3 upon treatment with IgG 95. Moreover, our findings suggest that down-regulation of RNF41 itself may be a mechanism for acquired resistance to treatment with IgG 95 and perhaps other anti-HER3 antibodies. Our work deepens our understanding of HER3 signaling by uncovering the mechanistic basis for the anti-proliferative effects of potential anti-HER3 antibody therapeutics.

Published

2019

10. An antagonistic monoclonal anti–Plexin-B1 antibody exerts therapeutic effects in mouse models of postmenopausal osteoporosis and multiple sclerosis

Author

Melanie Vogler, Arkadiusz Oleksy, Sabrina Schulze, Marina Fedorova, Baktybek Kojonazarov, Sharandip Nijjar, Seema Patel, Sian Jossi, Kovilen Sawmynaden, Maud Henry, Richard Brown, David Matthews, Stefan Offermanns, and Thomas Worzfeld

Subjects

Multiple Sclerosis, Antibodies, Monoclonal, Nerve Tissue Proteins, Receptors, Cell Surface, Semaphorins, Cell Biology, Ligands, Biochemistry, Disease Models, Animal, Mice, Antigens, CD, Animals, Humans, Female, Molecular Biology, Osteoporosis, Postmenopausal

Abstract

Osteoporosis and multiple sclerosis are highly prevalent diseases with limited treatment options. In light of these unmet medical needs, novel therapeutic approaches are urgently sought. Previously, the activation of the transmembrane receptor Plexin-B1 by its ligand semaphorin 4D (Sema4D) has been shown to suppress bone formation and promote neuroinflammation in mice. However, it is unclear whether inhibition of this receptor-ligand interaction by an anti-Plexin-B1 antibody could represent a viable strategy against diseases related to these processes. Here, we raised and systematically characterized a monoclonal antibody directed against the extracellular domain of human Plexin-B1, which specifically blocks the binding of Sema4D to Plexin-B1. In vitro, we show that this antibody inhibits the suppressive effects of Sema4D on human osteoblast differentiation and mineralization. To test the therapeutic potential of the antibody in vivo, we generated a humanized mouse line, which expresses transgenic human Plexin-B1 instead of endogenous murine Plexin-B1. Employing these mice, we demonstrate that the anti-Plexin-B1 antibody exhibits beneficial effects in mouse models of postmenopausal osteoporosis and multiple sclerosis in vivo. In summary, our data identify an anti-Plexin-B1 antibody as a potential therapeutic agent for the treatment of osteoporosis and multiple sclerosis.

Published

2022

11. Physiological C-terminal truncation of α-synuclein potentiates the prion-like formation of pathological inclusions

Author

Kimberly-Marie M. Gorion, Jason Caldwell, Cara J. Riffe, Niran Vijayaraghavan, Benoit I. Giasson, Zachary A. Sorrentino, and Kevin H. Strang

Subjects

0301 basic medicine, Amyloid, C terminal truncation, Fibril, Protein Aggregation, Pathological, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Prion protein, Molecular Biology, Mice, Inbred BALB C, Lewy body, Chemistry, Neurodegeneration, Antibodies, Monoclonal, Molecular Bases of Disease, Cell Biology, medicine.disease, Peptide Fragments, In vitro, Cell biology, HEK293 Cells, 030104 developmental biology, Proteolysis, alpha-Synuclein, α synuclein, Protein Multimerization, 030217 neurology & neurosurgery

Abstract

α-Synuclein (αsyn) aggregates into toxic fibrils in multiple neurodegenerative diseases where these fibrils form characteristic pathological inclusions such as Lewy bodies (LBs). The mechanisms initiating αsyn aggregation into fibrils are unclear, but ubiquitous post-translational modifications of αsyn present in LBs may play a role. Specific C-terminally (C)-truncated forms of αsyn are present within human pathological inclusions and form under physiological conditions likely in lysosome-associated pathways, but the roles for these C-truncated forms of αsyn in inclusion formation and disease are not well understood. Herein, we characterized the in vitro aggregation properties, amyloid fibril structures, and ability to induce full-length (FL) αsyn aggregation through prion-like mechanisms for eight of the most common physiological C-truncated forms of αsyn (1–115, 1–119, 1–122, 1–124, 1–125, 1–129, 1–133, and 1–135). In vitro, C-truncated αsyn aggregated more readily than FL αsyn and formed fibrils with unique morphologies. The presence of C-truncated αsyn potentiated aggregation of FL αsyn in vitro through co-polymerization. Specific C-truncated forms of αsyn in cells also exacerbated seeded aggregation of αsyn. Furthermore, in primary neuronal cultures, co-polymers of C-truncated and FL αsyn were potent prion-like seeds, but polymers composed solely of the C-truncated protein were not. These experiments indicated that specific physiological C-truncated forms of αsyn have distinct aggregation properties, including the ability to modulate the prion-like aggregation and seeding activity of FL αsyn. Proteolytic formation of these C-truncated species may have an important role in both the initiation of αsyn pathological inclusions and further progression of disease with strain-like properties.

Published

2018

12. Highly specific monoclonal antibodies for allosteric inhibition and immunodetection of the human pancreatic zinc transporter ZnT8

Author

Dax Fu, Chengfeng Merriman, Huilin Li, and Hua Li

Subjects

0301 basic medicine, medicine.drug_class, Allosteric regulation, Zinc Transporter 8, Monoclonal antibody, Biochemistry, Epitope, 03 medical and health sciences, Allosteric Regulation, Insulin-Secreting Cells, Drug Discovery, medicine, Humans, Genetic Predisposition to Disease, Molecular Biology, 030102 biochemistry & molecular biology, SLC30A8, biology, Chemistry, Drug discovery, Methods and Resources, Antibodies, Monoclonal, Transporter, Cell Biology, Solute carrier family, 030104 developmental biology, Diabetes Mellitus, Type 2, biology.protein

Abstract

Solute carrier family 30 member 8 (SLC30A8), encoding the pancreatic zinc transporter ZnT8, is a susceptibility gene for type 2 diabetes (T2D). Reducing ZnT8 transport activity or down-regulating its cellular expression is hypothesized to be an antidiabetogenic strategy mimicking the protective effect of SLC30A8 haploinsufficiency in humans. However, research tools to inhibit ZnT8 activity and measure cellular ZnT8 levels are not available. Here, we report the identification of two anti-ZnT8 mAbs applicable to addressing these unmet needs. Both mAbs exhibited subnanomolar affinities for human ZnT8 and were selective against homologous zinc transporters with distinct cross-species reactivities and epitope recognition. We showed that antigen-binding fragments (Fabs) protected ZnT8 from unfolding and inhibited ZnT8-mediated zinc transport in proteoliposomes. Negative-stain EM revealed a ternary binding complex of a ZnT8 monomer and two different Fabs at a 1:1:1 stoichiometry. Moreover, dual bindings of two different mAbs to a single ZnT8 protein multiplied the individual anti-ZnT8 specificities, enabling quantification of cellular ZnT8 levels by homogeneous time-resolved fluorescence (HTRF). Our results demonstrate the utilities of the two generated mAbs as allosteric inhibitors and highly specific biosensors of human ZnT8.

Published

2018

13. Are N- and C-terminally truncated Aβ species key pathological triggers in Alzheimer's disease?

Author

Frédéric Checler, Julie Dunys, Audrey Valverde, Institut de pharmacologie moléculaire et cellulaire (IPMC), Université Nice Sophia Antipolis (... - 2019) (UNS), COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Centre National de la Recherche Scientifique (CNRS), Centre National de la Recherche Scientifique (CNRS)-Université Nice Sophia Antipolis (... - 2019) (UNS), and COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Université Côte d'Azur (UCA)

Subjects

0301 basic medicine, Proteolysis, Protein domain, Gene Expression, tau Proteins, Biochemistry, Amyloid beta-Protein Precursor, Mice, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, Alzheimer Disease, Gene expression, medicine, Animals, Humans, CA1 Region, Hippocampal, Molecular Biology, Nootropic Agents, ComputingMilieux_MISCELLANEOUS, Neurons, Amyloid beta-Peptides, medicine.diagnostic_test, Chemistry, Neurodegeneration, Neurotoxicity, Antibodies, Monoclonal, Minireviews, Cell Biology, medicine.disease, Cell biology, Disease Models, Animal, Neuroprotective Agents, 030104 developmental biology, Biomarker (medicine), [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Amyloid Precursor Protein Secretases, Alzheimer's disease, 030217 neurology & neurosurgery, Function (biology)

Abstract

The histopathology of Alzheimer's disease (AD) is characterized by neuronal loss, neurofibrillary tangles, and senile plaque formation. The latter results from an exacerbated production (familial AD cases) or altered degradation (sporadic cases) of 40/42-amino acid–long β-amyloid peptides (Aβ peptides) that are produced by sequential cleavages of Aβ precursor protein (βAPP) by β- and γ-secretases. The amyloid cascade hypothesis proposes a key role for the full-length Aβ42 and the Aβ40/42 ratio in AD etiology, in which soluble Aβ oligomers lead to neurotoxicity, tau hyperphosphorylation, aggregation, and, ultimately, cognitive defects. However, following this postulate, during the last decade, several clinical approaches aimed at decreasing full-length Aβ42 production or neutralizing it by immunotherapy have failed to reduce or even stabilize AD-related decline. Thus, the Aβ peptide (Aβ40/42)-centric hypothesis is probably a simplified view of a much more complex situation involving a multiplicity of APP fragments and Aβ catabolites. Indeed, biochemical analyses of AD brain deposits and fluids have unraveled an Aβ peptidome consisting of additional Aβ-related species. Such Aβ catabolites could be due to either primary enzymatic cleavages of βAPP or secondary processing of Aβ itself by exopeptidases. Here, we review the diversity of N- and C-terminally truncated Aβ peptides and their biosynthesis and outline their potential function/toxicity. We also highlight their potential as new pharmaceutical targets and biomarkers.

Published

2018

14. Agonistic β-Klotho antibody mimics fibroblast growth factor 21 (FGF21) functions

Author

Xiaoshan Min, Sheree Johnstone, Wei Wang, Zhulun Wang, Xinchao Yu, Jennifer Weiszmann, William G. Romanow, Stephen T. Thibault, and Yang Li

Subjects

0301 basic medicine, Scaffold protein, Receptor complex, FGF21, Protein Conformation, medicine.drug_class, Antibody Affinity, CHO Cells, Crystallography, X-Ray, Fibroblast growth factor, Monoclonal antibody, Biochemistry, Mice, 03 medical and health sciences, Cricetulus, 0302 clinical medicine, TIM barrel, medicine, Animals, Humans, Receptor, Fibroblast Growth Factor, Type 1, Receptor, Klotho Proteins, Molecular Biology, Chemistry, Antibodies, Monoclonal, Membrane Proteins, Cell Biology, Cell biology, Fibroblast Growth Factors, Microscopy, Electron, 030104 developmental biology, Fibroblast growth factor receptor, 030217 neurology & neurosurgery, Protein Binding, Signal Transduction

Abstract

Fibroblast growth factor 21 (FGF21), an endocrine hormone in the FGF family, plays a critical role in regulating metabolic homeostasis and has emerged as a therapeutic target for metabolic diseases, including Type 2 diabetes mellitus. FGF21 functions through a receptor complex that consists of an FGF receptor (FGFR) and a co-receptor β-Klotho. Here, we identify and biochemically and structurally characterize 39F7, a high-affinity agonistic monoclonal antibody (mAb) against β-Klotho that mimics FGF21 function. The co-crystal structure of β-Klotho KL1 domain in complex with 39F7 Fab revealed that the recognition of 39F7 is centered on Trp-295 of β-Klotho in a FGF21 noncompetitive manner. KL1 adopts a (β/α)8 TIM barrel fold which resembles that of β-glycosylceramidase, but lacks molecular features for enzymatic activity, suggesting that KL1 functions as a scaffold protein instead. In vitro characterization demonstrated that, although 39F7 does not compete with FGF21, it is specific for β-Klotho/FGFR1c activation. Furthermore, the agonistic activity of 39F7 required the full IgG molecule to be bivalent, suggesting that 39F7 functions by promoting receptor/co-receptor dimerization. Supported by negative stain EM analysis of full-length β-Klotho, we propose a molecular model wherein the agonistic antibody 39F7 acts in a β-Klotho– and FGFR1c-dependent manner, mimicking FGF21 activity. More importantly, 39F7 offers promising therapeutic potential in the axis of FGF21 signaling as an antibody therapy alternative to FGF21 analogs for treatment of metabolic diseases.

