Your search keyword '"Fc fusion"' showing total 361 results

1. Efficient Expression of Functionally Active Aflibercept with Designed N-glycans.

Author

Keshvari, Tahereh, Melnik, Stanislav, Sun, Lin, Niazi, Ali, Aram, Farzaneh, Moghadam, Ali, Kogelmann, Benjamin, Wozniak-Knopp, Gordana, Kallolimath, Somanath, Ramezani, Amin, and Steinkellner, Herta

Subjects

*VASCULAR endothelial growth factor receptors, *AFLIBERCEPT

Abstract

Aflibercept is a therapeutic recombinant fusion protein comprising extracellular domains of human vascular endothelial growth factor receptors (VEGFRs) and IgG1-Fc. It is a highly glycosylated protein with five N-glycosylation sites that might impact it structurally and/or functionally. Aflibercept is produced in mammalian cells and exhibits large glycan heterogeneity, which hampers glycan-associated investigations. Here, we report the expression of aflibercept in a plant-based system with targeted N-glycosylation profiles. Nicotiana benthamiana-based glycoengineering resulted in the production of aflibercept variants carrying designed carbohydrates, namely, N-glycans with terminal GlcNAc and sialic acid residues, herein referred to as AFLIGnGn and AFLISia, respectively. Both variants were transiently expressed in unusually high amounts (2 g/kg fresh leaf material) in leaves and properly assembled to dimers. Mass spectrometric site-specific glycosylation analyses of purified aflibercept showed the presence of two to four glycoforms in a consistent manner. We also demonstrate incomplete occupancy of some glycosites. Both AFLIGnGn and AFLISia displayed similar binding potency to VEGF165, with a tendency of lower binding to variants with increased sialylation. Collectively, we show the expression of functionally active aflibercept in significant amounts with controlled glycosylation. The results provide the basis for further studies in order to generate optimized products in the best-case scenario. [ABSTRACT FROM AUTHOR]

Published

2024

2. An engineered Fc fusion protein that targets antigen-specific T cells and autoantibodies mitigates autoimmune disease

Author

Mathangi Janakiraman, Alexei Leliavski, Jeeva Varadarajulu, Dieter Jenne, and Gurumoorthy Krishnamoorthy

Subjects

Multiple sclerosis, EAE, Fc fusion, T cells, Autoantibodies, Tolerance, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Current effective therapies for autoimmune diseases rely on systemic immunomodulation that broadly affects all T and/or B cell responses. An ideal therapeutic approach would combine autoantigen-specific targeting of both T and B cell effector functions, including efficient removal of pathogenic autoantibodies. Albeit multiple strategies to induce T cell tolerance in an autoantigen-specific manner have been proposed, therapeutic removal of autoantibodies remains a significant challenge. Here, we devised an approach to target both autoantigen-specific T cells and autoantibodies by producing a central nervous system (CNS) autoantigen myelin oligodendrocyte glycoprotein (MOG)-Fc fusion protein. We demonstrate that MOG-Fc fusion protein has significantly higher bioavailability than monomeric MOG and is efficient in clearing anti-MOG autoantibodies from circulation. We also show that MOG-Fc promotes T cell tolerance and protects mice from MOG-induced autoimmune encephalomyelitis. This multipronged targeting approach may be therapeutically advantageous in the treatment of autoimmunity.

Published

2023

3. Development of an RBD-Fc fusion vaccine for COVID-19

Author

Yisheng Sun, Qiaomin Li, Yuanyuan Luo, Hanping Zhu, Fang Xu, Hangjing Lu, Pingping Yao, Zhen Wang, Wenbin Zhao, and Zhan Zhou

Subjects

SARS-CoV-2, Heterologous, RBD, Delta variant, Fc fusion, Immunologic diseases. Allergy, RC581-607

Abstract

Although the global pandemic of SARS-CoV-2 has passed, there are still regional outbreaks that continue to jeopardize human health. Hence, there is still a great deal of interest in developing an efficient vaccine that can quickly and effectively prevent reemerging outbreaks of SARS-CoV-2. Delta variant was once a dominant strain in the world in 2021, and we first constructed a recombinant RBDdelta-Fc fusion vaccine by coupling the RBD of Delta variant with the human Fc fragment. This Fc fusion strategy increases the immunogenicity of the recombinant RBD vaccine, with a long-lasting high level of IgG antibodies and neutralizing antibodies induced by RBDdelta-Fc vaccine. This RBDdelta-Fc vaccine, as well as the RBD-Fc vaccine prepared in our previously study, could trigger a durable immune effect by the heterologous boosting immunity, and the RBD-Fc induced a quicker humoral immune response than the homologous immunization with inactivated vaccines. In conclusion, the Fc fusion strategy has a significant role in enhancing the immunogenicity of recombinant protein vaccines, thus promising the development of a safe and efficient vaccine for the heterologous boosting against SARS-CoV-2.

Published

2024

4. An engineered Fc fusion protein that targets antigen-specific T cells and autoantibodies mitigates autoimmune disease.

Author

Janakiraman, Mathangi, Leliavski, Alexei, Varadarajulu, Jeeva, Jenne, Dieter, and Krishnamoorthy, Gurumoorthy

Subjects

*CHIMERIC proteins, *T cells, *AUTOANTIBODIES, *MYELIN oligodendrocyte glycoprotein, *AUTOIMMUNE diseases

Abstract

Current effective therapies for autoimmune diseases rely on systemic immunomodulation that broadly affects all T and/or B cell responses. An ideal therapeutic approach would combine autoantigen-specific targeting of both T and B cell effector functions, including efficient removal of pathogenic autoantibodies. Albeit multiple strategies to induce T cell tolerance in an autoantigen-specific manner have been proposed, therapeutic removal of autoantibodies remains a significant challenge. Here, we devised an approach to target both autoantigen-specific T cells and autoantibodies by producing a central nervous system (CNS) autoantigen myelin oligodendrocyte glycoprotein (MOG)-Fc fusion protein. We demonstrate that MOG-Fc fusion protein has significantly higher bioavailability than monomeric MOG and is efficient in clearing anti-MOG autoantibodies from circulation. We also show that MOG-Fc promotes T cell tolerance and protects mice from MOG-induced autoimmune encephalomyelitis. This multipronged targeting approach may be therapeutically advantageous in the treatment of autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2023

5. A novel nanobody-based HER2-targeting antibody exhibits potent synergistic antitumor efficacy in trastuzumab-resistant cancer cells.

Author

Xinlin Liu, Linli Luan, Xi Liu, Dingwen Jiang, Junwen Deng, Jiazhen Xu, Yang Yuan, Jiyao Xing, Bingguan Chen, Dongming Xing, and Haiming Huang

Subjects

CANCER cells, IMMUNOGLOBULINS, TRASTUZUMAB, ANTINEOPLASTIC agents, HUMAN growth, PHYLLODES tumors

Abstract

Human epithelial growth factor receptor-2 (HER2) plays an oncogenic role in numerous tumors, including breast, gastric, and various other solid tumors. While anti-HER2 therapies are approved for the treatment of HER2-positive tumors, a necessity persists for creating novel HER2-targeted agents to resolve therapeutic resistance. Utilizing a synthetic nanobody library and affinity maturation, our study identified four anti-HER2 nanobodies that exhibited high affinity and specificity. These nanobodies recognized three distinct epitopes of HER2-ECD. Additionally, we constructed VHH-Fc and discovered that they facilitated superior internalization and showed moderate growth inhibition. Compared to the combination of trastuzumab and pertuzumab, the VHH-Fc combos or their combination with trastuzumab demonstrated greater or comparable antitumor activity in both ligand-independent and ligand-driven tumors. Most remarkably, A9B5-Fc, which targeted domain I of HER2-ECD, displayed significantly enhanced trastuzumab-synergistic antitumor efficacy compared to pertuzumab under trastuzumab-resistant conditions. Our findings offer anti-HER2 nanobodies with high affinity and non-overlapping epitope recognition. The novel nanobody-based HER2-targeted antibody, A9B5-Fc, binding to HER2-ECD I, mediates promising receptor internalization. It possesses the potential to serve as a potent synergistic partner with trastuzumab, contributing to overcoming acquired resistance. [ABSTRACT FROM AUTHOR]

Published

2023

6. Efficient Expression of Functionally Active Aflibercept with Designed N-glycans

Author

Tahereh Keshvari, Stanislav Melnik, Lin Sun, Ali Niazi, Farzaneh Aram, Ali Moghadam, Benjamin Kogelmann, Gordana Wozniak-Knopp, Somanath Kallolimath, Amin Ramezani, and Herta Steinkellner

Subjects

aflibercept, plant expression, glycosylation, glycan engineering, Fc fusion, anti VEGF, Immunologic diseases. Allergy, RC581-607

Abstract

Aflibercept is a therapeutic recombinant fusion protein comprising extracellular domains of human vascular endothelial growth factor receptors (VEGFRs) and IgG1-Fc. It is a highly glycosylated protein with five N-glycosylation sites that might impact it structurally and/or functionally. Aflibercept is produced in mammalian cells and exhibits large glycan heterogeneity, which hampers glycan-associated investigations. Here, we report the expression of aflibercept in a plant-based system with targeted N-glycosylation profiles. Nicotiana benthamiana-based glycoengineering resulted in the production of aflibercept variants carrying designed carbohydrates, namely, N-glycans with terminal GlcNAc and sialic acid residues, herein referred to as AFLIGnGn and AFLISia, respectively. Both variants were transiently expressed in unusually high amounts (2 g/kg fresh leaf material) in leaves and properly assembled to dimers. Mass spectrometric site-specific glycosylation analyses of purified aflibercept showed the presence of two to four glycoforms in a consistent manner. We also demonstrate incomplete occupancy of some glycosites. Both AFLIGnGn and AFLISia displayed similar binding potency to VEGF165, with a tendency of lower binding to variants with increased sialylation. Collectively, we show the expression of functionally active aflibercept in significant amounts with controlled glycosylation. The results provide the basis for further studies in order to generate optimized products in the best-case scenario.

