Your search keyword '"Fc fragment"' showing total 381 results

1. Binding to the neonatal Fc receptor enhances the pathogenicity of antidesmoglein-3 antibodies in keratinocytes.

Author

Zakrzewicz, Anna, Vanderheyden, Katrien, Galaly, Yad, Feldhoff, Simon, Sips, Magdalena, Brinkhaus, Maximilian, and Tikkanen, Ritva

Subjects

RECOMBINANT antibodies, FC receptors, EPITHELIAL cells, PEMPHIGUS vulgaris, AUTOANTIBODIES

Abstract

The neonatal Fc receptor (FcRn) is important for numerous cellular processes that involve antibody recycling and trafficking. A major function of FcRn is IgG recycling and half-life prolongation, and FcRn blockade results in a reduction of autoantibodies in IgG-mediated autoimmune diseases. In epithelial cells, FcRn functions in processes different from IgG recycling, such as antibody transcytosis in intestinal cells. In pemphigus vulgaris, an autoimmune disease of the epidermis, IgG autoantibodies directed against desmosomal adhesion proteins, especially desmoglein-3 and -1, cause loss of keratinocyte adhesion. We have previously demonstrated that FcRn blockade with efgartigimod, a human Fc fragment with enhanced FcRn binding, significantly reduces the keratinocyte monolayer fragmentation caused by anti-desmoglein-3 antibodies. This points to a direct function of FcRn in keratinocytes, beyond IgG recycling, but the mechanisms have not yet been elucidated in detail. Here, we show that FcRn binding is required for the full pathogenicity of recombinant anti-desmoglein-3 antibodies in keratinocytes, and that antibodies that exhibit enhanced or reduced FcRn affinity due to targeted substitutions in their Fc region, as well as F(ab')2 fragments not binding to FcRn display different degrees of pathogenicity. Blockade of FcRn by efgartigimod only shows a protective effect on keratinocyte adhesion against antibodies capable of binding to FcRn. Furthermore, antibody-induced degradation of desmoglein-3 in keratinocytes does not depend on FcRn, demonstrating that desmoglein-3 degradation and acantholysis are functionally disconnected processes. Our data suggest that the role of FcRn in autoimmune diseases is likely to be versatile and cell-type dependent, thus stressing the importance of further studies on FcRn function in autoimmune diseases. [ABSTRACT FROM AUTHOR]

Published

2024

2. Binding to the neonatal Fc receptor enhances the pathogenicity of anti-desmoglein-3 antibodies in keratinocytes

Author

Anna Zakrzewicz, Katrien Vanderheyden, Yad Galaly, Simon Feldhoff, Magdalena Sips, Maximilian Brinkhaus, and Ritva Tikkanen

Subjects

autoimmune diseases, autoantibodies, bullous skin diseases, pemphigus, neonatal Fc receptor, Fc fragment, Immunologic diseases. Allergy, RC581-607

Abstract

The neonatal Fc receptor (FcRn) is important for numerous cellular processes that involve antibody recycling and trafficking. A major function of FcRn is IgG recycling and half-life prolongation, and FcRn blockade results in a reduction of autoantibodies in IgG-mediated autoimmune diseases. In epithelial cells, FcRn functions in processes different from IgG recycling, such as antibody transcytosis in intestinal cells. In pemphigus vulgaris, an autoimmune disease of the epidermis, IgG autoantibodies directed against desmosomal adhesion proteins, especially desmoglein-3 and -1, cause loss of keratinocyte adhesion. We have previously demonstrated that FcRn blockade with efgartigimod, a human Fc fragment with enhanced FcRn binding, significantly reduces the keratinocyte monolayer fragmentation caused by anti-desmoglein-3 antibodies. This points to a direct function of FcRn in keratinocytes, beyond IgG recycling, but the mechanisms have not yet been elucidated in detail. Here, we show that FcRn binding is required for the full pathogenicity of recombinant anti-desmoglein-3 antibodies in keratinocytes, and that antibodies that exhibit enhanced or reduced FcRn affinity due to targeted substitutions in their Fc region, as well as F(ab’)2 fragments not binding to FcRn display different degrees of pathogenicity. Blockade of FcRn by efgartigimod only shows a protective effect on keratinocyte adhesion against antibodies capable of binding to FcRn. Furthermore, antibody-induced degradation of desmoglein-3 in keratinocytes does not depend on FcRn, demonstrating that desmoglein-3 degradation and acantholysis are functionally disconnected processes. Our data suggest that the role of FcRn in autoimmune diseases is likely to be versatile and cell-type dependent, thus stressing the importance of further studies on FcRn function in autoimmune diseases.