Published

2018

15. Bacterially expressed HIV-1 gp120 outer-domain fragment immunogens with improved stability and affinity for CD4-binding site neutralizing antibodies

Author

Joanne DeStefano, Aditya Arun Kumar, Aaron J. Wilson, Celia C. La Branche, Sanchari Bhattacharyya, Heather Arendt, David C. Montefiori, Mansi Purwar, Christopher L. Parks, Venkada Subramanian Vignesh, Raghavan Varadarajan, Raksha Das, and Ujjwal Rathore

Subjects

0301 basic medicine, Immunogen, Immunology, Protein design, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Crystallography, X-Ray, Ligands, Biochemistry, Neutralization, Epitope, Epitopes, 03 medical and health sciences, Animals, Humans, Binding site, Neutralizing antibody, Molecular Biology, AIDS Vaccines, Binding Sites, biology, Chemistry, Immunogenicity, Antibodies, Monoclonal, Cell Biology, Antibodies, Neutralizing, Virology, 030104 developmental biology, CD4 Antigens, HIV-1, biology.protein, Rabbits, Antibody, Broadly Neutralizing Antibodies, Protein Binding

Abstract

Protein minimization is an attractive approach for designing vaccines against rapidly evolving pathogens such as human immunodeficiency virus, type 1 (HIV-1), because it can help in focusing the immune response toward conserved conformational epitopes present on complex targets. The outer domain (OD) of HIV-1 gp120 contains epitopes for a large number of neutralizing antibodies and therefore is a primary target for structure-based vaccine design. We have previously designed a bacterially expressed outer-domain immunogen (OD(EC)) that bound CD4-binding site (CD4bs) ligands with 3–12 μm affinity and elicited a modest neutralizing antibody response in rabbits. In this study, we have optimized OD(EC) using consensus sequence design, cyclic permutation, and structure-guided mutations to generate a number of variants with improved yields, biophysical properties, stabilities, and affinities (K(D) of 10–50 nm) for various CD4bs targeting broadly neutralizing antibodies, including the germline-reverted version of the broadly neutralizing antibody VRC01. In contrast to OD(EC), the optimized immunogens elicited high anti-gp120 titers in rabbits as early as 6 weeks post-immunization, before any gp120 boost was given. Following two gp120 boosts, sera collected at week 22 showed cross-clade neutralization of tier 1 HIV-1 viruses. Using a number of different prime/boost combinations, we have identified a cyclically permuted OD fragment as the best priming immunogen, and a trimeric, cyclically permuted gp120 as the most suitable boosting molecule among the tested immunogens. This study also provides insights into some of the biophysical correlates of improved immunogenicity.

Published

2018

16. Structure–function characterization of three human antibodies targeting the vaccinia virus adhesion molecule D8

Author

Dirk M. Zajonc, Shane Crotty, Yan Xiang, Jing Wang, Klaus Ley, Thomas Kaever, Zbigniew Mikulski, Xiangzhi Meng, Greg Miller, Matthias Hupfer, Michael H. Matho, Linda C. Hsieh-Wilson, Andrew Schlossman, Aruna Bitra, Bjoern Peters, Iuliia M. Gilchuk, Tzanko Doukov, and James E. Crowe

Subjects

0301 basic medicine, Viral protein, viruses, Immunology, Enzyme-Linked Immunosorbent Assay, Vaccinia virus, Plasma protein binding, Antibodies, Viral, Crystallography, X-Ray, medicine.disease_cause, Biochemistry, Antibodies, Epitope, Epitopes, Structure-Activity Relationship, 03 medical and health sciences, Protein structure, Viral Envelope Proteins, Neutralization Tests, medicine, Humans, Neutralizing antibody, Antigens, Viral, Molecular Biology, biology, Chemistry, Cell adhesion molecule, Antibodies, Monoclonal, virus diseases, Cell Biology, Protein engineering, Ligand (biochemistry), Antibodies, Neutralizing, Molecular biology, 030104 developmental biology, Antibody Formation, biology.protein, Cell Adhesion Molecules, Protein Binding

Abstract

Vaccinia virus (VACV) envelope protein D8 is one of three glycosaminoglycan adhesion molecules and binds to the linear polysaccharide chondroitin sulfate (CS). D8 is also a target for neutralizing antibody responses that are elicited by the smallpox vaccine, which has enabled the first eradication of a human viral pathogen and is a useful model for studying antibody responses. However, to date, VACV epitopes targeted by human antibodies have not been characterized at atomic resolution. Here, we characterized the binding properties of several human anti-D8 antibodies and determined the crystal structures of three VACV-mAb variants, VACV-66, VACV-138, and VACV-304, separately bound to D8. Although all these antibodies bound D8 with high affinity and were moderately neutralizing in the presence of complement, VACV-138 and VACV-304 also fully blocked D8 binding to CS-A, the low affinity ligand for D8. VACV-138 also abrogated D8 binding to the high-affinity ligand CS-E, but we observed residual CS-E binding was observed in the presence of VACV-304. Analysis of the VACV-138– and VACV-304–binding sites along the CS-binding crevice of D8, combined with different efficiencies of blocking D8 adhesion to CS-A and CS-E allowed us to propose that D8 has a high- and low-affinity CS-binding region within its central crevice. The crevice is amenable to protein engineering to further enhance both specificity and affinity of binding to CS-E. Finally, a wild-type D8 tetramer specifically bound to structures within the developing glomeruli of the kidney, which express CS-E. We propose that through structure-based protein engineering, an improved D8 tetramer could be used as a potential diagnostic tool to detect expression of CS-E, which is a possible biomarker for ovarian cancer.

Published

2018

17. Structural details of monoclonal antibody m971 recognition of the membrane-proximal domain of CD22

Author

Wei Li, Dorota Borovsky, Jean-Philippe Julien, Iga Kucharska, Taylor Sicard, Hong Cui, Dimiter S. Dimitrov, Yang Feng, Xianglei Liu, and June Ereño-Orbea

Subjects

crystal structure, Sialic Acid Binding Ig-like Lectin 2, CAR-T cell, Antigens, CD19, SLS, static light scattering, Immunoglobulin domain, m971, GAG, glycosaminoglycan, Biochemistry, MSLN, mesothelin, Epitope, HEK 293S, HEK 293 GnT I−/−, Fragment antigen-binding, B-ALL, B-cell acute lymphoblastic leukemia, Protein Domains, antibody, Siglec, sialic acid–binding immunoglobulin-like lectin, hemic and lymphatic diseases, BLI, biolayer interferometry, CD22, ITIMs, intracellular tyrosine-based inhibitory motifs, Molecular Biology, CD22, cluster of differentiation-22, Tonset, onset aggregation temperature, B-Lymphocytes, B cell, HCDRs, heavy-chain complementarity-determining regions, Tm, melting temperature, biology, Chemistry, Antibodies, Monoclonal, CAR-T cell, chimeric antigen receptor T cell, SIGLEC, Cell Biology, ECD, extracellular domain, Ig, immunoglobulin, Chimeric antigen receptor, Cell biology, Fab, fragment antigen-binding, biology.protein, CARs, chimeric antigen receptors, Paratope, Antibody, Research Article

Abstract

Cluster of differentiation-22 (CD22) belongs to the sialic acid–binding immunoglobulin (Ig)-like lectin family of receptors that is expressed on the surface of B cells. It has been classified as an inhibitory coreceptor for the B-cell receptor because of its function in establishing a baseline level of B-cell inhibition. The restricted expression of CD22 on B cells and its inhibitory function make it an attractive target for B-cell depletion in cases of B-cell malignancies. Genetically modified T cells with chimeric antigen receptors (CARs) derived from the m971 antibody have shown promise when used as an immunotherapeutic agent against B-cell acute lymphoblastic leukemia. A key aspect of the efficacy of this CAR-T was its ability to target a membrane-proximal epitope on the CD22 extracellular domain; however, the molecular details of m971 recognition of CD22 have thus far remained elusive. Here, we report the crystal structure of the m971 fragment antigen-binding in complex with the two most membrane-proximal Ig-like domains of CD22 (CD22d6–d7). The m971 epitope on CD22 resides at the most proximal Ig domain (d7) to the membrane, and the antibody paratope contains electrostatic surfaces compatible with interactions with phospholipid head groups. Together, our data identify molecular details underlying the successful transformation of an antibody epitope on CD22 into an effective CAR immunotherapeutic target.

Published

2021

18. Mechanisms of recognition of amyloid-β (Aβ) monomer, oligomer, and fibril by homologous antibodies

Author

Buyong Ma, Jun Zhao, and Ruth Nussinov

Subjects

Models, Molecular, 0301 basic medicine, Amyloid, Protein Conformation, Pentamer, Recombinant Fusion Proteins, Peptide, Molecular Dynamics Simulation, Antibodies, Monoclonal, Humanized, Protein Engineering, Fibril, Protein Aggregation, Pathological, Biochemistry, Oligomer, Antibodies, Protein Aggregates, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antibody Specificity, medicine, Animals, Humans, Solanezumab, Molecular Biology, Nootropic Agents, chemistry.chemical_classification, Amyloid beta-Peptides, Antibodies, Monoclonal, Cell Biology, Complementarity Determining Regions, Molecular Docking Simulation, Molecular Weight, 030104 developmental biology, Monomer, chemistry, Structural Homology, Protein, Drug Design, Protein Structure and Folding, Crenezumab, Biophysics, Binding Sites, Antibody, Protein Multimerization, 030217 neurology & neurosurgery, Entropy (order and disorder), medicine.drug

Abstract

Alzheimer's disease is one of the most devastating neurodegenerative diseases without effective therapies. Immunotherapy is a promising approach, but amyloid antibody structural information is limited. Here we simulate the recognition of monomeric, oligomeric, and fibril amyloid-β (Aβ) by three homologous antibodies (solanezumab, crenezumab, and their chimera, CreneFab). Solanezumab only binds the monomer, whereas crenezumab and CreneFab can recognize different oligomerization states; however, the structural basis for this observation is not understood. We successfully identified stable complexes of crenezumab with Aβ pentamer (oligomer model) and 16-mer (fibril model). It is noteworthy that solanezumab targets Aβ residues 16-26 preferentially in the monomeric state; conversely, crenezumab consistently targets residues 13-16 in different oligomeric states. Unlike the buried monomeric peptide in solanezumab's complementarity-determining region, crenezumab binds the oligomer's lateral and edge residues. Surprisingly, crenezumab's complementarity-determining region loops can effectively bind the Aβ fibril lateral surface around the same 13-16 region. The constant domain influences antigen recognition through entropy redistribution. Different constant domain residues in solanezumab/crenezumab/chimera influence the binding of Aβ aggregates. Collectively, we provide molecular insight into the recognition mechanisms facilitating antibody design.

Published

2017

19. Palmitoylation is a prerequisite for dimerization-dependent raftophilicity of rhodopsin

Author

Fumio Hayashi and Keiji Seno

Subjects

Models, Molecular, 0301 basic medicine, Rhodopsin, Light, Protein Conformation, G protein, Stereochemistry, Lipoylation, Dark Adaptation, Biochemistry, Amphibian Proteins, 03 medical and health sciences, Membrane Microdomains, Protein structure, Palmitoylation, Animals, Cysteine, Transducin, Molecular Biology, Lipid raft, G protein-coupled receptor, Rana catesbeiana, biology, Protein Stability, Chemistry, Antibodies, Monoclonal, Cell Biology, Rod Cell Outer Segment, Kinetics, 030104 developmental biology, biology.protein, Biophysics, Cystine, lipids (amino acids, peptides, and proteins), Protein Multimerization, Dimerization, Hydrophobic and Hydrophilic Interactions, Oxidation-Reduction, Protein Processing, Post-Translational, Signal Transduction, Visual phototransduction

Abstract

The visual photopigment rhodopsin (Rh) is a prototypical G protein–coupled receptor (GPCR) responsible for initiation of the phototransduction cascade in rod photoreceptors. Similar to other GPCRs, Rh can form dimers or even higher oligomers and tends to have a supramolecular organization that is likely important in the dim light response. Rh also exhibits high affinity for lipid rafts (i.e. raftophilicity) upon light-dependent binding with the cognate G protein transducin (Gt), suggesting the presence of lipid raft-like domains in the retinal disk membrane and their importance in phototransduction. However, the relationship between Rh oligomerization and lipid rafts in the disk membrane remains to be explored. Given previous findings that Gt binds to dimeric Rh and that Rh is posttranslationally modified with two highly raftophilic palmitoyl moieties, we hypothesized that Rh becomes raftophilic upon dimerization. Here, using biochemical assays, we found that Rh*–Gt complexes in the detergent-resistant membrane are partially resistant to cholesterol depletion by methyl-β-cyclodextrin and that the Rh-to-Gt stoichiometry in this methyl-β-cyclodextrin–resistant complex is 2:1. Next, we found that IgG-mediated Rh–Rh cross-linking renders Rh highly raftophilic, supporting the premise that Rh becomes raftophilic upon dimerization. Rh depalmitoylation via reduction of thioester linkages blocked the translocation of IgG–cross-linked Rh to the detergent-resistant membrane, highlighting that the two palmitoyl moieties are important for the dimerization-dependent raftophilicity of Rh. These results indicate that palmitoylated GPCRs such as Rh can acquire raftophilicity upon G protein–stabilized dimerization and thereby organize receptor-cluster rafts by recruiting raftophilic lipids.