Published

2024

7. Immunogenic fusion proteins induce neutralizing SARS-CoV-2 antibodies in the serum and milk of sheep

Author

Gregory M. Jacobson, Kirsty Kraakman, Olivia Wallace, Jolyn Pan, Alex Hennebry, Grant Smolenski, Ray Cursons, Steve Hodgkinson, Adele Williamson, and William Kelton

Subjects

Immune milk, Fc domain, Fc fusion, SARS-CoV-2, Antigen design, Biotechnology, TP248.13-248.65

Abstract

Antigen-specific polyclonal immunoglobulins derived from the serum, colostrum, or milk of immunized ruminant animals have potential as scalable therapeutics for the control of viral diseases including COVID-19. Here we show that the immunization of sheep with fusions of the SARS-CoV-2 receptor binding domain (RBD) to ovine IgG2a Fc domains promotes significantly higher levels of antigen-specific antibodies compared to native RBD or full-length spike antigens. This antibody population contained elevated levels of neutralizing antibodies that suppressed binding between the RBD and hACE2 receptors in vitro. A second immune-stimulating fusion candidate, Granulocyte-macrophage colony-stimulating factor (GM-CSF), induced high neutralizing responses in select animals but narrowly missed achieving significance. We further demonstrated that the antibodies induced by these fusion antigens were transferred into colostrum/milk and possessed cross-neutralizing activity against diverse SARS-CoV-2 variants. Our findings highlight a new pathway for recombinant antigen design in ruminant animals with applications in immune milk production and animal health.

Published

2023

8. Strategies for extending the half-life of biotherapeutics: successes and complications.

Author

Binder U and Skerra A

Abstract

Introduction: Engineering of the drug half-life in vivo has become an integral part of modern biopharmaceutical development due to the fact that many proteins/peptides with therapeutic potential are quickly cleared by kidney filtration after injection and, thus, circulate only a few hours in humans (or just minutes in mice)., Areas Covered: Looking at the growing list of clinically approved biologics that have been modified for prolonged activity, and also the plethora of such drugs under preclinical and clinical development, it is evident that not one solution fits all needs, owing to the vastly different structural features and functional properties of the pharmacologically active entities. This article provides an overview of established half-life extension strategies, as well as of emerging novel concepts for extending the in vivo stability of biologicals, and their pros and cons., Expert Opinion: Beyond the classical and still dominating technologies for improving drug pharmacokinetics and bioavailability, Fc fusion and PEGylation, various innovative approaches that offer advantages in different respects have entered the clinical stage. While the Fc fusion partner may be gradually superseded by engineered albumin-binding domains, chemical PEGylation may be replaced by biodegradable recombinant amino-acid polymers like PASylation, thus also offering a purely biotechnological manufacturing route.

Published

2024

9. Corrigendum: Anti-HIV-1 nanobody-IgG1 constructs with improved neutralization potency and the ability to mediate Fc effector functions

Author

Angela I. Schriek, Marlies M. van Haaren, Meliawati Poniman, Gillian Dekkers, Arthur E. H. Bentlage, Marloes Grobben, Gestur Vidarsson, Rogier W. Sanders, Theo Verrips, Teunis B. H. Geijtenbeek, Raimond Heukers, Neeltje A. Kootstra, Steven W. de Taeye, and Marit J. van Gils

Subjects

HIV-1, nanobodies, neutralization, Fc fusion, Fc-mediated effector functions, Immunologic diseases. Allergy, RC581-607

Published

2022

10. Lectibodies as antivirals.

Author

Santisteban Celis, Ian Carlosalberto and Matoba, Nobuyuki

Subjects

*ANTIVIRAL agents, *CHIMERIC proteins, *GLYCANS, *LECTINS, *VIRUS diseases, *CARBOHYDRATES

Abstract

Growing concerns regarding the emergence of highly transmissible viral diseases highlight the urgent need to expand the repertoire of antiviral therapeutics. For this reason, new strategies for neutralizing and inhibiting these viruses are necessary. A promising approach involves targeting the glycans present on the surfaces of enveloped viruses. Lectins, known for their ability to recognize specific carbohydrate molecules, offer the potential for glycan-targeted antiviral strategies. Indeed, numerous studies have reported the antiviral effects of various lectins of both endogenous and exogenous origins. However, many lectins in their natural forms, are not suitable for use as antiviral therapeutics due to toxicity, other unfavorable pharmacological effects, and/or unreliable manufacturing sources. Therefore, improvements are crucial for employing lectins as effective antiviral therapeutics. A novel approach to enhance lectins' suitability as pharmaceuticals could be the generation of recombinant lectin-Fc fusion proteins, termed "lectibodies." In this review, we discuss the scientific rationale behind lectin-based antiviral strategies and explore how lectibodies could facilitate the development of new antiviral therapeutics. We will also share our perspective on the potential of these molecules to transcend their potential use as antiviral agents. [ABSTRACT FROM AUTHOR]

Published

2024

11. Anti-HIV-1 Nanobody-IgG1 Constructs With Improved Neutralization Potency and the Ability to Mediate Fc Effector Functions.

Author

Schriek, Angela I., van Haaren, Marlies M., Poniman, Meliawati, Dekkers, Gillian, Bentlage, Arthur E. H., Grobben, Marloes, Vidarsson, Gestur, Sanders, Rogier W., Verrips, Theo, Geijtenbeek, Teunis B. H., Heukers, Raimond, Kootstra, Neeltje A., de Taeye, Steven W., and van Gils, Marit J.

Subjects

IMMUNE response, KILLER cells, PHAGOCYTOSIS, IMMUNOGLOBULINS, ANTIRETROVIRAL agents, CELL physiology

Abstract

The most effective treatment for HIV-1, antiretroviral therapy, suppresses viral replication and averts the disease from progression. Nonetheless, there is a need for alternative treatments as it requires daily administration with the possibility of side effects and occurrence of drug resistance. Broadly neutralizing antibodies or nanobodies targeting the HIV-1 envelope glycoprotein are explored as alternative treatment, since they mediate viral suppression and contribute to the elimination of virus-infected cells. Besides neutralization potency and breadth, Fc-mediated effector functions of bNAbs also contribute to the in vivo efficacy. In this study multivalent J3, 2E7 and 1F10 anti-HIV-1 broadly neutralizing nanobodies were generated to improve neutralization potency and IgG1 Fc fusion was utilized to gain Fc-mediated effector functions. Bivalent and trivalent nanobodies, coupled using long glycine-serine linkers, showed increased binding to the HIV-1 Env and enhanced neutralization potency compared to the monovalent variant. Fusion of an IgG1 Fc domain to J3 improved neutralization potency compared to the J3-bihead and restored Fc-mediated effector functions such as antibody-dependent cellular phagocytosis and trogocytosis, and natural killer cell activation. Due to their neutralization breadth and potency and their ability to induce effector functions these nanobody-IgG1 constructs may prove to be valuable towards alternative HIV-1 therapies. [ABSTRACT FROM AUTHOR]

Published

2022

12. Anti-HIV-1 Nanobody-IgG1 Constructs With Improved Neutralization Potency and the Ability to Mediate Fc Effector Functions

Author

Angela I. Schriek, Marlies M. van Haaren, Meliawati Poniman, Gillian Dekkers, Arthur E. H. Bentlage, Marloes Grobben, Gestur Vidarsson, Rogier W. Sanders, Theo Verrips, Teunis B. H. Geijtenbeek, Raimond Heukers, Neeltje A. Kootstra, Steven W. de Taeye, and Marit J. van Gils

Subjects

HIV-1, nanobodies, neutralization, Fc fusion, Fc-mediated effector functions, Immunologic diseases. Allergy, RC581-607

Abstract

The most effective treatment for HIV-1, antiretroviral therapy, suppresses viral replication and averts the disease from progression. Nonetheless, there is a need for alternative treatments as it requires daily administration with the possibility of side effects and occurrence of drug resistance. Broadly neutralizing antibodies or nanobodies targeting the HIV-1 envelope glycoprotein are explored as alternative treatment, since they mediate viral suppression and contribute to the elimination of virus-infected cells. Besides neutralization potency and breadth, Fc-mediated effector functions of bNAbs also contribute to the in vivo efficacy. In this study multivalent J3, 2E7 and 1F10 anti-HIV-1 broadly neutralizing nanobodies were generated to improve neutralization potency and IgG1 Fc fusion was utilized to gain Fc-mediated effector functions. Bivalent and trivalent nanobodies, coupled using long glycine-serine linkers, showed increased binding to the HIV-1 Env and enhanced neutralization potency compared to the monovalent variant. Fusion of an IgG1 Fc domain to J3 improved neutralization potency compared to the J3-bihead and restored Fc-mediated effector functions such as antibody-dependent cellular phagocytosis and trogocytosis, and natural killer cell activation. Due to their neutralization breadth and potency and their ability to induce effector functions these nanobody-IgG1 constructs may prove to be valuable towards alternative HIV-1 therapies.

Published

2022

13. Protein Engineering Strategies for Improved Pharmacokinetics.

Author

Rondon, Aurélie, Mahri, Sohaib, Morales‐Yanez, Francisco, Dumoulin, Mireille, and Vanbever, Rita

Subjects

*PROTEIN engineering, *BIOPOLYMERS, *PROTEIN structure, *CHIMERIC proteins, *SMALL molecules, *CHEMICAL engineering, *GENETIC engineering

Abstract

Protein therapeutics have gained momentum in recent years and become a pillar in treating many diseases and the only choice in several ailments. Protein therapeutics are highly specific, tunable, and less toxic than conventional small drug molecules. However, reaping the full benefits of therapeutic proteins in the clinics is often hindered by issues of immunogenicity and short half‐life due essentially to fast renal clearance and enzymatic degradation. Advances in polymer chemistry and protein engineering allowed overcoming some of these limitations. Strategies to prolong the half‐life of proteins rely on increasing their size and stability and/or fusing them to endogenous proteins (albumin, Fc fragment of antibody) to hijack physiological pathways involved in protein recycling. On the downside, these modifications might alter therapeutic proteins structure and function. Therefore, a compromise between half‐life and activity is sought. This review covers half‐life extension strategies using natural and synthetic polymers as well as fusion to other proteins and sheds light on genetic engineering strategies and chemical and enzymatic reactions to achieve this goal. Promising strategies and successful applications in the clinics are highlighted. [ABSTRACT FROM AUTHOR]

Published

2021

14. Structure-guided design of ultrapotent disruptive IgE inhibitors to rapidly terminate acute allergic reactions.

Author

Pennington, Luke F., Gasser, Pascal, Brigger, Daniel, Guntern, Pascal, Eggel, Alexander, and Jardetzky, Theodore S.