Published

2024

3. A fusion protein of vimentin with Fc fragment inhibits Japanese encephalitis virus replication.

Author

Taoping Zhang, Zhixin Chen, Lyu Xie, Ruixian Xu, Lu Chen, Ting Jia, Wengang Shi, Yongbo Wang, Yuzhu Song, Qinqin Han, Xueshan Xia, Tao Yuan, and Jinyang Zhang

Subjects

JAPANESE encephalitis viruses, CHIMERIC proteins, VIMENTIN, VIRAL replication, VIRAL proteins, VIRAL envelope proteins

Abstract

Japanese encephalitis virus (JEV), a member of the Flaviviridae family and a flavivirus, is known to induce acute encephalitis. Vimentin protein has been identified as a potential receptor for JEV, engaging in interactions with the viral membrane protein. The Fc fragment, an integral constituent of immunoglobulins, plays a crucial role in antigen recognition by dendritic cells (DCs) or phagocytes, leading to subsequent antigen presentation, cytotoxicity, or phagocytosis. In this study, we fused the receptor of JEV vimentin with the Fc fragment of IgG and expressed the resulting vimentin-Fc fusion protein in Escherichia coli. Pulldown experiments demonstrated the binding ability of the vimentin-Fc fusion protein to JEV virion in vitro. Additionally, we conducted inhibition assays at the cellular level, revealing the ability of vimentin-Fc protein suppressing JEV replication, it may be a promising passive immunotherapy agent for JEV. These findings pave the way for potential therapeutic strategies against JEV. [ABSTRACT FROM AUTHOR]

Published

2024

4. Application of a Novel Aptamer Beacon for Rapid Detection of IgG1 Antibody Drugs.

Author

Yang, Ke, Zheng, Wei-Wei, Huang, Xiu-Song, Chen, Kai-Ming, and Duan, Cai-Wen

Abstract

Antibody drugs have been widely used to treat many diseases and are the fastest-growing drug class. IgG1 is the most common type of antibody because of its good serum stability; however, effective methods for the rapid detection of IgG1-type antibodies are lacking. In this study, we designed two aptamer molecules derived from the reported aptamer probe that has been proven to bind to the Fc fragment of the IgG1 antibody. The results showed that Fc-1S could specifically bind to the human IgG1 Fc proteins. In addition, we modified the structure of Fc-1S and constructed three aptamer molecular beacons that could quantitatively detect IgG1-type antibodies within a short time. Furthermore, we unveiled that the Fc-1S37R beacon has the highest sensitivity for IgG1-type antibodies with a detection limit of 48.82813 ng/mL and can accurately detect serum antibody concentrations in vivo with consistent results to ELISA. Therefore, Fc-1S37R is an efficient method for the production monitoring and quality control of IgG1-type antibodies to enable the large-scale production and application of antibody drugs. [ABSTRACT FROM AUTHOR]

Published

2023

5. Antibody glycosylation in autoimmune diseases

Author

Zhou, Xing, Motta, Francesca, Selmi, Carlo, Ridgway, William M, Gershwin, M Eric, and Zhang, Weici

Subjects

Biomedical and Clinical Sciences, Immunology, Autoimmune Disease, Arthritis, Lupus, Digestive Diseases, Inflammatory and immune system, Good Health and Well Being, Arthritis, Rheumatoid, Autoimmune Diseases, Autoimmunity, Glycosylation, Humans, Lupus Erythematosus, Systemic, Antibody, Inflammation, Fc fragment, Clinical sciences

Abstract

The glycosylation of the fragment crystallizable (Fc) region of immunoglobulins (Ig) is critical for the modulation of antibody effects on inflammation. Moreover, antibody glycosylation may induce pathologic modifications and ultimately contribute to the development of autoimmune diseases. Thanks to progress in the analysis of glycosylation, more data are available on IgG and its subclass structures in the context of autoimmune diseases. In this review, we focused on the impact of Ig glycosylation in autoimmunity, describing how it modulates the immune response and how glycome profiles can be used as biomarkers of disease activity. The analysis of antibody glycosylation demonstrated specific features in human autoimmune and chronic inflammatory conditions, including rheumatoid arthritis, systemic lupus erythematosus, inflammatory bowel disease and autoimmune liver diseases, among others. Within the same disease, different patterns are associated with disease severity and treatment options. Future research may increase the information available on the distinct glycome profiles and expand their potential role as biomarkers and as targets for treatment, ultimately favoring an individualized approach.