Published

2017

20. Structural and functional analyses of pyroglutamate-amyloid-β-specific antibodies as a basis for Alzheimer immunotherapy

Author

Milton T. Stubbs, Stephan Schilling, Hans-Ulrich Demuth, Jens-Ulrich Rahfeld, Christoph Parthier, Martin Kleinschmidt, Anke Piechotta, Inge Lues, Kathrin Gnoth, and Thierry Pillot

Subjects

0301 basic medicine, medicine.drug_class, medicine.medical_treatment, Peptide, Monoclonal antibody, Biochemistry, Mice, 03 medical and health sciences, 0302 clinical medicine, Alzheimer Disease, In vivo, medicine, Animals, Molecular Biology, Cells, Cultured, chemistry.chemical_classification, Amyloid beta-Peptides, biology, Antibodies, Monoclonal, Cell Biology, Immunotherapy, medicine.disease, In vitro, Pyrrolidonecarboxylic Acid, N-terminus, 030104 developmental biology, chemistry, Protein Structure and Folding, biology.protein, Alzheimer's disease, Antibody, 030217 neurology & neurosurgery

Abstract

Alzheimer disease is associated with deposition of the amyloidogenic peptide Aβ in the brain. Passive immunization using Aβ-specific antibodies has been demonstrated to reduce amyloid deposition both in vitro and in vivo. Because N-terminally truncated pyroglutamate (pE)-modified Aβ species (AβpE3) exhibit enhanced aggregation potential and propensity to form toxic oligomers, they represent particularly attractive targets for antibody therapy. Here we present three separate monoclonal antibodies that specifically recognize AβpE3 with affinities of 1–10 nm and inhibit AβpE3 fibril formation in vitro. In vivo application of one of these resulted in improved memory in AβpE3 oligomer-treated mice. Crystal structures of Fab-AβpE3 complexes revealed two distinct binding modes for the peptide. Juxtaposition of pyroglutamate pE3 and the F4 side chain (the “pEF head”) confers a pronounced bulky hydrophobic nature to the AβpE3 N terminus that might explain the enhanced aggregation properties of the modified peptide. The deep burial of the pEF head by two of the antibodies explains their high target specificity and low cross-reactivity, making them promising candidates for the development of clinical antibodies.

Published

2017

21. Targeted Fcγ Receptor (FcγR)-mediated Clearance by a Biparatopic Bispecific Antibody

Author

Christine Fazenbaker, G. Jonah A. Rainey, Craig N. Jenne, Tracy Chen, Srinath Kasturirangan, Alyse D. Portnoff, Xinwei Wang, Changshou Gao, Helen Zhong, Jared S. Bee, Herren Wu, Linda Xu, and Zhutian Zeng

Subjects

0301 basic medicine, microscopic imaging, Kupffer Cells, medicine.drug_class, Immunology, Fc receptor, Antigen-Antibody Complex, macrophage, Monoclonal antibody, Biochemistry, Epitope, Mice, 03 medical and health sciences, Immune system, Antigen, antibody, Antibodies, Bispecific, medicine, Animals, Humans, Macrophage, Receptor, Molecular Biology, IL-6, antibody engineering, biology, Interleukin-6, protein complex, Receptors, IgG, Antibodies, Monoclonal, Cell Biology, Cell biology, HEK293 Cells, 030104 developmental biology, Liver, Immunoglobulin G, biology.protein, Antibody, electron microscopy (EM), pharmacokinetics, Protein Binding

Abstract

Soluble ligands have commonly been targeted by antibody therapeutics for cancers and other diseases. Although monoclonal antibodies targeting such ligands can block their interactions with their cognate receptors, they can also significantly increase the half-life of their ligands by FcRn-mediated antibody recycling, thereby evading ligand renal clearance and requiring increasingly high antibody doses to neutralize the increasing pool of target. To overcome this issue, we generated a bispecific/biparatopic antibody (BiSAb) that targets two different epitopes on IL-6 to block IL-6-mediated signaling. The BiSAb formed large immune complexes with IL-6 that can bind Fcγ receptors on phagocytic cells and are rapidly internalized. In addition, rapid clearance of the BiSAb·IL-6 complex was observed in mice while the parental antibodies prolonged the serum half-life of IL-6. Intravital imaging of the liver in mice confirmed that the rapid clearance of these large immune complexes was associated with Fcγ receptor-dependent binding to Kupffer cells in the liver. The approach described here provides a general strategy for therapeutic antibodies with the ability to not only neutralize but also actively drive clearance of their soluble antigens.

Published

2017

22. Biological Characterization of a Stable Effector Functionless (SEFL) Monoclonal Antibody Scaffold in Vitro

Author

Madeline M. Fort, Nancy E. Everds, Mai Phuong Nguyen, Linda O. Narhi, Darcey Clark, Yan Bin Yu, Padma K. Narayanan, Nianyu Li, Yao Zhuang, Riki Stevenson, Kannan Gunasekaran, Jeanine L. Bussiere, Ling Liu, Kei Kim, and Frederick W. Jacobsen

Subjects

Blood Platelets, 0301 basic medicine, medicine.drug_class, Immunology, Fc receptor, Monoclonal antibody, Biochemistry, Monocytes, Mice, 03 medical and health sciences, 0302 clinical medicine, Phagocytosis, Cell Line, Tumor, medicine, Animals, Humans, Platelet activation, Cytotoxicity, Molecular Biology, Antibody-dependent cell-mediated cytotoxicity, biology, Receptors, IgG, Antibodies, Monoclonal, Cell Biology, Platelet Activation, Molecular biology, In vitro, Complement-dependent cytotoxicity, Macaca fascicularis, 030104 developmental biology, Immunoglobulin G, 030220 oncology & carcinogenesis, biology.protein, Antibody

Abstract

The stable effector functionLess (SEFL) antibody was designed as an IgG1 antibody with a constant region that lacks the ability to interact with Fcγ receptors. The engineering and stability and pharmacokinetic assessments of the SEFL scaffold is described in the accompanying article (Jacobsen, F. W., Stevenson, R., Li, C., Salimi-Moosavi, H., Liu, L., Wen, J., Luo, Q., Daris, K., Buck, L., Miller, S., Ho, S-Y., Wang, W., Chen, Q., Walker, K., Wypych, J., Narhi, L., and Gunasekaran, K. (2017) J. Biol. Chem. 292). The biological properties of these SEFL antibodies were assessed in a variety of human and cynomolgus monkey in vitro assays. Binding of parent molecules and their SEFL variants to human and cynomolgus monkey FcγRs were evaluated using flow cytometry-based binding assays. The SEFL variants tested showed decreased binding affinity to human and cynomolgus FcγRs compared with the wild-type IgG1 antibody. In addition, SEFL variants demonstrated no antibody-dependent cell-mediated cytotoxicity in vitro against Daudi cells with cynomolgus monkey peripheral blood mononuclear cells, and had minimal complement-dependent cytotoxicity activity similar to that of the negative control IgG2 in a CD20+ human Raji lymphoma cell line. SEFL mutations eliminated off-target antibody-dependent monocyte phagocytosis of cynomolgus monkey platelets, and cynomolgus platelet activation in vitro. These experiments demonstrate that the SEFL modifications successfully eliminated Fc-associated effector binding and functions.

Published

2017

23. Reply to Cattoretti: Specificity of anti-MYC antibodies

Author

Ye Seul Son, Kyung-Bok Lee, Boon-Eng Teh, Janghwan Kim, Kwang Bo Jung, Mi-Young Son, Insoo Kang, and Ilkyun Im

Subjects

biology, business.industry, Antibodies, Monoclonal, Cell Biology, Cellular Reprogramming, Biochemistry, Virology, Proto-Oncogene Proteins c-myc, Text mining, biology.protein, Humans, Single-Cell Analysis, Antibody, Letters to the Editor, business, Molecular Biology, Biomarkers

Published

2020

24. Anti-GPR56 monoclonal antibody potentiates GPR56-mediated Src-Fak signaling to modulate cell adhesion

Author

Kendra S. Carmon, Ling Wu, Liezl E. Francisco, Joan Jacob, Tressie A. Posey, Sheng Zhang, Qingyun Liu, Wangsheng Yu, and Treena Chatterjee

Subjects

0301 basic medicine, Serum Response Factor, RHOA, ADGRG1, Carcinogenesis, focal adhesion kinase (Fak), Biochemistry, Receptors, G-Protein-Coupled, GPR56, G-protein-coupled receptor 56, RhoA, Ras homolog family member A, siRNA, small interfering ribonucleic acid, SRE, serum response element, Phosphorylation, biology, Chemistry, Antibodies, Monoclonal, Adhesion G-Protein Coupled Receptor G1, G-protein-coupled receptor (GPCR), Cell biology, Gene Expression Regulation, Neoplastic, src-Family Kinases, 7TM, seven-transmembrane, CRC, colorectal cancer, Pax, paxillin, shRNA, short hairpin ribonucleic acid, Colorectal Neoplasms, Signal Transduction, Research Article, Src, CTF, C-terminal fragment, Proto-oncogene tyrosine-protein kinase Src, GPS, GPCR Proteolysis Site, colorectal cancer (CRC), Focal adhesion, 03 medical and health sciences, Cell Line, Tumor, SRF-RE, serum response factor response element, Humans, mAb, monoclonal antibody, Cell adhesion, Molecular Biology, Paxillin, KD, knockdown, paxillin, 030102 biochemistry & molecular biology, STP, Serine–Threonine–Proline-rich, GAIN, GPCR-autoproteolysis inducing, PLL, Pentraxin/Laminin/neurexin/sex-hormone(LNS)-binding-globulin-Like, aGPCR, adhesion G-protein-coupled receptor, cell adhesion, Src, Src proto-oncogene, nonreceptor tyrosine kinase, Cell Biology, ECD, extracellular domain, WT, wild-type, Fak, focal adhesion kinase, NTF, N-terminal fragment, 030104 developmental biology, GPR56, monoclonal antibody, Focal Adhesion Kinase 1, ADGRG1, adhesion G protein-coupled receptor G1, ICC, immunocytochemistry, biology.protein, rhoA GTP-Binding Protein

Abstract

GPR56 is a member of the adhesion G-protein-coupled receptor family shown to play important roles in cell adhesion, brain development, immune function, and tumorigenesis. GPR56 is highly upregulated in colorectal cancer and correlates with poor prognosis. Several studies have shown GPR56 couples to the Gα12/13 class of heterotrimeric G-proteins to promote RhoA activation. However, due to its structural complexity and lack of a high-affinity receptor-specific ligand, the complete GPR56 signaling mechanism remains largely unknown. To delineate the activation mechanism and intracellular signaling functions of GPR56, we generated a monoclonal antibody (mAb) that binds with high affinity and specificity to the extracellular domain (ECD). Using deletion mutants, we mapped the mAb binding site to the GAIN domain, which mediates membrane-proximal autoproteolytic cleavage of the ECD. We showed that GPR56 overexpression in 293T cells leads to increased phosphorylation of Src, Fak, and paxillin adhesion proteins and activation of the Gα12/13-RhoA-mediated serum response factor (SRF) pathway. Treatment with the mAb potentiated Src-Fak phosphorylation, RhoA–SRF signaling, and cell adhesion. Consistently, GPR56 knockdown in colorectal cancer cells decreased Src–Fak pathway phosphorylation and cell adhesion. Interestingly, GPR56-mediated activation of Src–Fak phosphorylation occurred independent of RhoA, yet mAb-induced potentiation of RhoA–SRF signaling was Src-dependent. Furthermore, we show that the C-terminal portion of the Serine–Threonine–Proline-rich (STP) region, adjacent to the GAIN domain, was required for Src–Fak activation. However, autoproteolytic cleavage of the ECD was dispensable. These data support a new ECD-dependent mechanism by which GPR56 functions to regulate adhesion through activation of Src–Fak signaling.

