Your search keyword '"Janine Ferrant"' showing total 11 results

1. Assessing in vivo dynamics of multiple quality attributes from a therapeutic IgG4 monoclonal antibody circulating in cynomolgus monkey

Author

Yu Huang, Yue Emma Zhang, Janine Ferrant, Yelena Lyubarskaya, Yinyin Li, Shiaw-Lin Billy Wu, and Siyang Peter Li

Subjects

0301 basic medicine, medicine.drug_class, media_common.quotation_subject, Immunology, quality attributes, Biology, Pharmacology, Monoclonal antibody, 01 natural sciences, Peptide Mapping, 03 medical and health sciences, Affinity chromatography, In vivo, Report, medicine, Immunology and Allergy, Animals, Quality (business), Peptide sequence, media_common, mass spectrometry, 010401 analytical chemistry, Antibodies, Monoclonal, Affinity purification, In vitro, 0104 chemical sciences, in vivo, Macaca fascicularis, 030104 developmental biology, Biopharmaceutical, Immunoglobulin G, Models, Animal, monkey, Critical quality attributes

Abstract

Characterization of biopharmaceutical proteins and assessment and understanding of the critical quality attributes (CQAs) is a significant part of biopharmaceutical product development and is routinely performed in vitro. In contrast, systematic analysis of the quality attributes in vivo is not as widespread, although metabolism and clearance of multiple variants of therapeutic proteins administered to non-human primates and human subjects may have a different impact on safety, efficacy and exposure. The major hurdles of such studies are usually sample availability and technical capability. In this study, we used affinity purification coupled with liquid chromatography and mass spectrometric analysis of the digested protein for consistent and simultaneous detection of the full amino acid sequence of a therapeutic IgG4 monoclonal antibody, MAB1. This methodology allowed us to assess in vivo changes of all sequence-related modifications and quality attributes of MAB1 over the duration of a preclinical pharmacokinetic study in cynomolgus monkeys.

Published

2016

2. A Prodomain Fragment from the Proteolytic Activation of Growth Differentiation Factor 11 Remains Associated with the Mature Growth Factor and Keeps It Soluble

Author

Andreas Lehmann, Thomas Cameron, Yan Gao, Bang-Jian Gong, Dingyi Wen, Thomas Walz, Joseph Amatucci, Pepinsky R Blake, Martin Bush, Nels E. Pederson, Yaping Sun, and Janine Ferrant

Subjects

0301 basic medicine, Proteolysis, medicine.medical_treatment, Protein domain, Peptide, CHO Cells, Biology, Biochemistry, 03 medical and health sciences, Cricetulus, Protein Domains, Cricetinae, medicine, Animals, Humans, chemistry.chemical_classification, medicine.diagnostic_test, Growth factor, Chinese hamster ovary cell, Hydrogen-Ion Concentration, biology.organism_classification, Growth Differentiation Factors, 030104 developmental biology, chemistry, Solubility, GDF11, Bone Morphogenetic Proteins, Protein Multimerization, Peptides, Transforming growth factor

Abstract

Growth differentiation factor 11 (GDF11), a member of the transforming growth factor β (TGF-β) family, plays diverse roles in mammalian development. It is synthesized as a large, inactive precursor protein containing a prodomain, pro-GDF11, and exists as a homodimer. Activation requires two proteolytic processing steps that release the prodomains and transform latent pro-GDF11 into active mature GDF11. In studying proteolytic activation in vitro, we discovered that a 6-kDa prodomain peptide containing residues 60–114, PDP60–114, remained associated with the mature growth factor. Whereas the full-length prodomain of GDF11 is a functional antagonist, PDP60–114 had no impact on activity. The specific activity of the GDF11/PDP60–114 complex (EC50 = 1 nM) in a SMAD2/3 reporter assay was identical to that of mature GDF11 alone. PDP60–114 improved the solubility of mature GDF11 at neutral pH. As the growth factor normally aggregates/precipitates at neutral pH, PDP60–114 can be used as a solubility-enhancing form...