Published

2021

6. Development of the method for determinating ADCC biological activity of IVIG

Author

Liyuan ZHU, Qing LIU, Li MA, and Changqing LI

Subjects

human immunoglobulin (ph4)for intravenous injection, fc fragment, antibody-dependent cell-mediated cytotoxicity, biological activity, Diseases of the blood and blood-forming organs, RC633-647.5, Medicine

Abstract

Objective To establish a method for determinating the antigen-dependent cell-mediated cytotoxicity (ADCC) of human immunoglobulin (pH4)for intravenous injection (IVIG) on luciferase reporter gene-modified cell assay. Methods As effector cells, Jurkat-NFAT-Luc-CD16 cells were used in the assay, and PLC/PRF/5 cells were used as target cells. After incubation of effector cells and target cells with IVIG, the method for determinating ADCC biological activity of IVIG was established by detecting luciferase released by activated T nuclear factor after binding of IVIG Fc fragment to effector cells. Meanwhile, the experimental assay conditions were optimized, and the methodology was verified subsequently. Results IVIG had a dose-response relationship in this method, which was consistent with four parameter logistic model. And the PLC/PRF/5 cells were finally determined as the target cells. The initial dilution concentration of antibody was 20 mg/mL, and the ratio dilution was 1∶2, and the effector to target ratio was 1∶3, and co-incubation time of two cells and IVIG was 24 hours. Within-run and between-run analysis including three independent tests, initial working concentration relative light unit (RLU) and the relative standard deviation (RSD) of the concentration for 50% of maximal effect(EC50) were less than 11%. The relative titers of the recovery samples of the two different dilution groups were (23.50±1.69)% and (49.30±2.97)%, respectively, and the corresponding recovery rates were (93.50±6.30)% and (96.24±5.43)%, respectively, with RSD less than 11%. Conclusion The method for determinating ADCC biological activity of IVIG based on luciferase reporter gene-modified cell assay was successfully established. It could be applied in determinating the ADCC biological activity of IVIG, and has the advantages of satisfactory linearity, accuracy, precision and specificity.

Published

2023

7. Effect of IgG fragments in IVIG(pH4)on phagocytosis of sensitized erythrocytes by macrophage

Author

Liyuan ZHU, Wei ZHANG, Mingxia HOU, Qin LIU, Yuyan QIN, Li Ma, and Changqing LI

Subjects

human immunoglobulin (ph4)for intravenous injection, fc fragment, thp-1 cells, phagocytosis, Diseases of the blood and blood-forming organs, RC633-647.5, Medicine

Abstract

Objective To research the effect of the Fc, Fab and F(ab′)2 fragments of immunoglobulin G, the main components of Human Immunoglobulin(pH4) for Intravenous Injection(IVIG), on the phagocytic function of macrophages derived from THP-1 cells. Methods First of all, IVIG was digested with papain and pepsin to obtain Fc, Fab and F(ab′)2, and these components were then identified by sodium dodecyl sulfate polyacrylamide gel electrophoresis (SDS-PAGE). Afterwards, propylene glycol monomethyl ether acetate (PMA) was used to induce THP-1 cells to differentiate into M0 macrophages. Finally, the sensitized erythrocytes were labeled with carboxy fluorescein succinimidyl ester (CFSE), and the effect of the above components on the phagocytic ability of M0 macrophages to engulf sensitized erythrocytes was detected by flow cytometry. Results The identification results of SDS-PAGE showed that the prepared IgG fragments met the requirements of subsequent experiments. Flow cytometry performs showed that the phagocytosis model of M0 macrophages had been successfully established. When the concentration of Fc increased from 0.1μg/ mL to 10μg/ mL, the phagocytosis rate of erythrocytes sensitized by M0 macrophages decreased from (24.21±0.58) % to (12.27±0.19) %. When the concentration of IVIG protein increased from 0.1 μg/ml to 10 μg/ml, the phagocytosis rate decreased from (20.57±0.39) % to (0.20±0.03) %. Meanwhile, at the same protein concentration (10 μg/ml), the inhibitory effect of Fc on phagocytosis was only half that of IVIG. In addition, Fab, F(ab′)2, and human serum albumin could not inhibit phagocytosis of M0 macrophages. Conclusion IVIG can effectively inhibit the phagocytosis of THP-1 derived M0 macrophages, which is mainly dependent on the Fc, but not related to the Fab of IgG and F (ab′)2.