Published

2021

25. A novel anti-human IL-1R7 antibody reduces IL-18-mediated inflammatory signaling

Author

Jared J. Lindenberger, Nicholas E. Powers, Karsten Beckmann, Liqiong Jiang, Suzhao Li, Stephan Fischer, Dennis M. de Graaf, Ulrich Pessara, Charles A. Dinarello, Jesper F Højen, Elan Z. Eisenmesser, and Tania Azam

Subjects

Lipopolysaccharides, 0301 basic medicine, medicine.medical_treatment, Anti-Inflammatory Agents, Biochemistry, Candida albicans, Interferon gamma, Receptor, Research Articles, Receptors, Interleukin-18, Chemistry, Macrophage Activation Syndrome, Interleukin-18, NF-kappa B, Antibodies, Monoclonal, interleukin-18 (IL-18), Cytokine, Interleukin 18, Tumor necrosis factor alpha, medicine.symptom, Signal transduction, Signal Transduction, medicine.drug, Primary Cell Culture, Inflammation, macrophage activation syndrome (MAS), Proinflammatory cytokine, Interferon-gamma, 03 medical and health sciences, medicine, Humans, Immunologic Factors, Molecular Biology, 030102 biochemistry & molecular biology, Interleukin-6, SARS-CoV-2, Tumor Necrosis Factor-alpha, COVID-19, blockade, Cell Biology, Antibodies, Neutralizing, COVID-19 Drug Treatment, therapeutic, HEK293 Cells, 030104 developmental biology, Gene Expression Regulation, Immunology, Leukocytes, Mononuclear, IL-1 receptor 7 (IL-1R7), IFNγ

Abstract

Unchecked inflammation can result in severe diseases with high mortality, such as macrophage activation syndrome (MAS). MAS and associated cytokine storms have been observed in COVID-19 patients exhibiting systemic hyper-inflammation. Interleukin-18 (IL-18), a proinflammatory cytokine belonging to the IL-1 family, is elevated in both MAS and COVID-19 patients, and its level is known to correlate with the severity of COVID-19 symptoms. IL-18 binds its specific receptor IL-1 Receptor 5 (IL-1R5, also known as IL-18 Receptor alpha chain), leading to the recruitment of the co-receptor, IL-1 Receptor 7 (IL-1R7, also known as IL-18 Receptor beta chain). This heterotrimeric complex then initiates downstream signaling, resulting in systemic and local inflammation. Here, we developed a novel humanized monoclonal anti-IL-1R7 antibody to specifically block the activity of IL-18 and its inflammatory signaling. We characterized the function of this antibody in human cell lines, in freshly obtained peripheral blood mononuclear cells (PBMCs), and in human whole blood cultures. We found that the anti-IL-1R7 antibody significantly suppressed IL-18-mediated NFκB activation, reduced IL-18-stimulated IFNγ and IL-6 production in human cell lines, and reduced IL-18-induced IFNγ, IL-6 and TNFα production in PBMCs. Moreover, the anti-IL-1R7 antibody significantly inhibited LPS- and Candida albicans-induced IFNγ production in PBMCs, as well as LPS-induced IFNγ production in whole blood cultures. Our data suggest that blocking IL-1R7 could represent a potential therapeutic strategy to specifically modulate IL-18 signaling, and may warrant further investigation into its clinical potential for treating IL-18-mediated diseases, including MAS and COVID-19.

Published

2021

26. The chaperone GRP78 is a host auxiliary factor for SARS-CoV-2 and GRP78 depleting antibody blocks viral entry and infection

Author

Keigo Machida, Parkash S. Gill, Da-Wei Yeh, Chun-Chih Tseng, Dat P. Ha, Richard Van Krieken, Pu Zhang, Amy S. Lee, and Anthony J. Carlos

Subjects

GRP78, 0301 basic medicine, Accelerated Communication, medicine.drug_class, ACE2, Endoplasmic Reticulum, Monoclonal antibody, Biochemistry, 03 medical and health sciences, Protein Domains, Viral entry, Chlorocebus aethiops, medicine, Animals, Humans, RNA, Small Interfering, Endoplasmic Reticulum Chaperone BiP, Vero Cells, Molecular Biology, Heat-Shock Proteins, Antibody, Infectivity, Binding Sites, 030102 biochemistry & molecular biology, biology, SARS-CoV-2, Spike Protein, Endoplasmic reticulum, fungi, Antibodies, Monoclonal, Cell Biology, Virus Internalization, Cell biology, 030104 developmental biology, Gene Expression Regulation, Chaperone (protein), Host-Pathogen Interactions, Mutation, Spike Glycoprotein, Coronavirus, Unfolded Protein Response, biology.protein, Unfolded protein response, Angiotensin-Converting Enzyme 2, Protein Multimerization, Signal transduction, Protein Binding, Signal Transduction

Abstract

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), the causative agent of the COVID-19 global pandemic, utilizes the host receptor angiotensin-converting enzyme 2 (ACE2) for viral entry. However, other host factors might also play important roles in SARS-CoV-2 infection, providing new directions for antiviral treatments. GRP78 is a stress-inducible chaperone important for entry and infectivity for many viruses. Recent molecular docking analyses revealed putative interaction between GRP78 and the receptor binding domain (RBD) of the SARS-CoV-2 Spike protein (SARS-2-S). Here we report that GRP78 can form a complex with SARS-2-S and ACE2 on the surface and at the perinuclear region typical of the endoplasmic reticulum in VeroE6-ACE2 cells, and that the substrate binding domain of GRP78 is critical for this interaction. In vitro binding studies further confirmed that GRP78 can directly bind to the RBD of SARS-2-S and ACE2. To investigate the role of GRP78 in this complex, we knocked down GRP78 in VeroE6-ACE2 cells. Loss of GRP78 markedly reduced cell surface ACE2 expression and led to activation of markers of the unfolded protein response. Treatment of lung epithelial cells with a humanized monoclonal antibody (hMAb159) selected for its safe clinical profile in preclinical models, depleted cell surface GRP78 and reduced cell surface ACE2 expression, as well as SARS-2-S-driven viral entry and SARS-CoV-2 infection in vitro. Our data suggest that GRP78 is an important host auxiliary factor for SARS-CoV-2 entry and infection and a potential target to combat this novel pathogen and other viruses that utilize GRP78 in combination therapy.

Published

2021

27. Fc γ receptor compositional heterogeneity: Considerations for immunotherapy development

Author

Adam W. Barb

Subjects

Cytotoxicity, Immunologic, glycoprotein, 0301 basic medicine, medicine.medical_treatment, IgG, immunoglobulin G, Fc receptor, Reviews, Computational biology, Major histocompatibility complex, Biochemistry, Fc, crystallizable fragment, FcγRs, Fc γ receptors, Immunoglobulin G, 03 medical and health sciences, glycobiology, Antigens, CD, antibody, medicine, Animals, Humans, MHC, major histocompatibility complex, Receptor, Molecular Biology, Alleles, Receptors, Chimeric Antigen, 030102 biochemistry & molecular biology, biology, Mechanism (biology), Glycobiology, Receptors, IgG, Antibodies, Monoclonal, Cell Biology, Immunotherapy, Immunoglobulin Fc Fragments, Killer Cells, Natural, 030104 developmental biology, biology.protein, immunotherapy, LacNAc, N-acetyllactosamine, NK, natural killer, Function (biology)

Abstract

The antibody-binding crystallizable fragment (Fc) γ receptors (FcγRs) are expressed by leukocytes and activate or suppress a cellular response once engaged with an antibody-coated target. Therapeutic mAbs that require FcγR binding for therapeutic efficacy are now frontline treatments for multiple diseases. However, substantially fewer development efforts are focused on the FcγRs, despite accounting for half of the antibody–receptor complex. The recent success of engineered cell-based immunotherapies now provides a mechanism to introduce modified FcγRs into the clinic. FcγRs are highly heterogeneous because of multiple functionally distinct alleles for many genes, the presence of membrane-tethered and soluble forms, and a high degree of post-translational modification, notably asparagine-linked glycans. One significant factor limiting FcγR improvement is the fundamental lack of knowledge regarding endogenous receptor forms present in the human body. This review describes the composition of FcγRs isolated from primary human leukocytes, summarizes recent efforts to engineer FcγRs, and concludes with a description of potential FcγR features to enrich for enhanced function. Further understanding FcγR biology could accelerate the development of new clinical therapies targeting immune-related disease.

Published

2021

28. Competitively disrupting the neutrophil-specific receptor-autoantigen CD177:proteinase 3 membrane complex reduces anti-PR3 antibody-induced neutrophil activation.

Author

Marino SF, Jerke U, Rolle S, Daumke O, and Kettritz R

Subjects

Antibodies, Antineutrophil Cytoplasmic immunology, Antibodies, Monoclonal, Cell Membrane immunology, Humans, Isoantigens metabolism, Myeloblastin metabolism, Neutrophil Activation, Superoxides immunology, Autoantigens immunology, GPI-Linked Proteins immunology, Granulomatosis with Polyangiitis immunology, Neutrophils immunology, Receptors, Cell Surface immunology

Abstract

CD177 is a neutrophil-specific receptor presenting the proteinase 3 (PR3) autoantigen on the neutrophil surface. CD177 expression is restricted to a neutrophil subset, resulting in CD177 pos /mPR3 high and CD177 neg /mPR3 low populations. The CD177 pos /mPR3 high subset has implications for antineutrophil cytoplasmic autoantibody (ANCA)-associated autoimmune vasculitis, wherein patients harbor PR3-specific ANCAs that activate neutrophils for degranulation. Here, we generated high-affinity anti-CD177 monoclonal antibodies, some of which interfered with PR3 binding to CD177 (PR3 "blockers") as determined by surface plasmon resonance spectroscopy and used them to test the effect of competing PR3 from the surface of CD177 pos neutrophils. Because intact anti-CD177 antibodies also caused neutrophil activation, we prepared nonactivating Fab fragments of a PR3 blocker and nonblocker that bound specifically to CD177 pos neutrophils. We observed that Fab blocker clone 40, but not nonblocker clone 80, dose-dependently reduced anti-PR3 antibody binding to CD177 pos neutrophils. Importantly, preincubation with clone 40 significantly reduced respiratory burst in primed neutrophils challenged with either monoclonal antibodies to PR3 or PR3-ANCA immunoglobulin G from ANCA-associated autoimmune vasculitis patients. After separating the two CD177/mPR3 neutrophil subsets from individual donors by magnetic sorting, we found that PR3-ANCAs provoked significantly more superoxide production in CD177 pos /mPR3 high than in CD177 neg /mPR3 low neutrophils, and that anti-CD177 Fab clone 40 reduced the superoxide production of CD177 pos cells to the level of the CD177 neg cells. Our data demonstrate the importance of the CD177:PR3 membrane complex in maintaining a high ANCA epitope density and thereby underscore the contribution of CD177 to the severity of PR3-ANCA diseases., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

29. Agonistic Human Antibodies Binding to Lecithin-Cholesterol Acyltransferase Modulate High Density Lipoprotein Metabolism

Author

Ruwanthi N. Gunawardane, Stephanie Masterman, Dongming Liu, Derek E. Piper, Sophia Siu, Mingyue Zhou, David Park Meininger, Joyce Chi Yee Chan, Mei Lu, Michael A. Brown, Jie Tang, John M. Delaney, Margrit Schwarz, Tim Carlson, Andrew Gates, Preston Fordstrom, Cheng Janet D, Nigel Walker, and Richard Zhang

Subjects

0301 basic medicine, Immunogen, medicine.drug_class, High-throughput screening, high density lipoprotein (HDL), Antigen-Antibody Complex, CHO Cells, Monoclonal antibody, Biochemistry, drug discovery, Phosphatidylcholine-Sterol O-Acyltransferase, Mice, 03 medical and health sciences, chemistry.chemical_compound, Cricetulus, Cricetinae, medicine, Animals, Humans, Protein Structure, Quaternary, Molecular Biology, Dyslipidemias, chemistry.chemical_classification, antibody engineering, biology, Drug discovery, Cholesterol, Chinese hamster ovary cell, Cholesterol, HDL, Antibodies, Monoclonal, Cell Biology, Macaca fascicularis, enzyme, 030104 developmental biology, Enzyme, chemistry, Cardiovascular Diseases, Enzymology, cholesterol metabolism, biology.protein, Binding Sites, Antibody, Antibody

Abstract

Drug discovery opportunities where loss-of-function alleles of a target gene link to a disease-relevant phenotype often require an agonism approach to up-regulate or re-establish the activity of the target gene. Antibody therapy is increasingly recognized as a favored drug modality due to multiple desirable pharmacological properties. However, agonistic antibodies that enhance the activities of the target enzymes are rarely developed because the discovery of agonistic antibodies remains elusive. Here we report an innovative scheme of discovery and characterization of human antibodies capable of binding to and agonizing a circulating enzyme lecithin cholesterol acyltransferase (LCAT). Utilizing a modified human LCAT protein with enhanced enzymatic activity as an immunogen, we generated fully human monoclonal antibodies using the XenoMouse(TM) platform. One of the resultant agonistic antibodies, 27C3, binds to and substantially enhances the activity of LCAT from humans and cynomolgus macaques. X-ray crystallographic analysis of the 2.45 Å LCAT-27C3 complex shows that 27C3 binding does not induce notable structural changes in LCAT. A single administration of 27C3 to cynomolgus monkeys led to a rapid increase of plasma LCAT enzymatic activity and a 35% increase of the high density lipoprotein cholesterol that was observed up to 32 days after 27C3 administration. Thus, this novel scheme of immunization in conjunction with high throughput screening may represent an effective strategy for discovering agonistic antibodies against other enzyme targets. 27C3 and other agonistic human anti-human LCAT monoclonal antibodies described herein hold potential for therapeutic development for the treatment of dyslipidemia and cardiovascular disease.