Abstract

Anaphylaxis represents one of the most severe and fatal forms of allergic reactions. Like most other allergies, it is caused by activation of basophils and mast cells by allergen-mediated cross-linking of IgE bound to its high-affinity receptor, FcεRI, on the cell surface. The systemic release of soluble mediators induces an inflammatory cascade, rapidly causing symptoms with peak severity in minutes to hours after allergen exposure. Primary treatment for anaphylaxis consists of immediate intramuscular administration of adrenaline. While adrenaline alleviates life-threatening symptoms of an anaphylactic reaction, there are currently no disease-modifying interventions available. We sought to develop potent and fast-acting IgE inhibitors with the potential to rapidly terminate acute allergic reactions. Using affinity maturation by yeast display and structure-guided molecular engineering, we generated 3 optimized disruptive IgE inhibitors based on designed ankyrin repeat proteins and assessed their ability to actively remove IgE from allergic effector cells in vitro as well as in vivo in mice. The engineered IgE inhibitors rapidly dissociate preformed IgE:FcεRI complexes, terminate IgE-mediated signaling in preactivated human blood basophils in vitro, and shut down preinitiated allergic reactions and anaphylaxis in mice in vivo. Fast-acting disruptive IgE inhibitors demonstrate the feasibility of developing kinetically optimized inhibitors for the treatment of anaphylaxis and the rapid desensitization of allergic individuals. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2021

15. A single injection of CM1021, a long half-life hepatocyte growth factor mimetic, increases liver mass in mice

Author

James H. Kelly

Subjects

Hepatocyte growth factor, Hepatocyte growth factor mimetic, Fc fusion, Long half-life, Branching morphogenesis, Hepatocyte division, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

Despite years of positive animal data, hepatocyte growth factor (HGF) has never been developed into a useful pharmaceutical, primarily due to its poor pharmacological properties. CM1021 is a fusion protein containing the K1 loop of HGF and the human IgG1 Fc region. The experiments described here demonstrate that CM1021 has the biological properties of HGF and the pharmacological properties of a monoclonal antibody. CM1021 stimulates scattering and branching morphogenesis in MDCK cells and stimulates liver growth in vivo. Unlike HGF, it is available via intraperitoneal injection and has an estimated half-life similar to an antibody.

Published

2021

16. 'Fc Fusion Proteins'

Author

Heath, Carole, Pettit, Dean, Perrie, Yvonne, Series Editor, Warne, Nicholas W., editor, and Mahler, Hanns-Christian, editor

Published

2018

17. A VHH-Fc Fusion Targeted to the Chloroplast Thylakoid Lumen Assembles and Neutralizes Enterohemorrhagic E. coli O157:H7

Author

Adam Chin-Fatt and Rima Menassa

Subjects

enterohemorrhagic E. coli-EHEC, IgA, single domain antibody, VHH, Fc fusion, Fc engineering, Plant culture, SB1-1110

Abstract

Chimeric fusion proteins comprising a single domain antibody (VHH) fused to a crystallizable fragment (Fc) of an immunoglobulin are modular glycoproteins that are becoming increasingly in demand because of their value as diagnostics, research reagents and passive immunization therapeutics. Because ER-associated degradation and misfolding may potentially be limiting factors in the oxidative folding of VHH-Fc fusion proteins in the ER, we sought to explore oxidative folding in an alternative sub-compartment, the chloroplast thylakoid lumen, and determine its viability in a molecular farming context. We developed a set of in-house expression vectors for transient transformation of Nicotiana benthamiana leaves that target a VHH-Fc to the thylakoid lumen via either secretory (Sec) or twin-arginine translocation (Tat) import pathways. Compared to stromal [6.63 ± 3.41 mg/kg fresh weight (FW)], cytoplasmic (undetectable) and Tat-import pathways (5.43 ± 2.41 mg/kg FW), the Sec-targeted VHH-Fc showed superior accumulation (30.56 ± 5.19 mg/kg FW), but was less than that of the ER (51.16 ± 9.11 mg/kg FW). Additionally, the introduction of a rationally designed de novo disulfide bond enhances in planta accumulation when introduced into the Sec-targeted Fc fusion protein from 50.24 ± 4.08 mg/kg FW to 110.90 ± 6.46 mg/kg FW. In vitro immunofluorescent labeling assays on VHH-Fc purified from Sec, Tat, and stromal pathways demonstrate that the antibody still retains VHH functionality in binding Escherichia coli O157:H7 and neutralizing its intimate adherence to human epithelial type 2 cells. These results overall provide a proof of concept that the oxidative folding environment of the thylakoid lumen may be a viable compartment for stably folding disulfide-containing recombinant VHH-Fc proteins.

Published

2021

18. A Rationally Designed Bovine IgA Fc Scaffold Enhances in planta Accumulation of a VHH-Fc Fusion Without Compromising Binding to Enterohemorrhagic E. coli

Author

Adam Chin-Fatt, Reza Saberianfar, and Rima Menassa

Subjects

enterohemorrhagic E. coli-EHEC, IgA, VHH antibody fragment, single domain antibody (sdAb), Fc fusion, plant-made antibodies, Plant culture, SB1-1110

Abstract

We previously isolated a single domain antibody (VHH) that binds Enterohemorrhagic Escherichia coli (EHEC) with the end-goal being the enteromucosal passive immunization of cattle herds. To improve the yield of a chimeric fusion of the VHH with an IgA Fc, we employed two rational design strategies, supercharging and introducing de novo disulfide bonds, on the bovine IgA Fc component of the chimera. After mutagenizing the Fc, we screened for accumulation levels after transient transformation in Nicotiana benthamiana leaves. We identified and characterized five supercharging and one disulfide mutant, termed ‘(5 + 1)Fc’, that improve accumulation in comparison to the native Fc. Combining all these mutations is associated with a 32-fold increase of accumulation for the Fc alone, from 23.9 mg/kg fresh weight (FW) to 599.5 mg/kg FW, as well as a twenty-fold increase when fused to a VHH that binds EHEC, from 12.5 mg/kg FW tissue to 236.2 mg/kg FW. Co-expression of native or mutated VHH-Fc with bovine joining chain (JC) and bovine secretory component (SC) followed by co-immunoprecipitation suggests that the stabilizing mutations do not interfere with the capacity of VHH-Fc to assemble with JC and FC into a secretory IgA. Both the native and the mutated VHH-Fc similarly neutralized the ability of four of the seven most prevalent EHEC strains (O157:H7, O26:H11, O111:Hnm, O145:Hnm, O45:H2, O121:H19 and O103:H2), to adhere to HEp-2 cells as visualized by immunofluorescence microscopy and quantified by fluorometry. These results collectively suggest that supercharging and disulfide bond tethering on a Fc chain can effectively improve accumulation of a VHH-Fc fusion without impacting VHH functionality.

Published

2021

19. A VHH-Fc Fusion Targeted to the Chloroplast Thylakoid Lumen Assembles and Neutralizes Enterohemorrhagic E. coli O157:H7.

Author

Chin-Fatt, Adam and Menassa, Rima

Subjects

CHIMERIC proteins, RECOMBINANT proteins, ESCHERICHIA coli O157:H7, CHLOROPLASTS, GLYCOPROTEINS, NICOTIANA benthamiana

Abstract

Chimeric fusion proteins comprising a single domain antibody (VHH) fused to a crystallizable fragment (Fc) of an immunoglobulin are modular glycoproteins that are becoming increasingly in demand because of their value as diagnostics, research reagents and passive immunization therapeutics. Because ER-associated degradation and misfolding may potentially be limiting factors in the oxidative folding of VHH-Fc fusion proteins in the ER, we sought to explore oxidative folding in an alternative sub-compartment, the chloroplast thylakoid lumen, and determine its viability in a molecular farming context. We developed a set of in-house expression vectors for transient transformation of Nicotiana benthamiana leaves that target a VHH-Fc to the thylakoid lumen via either secretory (Sec) or twin-arginine translocation (Tat) import pathways. Compared to stromal [6.63 ± 3.41 mg/kg fresh weight (FW)], cytoplasmic (undetectable) and Tat-import pathways (5.43 ± 2.41 mg/kg FW), the Sec-targeted VHH-Fc showed superior accumulation (30.56 ± 5.19 mg/kg FW), but was less than that of the ER (51.16 ± 9.11 mg/kg FW). Additionally, the introduction of a rationally designed de novo disulfide bond enhances in planta accumulation when introduced into the Sec-targeted Fc fusion protein from 50.24 ± 4.08 mg/kg FW to 110.90 ± 6.46 mg/kg FW. In vitro immunofluorescent labeling assays on VHH-Fc purified from Sec, Tat, and stromal pathways demonstrate that the antibody still retains VHH functionality in binding Escherichia coli O157:H7 and neutralizing its intimate adherence to human epithelial type 2 cells. These results overall provide a proof of concept that the oxidative folding environment of the thylakoid lumen may be a viable compartment for stably folding disulfide-containing recombinant VHH-Fc proteins. [ABSTRACT FROM AUTHOR]

Published

2021

20. A Rationally Designed Bovine IgA Fc Scaffold Enhances in planta Accumulation of a VHH-Fc Fusion Without Compromising Binding to Enterohemorrhagic E. coli.