Published

2022

8. A nano-innate immune system activator for cancer therapy in a 4T1 tumor-bearing mouse model

Author

Xiang-Yu Liu, Mao-Hua Zhu, Xiao-Yu Wang, Xiao Dong, Hai-Jun Liu, Rui-Yang Li, Shi-Chong Jia, Qin Lu, Mei Zhao, Peng Sun, Hong-Zhuan Chen, and Chao Fang

Subjects

Nanoparticles, Innate immune system, Fc fragment, Immunotherapy, Breast cancer, Biotechnology, TP248.13-248.65, Medical technology, R855-855.5

Abstract

Abstract Background Harnessing the immune system to fight cancer has led to prominent clinical successes. Strategies to stimulate innate immune effectors are attracting considerable interest in cancer therapy. Here, through conjugating multivalent Fc fragments onto the surface of mesoporous silica nanoparticles (MSN), we developed a nanoparticle-based innate immune system activator (NISA) for breast cancer immunotherapy. Methods NISA was prepared through conjugating mouse IgG3 Fc to MSN surface. Then, long-chain PEG5000, which was used to shield Fc to confer nanoparticle colloidal stability, was linked to the MSN surface via matrix metalloprotease-2 (MMP-2)-cleavable peptide (GPLGIAGQC). The activation of multiple components of innate immune system, including complement and the innate cells (macrophages and dendritic cells) and the associated anticancer effect were investigated. Results Fc fragments of NISA can be exposed through hydrolysis of long-chain PEG5000 by highly expressed MMP-2 in tumor microenvironment. Then, effective stimulation and activation of multiple components of innate immune system, including complement, macrophages, and dendritic cells were obtained, leading to efficient antitumor effect in 4T1 breast cancer cells and orthotopic breast tumor model in mice. Conclusions The antitumor potency conferred by NISA highlights the significance of stimulating multiple innate immune elements in cancer immunotherapy. Graphical Abstract

Published

2022

9. Binding to the neonatal Fc receptor enhances the pathogenicity of anti-desmoglein-3 antibodies in keratinocytes.

Author

Zakrzewicz A, Vanderheyden K, Galaly Y, Feldhoff S, Sips M, Brinkhaus M, and Tikkanen R

Subjects

Humans, Animals, Protein Binding, Immunoglobulin G immunology, Immunoglobulin G metabolism, Mice, Cell Adhesion immunology, Keratinocytes immunology, Keratinocytes metabolism, Receptors, Fc metabolism, Receptors, Fc immunology, Histocompatibility Antigens Class I immunology, Histocompatibility Antigens Class I metabolism, Desmoglein 3 immunology, Desmoglein 3 metabolism, Autoantibodies immunology, Pemphigus immunology, Pemphigus metabolism

Abstract

The neonatal Fc receptor (FcRn) is important for numerous cellular processes that involve antibody recycling and trafficking. A major function of FcRn is IgG recycling and half-life prolongation, and FcRn blockade results in a reduction of autoantibodies in IgG-mediated autoimmune diseases. In epithelial cells, FcRn functions in processes different from IgG recycling, such as antibody transcytosis in intestinal cells. In pemphigus vulgaris, an autoimmune disease of the epidermis, IgG autoantibodies directed against desmosomal adhesion proteins, especially desmoglein-3 and -1, cause loss of keratinocyte adhesion. We have previously demonstrated that FcRn blockade with efgartigimod, a human Fc fragment with enhanced FcRn binding, significantly reduces the keratinocyte monolayer fragmentation caused by anti-desmoglein-3 antibodies. This points to a direct function of FcRn in keratinocytes, beyond IgG recycling, but the mechanisms have not yet been elucidated in detail. Here, we show that FcRn binding is required for the full pathogenicity of recombinant anti-desmoglein-3 antibodies in keratinocytes, and that antibodies that exhibit enhanced or reduced FcRn affinity due to targeted substitutions in their Fc region, as well as F(ab')2 fragments not binding to FcRn display different degrees of pathogenicity. Blockade of FcRn by efgartigimod only shows a protective effect on keratinocyte adhesion against antibodies capable of binding to FcRn. Furthermore, antibody-induced degradation of desmoglein-3 in keratinocytes does not depend on FcRn, demonstrating that desmoglein-3 degradation and acantholysis are functionally disconnected processes. Our data suggest that the role of FcRn in autoimmune diseases is likely to be versatile and cell-type dependent, thus stressing the importance of further studies on FcRn function in autoimmune diseases., Competing Interests: RT has received research funding from argenx within a bilateral Research Collaboration Agreement. KV, MS and MB are employees of argenx, and their role in this study was as required from eligible coauthors. These aforementioned argenx coworkers generated some of the data, participated in the design of the study and in the writing of the manuscript as coauthors. The argenx coworkers and the funders had no role beyond their role as coauthors in the interpretation of the data or in the decision to publish the results. 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. The author(s) declared that they were an editorial board member of Frontiers, at the time of submission. This had no impact on the peer review process and the final decision., (Copyright © 2024 Zakrzewicz, Vanderheyden, Galaly, Feldhoff, Sips, Brinkhaus and Tikkanen.)