Published

2017

3. A Monoclonal Antibody to α1β1 Blocks Antigen-induced Airway Responses in Sheep

Author

Amie N. Carmillo, Victor Koteliansky, Ashfaq Ahmed, Roy R. Lobb, Frederick R. Taylor, Philip Gotwals, Ellen Garber, William M. Abraham, Janine Ferrant, Antonin de Fougerolles, and Irakli Serebriakov

Subjects

Male, Pulmonary and Respiratory Medicine, Integrins, medicine.drug_class, Inflammation, Critical Care and Intensive Care Medicine, Monoclonal antibody, Sensitivity and Specificity, Bronchial Provocation Tests, CD49a, Antigen, Receptors, Very Late Antigen, Reference Values, Intensive care, Administration, Inhalation, medicine, Animals, Receptor, Sheep, Domestic, Probability, biology, business.industry, Airway Resistance, Antibodies, Monoclonal, CD29, Disease Models, Animal, Immunology, biology.protein, Female, Bronchial Hyperreactivity, Antibody, medicine.symptom, business

Abstract

The integrin alpha1beta1 (very late antigen-1; CD49a/CD29) is a major adhesion receptor for collagen I, IV, and VI, and its induced expression on activated monocytes and lymphocytes plays a central role in their retention and activation at inflammatory sites in autoimmune pathologies. However, the role of alpha1beta1 in allergic settings has not been explored. In this study, we show that a single 45-mg dose of aerosolized monoclonal antibody AQC2 to the alpha1 chain of human and sheep very late antigen-1, given 30 minutes before challenge, blocks both the allergen-induced late response and the associated airway hyperresponsiveness, functional indicators of allergen-induced inflammation, in sheep. AQC2 does not affect the early response. Consistent with these effects, AQC2 tended to reduce the cell response associated with local antigen instillation. An isotype-matched control antibody had no protective effects. Two humanized versions of AQC2, a wild-type IgG1 and an aglycosyl form of the same monoclonal antibody, which has reduced Fc receptor-mediated effector functions, are equally effective in blocking the antigen-induced late response and airway hyperresponsiveness in the sheep model. These data suggest that mononuclear leukocyte adhesion-dependent pathologies contribute to allergic lung disease and provide proof-of-concept that antagonists of alpha1 integrins may be useful in preventing these events.

Published

2004

4. Variation in the ordered structure of complexes between CD154 and anti-CD154 monoclonal antibodies

Author

Frederick R. Taylor, Christopher D. Benjamin, Cheryl A. Wilson, Yen-Ming Hsu, Kenneth H. Roux, Michael Karpusas, Janine Ferrant, and Hess Donna M

Subjects

medicine.drug_class, Chemistry, CD40 Ligand, Immunology, Size-exclusion chromatography, Cell, Antibodies, Monoclonal, Antigen-Antibody Complex, Monoclonal antibody, Ligand (biochemistry), Molecular biology, law.invention, Jurkat Cells, Microscopy, Electron, medicine.anatomical_structure, Dynamic light scattering, Confocal microscopy, law, medicine, Biophysics, Humans, CD154, Electron microscope, Molecular Biology

Abstract

The cell surface co-stimulatory protein CD154 (CD40L) is a target for monoclonal antibody (mAb) inhibitors of T-cell mediated immune diseases. This protein, like most other members of the TNF ligand family, forms homotrimeric complexes on the cell surface and in solution, with a three-fold axis of symmetry. We find that several different anti-CD154 monoclonal antibodies form distinctive complexes with soluble CD154. These soluble complexes have been analyzed using size exclusion chromatography, static and dynamic light scattering, and electron microscopy and shown to consist of caged structures of various geometries. The cell surface complexes have been analyzed by confocal microscopy and, depending on the mAb, remain as small, separate complexes or form large aggregates. The formation of these complexes in solution is likely to have an impact on measures of affinity, while the cell surface complexes could affect binding potency and provoke other biological effects.