Author

Chin-Fatt, Adam, Saberianfar, Reza, and Menassa, Rima

Subjects

IMMUNOGLOBULIN A, ESCHERICHIA coli O157:H7, BOS, CATTLE herding, IMMUNOFLUORESCENCE

Abstract

We previously isolated a single domain antibody (VHH) that binds Enterohemorrhagic Escherichia coli (EHEC) with the end-goal being the enteromucosal passive immunization of cattle herds. To improve the yield of a chimeric fusion of the VHH with an IgA Fc, we employed two rational design strategies, supercharging and introducing de novo disulfide bonds, on the bovine IgA Fc component of the chimera. After mutagenizing the Fc, we screened for accumulation levels after transient transformation in Nicotiana benthamiana leaves. We identified and characterized five supercharging and one disulfide mutant, termed '(5 + 1)Fc', that improve accumulation in comparison to the native Fc. Combining all these mutations is associated with a 32-fold increase of accumulation for the Fc alone, from 23.9 mg/kg fresh weight (FW) to 599.5 mg/kg FW, as well as a twenty-fold increase when fused to a VHH that binds EHEC, from 12.5 mg/kg FW tissue to 236.2 mg/kg FW. Co-expression of native or mutated VHH-Fc with bovine joining chain (JC) and bovine secretory component (SC) followed by co-immunoprecipitation suggests that the stabilizing mutations do not interfere with the capacity of VHH-Fc to assemble with JC and FC into a secretory IgA. Both the native and the mutated VHH-Fc similarly neutralized the ability of four of the seven most prevalent EHEC strains (O157:H7, O26:H11, O111:Hnm, O145:Hnm, O45:H2, O121:H19 and O103:H2), to adhere to HEp-2 cells as visualized by immunofluorescence microscopy and quantified by fluorometry. These results collectively suggest that supercharging and disulfide bond tethering on a Fc chain can effectively improve accumulation of a VHH-Fc fusion without impacting VHH functionality. [ABSTRACT FROM AUTHOR]

Published

2021

21. NKG2D-Fc fusion protein promotes antitumor immunity through the depletion of immunosuppressive cells.

Author

Feng, Po-Hao, Lam, Brandon, Tseng, Ssu-Hsueh, Kung, Yu-Jui, Farmer, Emily, Cheng, Max A., and Hung, Chien-Fu

Subjects

*CHIMERIC proteins, *SUPPRESSOR cells, *KILLER cells, *IMMUNITY, *CELLS

Abstract

A major factor impeding the success of numerous therapeutic approaches in cancer is the immunosuppressive nature of the tumor microenvironment (TME). Hence, methods capable of reverting tumor immunosuppression through depletion or reprogramming of myeloid-derived suppressive cells (MDSCs) and regulatory T cells (Tregs) are of great clinical need. Here, we explore NKG2D-Fc as a modality to modulate antitumor immunity through the depletion of immunosuppressive MDSCs and Tregs in the TME. We have generated the NKG2D-Fc fusion protein and characterized its potential to mediate tumor control and overall survival in LL2 and MC38 murine models. Upon treatment of LL2 or MC38 tumor-bearing mice with NKG2D-Fc, we observe significant tumor control and enhanced survival compared to Fc control. When characterizing MDCSs and Tregs from tumor-bearing mice, we observe clear expression of NKG2D-ligand RAE1γ and subsequent binding of NKG2D-Fc fusion protein to both MDSCs and Tregs. Examining the immune profile of mice treated with NKG2D-Fc reveals significant depletion of MDSCs and Tregs in the TME, as well as an increase in NK cells likely due to the reversed suppressive TME. In conclusion, NKG2D-Fc induces antitumor immunity and tumor control through the depletion of MDSCs and Tregs, subsequently providing a niche for the infiltration and expansion of proinflammatory cells, such as NK cells. Strategies capable of modulating the immunosuppressive state in cancer are in high clinical demand. NKG2D-Fc is a simple, single tool capable of depleting both MDSCs and Tregs and should be further investigated as a therapeutic agent for the treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2020

22. Measurements of eftrenonacog alfa by 19 different combinations reagents/instrument: A single‐centre study.

Author

Sinegre, Thomas, Trayaud, Adeline, Tardieu, Maryse, Fourneyron, Virginie, Talon, Laurie, Berger, Marc G., Tillier, Maxence, Senectaire, Stéphanie, Gembara, Piotr, Barbin, Anne‐Lise, Vaissade, Aurélie, and Lebreton, Aurélien

Subjects

*CHIMERIC proteins, *HEMOPHILIA, *ACTIN

Abstract

Introduction: Recombinant factor IX Fc fusion protein (rFIXFc) is an extended half‐life concentrate for the treatment of haemophilia B (HB). rFIXFc activity monitoring is crucial in several clinical situations. However, differences were observed between one‐stage clotting (OSC) and chromogenic assays, but not for all factor IX (FIX) concentrations. Aims: To compare rFIXFc measurements obtained using different instruments and common OSC and chromogenic asssays. Methods: FIX:C measurements were performed in rFIXFc‐spiked plasma aliquots (targeted FIX levels of 1.5, 1, 0.5, 0.2, 0.05, 0.02 and 0.01 IU/mL) and plasma samples collected from two patients with HB at various time points after rFIXFc infusion, using three instruments (STA‐R MAX, ACLTOP700 and CS2100i) and common clotting and chromogenic FIX:C assays. Results: The same reagent could give different FIX:C measurements when adapted to different instruments. Moreover, the same reagent/instrument combination could give different results depending of the FIX concentration. For OSC assays, only STA‐Cephascreen on STA‐R MAX and CS2100i, SynthAFax on ACLTOP 700 and Actin on CS2100i provided acceptable recoveries for all rFIXFc concentrations. The chromogenic assays ROX‐FIX and Biophen FIX:C underestimated rFIXFc for concentrations lower than 0.05 and 0.2 IU/mL, respectively. Conclusions: Our study demonstrates that the same reagent adapted to different instruments could lead to different rFIXFc values. As rFIXFc under/overestimation could be associated with inappropriate treatment or biased calculation of pharmacokinetic parameters, the reagent/instrument combination used by haemostasis laboratories should be considered and regularly evaluated by external quality assessment programmes. [ABSTRACT FROM AUTHOR]

Published

2020

23. Development of an RBD-Fc fusion vaccine for COVID-19.

Author

Sun Y, Li Q, Luo Y, Zhu H, Xu F, Lu H, Yao P, Wang Z, Zhao W, and Zhou Z

Abstract

Although the global pandemic of SARS-CoV-2 has passed, there are still regional outbreaks that continue to jeopardize human health. Hence, there is still a great deal of interest in developing an efficient vaccine that can quickly and effectively prevent reemerging outbreaks of SARS-CoV-2. Delta variant was once a dominant strain in the world in 2021, and we first constructed a recombinant RBD delta -Fc fusion vaccine by coupling the RBD of Delta variant with the human Fc fragment. This Fc fusion strategy increases the immunogenicity of the recombinant RBD vaccine, with a long-lasting high level of IgG antibodies and neutralizing antibodies induced by RBD delta -Fc vaccine. This RBD delta -Fc vaccine, as well as the RBD-Fc vaccine prepared in our previously study, could trigger a durable immune effect by the heterologous boosting immunity, and the RBD-Fc induced a quicker humoral immune response than the homologous immunization with inactivated vaccines. In conclusion, the Fc fusion strategy has a significant role in enhancing the immunogenicity of recombinant protein vaccines, thus promising the development of a safe and efficient vaccine for the heterologous boosting against SARS-CoV-2., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2024 The Author(s).)

Published

2024

24. Potential limits of AAV‐based gene therapy with the use of new transgenes expressing factor IX fusion proteins.

Author

Le Quellec, Sandra, Enjolras, Nathalie, Negrier, Claude, Dane, Allison, McIntosh, Jenny, Rosales, Cecilia, and Nathwani, Amit

Abstract

Introduction: The variety of treatment for haemophilia B (HB) has recently improved with the emergence of both AAV‐based gene therapy and bioengineered human factor IX (hFIX) molecules with prolonged half‐life due to fusion to either albumin (Alb) or immunoglobulin Fc fragment (Fc). Aim: Adeno‐associated viral vectors (AAV) mediating expression of hFIX‐Alb and hFIX‐Fc fusion proteins was investigated for gene therapy of HB to explore if their extended half‐life translates to higher plasma levels of FIX. Methods: Single‐stranded cross‐packaged AAV2/8 vectors expressing hFIX‐Alb, hFIX‐Fc and hFIX were evaluated in vitro, and in mice. Results: Both hFIX‐Alb and hFIX‐Fc fusion proteins were synthesized and expressed as single chains of expected size following AAV‐mediated gene transfer in vitro and in vivo. The procoagulant properties of these hFIX‐fusion proteins were comparable to wild‐type hFIX. However, their expression levels were threefold lower than wild‐type hFIX in vivo most likely due to inefficient secretion. Conclusion: This, the first, evaluation of hFIX‐fusion proteins in the context of AAV gene transfer suggests that the hFIX‐fusion proteins are secreted inefficiently from the liver, thus preventing their optimal use in gene therapy approaches. [ABSTRACT FROM AUTHOR]

Published

2019

25. Optimized Production of Fc Fusion Proteins by Sortase Enzymatic Ligation

Author

Kyle D. Apley, Stephanie N. Johnson, Brandon J. DeKosky, Cory Berkland, Noora Batrash, Amy D. Laflin, and J. Daniel Griffin

Subjects

chemistry.chemical_classification, biology, General Chemical Engineering, food and beverages, A protein, Peptide, General Chemistry, Industrial and Manufacturing Engineering, Fc domain, Fc fusion, Enzyme, chemistry, Biochemistry, Sortase, biology.protein, Antibody, Ligation

Abstract

Fc fusions are a growing class of drugs comprising an antibody Fc domain covalently linked to a protein or peptide and can pose manufacturing challenges. In this study we evaluated three synthetic ...

Published

2021

26. A novel nanobody-based HER2-targeting antibody exhibits potent synergistic antitumor efficacy in trastuzumab-resistant cancer cells.

Author

Liu X, Luan L, Liu X, Jiang D, Deng J, Xu J, Yuan Y, Xing J, Chen B, Xing D, and Huang H

Subjects

Humans, Trastuzumab pharmacology, Trastuzumab therapeutic use, Receptor, ErbB-2, Ligands, Epitopes, Single-Domain Antibodies pharmacology, Single-Domain Antibodies therapeutic use, Neoplasms pathology

Abstract

Human epithelial growth factor receptor-2 (HER2) plays an oncogenic role in numerous tumors, including breast, gastric, and various other solid tumors. While anti-HER2 therapies are approved for the treatment of HER2-positive tumors, a necessity persists for creating novel HER2-targeted agents to resolve therapeutic resistance. Utilizing a synthetic nanobody library and affinity maturation, our study identified four anti-HER2 nanobodies that exhibited high affinity and specificity. These nanobodies recognized three distinct epitopes of HER2-ECD. Additionally, we constructed VHH-Fc and discovered that they facilitated superior internalization and showed moderate growth inhibition. Compared to the combination of trastuzumab and pertuzumab, the VHH-Fc combos or their combination with trastuzumab demonstrated greater or comparable antitumor activity in both ligand-independent and ligand-driven tumors. Most remarkably, A9B5-Fc, which targeted domain I of HER2-ECD, displayed significantly enhanced trastuzumab-synergistic antitumor efficacy compared to pertuzumab under trastuzumab-resistant conditions. Our findings offer anti-HER2 nanobodies with high affinity and non-overlapping epitope recognition. The novel nanobody-based HER2-targeted antibody, A9B5-Fc, binding to HER2-ECD I, mediates promising receptor internalization. It possesses the potential to serve as a potent synergistic partner with trastuzumab, contributing to overcoming acquired resistance., Competing Interests: XLL is a visiting scholar of Noventi Biopharmaceuticals Co., Ltd. LL, DJ, BC, and HH are employed by Noventi Biopharmaceuticals Co., Ltd. XL is employed by Bioworkshops Suzhou Limited. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Liu, Luan, Liu, Jiang, Deng, Xu, Yuan, Xing, Chen, Xing and Huang.)