Published

2024

10. The Selection of DNA Aptamers Against the Fc Region of Human IgG

Author

Hu, Wen-Pin, Lin, Hui-Ting, Su, Wen-Yu, Hu, Rouh-Mei, Yang, Wei, Chen, Wen-Yih, Tsai, Jeffrey J. P., Angrisani, Leopoldo, Series Editor, Arteaga, Marco, Series Editor, Panigrahi, Bijaya Ketan, Series Editor, Chakraborty, Samarjit, Series Editor, Chen, Jiming, Series Editor, Chen, Shanben, Series Editor, Chen, Tan Kay, Series Editor, Dillmann, Rüdiger, Series Editor, Duan, Haibin, Series Editor, Ferrari, Gianluigi, Series Editor, Ferre, Manuel, Series Editor, Hirche, Sandra, Series Editor, Jabbari, Faryar, Series Editor, Jia, Limin, Series Editor, Kacprzyk, Janusz, Series Editor, Khamis, Alaa, Series Editor, Kroeger, Torsten, Series Editor, Liang, Qilian, Series Editor, Martin, Ferran, Series Editor, Ming, Tan Cher, Series Editor, Minker, Wolfgang, Series Editor, Misra, Pradeep, Series Editor, Möller, Sebastian, Series Editor, Mukhopadhyay, Subhas, Series Editor, Ning, Cun-Zheng, Series Editor, Nishida, Toyoaki, Series Editor, Pascucci, Federica, Series Editor, Qin, Yong, Series Editor, Seng, Gan Woon, Series Editor, Speidel, Joachim, Series Editor, Veiga, Germano, Series Editor, Wu, Haitao, Series Editor, Zhang, Junjie James, Series Editor, Hung, Jason C., editor, Yen, Neil Y., editor, and Hui, Lin, editor

Published

2019

11. A nano-innate immune system activator for cancer therapy in a 4T1 tumor-bearing mouse model.

Author

Liu, Xiang-Yu, Zhu, Mao-Hua, Wang, Xiao-Yu, Dong, Xiao, Liu, Hai-Jun, Li, Rui-Yang, Jia, Shi-Chong, Lu, Qin, Zhao, Mei, Sun, Peng, Chen, Hong-Zhuan, and Fang, Chao

Subjects

*IMMUNE system, *LABORATORY mice, *CANCER treatment, *ANIMAL disease models, *MESOPOROUS silica, *CANCER cells

Abstract

Background: Harnessing the immune system to fight cancer has led to prominent clinical successes. Strategies to stimulate innate immune effectors are attracting considerable interest in cancer therapy. Here, through conjugating multivalent Fc fragments onto the surface of mesoporous silica nanoparticles (MSN), we developed a nanoparticle-based innate immune system activator (NISA) for breast cancer immunotherapy. Methods: NISA was prepared through conjugating mouse IgG3 Fc to MSN surface. Then, long-chain PEG5000, which was used to shield Fc to confer nanoparticle colloidal stability, was linked to the MSN surface via matrix metalloprotease-2 (MMP-2)-cleavable peptide (GPLGIAGQC). The activation of multiple components of innate immune system, including complement and the innate cells (macrophages and dendritic cells) and the associated anticancer effect were investigated. Results: Fc fragments of NISA can be exposed through hydrolysis of long-chain PEG5000 by highly expressed MMP-2 in tumor microenvironment. Then, effective stimulation and activation of multiple components of innate immune system, including complement, macrophages, and dendritic cells were obtained, leading to efficient antitumor effect in 4T1 breast cancer cells and orthotopic breast tumor model in mice. Conclusions: The antitumor potency conferred by NISA highlights the significance of stimulating multiple innate immune elements in cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2022

12. 牛免疫球蛋白G的体外人源唾液酸化及 Fc片段的制备.