Published

2002

5. Structure of CD40 Ligand in Complex with the Fab Fragment of a Neutralizing Humanized Antibody

Author

Kathy Strauch, Janine Ferrant, Yen-Ming Hsu, Michael Karpusas, Jodie Lucci, Christopher D. Benjamin, Frederick R. Taylor, and Ellen Garber

Subjects

Models, Molecular, crystal structure, medicine.drug_class, Protein Conformation, CD40 Ligand, Molecular Sequence Data, Static Electricity, Antibody Affinity, Humanized antibody, Monoclonal antibody, Crystallography, X-Ray, Epitope, Epitopes, Immunoglobulin Fab Fragments, Mice, antigen, Antigen, Neutralization Tests, Structural Biology, medicine, Animals, Humans, Amino Acid Sequence, CD154, Molecular Biology, B cell, epitope, Microscopy, Confocal, biology, Antibodies, Monoclonal, hemic and immune systems, Molecular biology, medicine.anatomical_structure, Immunoglobulin class switching, biology.protein, Biophysics, Mutagenesis, Site-Directed, Binding Sites, Antibody, Antibody, mutagenesis

Abstract

Background: CD40 ligand (CD40L or CD154), a member of the tumor necrosis factor (TNF) family, plays a critical role in both humoral and cellular immune responses and has been implicated in biological pathways involving epithelial cells, fibroblasts, and platelets. Such a pathway is T cell-mediated B cell activation, a process that occurs through the interaction of CD40L with CD40 receptor expressed on B cells. It results in various B cell responses, including immunoglobulin isotype switching and B cell differentiation and proliferation. These responses can be inhibited by the monoclonal antibody 5c8, which binds with high affinity to CD40L. Results: To understand the structural basis of the inhibition, we determined the crystal structure of the complex of the extracellular domain of CD40L and the Fab fragment of humanized 5c8 antibody. The structure shows that the complex has the shape of a three-bladed propeller with three Fab fragments bound symmetrically to a CD40L homotrimer. To further study the nature of the antibody-antigen interface, we assessed the ability of 23 site-directed mutants of CD40L to bind to 5c8 and CD40 and analyzed the results in the context of the crystal structure. Finally, we observed via confocal microscopy that 5c8 binding to CD40L on the cell surface results in the formation of patches of clustered complexes. Conclusions: The structure reveals that 5c8 neutralizes CD40L function by sterically blocking CD40 binding. The antigenic epitope is localized in a region of the surface that is likely to be structurally perturbed as a result of genetic mutations that cause hyper-IgM syndrome. The symmetric trimeric arrangement of the Fab fragments in the complex results in a geometry that facilitates the formation of large clusters of complexes on the cell surface.

Published

2001

6. Long-term anti-CD154 dosing in nephritic mice is required to maintain survival and inhibit mediators of renal fibrosis

Author

Anne H. Cutler, Janine Ferrant, and Susan L. Kalled

Subjects

medicine.medical_specialty, CD40 Ligand, Lupus nephritis, Renal function, 030204 cardiovascular system & hematology, Kidney, Antibodies, Mice, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, Fibrosis, Internal medicine, medicine, Renal fibrosis, Animals, 030203 arthritis & rheumatology, Proteinuria, business.industry, medicine.disease, Lupus Nephritis, medicine.anatomical_structure, Endocrinology, Renal pathology, Immunotherapy, medicine.symptom, business, Nephritis

Abstract

The CD154=CD40 pathway is required for the development and progression of disease in a variety of autoimmune model systems. We have demonstrated previously that long-term anti-CD154 treatment of nephritic (SWR×NZB)F1 mice prolonged survival and preserved kidney function. Herein we ask if long-term treatment is required and further characterize the protective effect on renal pathology by examining a-smooth muscle actin, collagen and TGF-b1 expression in renal tissue. The effects of anti-CD154 on brain and heart inflammation are also examined. Three dosing strategies of anti-CD154 mAb were compared in SNF1 mice that exhibited moderate or severe nephritis: (1) weekly for 6 weeks; (2) monthly; (3) weekly for 6-12 weeks followed by monthly dosing. Proteinuria, serum anti-DNA, anti-CD154 pharmacokinetics and serum soluble CD154 analyses were performed. Anti-CD154 treatment of moderate disease increased survival across all regimens, although weekly followed by monthly maintenance dosing proved most efficacious. This regime also inhibited renal a-smooth muscle actin and collagen deposition. Only the most aggressive anti-CD154 treatment protocol increased survival in severely nephritic mice. Long-term anti-CD154 treatment significantly inhibits key mediators of kidney fibrosis and is required to maximize survival and renal function. Potential reasons for differential therapeutic efficacy in moderately vs severely nephritic mice are discussed.