Published

2023

27. Corrigendum: Anti-HIV-1 nanobody-IgG1 constructs with improved neutralization potency and the ability to mediate Fc effector functions (Front. Immunol., (2022), 13, 893648, 10.3389/fimmu.2022.893648)

Author

Schriek, Angela I., van Haaren, Marlies M., Poniman, Meliawati, Dekkers, Gillian, Bentlage, Arthur E. H., Grobben, Marloes, Vidarsson, Gestur, Sanders, Rogier W., Verrips, Theo, Geijtenbeek, Teunis B. H., Heukers, Raimond, Kootstra, Neeltje A., de Taeye, Steven W., van Gils, Marit J., Experimental Immunology, Graduate School, AII - Infectious diseases, Medical Microbiology and Infection Prevention, Infectious diseases, AII - Cancer immunology, APH - Aging & Later Life, and Molecular cell biology and Immunology

Subjects

Fc fusion, Fc-mediated effector functions, HIV-1, neutralization, nanobodies

Abstract

In the published article, there was an error in the Funding statement. The funder was mentioned as AIDSfonds and Aids fonds instead of Aidsfonds. The correct Funding statement appears below. Funding This work was supported by HealthHolland/Aidsfonds: LSHM19101/P-44802, by HealthHolland/AMC: 2019-1167 and the AMC Fellowship from Amsterdam UMC received by MJG. ST is supported by Young investigator grant P-53301 Aidsfonds. The authors apologize for this error and state that this does not change the scientific conclusions of the article in any way. The original article has been updated.

Published

2022

28. Corrigendum

Subjects

Fc fusion, Fc-mediated effector functions, HIV-1, neutralization, nanobodies

Abstract

In the published article, there was an error in the Funding statement. The funder was mentioned as AIDSfonds and Aids fonds instead of Aidsfonds. The correct Funding statement appears below. Funding This work was supported by HealthHolland/Aidsfonds: LSHM19101/P-44802, by HealthHolland/AMC: 2019-1167 and the AMC Fellowship from Amsterdam UMC received by MJG. ST is supported by Young investigator grant P-53301 Aidsfonds. The authors apologize for this error and state that this does not change the scientific conclusions of the article in any way. The original article has been updated.

Published

2022

29. Battle of GLP-1 delivery technologies.

Author

Yu, Minzhi, Benjamin, Mason M., Srinivasan, Santhanakrishnan, Morin, Emily E., Shishatskaya, Ekaterina I., Schwendeman, Steven P., and Schwendeman, Anna

Subjects

*DRUG delivery systems, *GLUCAGON-like peptide-1 receptor, *TYPE 2 diabetes treatment, *MONOCLONAL antibodies, *PHARMACOKINETICS

Abstract

Glucagon-like peptide-1 receptor agonists (GLP-1 RAs) belong to an important therapeutic class for treatment of type 2 diabetes. Six GLP-1 RAs, each utilizing a unique drug delivery strategy, are now approved by the Food and Drug Administration (FDA) and additional, novel GLP-1 RAs are still under development, making for a crowded marketplace and fierce competition among the manufacturers of these products. As rapid elimination is a major challenge for clinical application of GLP-1 RAs, various half-life extension strategies have been successfully employed including sequential modification, attachment of fatty-acid to peptide, fusion with human serum albumin, fusion with the fragment crystallizable (Fc) region of a monoclonal antibody, sustained drug delivery systems, and PEGylation. In this review, we discuss the scientific rationale of the various half-life extension strategies used for GLP-1 RA development. By analyzing and comparing different approved GLP-1 RAs and those in development, we focus on assessing how half-life extending strategies impact the pharmacokinetics, pharmacodynamics, safety, patient usability and ultimately, the commercial success of GLP-1 RA products. We also anticipate future GLP-1 RA development trends. Since similar drug delivery strategies are also applied for developing other therapeutic peptides, we expect this case study of GLP-1 RAs will provide generalizable concepts for the rational design of therapeutic peptides products with extended duration of action. [ABSTRACT FROM AUTHOR]

Published

2018

30. Final results of the PUPs B-LONG study: evaluating safety and efficacy of rFIXFc in previously untreated patients with hemophilia B

Author

Raina Liesner, Krista Fischer, Antoine Rauch, Deepthi Jayawardene, Michael Recht, Bent Winding, Beatrice Nolan, Anna Klukowska, Sriya Gunawardena, Amy D. Shapiro, Margaret V. Ragni, Julie Curtin, and Sutirtha Mukhopadhyay

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Clinical Trials and Observations, Population, Phases of clinical research, Hemorrhage, 030204 cardiovascular system & hematology, Hemophilia A, Hemophilia B, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Child, education, Adverse effect, Blood coagulation test, Bleeding episodes, education.field_of_study, business.industry, Hematology, Bleed, Fc fusion, 030104 developmental biology, Blood Coagulation Tests, business, Recombinant factor IX

Abstract

PUPs B-LONG evaluated the safety and efficacy of recombinant factor IX Fc fusion protein (rFIXFc) in previously untreated patients (PUPs) with hemophilia B. In this open-label, phase 3 study, male PUPs (age 85%) bleeding episodes required only 1 infusion for bleed resolution. In this first study reporting results with rFIXFc in pediatric PUPs with hemophilia B, rFIXFc was well tolerated, with the adverse event profile as expected in a pediatric hemophilia population. rFIXFc was effective, both as prophylaxis and in the treatment of bleeding episodes. This trial was registered at www.clinicaltrials.gov as #NCT02234310.

Published

2021

31. Creation of Severe Acute Respiratory Syndrome- Coronavirus-2 Spike (AA 14Q-685R) --Fc Fusion Protein

Author

Marjana, Lea and Marjana, Lea

Published

2022

32. Clinical studies of extended-half-life recombinant FVIII products for prophylaxis in adults and children: A critical review from the physician's perspective.

Author

UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Centre de malformations vasculaires congénitales, UCL - (SLuc) Service d'hématologie, Hermans, Cédric, Reding, Mark T, Astermark, Jan, Klamroth, Robert, Mancuso, Maria Elisa, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Centre de malformations vasculaires congénitales, UCL - (SLuc) Service d'hématologie, Hermans, Cédric, Reding, Mark T, Astermark, Jan, Klamroth, Robert, and Mancuso, Maria Elisa

Abstract

This review compares the methodology of published clinical studies investigating the extended-half-life (EHL) factor VIII (FVIII) products, rFVIIIFc (efmoroctocog alfa, Elocta®/Eloctate®), BAY 94-9027 (damoctocog alfa pegol, Jivi®), BAX 855 (rurioctocog alfa pegol, Adynovate®) and N8-GP (turoctocog alfa pegol, Esperoct®) including the phase 2/3 studies, A-LONG (NCT01181128), PROTECT VIII (NCT01580293), PROLONG-ATE (NCT01736475) and pathfinder2 (NCT01480180), respectively, and their corresponding pediatric studies and extensions. Study results are interpreted from a treating physician's perspective, translating into evidence-based, real-life use of the different EHL recombinant FVIII products for personalized prophylaxis. The similarities between the studies include methodology, objectives, study design and cohort size. The differences include duration, prophylactic dosing intervals, number of patient arms, use of control group and randomization, and treatment allocation. Comparing these studies broadens physicians' understanding of each treatment's applicability. Further evaluation of study data and future real-world studies should help physicians to confidently individualize and select treatment for each patient.

Published

2022

33. Corrigendum: Anti-HIV-1 nanobody-IgG1 constructs with improved neutralization potency and the ability to mediate Fc effector functions.

Subjects

IMMUNE response, IMMUNOGLOBULINS

Published

2022

34. Real-world clinical experience of extended half-life recombinant factor VIII Fc fusion protein (rFVIIIFc) in comparison to conventional factor products in patients with severe hemophilia A

Author

Ruwan Perera, Claudia Klein, T. Albert, Silvia Horneff, Georg Goldmann, Natascha Marquardt, and Johannes Oldenburg

Subjects

Clinical trial, medicine.medical_specialty, Fc fusion, business.industry, Internal medicine, Extension study, Fviii inhibitor, Medicine, Half-life, In patient, business, Severe hemophilia A, Recombinant factor viii

Abstract

Introduction: The recombinant factor FVIII Fc fusion protein (rFVIIIFc) is a first-in-class extended half-life FVIII product to treat patients with hemophilia A. The safety, efficacy and prolonged half-life of rFVIIIFc was demonstrated in the phase 3 studies A-LONG, Kids A-LONG and the extension study ASPIRE. Despite robust efficacy and safety data of rFVIIIFc therapy from clinical trials, evidence on the effectiveness of rFVIIIFc use in real-world remains scarce. Our analysis aimed at investigating the effectiveness of prophylactic rFVIIIFc treatment in routine clinical use in Germany. Material and Methods: Twenty-seven patients with severe hemophilia A, who switched from prophylaxis with conventional recombinant factor VIII (rFVIII) products to rFVIIIFc, were included. Annualized bleeding rates, factor consumption, number of injections and adherence to prophylaxis were compared. The retrospective period prior switching to rFVIIIFc was three years, while the mean follow-up period after switching to rFVIIIFc was 24.9 months. Results: Switching to rFVIIIFc led to a 33.7% reduction in mean annualized number of injections and a 18.3% reduction in mean annualized factor consumption while maintaining low bleeding rates. The mean annualized bleeding rate (ABR) was 2.5 and 1.7 for rFVIII and rFVIIIFc, respectively. The adherence improved from 87% to 94%. During the follow-up period eleven surgeries were performed; all with a hemostatic response rated as excellent. No FVIII inhibitor formation after switching to rFVIIIFc has been detected. Conclusion: Real-world treatment with rFVIIIFc was associated with substantial reductions in consumption and injection frequenies while maintaining low bleeding rates supporting safety and efficacy data from clinical trials.