Author

李天慧, 陈春旭, 陈贵杰, 孙 怡, and 曾晓雄

Subjects

PAPAIN, GALACTOSE, SIALIC acids, CYSTEINE, BOS, ETHYLENEDIAMINETETRAACETIC acid, IMMUNOGLOBULIN G, NEURAMINIDASE

Abstract

Copyright of Shipin Kexue/ Food Science is the property of Food Science Editorial Department and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

13. The Dual Targeting of FcRn and FcγRs via Monomeric Fc Fragments Results in Strong Inhibition of IgG-Dependent Autoimmune Pathologies

Author

Céline Monnet, Emilie Jacque, Christophe de Romeuf, Alexandre Fontayne, Toufik Abache, Nathalie Fournier, Gilles Dupont, Delphine Derache, Anais Engrand, Aurélie Bauduin, Aurélie Terrier, Alexander Seifert, Cécile Beghin, Alain Longue, Nicholas Masiello, Laetitia Danino, Michel Nogre, Anais Raia, Frederic Dhainaut, Louis Fauconnier, Dieudonnée Togbe, Carmen Reitinger, Falk Nimmerjahn, Wil Stevens, Sami Chtourou, and Philippe Mondon

Subjects

FcRn, Fc fragment, Fc engineering, autoantibodies, autoimmune disease, immune complex (IC), Immunologic diseases. Allergy, RC581-607

Abstract

Novel molecules that directly target the neonatal Fc receptor (FcRn) and/or Fc gamma receptors (FcγRs) are emerging as promising treatments for immunoglobulin G (IgG)-dependent autoimmune pathologies. Mutated Fc regions and monoclonal antibodies that target FcRn are currently in clinical development and hold promise for reducing the levels of circulating IgG. Additionally, engineered structures containing multimeric Fc regions allow the dual targeting of FcRn and FcγRs; however, their tolerance needs to first be validated in phase I clinical studies. Here, for the first time, we have developed a modified monomeric recombinant Fc optimized for binding to all FcRns and FcγRs without the drawback of possible tolerance associated with FcγR cross-linking. A rational approach using Fc engineering allowed the selection of LFBD192, an Fc with a combination of six mutations that exhibits improved binding to human FcRn and FcγR as well as mouse FcRn and FcγRIV. The potency of LFBD192 was compared with that of intravenous immunoglobulin (IVIg), an FcRn blocker (Fc-MST-HN), and a trimeric Fc that blocks FcRn and/or immune complex-mediated cell activation through FcγR without triggering an immune reaction in several in vitro tests and validated in three mouse models of autoimmune disease.

Published

2021

14. The Dual Targeting of FcRn and FcγRs via Monomeric Fc Fragments Results in Strong Inhibition of IgG-Dependent Autoimmune Pathologies.

Author

Monnet, Céline, Jacque, Emilie, de Romeuf, Christophe, Fontayne, Alexandre, Abache, Toufik, Fournier, Nathalie, Dupont, Gilles, Derache, Delphine, Engrand, Anais, Bauduin, Aurélie, Terrier, Aurélie, Seifert, Alexander, Beghin, Cécile, Longue, Alain, Masiello, Nicholas, Danino, Laetitia, Nogre, Michel, Raia, Anais, Dhainaut, Frederic, and Fauconnier, Louis

Subjects

FC receptors, IMMUNOGLOBULIN G, MONOCLONAL antibodies, LABORATORY mice, PATHOLOGY

Abstract

Novel molecules that directly target the neonatal Fc receptor (FcRn) and/or Fc gamma receptors (FcγRs) are emerging as promising treatments for immunoglobulin G (IgG)-dependent autoimmune pathologies. Mutated Fc regions and monoclonal antibodies that target FcRn are currently in clinical development and hold promise for reducing the levels of circulating IgG. Additionally, engineered structures containing multimeric Fc regions allow the dual targeting of FcRn and FcγRs; however, their tolerance needs to first be validated in phase I clinical studies. Here, for the first time, we have developed a modified monomeric recombinant Fc optimized for binding to all FcRns and FcγRs without the drawback of possible tolerance associated with FcγR cross-linking. A rational approach using Fc engineering allowed the selection of LFBD192, an Fc with a combination of six mutations that exhibits improved binding to human FcRn and FcγR as well as mouse FcRn and FcγRIV. The potency of LFBD192 was compared with that of intravenous immunoglobulin (IVIg), an FcRn blocker (Fc-MST-HN), and a trimeric Fc that blocks FcRn and/or immune complex-mediated cell activation through FcγR without triggering an immune reaction in several in vitro tests and validated in three mouse models of autoimmune disease. [ABSTRACT FROM AUTHOR]

Published

2021

15. A fusion protein of vimentin with Fc fragment inhibits Japanese encephalitis virus replication.

Author

Zhang T, Chen Z, Xie L, Xu R, Chen L, Jia T, Shi W, Wang Y, Song Y, Han Q, Xia X, Yuan T, and Zhang J