Published

2001

7. Biochemical analysis of retroviral structural proteins to identify and quantify retrovirus expressed by an NS0 murine myeloma cell line

Author

Frederick R. Taylor, R. Blake Pepinsky, Chenhui Zeng, Judith Sernatinger, Janine Ferrant, Susan F. Foley, and Robert Juffras

Subjects

medicine.drug_class, viruses, Blotting, Western, Molecular Sequence Data, Retroviridae Proteins, Gene Products, gag, Bioengineering, Biology, Monoclonal antibody, Applied Microbiology and Biotechnology, Mass Spectrometry, Virus, Mice, Bioreactors, Capsid, Retrovirus, Western blot, Murine leukemia virus, Tumor Cells, Cultured, medicine, Animals, Amino Acid Sequence, Chromatography, High Pressure Liquid, Leukemia, Experimental, medicine.diagnostic_test, General Medicine, Viral Load, biology.organism_classification, Virology, Molecular biology, Leukemia Virus, Murine, Microscopy, Electron, Tumor Virus Infections, Titer, Cell culture, Multiple Myeloma, Retroviridae Infections, Biotechnology

Abstract

A subclone of the NS0 murine myeloma cell line, frequently used to produce recombinant monoclonal antibodies, was found by a transmission electron microscopy method to express a surprisingly high titer of 10 11 retroviral particles per ml of culture supernatant. Infectivity assays showed a very low infectious titer with the restricted host range expected for a murine amphotropic retrovirus. A Western blot assay for the viral capsid protein was developed to confirm the high titer values and provide a means for monitoring batch consistency and virus removal during the purification process. Mass spectrometry of several of the viral Gag proteins demonstrated that the cell line appeared to produce at least two closely related retroviruses. N-terminal sequencing of three of the Gag proteins demonstrated that these retroviruses were members of the murine leukemia retroviral family. Western blot detection with an antibody for the capsid protein gave a linear standard curve over the range of 0.1–3 ng per lane. This allows the detection of viral titers as low as 6×10 7 virions per ml without the need to concentrate the sample. The Western blot method has higher throughput and less variability than transmission electron microscopy methods and has potential for monitoring viral titer and clearance during development of manufacturing processes.

Published

2000

8. The contribution of Fc effector mechanisms in the efficacy of anti-CD154 immunotherapy depends on the nature of the immune challenge

Author

Christopher D. Benjamin, Ellen Garber, Norma S. Kenyon, Yen Ming Hsu, Renee I. Shapiro, Linda C. Burkly, David M. Harlan, Janine Ferrant, Frederick R. Taylor, Susan L. Kalled, Anne H. Cutler, Hess Donna M, and Allan D. Kirk

Subjects

Glycosylation, medicine.medical_treatment, Immunology, CD40 Ligand, Islets of Langerhans Transplantation, chemical and pharmacologic phenomena, medicine.disease_cause, Antibodies, Monoclonal, Humanized, Autoimmunity, Mice, Immune system, Co-stimulation, immune system diseases, medicine, Immunology and Allergy, Animals, Humans, Lupus Erythematosus, Systemic, Transplantation, Homologous, CD40 Antigens, Lupus erythematosus, biology, Effector, Receptors, IgG, Immunization, Passive, Antibodies, Monoclonal, hemic and immune systems, General Medicine, Immunotherapy, medicine.disease, Kidney Transplantation, Immunoglobulin Fc Fragments, Transplantation, Disease Models, Animal, Macaca fascicularis, biology.protein, Antibody, Thrombocythemia, Essential

Abstract

Blockade of the CD154-CD40 co-stimulatory pathway with anti-CD154 mAbs has shown impressive efficacy in models of autoimmunity and allotransplantation. Clinical benefit was also demonstrated in systemic lupus erythematosus (SLE) and idiopathic thrombocytopenia patients with the humanized anti-CD154 mAb, 5C8 (hu5C8). However, thromboembolic complications that occurred during the course of the hu5C8 clinical trials have proven to be a major setback to the field and safe alternative therapeutics targeting the CD154-CD40 pathway are of great interest. Recently, effector mechanisms have been shown to play a part in anti-CD154 mAb-induced transplant acceptance in murine models, while this issue remains unresolved for humoral-mediated models. Herein, aglycosyl anti-CD154 mAbs with reduced binding to FcgammaR and complement were used as a novel means to test the role of effector mechanisms in non-human primate and murine models not amenable to gene knockout technology. While aglycosyl hu5C8 mAb was relatively ineffective in rhesus renal and islet allotransplantation, it inhibited primary and secondary humoral responses to a protein immunogen in cynomolgus monkeys. Moreover, an aglycosyl, chimeric MR1 mAb (muMR1) prolonged survival and inhibited pathogenic auto-antibody production in a murine model of SLE. Thus, the mechanisms required for efficacy of anti-CD154 mAbs depend on the nature of the immune challenge.