Published

2021

35. Real‐world outcomes with recombinant factor IX Fc fusion protein (rFIXFc) prophylaxis: Longitudinal follow‐up in a national adult cohort

Author

Niamh M O'Connell, Catherine Bergin, Mary Byrne, Julie Benson, Kevin M. Ryan, Rachel Bird, Evelyn Singleton, Sheila Roche, Eimear Quinn, Cleona Duggan, Ruth Gilmore, Mairead O'Donovan, and James S. O’Donnell

Subjects

Adult, medicine.medical_specialty, Recombinant Fusion Proteins, 030204 cardiovascular system & hematology, Hemophilia B, Factor IX, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Haemophilia B, Genetics (clinical), Retrospective Studies, Episodic treatment, business.industry, Real world outcomes, Hematology, General Medicine, Bleed, medicine.disease, Immunoglobulin Fc Fragments, Fc fusion, Cohort, Trough level, business, Follow-Up Studies, 030215 immunology, Recombinant factor IX

Abstract

Introduction In 2017, all people with severe haemophilia B (PWSHB) in Ireland switched from standard half-life (SHL) recombinant FIX (rFIX) to rFIX Fc fusion protein (rFIXFc) prophylaxis. Aims To evaluate prophylaxis regimens, bleeding rates and factor usage for two years of rFIXFc prophylaxis in a real-world setting. Methods Data collected retrospectively from electronic diaries and medical records of PWSHB for a two-year period on rFIXFc prophylaxis were compared with paired baseline data on SHL rFIX treatment. Results 28 PWSHB (≥18 years) were enrolled, and at switchover 79% were receiving prophylaxis and 21% episodic treatment with SHL rFIX. At 24 months following switchover, all remained on rFIXFc prophylaxis with reduced infusion frequency; median dose per infusion once weekly (55 IU/kg, 20/28), every 10 days (63 IU/kg, 2/28) or every 14 days (98 IU/kg, 6/28). Median annualised bleed rate improved significantly on rFIXFc prophylaxis (2.0 versus 3.3 on SHL FIX) (p = 0.01). Median FIX trough level with once-weekly infusions was 0.09 IU/ml (0.06-0.14 IU/ml). Management of bleeding episodes was similar with rFIXFc and SHL rFIX; one infusion was sufficient to treat 74% and 77% of bleeds, respectively, with similar total median treatment per bleeding episode. Factor consumption reduced by 28% with rFIXFc prophylaxis (57 IU/kg/week, range 40-86 IU/kg/week) compared with SHL rFIX (79 IU/kg/week, range 44-210 IU/kg/week) (p = 0.002). Conclusion This study provides important insights into real-world experience of switching to rFIXFc prophylaxis in an adult population, demonstrating high rates of prophylaxis, with reduced infusion frequency, bleeding and FIX consumption.

Published

2021

36. Recombinant vaccine containing an RBD-Fc fusion induced protection against SARS-CoV-2 in nonhuman primates and mice

Author

Yansong Sun, Xiaoling Lang, Chunrun Gao, Shaolong Chen, Hao Li, Shihui Sun, Peng He, Xin Wang, Yuwei Gao, Jiangfan Li, Guoqiang Fei, Gencheng Han, Shusheng Geng, Xin Fang, Li Liang, Ge Li, Xinwang Li, Tiecheng Wang, Yan Li, Jian Zhao, Yongqiang Deng, Lei He, Gu Hongjing, Wenjin Wei, Xiaolan Yang, Zhongyu Hu, Yuee Zhao, and Zhongpeng Zhao

Subjects

2019-20 coronavirus outbreak, COVID-19 Vaccines, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, CHO Cells, Predictive markers, Antibodies, Viral, law.invention, Mice, Cricetulus, Protein Domains, law, Correspondence, Animals, Immunology and Allergy, Viral immunology, Mice, Inbred BALB C, Vaccines, Synthetic, biology, SARS-CoV-2, Chinese hamster ovary cell, COVID-19, Antibodies, Neutralizing, Virology, Immunoglobulin Fc Fragments, Molecular Docking Simulation, Macaca fascicularis, Fc fusion, Infectious Diseases, Viral infection, Spike Glycoprotein, Coronavirus, biology.protein, Recombinant DNA, Angiotensin-Converting Enzyme 2, Antibody, Synthetic immunology

Published

2021

37. CLINICAL EFFICACY OF RECOMBINANT FACTOR VIII FC FUSION PROTEIN IN HAEMOPHILIA A PATIENT RECEIVING ON DEMAND TREATMENT ONLY

Author

Saima Zahir, Hamid Saeed Malik, Saleem Ahmed Khan, Pervez Ahmed, Tahira Zafar, and Altaf Hussain

Subjects

medicine.medical_specialty, Medicine (General), Hematology, business.industry, Cross-sectional study, Haemophilia A, Bleed, medicine.disease, Gastroenterology, Recombinant factor viii, Eighty Nine, Fc fusion, Basal (phylogenetics), R5-920, recombinant factor viii, Internal medicine, medicine, Medicine, hemophilia a, business, recombinant factor viii fc fusion protein

Abstract

Objective: To evaluate the efficacy of recombinant factor VIII FC fusion protein in haemophilia A patientreceiving on demand treatment only. Study Design: Comparative cross sectional study. Place and Duration of Study: Department of Hematology, Armed Forces Institute of Pathology and PakistanHemophilia Welfare Society, Rawalpindi, from Jun to Dec 2017. Methodology: Eighty-nine male patients of Hemophilia A already receiving recombinant factor VIII (20-30 Units/kg) on demand, with no history of inhibitors were included in study. Patients were divided as per age into paediatric and adult group and also on the basis of their basal factor VIII levels into severe, moderate and mild groups. Same patients were switched to recombinant factor VIII FC fusion protein (20-30 Units/kg) and its efficacy was measured and compared with recombinant Factor VIII in terms of dose requirement, injections, bleeds in six month period, presence of inhibitors and side effects. Results: Eighty nine male patients were studied. There was significant reduction in dose from median value of5750 units for group I to 4000 units for group II. Number of bleed in six month period were reduced from 5.3 ingroup I to 4.5 in group II. Number of injections were reduced on average to 1-2 injection per bleed in group II. No inhibitors were detected in group II. Conclusion: rFVIII Fc fusion protein has prolong activity and results in reduction of total dose, number of bleed,dose per bleed and has reduced antigenecity.

Published

2021

38. Magnetic bead extraction with acid dissociation immunoassay for the determination of serum CD80-Fc fusion protein

Author

Mason Brown, Christopher Hunter, Ago B Ahene, and Rosanna Kwok

Subjects

Recombinant Fusion Proteins, Clinical Biochemistry, Enzyme-Linked Immunosorbent Assay, 030226 pharmacology & pharmacy, Acid dissociation constant, Analytical Chemistry, 03 medical and health sciences, 0302 clinical medicine, Phase (matter), medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, 030203 arthritis & rheumatology, Chromatography, medicine.diagnostic_test, Chemistry, Magnetic Phenomena, Extraction (chemistry), General Medicine, Hydrogen-Ion Concentration, Fusion protein, Immunoglobulin Fc Fragments, Medical Laboratory Technology, Fc fusion, Magnetic bead, Immunoassay, B7-1 Antigen, CD80

Abstract

Background: To detect concentrations of subtherapeutic doses of the CD80-Fc fusion protein FPT155 in serum in Phase I studies, a highly sensitive assay was developed. Materials & methods: FPT155 was purified from human serum using magnetic beads coupled to cytotoxic T-lymphocyte-associated antigen-4. After washing away the serum components, FTP155 was released by acid dissociation and neutralization. The eluted drug was quantified in an ELISA using cytotoxic T-lymphocyte-associated antigen-4 as a capture reagent and biotinylated anti-human Fc for detection. The assay was validated with a calibration range of 5–40 ng/ml and a dilutional integrity of up to 100,000 ng/ml. Conclusion: A highly sensitive assay to determine serum concentrations of FPT155 using readily available reagents was developed. The results were in conformity with theoretical calculations.

Published

2021

39. Development of a nano-luciferase based assay to measure the binding of SARS-CoV-2 spike receptor binding domain to ACE-2

Author

Mark A. Skidmore, Alan Richardson, Farhat L. Khanim, and Marcelo A. Lima

Subjects

0301 basic medicine, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Biophysics, ACE2, medicine.disease_cause, Antiviral Agents, Biochemistry, Article, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, HiBIT tag, medicine, Humans, Nanotechnology, Luciferase, Secretion, Luciferases, Receptor, Molecular Biology, Binding assay, Mutation, Binding Sites, SARS-CoV-2, Chemistry, Ligand binding assay, COVID-19, Cell Biology, R1, Nano-luciferase, COVID-19 Drug Treatment, Cell biology, Fc fusion, 030104 developmental biology, 030220 oncology & carcinogenesis, Spike Glycoprotein, Coronavirus, Angiotensin-converting enzyme 2, Receptors, Virus, Angiotensin-Converting Enzyme 2, hormones, hormone substitutes, and hormone antagonists, QD415, Protein Binding

Abstract

To identify drugs that could potentially be used to treat infection with SARS-CoV-2, a high throughput 384-well assay was developed to measure the binding of the receptor binding domain (RBD) of the viral S1 protein to its main receptor, angiotensin converting enzyme 2 (ACE2). The RBD was fused to both a HiBIT tag and an IL6 secretion signal to enable facile collection from the cell culture media. The addition of culture media containing this protein, termed HiBIT-RBD, to cells expressing ACE2 led to binding that was specific to ACE2 and both time and concentration dependant, Binding could be inhibited by both RBD expressed in E. coli and by a full length S1 - Fc fusion protein (Fc-fused S1) expressed in eukaryotic cells. The mutation of residues that are known to play a role in the interaction of RBD with ACE2 also reduced binding. This assay may be used to identify drugs which inhibit the viral uptake into cells mediated by binding to ACE2., Graphical abstract Image 1, Highlights 1.A high-throughput, 384-well plate assay was developed to measure the binding S1 RBD to ACE2; 2.HiBIT-RBD binds to cells expressing ACE2 specifically and in a time dependant fashion; 3.The binding of HiBIT-RBD to ACE2 can be inhibited using recombinantly expressed SARS-CoV-2 RBD and full-length, Spike S1; 4.Site specific mutations within the RBD demonstrate the specificity of this assay.