Abstract

Japanese encephalitis virus (JEV), a member of the Flaviviridae family and a flavivirus, is known to induce acute encephalitis. Vimentin protein has been identified as a potential receptor for JEV, engaging in interactions with the viral membrane protein. The Fc fragment, an integral constituent of immunoglobulins, plays a crucial role in antigen recognition by dendritic cells (DCs) or phagocytes, leading to subsequent antigen presentation, cytotoxicity, or phagocytosis. In this study, we fused the receptor of JEV vimentin with the Fc fragment of IgG and expressed the resulting vimentin-Fc fusion protein in Escherichia coli . Pull-down experiments demonstrated the binding ability of the vimentin-Fc fusion protein to JEV virion in vitro . Additionally, we conducted inhibition assays at the cellular level, revealing the ability of vimentin-Fc protein suppressing JEV replication, it may be a promising passive immunotherapy agent for JEV. These findings pave the way for potential therapeutic strategies against JEV., Competing Interests: The 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 © 2024 Zhang, Chen, Xie, Xu, Chen, Jia, Shi, Wang, Song, Han, Xia, Yuan and Zhang.)

Published

2024

16. Fc-Mediated E2-Dimer Subunit Vaccines of Atypical Porcine Pestivirus Induce Efficient Humoral and Cellular Immune Responses in Piglets

Author

Xujiao Ren, Ping Qian, Shudan Liu, Huanchun Chen, and Xiangmin Li

Subjects

APPV, congenital tremor, subunit vaccine, Fc fragment, dimer, Microbiology, QR1-502

Abstract

Congenital tremor (CT) type A-II in piglets is caused by an emerging atypical porcine pestivirus (APPV), which is prevalent in swine herds and a serious threat to the pig production industry. This study aimed to construct APPV E2 subunit vaccines fused with Fc fragments and evaluate their immunogenicity in piglets. Here, APPV E2Fc and E2ΔFc fusion proteins expressed in Drosophila Schneider 2 (S2) cells were demonstrated to form stable dimers in SDS-PAGE and western blotting assays. Functional analysis revealed that aE2Fc and aE2ΔFc fusion proteins could bind to FcγRI on antigen-presenting cells (APCs), with the affinity of aE2Fc to FcγRI being higher than that of aE2ΔFc. Moreover, subunit vaccines based on aE2, aE2Fc, and aE2ΔFc fusion proteins were prepared, and their immunogenicity was evaluated in piglets. The results showed that the Fc fusion proteins emulsified with the ISA 201VG adjuvant elicited stronger humoral and cellular immune responses than the IMS 1313VG adjuvant. These findings suggest that APPV E2 subunit vaccines fused with Fc fragments may be a promising vaccine candidate against APPV.

Published

2021

17. Assessment of Computational Modeling of Fc-Fc Receptor Binding Through Protein-protein Docking Tool.

Author

Jebamani, Petrina, Sokalingam, Sriram, Sriramulu, Dinesh Kumar, Jung, Sang Taek, and Lee, Sun-Gu

Subjects

*MOLECULAR interactions, *HYDROGEN bonding interactions, *DRUG design, *PROTEIN-protein interactions, *FORECASTING

Abstract

Structural information of Fc-Fc receptor interaction may contribute to the design of drugs or therapeutic antibodies associated with the interaction. Computational protein-protein docking can be employed in structural study of protein-protein interaction, but its efficiency and reliability are still unstable and need to be validated and optimized for respective target protein complexes. In this study, we investigated and assessed the computational modeling efficiency of Fc-FcγR complex through HADDOCK by defining five different sets of active residues, a major parameter to determine the prediction efficiency of HADDOCK. The binding residues identified experimentally or the residues in the binding pocket were confirmed to be efficient active residues to achieve a high prediction efficiency, and too narrower or wider specification of active residues led to poor prediction efficiency. Most binding residues and crucial molecular interactions such as conserved interactions and hydrogen bonds in the crystal structure were reproduced in the best model. The HADDOCK docking condition determined in this study is expected to be applied to the computational characterization of various Fc-Fc receptor complexes and mutants. [ABSTRACT FROM AUTHOR]

Published

2020

18. Production of biologically active human factor IX-Fc fusion protein in the milk of transgenic mice.

Author

Yan, Hong, Gong, Xiuli, Xu, Miao, Guo, Xinbing, Chen, Yanwen, Xue, Yan, Zeng, Yitao, and Zeng, Fanyi