Published

2004

9. FcR interactions do not play a major role in inhibition of experimental autoimmune encephalomyelitis by anti-CD154 monoclonal antibodies

Author

Ellen Garber, Wouter van Rijs, Linda C. Burkly, Janine Ferrant, Lex Nagelkerken, Inge Haspels, Frederick R. Taylor, Hess Donna M, and Bep Blauw

Subjects

Proteolipid protein 1, Encephalomyelitis, Autoimmune, Experimental, Glycosylation, medicine.drug_class, T-Lymphocytes, Immunology, CD40 Ligand, Receptors, Fc, Monoclonal antibody, Mice, immune system diseases, medicine, Immunology and Allergy, Animals, CD154, Receptor, Myelin Proteolipid Protein, B-Lymphocytes, CD40, biology, Chemistry, Experimental autoimmune encephalomyelitis, Antibodies, Monoclonal, medicine.disease, Peptide Fragments, Myelin proteolipid protein, biology.protein, Female, Antibody

Abstract

It has been demonstrated that anti-CD154 mAb treatment effectively inhibits the development of experimental autoimmune encephalomyelitis (EAE). However, although it appears to prevent the induction of Th1 cells and reactivation of encephalitogenic T cells within the CNS, little information is available regarding the involvement of alternative mechanisms, nor has the contribution of Fc effector mechanisms in this context been addressed. By contrast, efficacy of anti-CD154 mAbs in models of allotransplantation has been reported to involve long-term unresponsiveness, potentially via activation of T regulatory cells, and recently was reported to depend on Fc-dependent functions, such as activated T cell depletion through FcγR or complement. In this study we demonstrate that anti-CD154 mAb treatment inhibits EAE development in SJL mice without apparent long-term unresponsiveness or active suppression of disease. To address whether the mechanism of inhibition of EAE by anti-CD154 mAb depends on its Fc effector interactions, we compared an anti-CD154 mAb with its aglycosyl counterpart with severely impaired FcγR binding and reduced complement binding activity with regard to their ability to inhibit clinical signs of EAE and report that both forms of the Ab are similarly protective. This observation was largely confirmed by the extent of leukocyte infiltration of the CNS; however, mice treated with the aglycosyl form may display slightly more proteolipid protein 139-151-specific immune reactivity. It is concluded that FcR interactions do not play a major role in the protective effect of anti-CD154 mAb in the context of EAE, though they may contribute to the full abrogation of peripheral peptide-specific lymphocyte responses. Chemicals / CAS: Antibodies, Monoclonal; CD40 Ligand, 147205-72-9; Myelin Proteolipid Protein; Peptide Fragments; proteolipid protein 139-151; Receptors, Fc

Published

2004

10. Crystal structure of the alpha1beta1 integrin I domain in complex with an antibody Fab fragment

Author

Paul H. Weinreb, Ellen Garber, Janine Ferrant, Michael Karpusas, Amie N. Carmillo, and Frederick R. Taylor

Subjects

Alanine, biology, medicine.drug_class, Stereochemistry, Chemistry, Protein Conformation, Recombinant Fusion Proteins, Integrin, Monoclonal antibody, Crystallography, X-Ray, Epitope, Integrin alpha1beta1, Residue (chemistry), Immunoglobulin Fab Fragments, Structural Biology, Laminin, Mutagenesis, biology.protein, medicine, Humans, Binding site, Antibody, Molecular Biology

Abstract

The alpha1beta1 (VLA-1) integrin is a cell-surface receptor for collagen and laminin and has been implicated in biological pathways involved in several pathological processes. These processes may be inhibited by the monoclonal antibody AQC2, which binds with high affinity to human alpha1beta1 integrin. To understand the structural basis of the inhibition we determined the crystal structure of the complex of a chimeric rat/human I domain of the alpha1beta1 integrin and the Fab fragment of humanized AQC2 antibody. The structure of the complex shows that the antibody blocks the collagen binding site of the I domain. An aspartate residue, from the CDR3 loop of the antibody heavy chain, coordinates the MIDAS metal ion in a manner similar to that of a glutamate residue from collagen. Substitution of the aspartate residue by alanine or arginine results in significant reduction of antibody binding affinity. Interestingly, although the mode of metal ion coordination resembles that of the open conformation, the I domain maintains an overall closed conformation previously observed only for unliganded I domains.