Published

2016

30. Antibody Response to Serpin B13 Induces Adaptive Changes in Mouse Pancreatic Islets and Slows Down the Decline in the Residual Beta Cell Function in Children with Recent Onset of Type 1 Diabetes Mellitus

Author

Nicholas Jospe, Yury Kryvalap, Chi-Wen Lo, Ekaterina Manuylova, Jan Czyzyk, and Raman Baldzizhar

Subjects

Blood Glucose, Male, 0301 basic medicine, endocrine system, medicine.medical_specialty, endocrine system diseases, T cell, Immunology, Biochemistry, Diabetes Mellitus, Experimental, 03 medical and health sciences, Mice, Inbred NOD, Insulin-Secreting Cells, Internal medicine, medicine, Animals, Humans, Child, Molecular Biology, Serpins, Cell Proliferation, Mice, Inbred BALB C, Type 1 diabetes, geography, geography.geographical_feature_category, C-Peptide, biology, Cell growth, Pancreatic islets, Immunization, Passive, Antibodies, Monoclonal, Cell Biology, medicine.disease, Islet, Deoxyuridine, Up-Regulation, Diabetes Mellitus, Type 1, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Antibody Formation, Linear Models, biology.protein, Female, Antibody, Beta cell, Pancreas

Abstract

Type 1 diabetes mellitus (T1D) is characterized by a heightened antibody (Ab) response to pancreatic islet self-antigens, which is a biomarker of progressive islet pathology. We recently identified a novel antibody to clade B serpin that reduces islet-associated T cell accumulation and is linked to the delayed onset of T1D. As natural immunity to clade B arises early in life, we hypothesized that it may influence islet development during that time. To test this possibility healthy young Balb/c male mice were injected with serpin B13 mAb or IgG control and examined for the number and cellularity of pancreatic islets by immunofluorescence and FACS. Beta cell proliferation was assessed by measuring nucleotide analog 5-ethynyl-2′-deoxyuridine (5-EdU) incorporation into the DNA and islet Reg gene expression was measured by real time PCR. Human studies involved measuring anti-serpin B13 autoantibodies by Luminex. We found that injecting anti-serpin B13 monoclonal Ab enhanced beta cell proliferation and Reg gene expression, induced the generation of ∼80 pancreatic islets per animal, and ultimately led to increase in the beta cell mass. These findings are relevant to human T1D because our analysis of subjects just diagnosed with T1D revealed an association between baseline anti-serpin activity and slower residual beta cell function decline in the first year after the onset of diabetes. Our findings reveal a new role for the anti-serpin immunological response in promoting adaptive changes in the endocrine pancreas and suggests that enhancement of this response could potentially help impede the progression of T1D in humans.

Published

2016

31. Novel Insights into Interleukin 6 (IL-6) Cis- and Trans-signaling Pathways by Differentially Manipulating the Assembly of the IL-6 Signaling Complex

Author

Vanessa Buatois, Jürgen Scheller, Gareth W. Jones, Zoë Johnson, Simon Arnett Jones, Marine Lacroix, Giovanni Magistrelli, Walter Ferlin, Marie Kosco-Vilbois, Florence Guilhot, Pauline Malinge, François Rousseau, Suzanne Herren, and Rami Lissilaa

Subjects

Male, Models, Molecular, Receptor complex, Stereochemistry, Immunology, Molecular Sequence Data, Biology, Biochemistry, Epitope, Mice, Cytokine Receptor gp130, Animals, Humans, Protein Interaction Domains and Motifs, Amino Acid Sequence, Protein Structure, Quaternary, Receptor, Molecular Biology, Peptide sequence, Mice, Knockout, Sequence Homology, Amino Acid, Interleukin-6, Genetic Complementation Test, Antibodies, Monoclonal, Cell Biology, Glycoprotein 130, Receptors, Interleukin-6, Rats, Cell biology, Mice, Inbred C57BL, A-site, Epitope mapping, Mice, Inbred DBA, Multiprotein Complexes, NIH 3T3 Cells, Female, Protein Multimerization, Signal transduction, Signal Transduction

Abstract

The IL-6 signaling complex is described as a hexamer, formed by the association of two IL-6·IL-6 receptor (IL-6R)·gp130 trimers, with gp130 being the signal transducer inducing cis- and trans-mediated signaling via a membrane-bound or soluble form of the IL-6R, respectively. 25F10 is an anti-mouse IL-6R mAb that binds to both membrane-bound IL-6R and soluble IL-6R with the unique property of specifically inhibiting trans-mediated signaling events. In this study, epitope mapping revealed that 25F10 interacts at site IIb of IL-6R but allows the binding of IL-6 to the IL-6R and the recruitment of gp130, forming a trimer complex. Binding of 25F10 to IL-6R prevented the formation of the hexameric complex obligate for trans-mediated signaling, suggesting that the cis- and trans-modes of IL-6 signaling adopt different mechanisms for receptor complex assembly. To study this phenomenon also in the human system, we developed NI-1201, a mAb that targets, in the human IL-6R sequence, the epitope recognized by 25F10 for mice. Interestingly, NI-1201, however, did not selectively inhibit human IL-6 trans-signaling, although both mAbs produced beneficial outcomes in conditions of exacerbated IL-6 as compared with a site I-directed mAb. These findings shed light on the complexity of IL-6 signaling. First, triggering cis- versus trans-mediated IL-6 signaling occurs via distinctive mechanisms for receptor complex assembly in mice. Second, the formation of the receptor complex leading to cis- and trans-signaling biology in mice and humans is different, and this should be taken into account when developing strategies to inhibit IL-6 clinically.

Published

2015

32. Deep Sequencing-guided Design of a High Affinity Dual Specificity Antibody to Target Two Angiogenic Factors in Neovascular Age-related Macular Degeneration

Author

Sarah Sanowar, Jeremy Stinson, Ping Wu, Germaine Fuh, Chingwei V. Lee, Patrick Koenig, and Seth F. Harris

Subjects

Models, Molecular, Vascular Endothelial Growth Factor A, Antibody Affinity, Cooperativity, Complementarity determining region, Protein Engineering, medicine.disease_cause, Biochemistry, Deep sequencing, Angiopoietin-2, Immunoglobulin Fab Fragments, Macular Degeneration, Antigen, Antibody Specificity, medicine, Humans, Molecular Targeted Therapy, Binding site, Molecular Biology, Mutation, biology, Drug discovery, Antibodies, Monoclonal, High-Throughput Nucleotide Sequencing, Reproducibility of Results, Cell Biology, Complementarity Determining Regions, Molecular biology, Protein Structure, Tertiary, Kinetics, Drug Design, Protein Structure and Folding, biology.protein, Feasibility Studies, Angiogenesis Inducing Agents, Antibody, Protein Binding

Abstract

The development of dual targeting antibodies promises therapies with improved efficacy over mono-specific antibodies. Here, we engineered a Two-in-One VEGF/angiopoietin 2 antibody with dual action Fab (DAF) as a potential therapeutic for neovascular age-related macular degeneration. Crystal structures of the VEGF/angiopoietin 2 DAF in complex with its two antigens showed highly overlapping binding sites. To achieve sufficient affinity of the DAF to block both angiogenic factors, we turned to deep mutational scanning in the complementarity determining regions (CDRs). By mutating all three CDRs of each antibody chain simultaneously, we were able not only to identify affinity improving single mutations but also mutation pairs from different CDRs that synergistically improve both binding functions. Furthermore, insights into the cooperativity between mutations allowed us to identify fold-stabilizing mutations in the CDRs. The data obtained from deep mutational scanning reveal that the majority of the 52 CDR residues are utilized differently for the two antigen binding function and permit, for the first time, the engineering of several DAF variants with sub-nanomolar affinity against two structurally unrelated antigens. The improved variants show similar blocking activity of receptor binding as the high affinity mono-specific antibodies against these two proteins, demonstrating the feasibility of generating a dual specificity binding surface with comparable properties to individual high affinity mono-specific antibodies.

Published

2015

33. An Early and Robust Activation of Caspases Heads Cells for a Regulated Form of Necrotic-like Cell Death

Author

Victoria Iglesias-Guimarais, Mercè Garcia-Belinchón, María Sánchez-Osuna, Carla Granados-Colomina, Elisenda Casanelles, Judit Ribas, Victor J. Yuste, Laura Martínez-Escardó, and Sònia Pascual-Guiral

Subjects

Programmed cell death, Necrosis, Antineoplastic Agents, Apoptosis, DNA and Chromosomes, Biochemistry, Amino Acid Chloromethyl Ketones, chemistry.chemical_compound, Cell Line, Tumor, Rotenone, medicine, Humans, Enzyme Inhibitors, Fragmentation (cell biology), Molecular Biology, Caspase, Benzophenanthridines, Neurons, biology, Nocodazole, Microfilament Proteins, Intrinsic apoptosis, Antibodies, Monoclonal, Cell Biology, Staurosporine, Chromatin, Cell biology, Enzyme Activation, Chelerythrine, Gene Expression Regulation, chemistry, Caspases, Quinolines, biology.protein, Thapsigargin, Peptidomimetics, medicine.symptom, Carrier Proteins, Colchicine, Intracellular, Signal Transduction

Abstract

Apoptosis is triggered by the activation of caspases and characterized by chromatin condensation and nuclear fragmentation (type II nuclear morphology). Necrosis is depicted by a gain in cell volume (oncosis), swelling of organelles, plasma membrane leakage, and subsequent loss of intracellular contents. Although considered as different cell death entities, there is an overlap between apoptosis and necrosis. In this sense, mounting evidence suggests that both processes can be morphological expressions of a common biochemical network known as "apoptosis-necrosis continuum." To gain insight into the events driving the apoptosis-necrosis continuum, apoptotically proficient cells were screened facing several apoptotic inducers for the absence of type II apoptotic nuclear morphologies. Chelerythrine was selected for further studies based on its cytotoxicity and the lack of apoptotic nuclear alterations. Chelerythrine triggered an early plasma membrane leakage without condensed chromatin aggregates. Ultrastructural analysis revealed that chelerythrine-mediated cytotoxicity was compatible with a necrotic-like type of cell death. Biochemically, chelerythrine induced the activation of caspases. Moreover, the inhibition of caspases prevented chelerythrine-triggered necrotic-like cell death. Compared with staurosporine, chelerythrine induced stronger caspase activation detectable at earlier times. After using a battery of chemicals, we found that high concentrations of thiolic antioxidants fully prevented chelerythrine-driven caspase activation and necrotic-like cell death. Lower amounts of thiolic antioxidants partially prevented chelerythrine-mediated cytotoxicity and allowed cells to display type II apoptotic nuclear morphology correlating with a delay in caspase-3 activation. Altogether, these data support that an early and pronounced activation of caspases can drive cells to undergo a form of necrotic-like regulated cell death.

Published

2015

34. Structural Insights into the Neutralization Properties of the Fully Human, Anti-interferon Monoclonal Antibody Sifalimumab

Author

Vaheh Oganesyan, William Dall'acqua, Li Peng, Robert M. Woods, and Herren Wu

Subjects

Models, Molecular, Protein Conformation, medicine.drug_class, Alpha interferon, Interferon alpha-2, Biology, Antibodies, Monoclonal, Humanized, Crystallography, X-Ray, Monoclonal antibody, Biochemistry, Interferon, medicine, Molecular replacement, Molecular Biology, autoimmune disease, epitope mapping, interferon, monoclonal antibody, nuclear magnetic resonance (NMR), protein expression, sifalimumab, structural biology, systemic lupus erythematosus, x-ray crystallography, Antibodies, Monoclonal, Interferon-alpha, Cell Biology, Molecular biology, Recombinant Proteins, Epitope mapping, Mechanism of action, Structural biology, Protein Structure and Folding, Sifalimumab, medicine.symptom, medicine.drug

Abstract

Background: We investigated the molecular basis of human IFN-α2A recognition by sifalimumab. Results: We determined the structure of the complex between the Fab of sifalimumab and IFN-α2A. Conclusion: The interferon-neutralizing properties of sifalimumab result from direct competition for IFN-α2A binding to IFN receptor subunit 1 and not IFN receptor subunit 2. Significance: These data provide the basis for the mechanism of action of sifalimumab., We report the three-dimensional structure of human interferon α-2A (IFN-α2A) bound to the Fab fragment of a therapeutic monoclonal antibody (sifalimumab; IgG1/κ). The structure of the corresponding complex was solved at a resolution of 3.0 Å using molecular replacement and constitutes the first reported structure of a human type I IFN bound to a therapeutic antibody. This study revealed the major contribution made by the first complementarity-determining region in each of sifalimumab light and heavy chains. These data also provided the molecular basis for sifalimumab mechanism of action. We propose that its interferon-neutralizing properties are the result of direct competition for IFN-α2A binding to the IFN receptor subunit 1 (IFNAR1) and do not involve inhibiting IFN-α2A binding to the IFN receptor subunit 2 (IFNAR2).