Published

2021

40. Outcome of Clinical Trials with New Extended Half-Life FVIII/IX Concentrates.

Author

Mancuso, Maria Elisa and Santagostino, Elena

Subjects

*CLINICAL trials, *HEMOPHILIA treatment, *PHARMACOKINETICS, *POLYETHYLENE glycol, *FEASIBILITY studies

Abstract

The development of a new generation of coagulation factors with improved pharmacokinetic profile will change the paradigm of treatment of persons with hemophilia (PWH). The standard treatment in PWH is represented by regular long-term prophylaxis that, given intravenously twice or thrice weekly, is associated with a not-negligible burden on patients' quality of life. The availability of drugs with improved pharmacokinetic profile may improve prophylaxis feasibility and protection against bleeding episodes. This article summarizes the main results obtained from clinical trials with modified factor VIII (FVIII) and factor IX (FIX) molecules. Published literature on new molecules for replacement treatment in hemophilia A and B was retrieved using PubMed search, and all ongoing clinical trials have been researched via www.clinicaltrials.gov. Such new molecules are usually engineered to have a longer plasma half-life than that which has been obtained by chemical modification (i.e., conjugation with polyethylene glycol, PEG) or by creating recombinant fusion proteins. Results from phase I/III studies in previously treated adults and children are now available for the vast majority of new products, including the results of their use in a surgical setting. On the contrary, trials involving previously untreated patients are still ongoing for all and results not yet available. [ABSTRACT FROM AUTHOR]

Published

2017

41. Single chain Fc-dimer-human growth hormone fusion protein for improved drug delivery.

Author

Zhou, Li, Wang, Hsuan-Yao, Tong, Shanshan, Okamoto, Curtis T., Shen, Wei-Chiang, and Zaro, Jennica L.

Subjects

*HUMAN growth hormone, *DRUG delivery systems, *FC receptors, *CHIMERIC proteins, *DRUG design, *PHARMACOKINETICS, *BIOACTIVE compounds

Abstract

Fc fusion protein technology has been successfully used to generate long-acting forms of several protein therapeutics. In this study, a novel Fc-based drug carrier, single chain Fc-dimer (sc(Fc) 2 ), was designed to contain two Fc domains recombinantly linked via a flexible linker. Since the Fc dimeric structure is maintained through the flexible linker, the hinge region was omitted to further stabilize it against proteolysis and reduce FcγR-related effector functions. The resultant sc(Fc) 2 candidate preserved the neonatal Fc receptor (FcRn) binding. sc(Fc) 2 -mediated delivery was then evaluated using a therapeutic protein with a short plasma half-life, human growth hormone (hGH), as the protein drug cargo. This novel carrier protein showed a prolonged in vivo half-life and increased hGH-mediated bioactivity compared to the traditional Fc-based drug carrier. sc(Fc) 2 technology has the potential to greatly advance and expand the use of Fc-technology for improving the pharmacokinetics and bioactivity of protein therapeutics. [ABSTRACT FROM AUTHOR]

Published

2017

42. Feasibility and outcomes of low‐dose and low‐frequency prophylaxis with recombinant extended half‐life products (Fc‐rFVIII and Fc‐rFIX) in Ivorian children with hemophilia: Two‐year experience in the setting of World Federation of Haemophilia humanitarian aid programme

Author

Ibrahima Sanogo, Sébastien Lobet, Catherine Lambert, Cedric Hermans, and N'Dogomo Meité

Subjects

Male, Pediatrics, medicine.medical_specialty, Haemophilia A, 030204 cardiovascular system & hematology, Hemophilia A, Haemophilia, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, medicine, Humans, Joint bleeding, Child, Genetics (clinical), Clotting factor, Factor VIII, Humanitarian aid, business.industry, Low dose, Hematology, General Medicine, Relief Work, medicine.disease, Fc fusion, Regimen, Child, Preschool, Feasibility Studies, business, Half-Life, 030215 immunology

Abstract

Introduction In sub-Saharan Africa, access to clotting factor concentrates (CFCs) is often extremely limited and published data on people with haemophilia on prophylaxis are almost not existent. Aims and methods To assess the feasibility, barriers and outcomes of a low-dose and low-frequency prophylaxis with extended half-life (EHL) recombinant Fc fusion FVIII and FIX in Ivorian children on a two-year period in the setting of the World Federation of Hemophilia's (WFH) humanitarian aid programme. Results Twenty-five boys with haemophilia were included. Mean (SD) age at inclusion was 5.6 (2.5) years. The median [range] follow-up duration was 17 [11-24] months. Regimen of prophylaxis was 20 IU kg-1 1×/week in haemophilia A and every 10 days in haemophilia B. We observed a maximal reduction by 87.6% of the annual spontaneous joint bleeding rate and a slight decrease in the total HJHS scores (p = .047). Adherence problems related to parents' low education level and shortage in CFCs were the main issues to carry out the programme. Inhibitors occurred in 12.5%. Conclusion This study confirms the feasibility and efficacy of low-dose and low-frequency prophylaxis in young Ivorian children with haemophilia treated with EHL CFCs donated through the WFH humanitarian aid programme. This work also highlights the crucial role of adherence and the need for appropriate education to achieve prophylaxis. Finally, it reminds the paramount objective of achieving self-sufficient, sustainable and available haemophilia replacement therapy for all worldwide.

Published

2020

43. Real‐world data of immune tolerance induction using recombinant factor VIII Fc fusion protein in patients with severe haemophilia A with inhibitors at high risk for immune tolerance induction failure: A follow‐up retrospective analysis

Author

Victoria Price, Haowei Linda Sun, Nisha Jain, Elisa Tsao, Jennifer A. Dumont, Janice M. Staber, Hilda Ding, Manuel Carcao, Zahra Al-Khateeb, Mark Belletrutti, Sanjay P Ahuja, MacGregor Steele, Steven W. Pipe, Amy D. Shapiro, Michael Wang, Jing Feng, Nina Hwang, and Kenneth Lieuw

Subjects

Haemophilia A, MEDLINE, recombinant factor VIII Fc fusion protein, haemophilia A, Hemophilia A, Recombinant factor viii, Immune tolerance, Retrospective analysis, Immune Tolerance, Medicine, Humans, In patient, Letter to the Editor, Genetics (clinical), Retrospective Studies, immune tolerance induction, Factor VIII, business.industry, Hematology, General Medicine, medicine.disease, rescue therapy, inhibitor, Fc fusion, Immunology, retrospective chart review, Severe haemophilia A, business, Follow-Up Studies

Published

2020

44. Real‐world data demonstrate improved bleed control and extended dosing intervals for patients with haemophilia B after switching to recombinant factor IX Fc fusion protein (rFIXFc) for up to 5 years

Author

Christopher Barnowski, Miguel A. Escobar, Amy D. Shapiro, Doris Quon, Ateefa Chaudhury, Nisha Jain, Michael Wang, Elisa Tsao, and Jing Feng

Subjects

Adult, Male, medicine.medical_specialty, Time Factors, Adolescent, Recombinant Fusion Proteins, Hemorrhage, haemophilia B, 030204 cardiovascular system & hematology, Haemophilia, Hemophilia B, Factor IX, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Internal medicine, medicine, Humans, Haemophilia B, Dosing, Clinical Haemophilia, Child, Genetics (clinical), extended half‐life factor, Aged, Retrospective Studies, business.industry, prolonged factor IX activity, Hematology, General Medicine, Original Articles, Bleed, Middle Aged, medicine.disease, Immunoglobulin Fc Fragments, Clinical trial, Fc fusion, rFIXFc, Child, Preschool, Original Article, factor IX switching, Female, business, Real world data, 030215 immunology, Recombinant factor IX

Abstract

Introduction In clinical trials, recombinant factor IX fusion protein (rFIXFc) has demonstrated safety, efficacy and prolonged activity with extended dosing intervals for treatment of haemophilia B. Aim To assess the real-world clinical utility of rFIXFc in a variable patient population and routine clinical practice. Methods A multicentre, retrospective chart review was conducted of patients with haemophilia B who had received rFIXFc prophylaxis or on-demand treatment for ≥6 months across six sites in the United States. Results Sixty-four eligible patients were identified who had a median (range) duration on rFIXFc of 2.7 (0.5-5.0) years. Of 32 patients on rFIXFc prophylaxis who switched from prophylaxis with another factor treatment (ie pre-rFIXFc) and had a known pre-rFIXFc dosing interval, the initial dosing interval was lengthened for 26 (81%) patients and maintained for the remaining 6 (19%) patients. Most (n = 48 [91%]) patients who received rFIXFc prophylaxis from the beginning to the end of the chart review period (n = 53) maintained or lengthened the dosing interval from first through last dose of rFIXFc. For patients receiving rFIXFc prophylaxis, there was an approximate 50% reduction in weekly factor consumption compared with pre-rFIXFc prophylaxis. Overall annualized bleed rates, annualized spontaneous bleed rates and annualized joint bleed rates decreased after switching to rFIXFc prophylaxis (n = 24 with bleed data). Compliance to recommended treatment improved or remained stable in most patients with available data (30/31). Conclusion Recombinant factor IX fusion protein prophylaxis improved bleed control, reduced overall consumption, reduced frequency of infusion and improved compliance for patients with haemophilia B in a real-world setting.

Published

2020

45. Signal Peptide Optimization to Prevent N-terminal Truncation of Glucagon Like Peptide-1/IgG-Fc Fusion Protein

Author

Suqin Song, Suzhen Wei, Cao Chunlai, Yongjie Lai, Xukun Xu, and Jing Li

Subjects

Signal peptide, Agonist, endocrine system, 010405 organic chemistry, Chemistry, medicine.drug_class, Chinese hamster ovary cell, digestive, oral, and skin physiology, Bioengineering, 01 natural sciences, Biochemistry, Fusion protein, Glucagon-like peptide-1, Molecular biology, Glucagon, 0104 chemical sciences, Analytical Chemistry, Fc fusion, Drug Discovery, medicine, Molecular Medicine, Dulaglutide, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

Dulaglutide (glucagon like peptide-1/IgG-Fc fusion protein, GLP-1-Fc) is a long lasting GLP-1 agonist, which consists of two arms of GLP-1 moieties fused to IgG Fc fragment. Dulaglutide is a safe and effective medication for type 2 diabetes. In an attempt to develop a biosimilar version of dulaglutide, we found that up to 75% of GLP-1-Fc displayed N-terminal truncations in one or both GLP-1 arms. We proposed that the N-terminal heterogeneity was caused by mis-cleavage of signal peptide and solved this problem through signal peptide optimization. Murine immunoglobulin kappa light chain signal peptide (KASP) significantly improves GLP-1-Fc N-terminal integrity and homogeneity. 92.8–95.7% of GLP-1-Fc molecules directed by KASP contain intact N-terminus. The productivity of GLP-1-Fc could reach 2.2 g/L in shaking flask fed batch culture. KASP is an optimal signal peptide for GLP-1-Fc expression in Chinese hamster ovary (CHO) cells.