Published

2003

11. CDP7657, an anti-CD40L antibody lacking an Fc domain, inhibits CD40L-dependent immune responses without thrombotic complications: an in vivo study

Author

Ellen Garber, Christopher Peters, Alison Maloney, Ali Amirkhosravi, David L. Hutto, Linda C. Burkly, Roland Foulkes, Neil Weir, Alastair D. G. Lawson, Frederick R. Taylor, Derek Thomas Brown, Martyn K. Robinson, Todd Meyer, Olivier A. Harari, John L. Francis, Ian Wakefield, Janine Ferrant, Timothy Bourne, Sarah Malcolm, Yen-Ming Hsu, Stevan Shaw, Lihe Su, and Anthony Shock

Subjects

CD40 Ligand, Immunology, Autoimmune Diseases, Polyethylene Glycols, Immunoglobulin Fab Fragments, Immune system, Antigen, Rheumatology, immune system diseases, In vivo, Tetanus Toxoid, Animals, Humans, Lupus Erythematosus, Systemic, Medicine, Immunology and Allergy, Platelet activation, Lupus erythematosus, Mice, Inbred NZB, biology, business.industry, Antibodies, Monoclonal, Thrombosis, medicine.disease, Macaca mulatta, Fragment crystallizable region, Immunity, Humoral, Disease Models, Animal, Macaca fascicularis, Antibody Formation, Humoral immunity, biology.protein, Antibody, business, Research Article

Abstract

Introduction CD40 ligand (CD40L) blockade has demonstrated efficacy in experimental autoimmune models. However, clinical trials of hu5c8, an anti-human CD40L IgG1 antibody, in systemic lupus erythematosus (SLE) were halted due to an increased incidence of thrombotic events. This study evaluated CDP7657, a high affinity PEGylated monovalent Fab' anti-CD40L antibody fragment, to assess whether an Fc-deficient molecule retains efficacy while avoiding the increased risk of thrombotic events observed with hu5c8. Methods The potency and cross-reactivity of CDP7657 was assessed in in vitro assays employing human and non-human primate leukocytes, and the capacity of different antibody formats to activate platelets in vitro was assessed using aggregometry and dense granule release assays. Given the important role CD40L plays in regulating humoral immunity, in vivo efficacy was assessed by investigating the capacity of Cynomolgus monkeys to generate immune responses to the tetanus toxoid antigen while the potential to induce thrombotic events in vivo was evaluated after repeat dosing of antibodies to Rhesus monkeys. A PEGylated anti-mouse CD40L was generated to assess efficacy in the New Zealand Black/White (NZB/W) mouse model of SLE. Results CDP7657 dose-dependently inhibited antigen-specific immune responses to tetanus toxoid in Cynomolgus monkeys, and in contrast to hu5c8, there was no evidence of pulmonary thrombovasculopathy in Rhesus monkeys. Aglycosyl hu5c8, which lacks Fc receptor binding function, also failed to induce thrombotic events in Rhesus monkeys. In vitro experiments confirmed that antibody constructs lacking an Fc, including CDP7657, did not induce human or monkey platelet activation. A PEGylated monovalent Fab' anti-mouse CD40L antibody also inhibited disease activity in the NZB/W mouse model of SLE after administration using a therapeutic dosing regimen where mice received antibodies only after they had displayed severe proteinuria. Conclusions These findings demonstrate for the first time that anti-CD40L antibodies lacking a functional Fc region do not induce thrombotic events in Rhesus monkeys and fail to activate platelets in vitro but, nevertheless retain pharmacological activity and support the investigation of CDP7657 as a potential therapy for systemic lupus erythematosus and other autoimmune diseases. Electronic supplementary material The online version of this article (doi:10.1186/s13075-015-0757-4) contains supplementary material, which is available to authorized users.