Published

2015

35. Variable Region Identical IgA and IgE to Cryptococcus neoformans Capsular Polysaccharide Manifest Specificity Differences

Author

Mary Ann Pohl, Alena Janda, Ertan Eryilmaz, Antonio Nakouzi, Arturo Casadevall, and Anthony Bowen

Subjects

Immunoglobulin A, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Immunology, Immunoglobulin Variable Region, Enzyme-Linked Immunosorbent Assay, Immunoglobulin E, Biochemistry, Immunoglobulin G, Microbiology, Mice, Antibody Specificity, Polysaccharides, Sequence Homology, Nucleic Acid, Animals, Molecular Biology, Antibodies, Fungal, Cryptococcus neoformans, Mice, Inbred BALB C, Base Sequence, biology, Macrophages, Antibodies, Monoclonal, Cryptococcosis, Cell Biology, biology.organism_classification, Isotype, Microscopy, Fluorescence, Immunoglobulin class switching, biology.protein, Paratope, Binding Sites, Antibody, Antibody, Peptides

Abstract

In recent years several groups have shown that isotype switching from IgM to IgG to IgA can affect the affinity and specificity of antibodies sharing identical variable (V) regions. However, whether the same applies to IgE is unknown. In this study we compared the fine specificity of V region-identical IgE and IgA to Cryptococcus neoformans capsular polysaccharide and found that these differed in specificity from each other. The IgE and IgA paratopes were probed by nuclear magnetic resonance spectroscopy with (15)N-labeled peptide mimetics of cryptococcal polysaccharide antigen (Ag). IgE was found to cleave the peptide at a much faster rate than V region-identical IgG subclasses and IgA, consistent with an altered paratope. Both IgE and IgA were opsonic for C. neoformans and protected against infection in mice. In summary, V-region expression in the context of the ϵ constant (C) region results in specificity changes that are greater than observed for comparable IgG subclasses. These results raise the possibility that expression of certain V regions in the context of α and ϵ C regions affects their function and contributes to the special properties of those isotypes.

Published

2015

36. Neurons and Glia Modify Receptor Protein-tyrosine Phosphatase ζ (RPTPζ)/Phosphacan with Cell-specific O-Mannosyl Glycans in the Developing Brain

Author

Russell T. Matthews, Toshihiko Katoh, Michael Tiemeyer, and Chrissa A. Dwyer

Subjects

Glycan, Glycosylation, medicine.drug_class, Molecular Sequence Data, Phosphatase, Glycobiology and Extracellular Matrices, Protein tyrosine phosphatase, Biology, N-Acetylglucosaminyltransferases, Monoclonal antibody, Biochemistry, Epitope, Mice, chemistry.chemical_compound, medicine, Animals, Molecular Biology, Mice, Knockout, Neurons, Receptor-Like Protein Tyrosine Phosphatases, Class 5, Antibodies, Monoclonal, Brain, Gene Expression Regulation, Developmental, Walker-Warburg Syndrome, Amino Sugars, Cell Biology, Isoenzymes, carbohydrates (lipids), Disease Models, Animal, Animals, Newborn, Carbohydrate Sequence, Proteoglycan, chemistry, Organ Specificity, biology.protein, lipids (amino acids, peptides, and proteins), Signal transduction, Mannose, Neuroglia, Signal Transduction

Abstract

Protein O-mannosylation is a glycan modification that is required for normal nervous system development and function. Mutations in genes involved in protein O-mannosyl glycosylation give rise to a group of neurodevelopmental disorders known as congenital muscular dystrophies (CMDs) with associated CNS abnormalities. Our previous work demonstrated that receptor protein-tyrosine phosphatase ζ (RPTPζ)/phosphacan is hypoglycosylated in a mouse model of one of these CMDs, known as muscle-eye-brain disease, a disorder that is caused by loss of an enzyme (protein O-mannose β-1,2-N-acetylglucosaminyltransferase 1) that modifies O-mannosyl glycans. In addition, monoclonal antibodies Cat-315 and 3F8 were demonstrated to detect O-mannosyl glycan modifications on RPTPζ/phosphacan. Here, we show that O-mannosyl glycan epitopes recognized by these antibodies define biochemically distinct glycoforms of RPTPζ/phosphacan and that these glycoforms differentially decorate the surface of distinct populations of neural cells. To provide a further structural basis for immunochemically based glycoform differences, we characterized the O-linked glycan heterogeneity of RPTPζ/phosphacan in the early postnatal mouse brain by multidimensional mass spectrometry. Structural characterization of the O-linked glycans released from purified RPTPζ/phosphacan demonstrated that this protein is a significant substrate for protein O-mannosylation and led to the identification of several novel O-mannose-linked glycan structures, including sulfo-N-acetyllactosamine containing modifications. Taken together, our results suggest that specific glycan modifications may tailor the function of this protein to the unique needs of specific cells. Furthermore, their absence in CMDs suggests that hypoglycosylation of RPTPζ/phosphacan may have different functional consequences in neurons and glia.

Published

2015

37. Receptor Tyrosine Kinase EphA5 Is a Functional Molecular Target in Human Lung Cancer

Author

Wadih Arap, Martin J. Edelman, Andrew Bradbury, Daniel F. Cimino, Maria I. Nunez, Ming D. Qian, Julianna K. Edwards, Ignacio I. Wistuba, Andrey S. Dobroff, Ximing Tang, Fortunato Ferrara, Roy R. Lobb, Waun Ki Hong, Richard L. Sidman, Fernanda I. Staquicini, Renata Pasqualini, Diane D. Liu, J. Jack Lee, Patrick J. Kelly, Ahmad Salameh, and Benjamin J. Moeller

Subjects

Lung Neoplasms, DNA Repair, DNA repair, medicine.drug_class, DNA damage, Monoclonal Antibody, medicine.medical_treatment, Mice, Nude, Biology, Monoclonal antibody, Radiation Tolerance, Receptor Tyrosine Kinase, Biochemistry, Receptor tyrosine kinase, Mice, Rats, Nude, Cell Line, Tumor, medicine, Animals, Humans, Molecular Targeted Therapy, Lung cancer, Molecular Biology, Mice, Inbred BALB C, Cell Cycle, Antibodies, Monoclonal, Receptor, EphA5, Cell Biology, Cell cycle, medicine.disease, S cell, Rats, Radiation therapy, Ionizing Radiation, Cancer research, biology.protein, DNA Damage Response, DNA Damage

Abstract

Background: EphA5 is a functional target in lung cancer, the most common cause of tumor-related death in mankind. Results: EphA5 regulates cell cycle checkpoints and DNA damage repair induced by ionizing radiation. Conclusion: EphA5 is a novel regulator of DNA damage repair with clinical implications. Significance: EphA5 may serve as a novel biomarker of radioresistance and a candidate target for therapeutic intervention in human lung cancer., Lung cancer is often refractory to radiotherapy, but molecular mechanisms of tumor resistance remain poorly defined. Here we show that the receptor tyrosine kinase EphA5 is specifically overexpressed in lung cancer and is involved in regulating cellular responses to genotoxic insult. In the absence of EphA5, lung cancer cells displayed a defective G1/S cell cycle checkpoint, were unable to resolve DNA damage, and became radiosensitive. Upon irradiation, EphA5 was transported into the nucleus where it interacted with activated ATM (ataxia-telangiectasia mutated) at sites of DNA repair. Finally, we demonstrate that a new monoclonal antibody against human EphA5 sensitized lung cancer cells and human lung cancer xenografts to radiotherapy and significantly prolonged survival, thus suggesting the likelihood of translational applications.

Published

2015

38. pH-dependent Binding Engineering Reveals an FcRn Affinity Threshold That Governs IgG Recycling

Author

M. Jack Borrok, Xiang-Qing Yu, Ping Tsui, Vaheh Oganesyan, Yanli Wu, William Dall'acqua, and Nurten Beyaz

Subjects

Male, Phage display, Protein Conformation, medicine.drug_class, Stereochemistry, Immunology, Antibody Affinity, Fc receptor, Mice, Transgenic, Receptors, Fc, Plasma protein binding, Protein Engineering, Monoclonal antibody, Biochemistry, Immunoglobulin G, Mice, Peptide Library, In vivo, medicine, Animals, Humans, Bacteriophages, Tissue Distribution, Molecular Biology, biology, Chemistry, Histocompatibility Antigens Class I, Antibodies, Monoclonal, Cell Biology, Protein engineering, Hydrogen-Ion Concentration, Surface Plasmon Resonance, Peptide Fragments, Macaca fascicularis, biology.protein, Biophysics, Female, Antibody, Protein Binding

Abstract

The Fc domain of IgG has been the target of multiple mutational studies aimed at altering the pH-dependent IgG/FcRn interaction to modulate IgG pharmacokinetics. These studies have yielded antibody variants with disparate pharmacokinetic characteristics, ranging from extended in vivo half-life to those exhibiting extremely rapid clearance. To better understand pH-dependent binding parameters that govern these outcomes and limit FcRn-mediated half-life extension, we generated a panel of novel Fc variants with high affinity binding at acidic pH that vary in pH 7.4 affinities and assessed pharmacokinetic outcomes. Pharmacokinetic studies in human FcRn transgenic mice and cynomolgus monkeys showed that multiple variants with increased FcRn affinities at acidic pH exhibited extended serum half-lives relative to the parental IgG. Importantly, the results reveal an underappreciated affinity threshold of neutral pH binding that determines IgG recycling efficiency. Variants with pH 7.4 FcRn affinities below this threshold recycle efficiently and can exhibit increased serum persistence. Increasing neutral pH FcRn affinity beyond this threshold reduced serum persistence by offsetting the benefits of increased pH 6.0 binding. Ultra-high affinity binding to FcRn at both acidic and neutral pH leads to rapid serum clearance.

Published

2015

39. Mechanisms of Neutralization of a Human Anti-α-toxin Antibody

Author

Agnieszka Sadowska, William Dall'acqua, Li Peng, Melissa Damschroder, Herren Wu, Bret R. Sellman, Christine Tkaczyk, Li Cheng, and Vaheh Oganesyan

Subjects

Models, Molecular, medicine.drug_class, Bacterial Toxins, Infectious Disease, Plasma protein binding, Antibodies, Monoclonal, Humanized, Crystallography, X-Ray, Monoclonal antibody, Biochemistry, Alpha Toxin, Epitope, Cell Line, Hemolysin Proteins, Immunoglobulin Fab Fragments, Neutralization Tests, medicine, Humans, Fab, Molecular Biology, Antibody, Linear epitope, biology, Antibodies, Monoclonal, Cell Biology, Surface Plasmon Resonance, Antibodies, Neutralizing, Molecular biology, Recombinant Proteins, Staphylococcus aureus (S. aureus), Epitope mapping, Lytic cycle, Mutagenesis, Protein Structure and Folding, Crystal Structure, biology.protein, Biophysics, Broadly Neutralizing Antibodies, Epitope Mapping, Protein Binding

Abstract

Background: MEDI4893 is an anti-α-toxin (AT) antibody currently in clinical trial in the field of Staphylococcus aureus-mediated diseases. Results: Structure/function studies of MEDI4893 reveal its epitope and mechanisms of action. Conclusion: MEDI4893 recognizes a novel epitope and exhibits a possible dual neutralization mechanism. Significance: Understanding the molecular basis of AT/MEDI4893 interaction has important implications to design potent antibodies targeting Staphylococcus aureus., MEDI4893 is a neutralizing human monoclonal antibody that targets α-toxin (AT) and is currently undergoing evaluation in the field of Staphylococcus aureus-mediated diseases. We have solved the crystal structure of MEDI4893 Fab bound to monomeric AT at a resolution of 2.56 Å and further characterized its epitope using various engineered AT variants. We have found that MEDI4893 recognizes a novel epitope in the so-called “rim” domain of AT and exerts its neutralizing effect through a dual mechanism. In particular, MEDI4893 not only sterically blocks binding of AT to its cell receptor but also prevents it from adopting a lytic heptameric trans-membrane conformation.