Published

2020

46. QL0902, a proposed etanercept biosimilar: pharmacokinetic and immunogenicity profile to its reference product in healthy Chinese male subjects

Author

Zhijun Huang, Shuang Yang, Chang Cui, Saqib Ali, Zeyu Zhang, Guoping Yang, Jie Huang, and Yun Zeng

Subjects

Male, 0301 basic medicine, China, Clinical Biochemistry, Pharmacology, Etanercept, law.invention, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, law, Drug Discovery, medicine, Humans, Receptor, Biosimilar Pharmaceuticals, Cross-Over Studies, business.industry, Immunogenicity, Biosimilar, Healthy Volunteers, Fc fusion, Reference product, 030104 developmental biology, Therapeutic Equivalency, 030220 oncology & carcinogenesis, Recombinant DNA, business, medicine.drug

Abstract

Objectives: To study the pharmacokinetics, safety and immunogenicity of Recombinant Human Tumor Necrosis Factor-α Receptor II: IgG Fc Fusion Protein for Injection (QL0902) and evaluate the pharmaco...

Published

2020

47. Recombinant factor VIII Fc fusion protein for the treatment of severe haemophilia A: Final results from the ASPIRE extension study

Author

Bent Winding, Keiji Nogami, Guy Young, Chris Barnes, Huixing Yuan, Johannes Oldenburg, Elena Santagostino, Liane Khoo, Beatrice Nolan, Barbara A. Konkle, Joachim Fruebis, K. John Pasi, Ingrid Pabinger, Dan Rudin, and Johnny Mahlangu

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Recombinant Fusion Proteins, 030204 cardiovascular system & hematology, Haemophilia, Hemophilia A, Recombinant factor viii, bleed rate, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Internal medicine, medicine, Clinical endpoint, Humans, Clinical Haemophilia, Child, Genetics (clinical), rFVIIIFc, Aged, extended half‐life, Factor VIII, business.industry, Hematology, General Medicine, Original Articles, Bleed, Middle Aged, medicine.disease, Confidence interval, Immunoglobulin Fc Fragments, Regimen, Fc fusion, Treatment Outcome, individualized prophylaxis, Child, Preschool, Severe haemophilia A, Original Article, Female, business, perioperative haemostasis, 030215 immunology

Abstract

Introduction The efficacy and safety of recombinant factor VIII Fc fusion protein (rFVIIIFc) as an extended half‐life treatment for severe haemophilia A were demonstrated in the Phase 3 A‐LONG and Kids A‐LONG studies. Eligible subjects who completed A‐LONG and Kids A‐LONG could enrol in ASPIRE (NCT01454739), an open‐label extension study. Aim To report the long‐term safety and efficacy of rFVIIIFc in subjects with severe haemophilia A who enrolled in ASPIRE. Methods Previously treated subjects received one or more of the following regimens: individualized prophylaxis (IP), weekly prophylaxis, modified prophylaxis or episodic treatment. Subjects could switch treatment regimen at any time. The primary endpoint was inhibitor development. Results A total of 150 subjects from A‐LONG and 61 subjects from Kids A‐LONG enrolled in ASPIRE. Most subjects received the IP regimen (A‐LONG: n = 110; Kids A‐LONG: n = 59). Median (range) treatment duration in ASPIRE for subjects from A‐LONG and Kids A‐LONG was 3.9 (0.1‐5.3) years and 3.2 (0.3‐3.9) years, respectively. No inhibitors were observed (0 per 1000 subject‐years; 95% confidence interval, 0‐5.2) and the overall rFVIIIFc safety profile was consistent with prior studies. For subjects on the IP regimen, annualized bleed rates (ABR) remained low (median overall ABR for adults and adolescents was

Published

2020

48. Is Low Dose a New Dose to Initiate Hemophilia A Prophylaxis? – A Systematic Study in Eastern India

Author

Abhijit Phukan, Rajib De, Shazia Gulshan, Prantar Chakrabarti, Tuphan Kanti Dolai, Shuvraneel Baul, and Prakas Kumar Mandal

Subjects

Pediatrics, medicine.medical_specialty, business.industry, Cost-Benefit Analysis, Low dose, India, Hemorrhage, School absenteeism, Hemophilia A, Severe hemophilia A, Eastern india, Activity participation, 03 medical and health sciences, Fc fusion, 0302 clinical medicine, Long acting, 030225 pediatrics, Hemarthrosis, Pediatrics, Perinatology and Child Health, medicine, Humans, Health score, Child, business, 030217 neurology & neurosurgery

Abstract

To investigate the effectiveness of low dose secondary/tertiary prophylaxis in severe Hemophilia A children and determine improvements in their daily life. Thirty Hemophilia A children (≤ 12 y) with factor VIII

Published

2020

49. rFIXFc prophylaxis improves pain and levels of physical activity in haemophilia B: Post hoc analysis of B-LONG using haemophilia-specific quality of life questionnaires

Author

Jan Astermark, Cédric Hermans, Elena Santagostino, Samuel Aballéa, Monia Ezzalfani, Jameel Nazir, Zalmai Hakimi, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Centre de malformations vasculaires congénitales, and UCL - (SLuc) Service d'hématologie

Subjects

Adult, medicine.medical_specialty, Adolescent, Population, Physical activity, Pain, physical activity, haemophilia B, Haemophilia, Hemophilia A, Hemophilia B, patient reported outcomes measures, McNemar's test, Quality of life, Internal medicine, Surveys and Questionnaires, Post-hoc analysis, medicine, Humans, Haemophilia B, education, Exercise, Genetics (clinical), education.field_of_study, quality of Life, factor IX, business.industry, Hematology, General Medicine, medicine.disease, Fc fusion, Quality of Life, rFIXFc protein, business

Abstract

INTRODUCTION: Recurrent bleeding in severe haemophilia B causes painful hemarthroses and reduces capacity for physical activity. Recombinant factor IX Fc fusion protein (rFIXFc) prophylaxis results in low annualised bleeding rates, with the potential to improve patients' health-related quality of life (HRQoL). AIM: To present a post hoc analysis of data from B-LONG describing change over time in patient-reported outcomes associated with pain and physical activity. METHODS: Patients (≥12 years) who received weekly dose-adjusted or interval-adjusted rFIXFc prophylaxis and completed the Haemophilia-Specific QoL questionnaire for adolescents (Haemo-QoL) or adults (Haem-A-QoL) at baseline (BL) and end of study (EoS). Individual level changes in items of the 'Physical Health' and 'Sports and Leisure' domains, categorised as 'never/rarely/seldom' or 'sometimes/often/all the time', were analysed using McNemar's test to compare distribution of responses at EoS versus BL. RESULTS: At EoS versus BL, a significantly greater proportion of patients did not experience painful swellings (64% vs. 44%; P = .004), painful joints (44% vs. 28%; P = .003) or pain when moving (54% vs. 41%; P = .026). Additionally, at EoS versus BL, patients were less likely to avoid participating in sports like football (30% vs. 8%; P = .002), avoid sports due to their haemophilia (47% vs. 27%; P = .007), or experience difficulty walking as far as they wanted (63% vs. 43%; P = .001). The proportion of patients who played sports as much as the general population was numerically increased (52% vs. 37%; P = .033) at EoS versus BL. CONCLUSION: Results of the analysis suggest that over time, rFIXFc prophylaxis is associated with significant improvements in pain and physical functioning. This contributes to previous evidence of overall HRQoL improvements in patients with haemophilia B treated with rFIXFc.

Published

2022

50. Recombinant Factor VIII Fc Fusion Protein (rFVIIIFc) in Real Life: One-Year Clinical and Economic Outcomes

Author

Martine Roche, Romain Giraud, Manon Roche, Hervé Chambost, Céline Falaise, Nicolas Delmotte, Sophie Gensollen, Hôpital de la Conception [CHU - APHM] (LA CONCEPTION), Centre Régional de Traitement de l'Hémophilie, Centre recherche en CardioVasculaire et Nutrition = Center for CardioVascular and Nutrition research (C2VN), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Assistance Publique - Hôpitaux de Marseille (APHM), Institut de Chimie Radicalaire (ICR), and Aix Marseille Université (AMU)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Clotting factor, medicine.medical_specialty, business.industry, [SDV]Life Sciences [q-bio], 030226 pharmacology & pharmacy, Recombinant factor viii, 03 medical and health sciences, Fc fusion, Regimen, 0302 clinical medicine, Pharmacotherapy, Internal medicine, Weekly dose, medicine, In real life, Pharmacology (medical), In patient, 030212 general & internal medicine, Original Research Article, business

Abstract

International audience; Background: Recombinant factor VIII Fc fusion protein (rFVIIIFc) is the first extended half-life (EHL) recombinant clotting factor with marketing authorization; it has been available in France since October 2016. However, data and literature about rFVIIIFc in clinical practice are scarce.Objective: We propose a 1-year clinical and economic outcome evaluation in patients with hemophilia A taking into consideration treatment adherence.Patients and methods: We reviewed the diaries of all patients treated with rFVIIIFc at Marseille Hemophilia Center for 1 year. All the data were related to the patients' infusion (i.e., annual number of infusions, weekly dose/kg, and annual consumption) and bleeding reports. The clotting factor costs were considered, whereas additional costs (e.g., infusion devices and nurse intervention) were neglected.Results: A total of 34 patients were evaluated. Their median age was 18 years (IQR = 18). Treatment adherence was observed in 62% for FVIII and 66% for rFVIIIFc. The analysis revealed a negligible decrease in the annual clotting factor consumption following the switch (- 2%, p = 0.7339). These data were combined with a significant reduction in the annual number of infusion (- 22.5%, median = 138.5, IQR = 65.8 for FVIII; median = 105, IQR = 24 for rFVIIIFc, p < 0.0001) and bleeding (- 50%, median = 5, IQR = 7.5 for FVIII; median = 1, IQR = 4 for rFVIIIFc, p < 0.0001). With regard to the cost, a decreasing trend was observed (- 8%, p = 0.1300).Conclusion: The analysis in a real-life setting revealed that the input of switches toward rFVIIIFc in different treatment (age of patients and regimen) patterns seems to corroborate previous studies. The results suggest that switches have a beneficial effect in terms of efficacy, clotting factor consumption, and cost.

Published

2021