Published

2014

40. Specific Targeting of a Naturally Presented Osteosarcoma Antigen, Papillomavirus Binding Factor Peptide, Using an Artificial Monoclonal Antibody

Author

Hiroshi Matsumiya, Toshihiko Torigoe, Noriyuki Sato, Shingo Ichimiya, Vitaly Kochin, Masanori Kyono, Makoto Emori, Tadashi Hasegawa, Tetsuo Himi, Takahisa Hirano, Norihiro Muroi, Toshihiko Yamashita, Takuro Wada, Hiroko Asanuma, Shingo Toji, Keiji Yamashita, Kenji Murata, Kazue Watanabe, and Tomohide Tsukahara

Subjects

medicine.drug_class, Molecular Sequence Data, Immunology, Antigen presentation, Bone Neoplasms, Monoclonal antibody, Cancer Vaccines, Biochemistry, Epitope, Antigen, Antigens, Neoplasm, Peptide Library, Cell Line, Tumor, HLA-A2 Antigen, medicine, Humans, Single-chain variable fragment, Cytotoxic T cell, Amino Acid Sequence, Peptide library, Papillomaviridae, Molecular Biology, Antigen Presentation, Osteosarcoma, Base Sequence, Chemistry, Antibodies, Monoclonal, Immunotherapy, Active, Cell Biology, Virology, HLA-B Antigens, Cancer research, Clone (B-cell biology), Single-Chain Antibodies, T-Lymphocytes, Cytotoxic

Abstract

Osteosarcoma is a rare but highly malignant tumor occurring most frequently in adolescents. The prognosis of non-responders to chemotherapy is still poor, and new treatment modalities are needed. To develop peptide-based immunotherapy, we previously identified autologous cytotoxic T lymphocyte-defined osteosarcoma antigen papillomavirus binding factor (PBF) in the context of HLA-B55 and the cytotoxic T lymphocyte epitope (PBF A2.2) presented by HLA-A2. PBF and HLA class I are expressed in ∼90 and 70% of various sarcomas, respectively. However, the expression status of peptide PBF A2.2 presented by HLA-A2 on osteosarcoma cells has remained unknown because it is difficult to generate a specific probe that reacts with the HLA·peptide complex. For detection and qualification of the HLA-A*02:01·PBF A2.2 peptide complex on osteosarcoma cells, we tried to isolate a single chain variable fragment (scFv) antibody directed to the HLA-*A0201·PBF A2.2 complex using a naïve scFv phage display library. As a result, scFv clone D12 with high affinity (KD = 1.53 × 10(-9) M) was isolated. D12 could react with PBF A2.2 peptide-pulsed T2 cells and HLA-A2+PBF+ osteosarcoma cell lines and simultaneously demonstrated that the HLA·peptide complex was expressed on osteosarcoma cells. In conclusion, scFv clone D12 might be useful to select candidate patients for PBF A2.2 peptide-based immunotherapy and develop antibody-based immunotherapy.

Published

2014

41. Mutagenesis Studies of the H5 Influenza Hemagglutinin Stem Loop Region

Author

Michael Caffrey, Lijun Rong, Arnab Basu, Aleksandar Antanasijevic, Rama K. Mishra, and Terry L. Bowlin

Subjects

Models, Molecular, viruses, Molecular Sequence Data, Mutagenesis (molecular biology technique), Hemagglutinin (influenza), Hemagglutinin Glycoproteins, Influenza Virus, Molecular Dynamics Simulation, Biology, Antibodies, Viral, Crystallography, X-Ray, Biochemistry, Virus, Viral entry, Animals, Humans, Amino Acid Sequence, Binding site, Site-directed mutagenesis, Molecular Biology, Influenza A Virus, H5N1 Subtype, virus diseases, Antibodies, Monoclonal, Cell Biology, Virus Internalization, Stem-loop, Antibodies, Neutralizing, Virology, A-site, Protein Structure and Folding, Mutagenesis, Site-Directed, biology.protein

Abstract

Influenza outbreaks, particularly the pandemic 1918 H1 and avian H5 strains, are of high concern to public health. The hemagglutinin envelope protein of influenza plays a critical role in viral entry and thus is an attractive target for inhibition of virus entry. The highly conserved stem loop region of hemagglutinin has been shown to undergo critically important conformational changes during the entry process and, moreover, to be a site for inhibition of virus entry by antibodies, small proteins, and small drug-like molecules. In this work we probe the structure-function properties of the H5 hemagglutinin stem loop region by site-directed mutagenesis. We find that most mutations do not disrupt expression, proteolytic processing, incorporation into virus, or receptor binding; however, many of the mutations disrupt the entry process. We further assess the effects of mutations on inhibition of entry by a neutralizing monoclonal antibody (C179) and find examples of increased and decreased sensitivity to the antibody, consistent with the antibody binding site observed by x-ray crystallography. In addition, we tested the sensitivity of the mutants to MBX2329, a small molecule inhibitor of influenza entry. Interestingly, the mutants exhibit increased and decreased sensitivities to MBX2329, which gives further insight into the binding site of the compound on HA and potential mechanisms of escape. Finally, we have modeled the binding site of MBX2329 using molecular dynamics and find that the resulting structure is in good agreement with the mutagenesis results. Together these studies underscore the importance of the stem loop region to HA function and suggest potential sites for therapeutic intervention of influenza entry.

Published

2014

42. A Cryptic Polyreactive Antibody Recognizes Distinct Clades of HIV-1 Glycoprotein 120 by an Identical Binding Mechanism

Author

Delphine Ohayon, Sébastien Lacroix-Desmazes, Tobias Scheel, Stéphane Mesnage, Cyril Planchais, Jordan D. Dimitrov, Claudia Berek, and Srinivas V. Kaveri

Subjects

Immunology, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Biochemistry, Protein–protein interaction, chemistry.chemical_compound, Immune system, HIV-1 protease, Humans, Molecular Biology, Heme, chemistry.chemical_classification, biology, fungi, virus diseases, food and beverages, Antibodies, Monoclonal, Cell Biology, Antibodies, Neutralizing, Primary and secondary antibodies, Molecular biology, Receptor–ligand kinetics, Kinetics, chemistry, HIV-1, biology.protein, Thermodynamics, Binding Sites, Antibody, Antibody, Glycoprotein

Abstract

Polyreactive antibodies play an important role for neutralization of human immunodeficiency virus (HIV). In addition to intrinsic polyreactive antibodies, the immune system of healthy individuals contains antibodies with cryptic polyreactivity. These antibodies acquire promiscuous antigen binding potential post-translationally, after exposure to various redox-active substances such as reactive oxygen species, iron ions, and heme. Here, we characterized the interaction of a prototypic human antibody that acquires binding potential to glycoprotein (gp) 120 after exposure to heme. The kinetic and thermodynamic analyses of interaction of the polyreactive antibody with distinct clades of gp120 demonstrated that the antigen-binding promiscuity of the antibody compensates for the molecular heterogeneity of the target antigen. Thus, the polyreactive antibody recognized divergent gp120 clades with similar values of the binding kinetics and quantitatively identical changes in the activation thermodynamic parameters. Moreover, this antibody utilized the same type of noncovalent forces for formation of complexes with gp120. In contrast, HIV-1-neutralizing antibodies isolated from HIV-1-infected individuals, F425 B4a1 and b12, demonstrated different binding behavior upon interaction with distinct variants of gp120. This study contributes to a better understanding of the physiological role and binding mechanism of antibodies with cryptic polyreactivity. Moreover, this study might be of relevance for understanding the basic aspects of HIV-1 interaction with human antibodies.

Published

2014

43. Mechanism of Action and Epitopes of Clostridium difficile Toxin B-neutralizing Antibody Bezlotoxumab Revealed by X-ray Crystallography

Author

Payal R. Sheth, Maribel Beaumont, Edward DiNunzio, Fred Racine, Li Xiao, Paul Reichert, Xiaoyu Yang, Jerzy Karczewski, Corey Strickland, Nicholas Murgolo, Susan Secore, Richard N. Ingram, Peter Orth, Todd Mayhood, Lorraine D. Hernandez, Grigori Ermakov, and Alex G. Therien

Subjects

Models, Molecular, Bacterial Toxins, Molecular Sequence Data, Clostridium difficile toxin B, Crystallography, X-Ray, Microbiology, Biochemistry, Epitope, Epitopes, Bacterial Proteins, Amino Acid Sequence, Binding site, Neutralizing antibody, Molecular Biology, Peptide sequence, Oligopeptide, Binding Sites, biology, Clostridioides difficile, Antibodies, Monoclonal, Cell Biology, Antibodies, Bacterial, Antibodies, Neutralizing, Protein Structure, Tertiary, Epitope mapping, Bezlotoxumab, biology.protein, Broadly Neutralizing Antibodies, Epitope Mapping

Abstract

The symptoms of Clostridium difficile infections are caused by two exotoxins, TcdA and TcdB, which target host colonocytes by binding to unknown cell surface receptors, at least in part via their combined repetitive oligopeptide (CROP) domains. A combination of the anti-TcdA antibody actoxumab and the anti-TcdB antibody bezlotoxumab is currently under development for the prevention of recurrent C. difficile infections. We demonstrate here through various biophysical approaches that bezlotoxumab binds to specific regions within the N-terminal half of the TcdB CROP domain. Based on this information, we solved the x-ray structure of the N-terminal half of the TcdB CROP domain bound to Fab fragments of bezlotoxumab. The structure reveals that the TcdB CROP domain adopts a β-solenoid fold consisting of long and short repeats and that bezlotoxumab binds to two homologous sites within the CROP domain, partially occluding two of the four putative carbohydrate binding pockets located in TcdB. We also show that bezlotoxumab neutralizes TcdB by blocking binding of TcdB to mammalian cells. Overall, our data are consistent with a model wherein a single molecule of bezlotoxumab neutralizes TcdB by binding via its two Fab regions to two epitopes within the N-terminal half of the TcdB CROP domain, partially blocking the carbohydrate binding pockets of the toxin and preventing toxin binding to host cells.

Published

2014

44. Mechanism and Function of Monoclonal Antibodies Targeting Siglec-15 for Therapeutic Inhibition of Osteoclastic Bone Resorption

Author

Aida Kalbakji, Annie Fortin, Gilles Tremblay, Matthew Stuible, Mario Filion, Anna N. Moraitis, and Stefan Saragosa

Subjects

musculoskeletal diseases, medicine.medical_specialty, Cell signaling, medicine.drug_class, Immunoglobulins, Osteoclasts, Monoclonal antibody, Biochemistry, Bone and Bones, Bone resorption, Cell Line, Mice, Bone Density, Osteoclast, Internal medicine, medicine, Animals, Humans, Bone Resorption, Molecular Biology, Adaptor Proteins, Signal Transducing, biology, musculoskeletal, neural, and ocular physiology, RANK Ligand, Antibodies, Monoclonal, Membrane Proteins, SIGLEC, Osteoblast, Cell Biology, respiratory system, musculoskeletal system, Cell biology, Radiography, medicine.anatomical_structure, Endocrinology, RANKL, biology.protein

Abstract

The use of monoclonal antibodies to target functionally important cell-surface proteins on bone-resorbing osteoclasts represents a promising approach for treatment of cancer-associated bone loss and other skeletal pathologies. Previously, we identified Siglec-15, a little studied sialic acid-binding receptor, as a candidate target that is highly up-regulated during osteoclast differentiation induced by the cytokine receptor activator of NF-κB ligand (RANKL). In this report, we confirm that Siglec-15 is localized to the plasma membrane where it can be targeted by monoclonal antibodies to inhibit differentiation of functional osteoclasts in vitro. Furthermore, we found that treatment of mice with these antibodies led to a marked increase in bone mineral density, consistent with inhibition of osteoclast activity. Interestingly, osteoblast numbers were maintained despite the anti-resorptive activity. At the molecular level, Siglec-15 interacts with the adapter protein DAP12 and can induce Akt activation when clustered on the osteoclast cell surface, which likely represents its normal signaling function. Importantly, we discovered that monoclonal antibodies induce rapid internalization, lysosomal targeting, and degradation of Siglec-15 by inducing receptor dimerization. This study defines a key regulatory node that controls osteoclast differentiation and activity downstream of RANKL and supports further development of Siglec-15 antibodies as a novel class of bone loss therapeutics.

Published

2014

45. Inhibitory Mechanism of an Allosteric Antibody Targeting the Glucagon Receptor

Author

Vicky Chiang, Ganesh Kolumam, Jacob E. Corn, Jeremy Murray, Yonglei Shang, Bernard B. Allan, Isidro Hötzel, Yingnan Zhang, Elizabeth Luis, Holly J. Clarke, Lance Kates, Azadeh Madjidi, Christopher M. Koth, and Susmith Mukund

Subjects

Male, Molecular Sequence Data, Allosteric regulation, Glucagon binding, Molecular Dynamics Simulation, Biology, Crystallography, X-Ray, Biochemistry, Glucagon, Mice, Antibody Engineering, Allosteric Regulation, Glucose Metabolism, Structural Biology, Receptors, Glucagon, Animals, Humans, Amino Acid Sequence, Binding site, Receptor, Molecular Biology, G protein-coupled receptor, Diabetes, Antibodies, Monoclonal, Cell Biology, Molecular biology, Protein Structure, Tertiary, Docking (molecular), Protein Structure and Folding, Extracellular Space, G Protein-coupled Receptors (GPCR), Glucagon receptor, hormones, hormone substitutes, and hormone antagonists

Abstract

Background: Allosteric regulators of GPCRs provide unique pharmacological properties. Results: The mechanism of allosteric inhibition of the glucagon receptor by an antibody, which is uniquely sensitive to a naturally occurring G40S mutation, is detailed. Conclusion: Allosteric sites on the glucagon receptor extracellular domain regulate receptor activity. Significance: Mechanisms of allosteric regulation of GPCRs aid discovery of drugs with improved selectivity., Elevated glucagon levels and increased hepatic glucagon receptor (GCGR) signaling contribute to hyperglycemia in type 2 diabetes. We have identified a monoclonal antibody that inhibits GCGR, a class B G-protein coupled receptor (GPCR), through a unique allosteric mechanism. Receptor inhibition is mediated by the binding of this antibody to two distinct sites that lie outside of the glucagon binding cleft. One site consists of a patch of residues that are surface-exposed on the face of the extracellular domain (ECD) opposite the ligand-binding cleft, whereas the second binding site consists of residues in the αA helix of the ECD. A docking model suggests that the antibody does not occlude the ligand-binding cleft. We solved the crystal structure of GCGR ECD containing a naturally occurring G40S mutation and found a shift in the register of the αA helix that prevents antibody binding. We also found that alterations in the αA helix impact the normal function of GCGR. We present a model for the allosteric inhibition of GCGR by a monoclonal antibody that may form the basis for the development of allosteric modulators for the treatment of diabetes and other class B GPCR-related diseases.

Published

2013

46. Cysteine Racemization on IgG Heavy and Light Chains

Author

Gregory C. Flynn and Qingchun Zhang

Subjects

Reaction mechanism, medicine.drug_class, Stereochemistry, CHO Cells, Sulfides, Immunoglobulin light chain, Monoclonal antibody, Biochemistry, chemistry.chemical_compound, Cricetulus, Thioether, mental disorders, medicine, Animals, Humans, Organic chemistry, Cysteine, Disulfides, Molecular Biology, Racemization, biology, Chemistry, Antibodies, Monoclonal, Cell Biology, Hydrogen-Ion Concentration, Protein Synthesis and Degradation, biology.protein, Antibody, Carrier Proteins, Immunoglobulin Heavy Chains, Chirality (chemistry), Protein Processing, Post-Translational

Abstract

Under basic pH conditions, the heavy chain 220-light chain 214 (H220-L214) disulfide bond, found in the flexible hinge region of an IgG1, can convert to a thioether. Similar conditions also result in racemization of the H220 cysteine. Here, we report that racemization occurs on both H220 and L214 on an IgG1 with a λ light chain (IgG1λ) but almost entirely on H220 of an IgGl with a κ light chain (IgG1κ) under similar conditions. Likewise, racemization was detected at significant levels on H220 and L214 on endogenous human IgG1λ but only at the H220 position on IgG1κ. Low but measurable levels of D-cysteines were found on IgG2 cysteines in the hinge region, both with monoclonal antibodies incubated under basic pH conditions and on antibodies isolated from human serum. A simplified reaction mechanism involving reversible β-elimination on the cysteine is presented that accounts for both base-catalyzed racemization and thioether formation at the hinge disulfide.

Published

2013

47. Engineered Protease-resistant Antibodies with Selectable Cell-killing Functions

Author

Heeringa Katharine, Allison R. Greenplate, Meredith Perpetua, Randall J. Brezski, Gregory Bannish, Robert Jordan, Frank Lynch, Stephen G. McCarthy, Katharine D. Grugan, Michelle Kinder, William R. Strohl, and Keri L. Soring

Subjects

Proteases, medicine.drug_class, medicine.medical_treatment, Immunology, Biology, Protein Engineering, Monoclonal antibody, medicine.disease_cause, Biochemistry, Immunoglobulin G, Cell Line, medicine, Humans, Molecular Biology, Mutation, Protease, fungi, Receptors, IgG, Antibody-Dependent Cell Cytotoxicity, food and beverages, Antibodies, Monoclonal, Cell Biology, Protein engineering, Molecular biology, Cell biology, Cell killing, Proteolysis, biology.protein, Binding Sites, Antibody, Antibody

Abstract

Molecularly engineered antibodies with fit-for-purpose properties will differentiate next generation antibody therapeutics from traditional IgG1 scaffolds. One requirement for engineering the most appropriate properties for a particular therapeutic area is an understanding of the intricacies of the target microenvironment in which the antibody is expected to function. Our group and others have demonstrated that proteases secreted by invasive tumors and pathological microorganisms are capable of cleaving human IgG1, the most commonly adopted isotype among monoclonal antibody therapeutics. Specific cleavage in the lower hinge of IgG1 results in a loss of Fc-mediated cell-killing functions without a concomitant loss of antigen binding capability or circulating antibody half-life. Proteolytic cleavage in the hinge region by tumor-associated or microbial proteases is postulated as a means of evading host immune responses, and antibodies engineered with potent cell-killing functions that are also resistant to hinge proteolysis are of interest. Mutation of the lower hinge region of an IgG1 resulted in protease resistance but also resulted in a profound loss of Fc-mediated cell-killing functions. In the present study, we demonstrate that specific mutations of the CH2 domain in conjunction with lower hinge mutations can restore and sometimes enhance cell-killing functions while still retaining protease resistance. By identifying mutations that can restore either complement- or Fcγ receptor-mediated functions on a protease-resistant scaffold, we were able to generate a novel protease-resistant platform with selective cell-killing functionality.

Published

2013

48. Structural and Functional Properties of the Membranotropic HIV-1 Glycoprotein gp41 Loop Region Are Modulated by Its Intrinsic Hydrophobic Core

Author

Yechiel Shai, Avraham Ashkenazi, Jiayin Qiu, and Shuwen Liu

Subjects

viruses, Molecular Sequence Data, Mutant, Plasma protein binding, HIV Antibodies, Biology, medicine.disease_cause, Gp41, Membrane Fusion, Biochemistry, Protein Structure, Secondary, Cell membrane, Structure-Activity Relationship, medicine, Humans, Amino Acid Sequence, Disulfides, Molecular Biology, Ions, Mutation, Circular Dichroism, Cell Membrane, virus diseases, Antibodies, Monoclonal, Computational Biology, Lipid bilayer fusion, Cell Biology, Lipids, Fusion protein, HIV Envelope Protein gp41, medicine.anatomical_structure, Membrane protein, Mutagenesis, HIV-1, Biophysics, Simian Immunodeficiency Virus, Hydrophobic and Hydrophilic Interactions, Molecular Biophysics, Protein Binding

Abstract

Background: HIV-1 infectivity is decreased by specific mutations that alter the hydrophobicity level in the HIV-1 gp41 loop core. Results: Antibody recognition, disulfide-bond formation, and lipid mixing of loop domain peptides are strongly affected by these mutations. Conclusion: The hydrophobic core maintains proper function and structure of the loop region. Significance: A better understanding of the membrane fusion mechanism of HIV and similar viruses is provided. The gp41 disulfide loop region switches from a soluble state to a membrane-bound state during the human immunodeficiency virus type 1 (HIV-1) envelope-mediated membrane fusion process. The loop possesses a hydrophobic core at the center of the region with an unusual basic residue (Lys-601). Furthermore, two loop core mutations, K601A and L602A, are found to inhibit HIV-1 infectivity while keeping wild type-like levels of the envelope, implying that they exert an inhibitory effect on gp41 during the membrane fusion event. Here, we investigated the mode of action of these mutations on the loop region. We show that the K601A mutation, but not the L602A mutation, abolished the binding of a loop-specific monoclonal antibody to a loop domain peptide. Additionally, the K601A, but not the L602A, impaired disulfide bond formation in the peptides. This was correlated with changes in the circular dichroism spectrum imposed by the K601A mutation. In the membrane, however, the L602A, but not the K601A, reduced the lipid mixing ability of the loop peptides, which was correlated with decreased α-helical content of the L602A mutant. The results suggest that the Lys-601 residue provides a moderate hydrophobicity level within the gp41 loop core that contributes to the proper structure and function of the loop inside and outside the membrane. Because basic residues are found between the loop Cys residues of several lentiviral fusion proteins, the findings may contribute to understanding the fusion mechanism of other viruses as well.

Published

2013

49. Implications of a Vasodilatory Human Monoclonal Autoantibody in Postural Hypotension

Author

Caitlin Zillner, David C. Kem, Jonathan Zuccolo, Madeleine W. Cunningham, Xichun Yu, Judith A. James, Kenneth J. Smith, Jiyeon Lee, and Hongliang Li

Subjects

Male, medicine.medical_specialty, Adrenergic receptor, medicine.drug_class, Vasodilator Agents, Adrenergic beta-Antagonists, CHO Cells, Biology, medicine.disease_cause, Monoclonal antibody, Biochemistry, Epitope, Immunoglobulin G, Autoimmunity, Propanolamines, Hypotension, Orthostatic, Cricetulus, Cricetinae, Internal medicine, medicine, Animals, Humans, Myocytes, Cardiac, Receptor, Molecular Biology, Aorta, Autoantibodies, Autoantibody, Antibodies, Monoclonal, Molecular Bases of Disease, Cell Biology, Surface Plasmon Resonance, Rats, Arterioles, Endocrinology, Monoclonal, biology.protein, Receptors, Adrenergic, beta-2, Peptides

Abstract

Functional autoantibodies to the autonomic receptors are increasingly recognized in the pathophysiology of cardiovascular diseases. To date, no human activating monoclonal autoantibodies to these receptors have been available. In this study, we describe for the first time a β2-adrenergic receptor (β2AR)-activating monoclonal autoantibody (C5F2) produced from the lymphocytes of a patient with idiopathic postural hypotension. C5F2, an IgG3 isotype, recognizes an epitope in the N terminus of the second extracellular loop (ECL2) of β2AR. Surface plasmon resonance analysis revealed high binding affinity for the β2AR ECL2 peptide. Immunoblotting and immunofluorescence demonstrated specific binding to β2AR in H9c2 cardiomyocytes, CHO cells expressing human β2AR, and rat aorta. C5F2 stimulated cyclic AMP production in β2AR-transfected CHO cells and induced potent dilation of isolated rat cremaster arterioles, both of which were specifically blocked by the β2AR-selective antagonist ICI-118551 and by the β2AR ECL2 peptide. This monoclonal antibody demonstrated sufficient activity to produce postural hypotension in its host. Its availability provides a unique opportunity to identify previously unrecognized causes and new pharmacological management of postural hypotension and other cardiovascular diseases.

Published

2013

50. Prefoldin Plays a Role as a Clearance Factor in Preventing Proteasome Inhibitor-induced Protein Aggregation

Author

Yuka Takekoshi, Takashi Shimizu, Akira Abe, Kazuko Takahashi-Niki, Hiroshi Maita, Hirotake Kitaura, Sanae M.M. Iguchi-Ariga, and Hiroyoshi Ariga

Subjects

Male, Proteasome Endopeptidase Complex, Protein Denaturation, Cell Survival, Protein subunit, Lactacystin, Mutation, Missense, Protein aggregation, Biology, Endoplasmic Reticulum, Biochemistry, Mice, chemistry.chemical_compound, Cell Line, Tumor, medicine, Animals, Humans, Molecular Biology, Cell Death, Endoplasmic reticulum, Antibodies, Monoclonal, Brain, Neurodegenerative Diseases, Cell Biology, Prefoldin complex, Ubiquitinated Proteins, Acetylcysteine, Protein Structure, Tertiary, Prefoldin, Cell biology, Proteasome, chemistry, Protein Synthesis and Degradation, Proteasome inhibitor, Thapsigargin, Proteasome Inhibitors, HeLa Cells, Molecular Chaperones, Protein Binding, medicine.drug

Abstract

Prefoldin is a molecular chaperone composed of six subunits, PFD1–6, and prevents misfolding of newly synthesized nascent polypeptides. Although it is predicted that prefoldin, like other chaperones, modulates protein aggregation, the precise function of prefoldin against protein aggregation under physiological conditions has never been elucidated. In this study, we first established an anti-prefoldin monoclonal antibody that recognizes the prefoldin complex but not its subunits. Using this antibody, it was found that prefoldin was localized in the cytoplasm with dots in co-localization with polyubiquitinated proteins and that the number and strength of dots were increased in cells that had been treated with lactacystin, a proteasome inhibitor, and thapsigargin, an inducer of endoplasmic reticulum stress. Knockdown of prefoldin increased the level of SDS-insoluble ubiquitinated protein and reduced cell viability in lactacystin and thapsigargin-treated cells. Opposite results were obtained in prefoldin-overexpressed cells. It has been reported that mice harboring a missense mutation L110R of MM-1α/PFD5 exhibit neurodegeneration in the cerebellum. Although the prefoldin complex containing L110R MM-1α was properly formed in vitro and in cells derived from L110R MM-1α mice, the levels of ubiquitinated proteins and cytotoxicity were higher in L110R MM-1α cells than in wild-type cells under normal conditions and were increased by lactacystin and thapsigargin treatment, and growth of L110R MM-1α cells was attenuated. Furthermore, the polyubiquitinated protein aggregation level was increased in the brains of L110R MM-1α mice. These results suggest that prefoldin plays a role in quality control against protein aggregation and that dysfunction of prefoldin is one of the causes of neurodegenerative diseases. Background: Prefoldin consisting of six subunits prevents protein misfolding. Results: Prefoldin prevented proteasome inhibitor- and endoplasmic reticulum stress-induced protein aggregation, and mutation of a prefoldin subunit resulted in loss of its activity. Conclusion: In addition to its protein folding activity, prefoldin protects cells from aggregated protein-induced cell death. Significance: Prefoldin is a quality control protein against protein aggregation.

Published

2013