Subjects

TRANSGENIC mice, MILK proteins, CHIMERIC proteins, TRANSGENIC animals, MAMMARY glands, HEMOPHILIA treatment, BLOOD coagulation factor IX

Abstract

Objective: To investigate the feasibility of producing human IgG1 Fc fragment fused factor IX (FIX-Fc) in the milk of transgenic animals, for an alternative possible solution to the unmet need of FIX-Fc products for hemophilia B treatment. Results: Six founder lines of transgenic mice harboring FIX-Fc cassette designed to be expressed specifically in the mammary gland were generated. FIX-Fc protein was secreted into the milk of transgenic mice with preserved biological activity (with the highest value of 6.2 IU/mL), similar to that of the non-fused FIX transgenic milk. RT-PCR and immunofluorescence analysis confirmed that FIX-Fc was specifically expressed in the mammary gland. The blood FIX clotting activities were unchanged, and no apparent health defects were observed in the transgenic mice. Moreover, the stability of FIX protein in milk was increased by the Fc fusion. Conclusions: It is feasible to produce biologically functional FIX-Fc in the mammary gland of transgenic mice. Our preliminary results provide a foundation for the potential scale-up production of FIX-Fc in the milk of dairy animals. [ABSTRACT FROM AUTHOR]

Published

2020

19. Monoclonal Antibodies as Therapeutic Agents

Author

Khan, Manzoor M. and Khan, Manzoor M

Published

2016

20. Fc fragment of immunoglobulin G receptor IIa (FCGR2A) as a new potential prognostic biomarker of esophageal squamous cell carcinoma

Author

Nan Li, Zhi-Qiang Peng, Wen-Geng Zhang, Si-Fen Lu, Lu Zuhong, Xing-Yue Tu, and Kang Yulin

Subjects

Text mining, business.industry, Cancer research, Fc-Gamma Receptor, Medicine, Prognostic biomarker, General Medicine, FCGR2A, business, Esophageal squamous cell carcinoma, Fc fragment

Published

2021

21. Selectivity evaluation and separation of human immunoglobulin G, Fab and Fc fragments with mixed-mode resins.

Author

Luo, Ying-Di, Zhang, Qi-Lei, Yuan, Xiao-Ming, Shi, Wei, Yao, Shan-Jing, and Lin, Dong-Qiang

Subjects

*IMMUNOGLOBULIN G, *ADSORPTION (Chemistry), *CHROMATOGRAPHIC analysis, *PROTEIN-ligand interactions, *ISOTHERMAL titration calorimetry

Abstract

Adsorption selectivity is critical important for mixed-mode chromatography with specially-designed ligands. Human immunoglobulin G (hIgG), Fc and Fab fragments were used in the present work to evaluate adsorption behavior and binding selectivity of four mixed-mode resins with the ligands of 4-mercatoethyl-pyridine (MEP), 2-mercapto-1-methylimidazole (MMI), 5-aminobenzimidazole (ABI) and tryptophan-5-aminobenzimidazole (W-ABI), respectively. The resins showed an obvious pH-dependent adsorption behavior. High adsorption capacities were found at neutral pH for hIgG, Fc and Fab, and almost no adsorption happened under acidic conditions. An adsorption selectivity index was proposed to evaluate separation efficiency. High specificity of hIgG/Fc was found at pH 8.9 for MEP resin, and for W-ABI resin at pH 8.0 and 8.9. In addition, isothermal titration calorimetry was used to evaluate ligand-protein interactions. Finally, the separation of hIgG and Fc (1:1) was optimized with mixed-mode resins, and the best separation performance was obtained with W-ABI-based resin. Loading at pH 8.0 resulted in the flow through of Fc with purity of 90.4% and recovery of 98.8%, while elution at pH 3.6 provided hIgG with purity of 99.7% and recovery of 86.5%. [ABSTRACT FROM AUTHOR]

Published

2017

22. Effects of intravitreally injected Fc fragment on rat eyes.

Author

Taubitz, Tatjana, Steinbrenner, Laura-Pia, Tschulakow, Alexander, Biesemeier, Antje, Julien-Schraermeyer, Sylvie, and Schraermeyer, Ulrich

Subjects

*TREATMENT of eye diseases, *VASCULAR endothelial growth factors, *ELECTRON microscopy, *IMMUNOHISTOCHEMISTRY, *BIOCHEMICAL mechanism of action, *LABORATORY rats, *THERAPEUTICS

Abstract

Purpose: Anti-vascular endothelial growth factor (VEGF) drugs are used to treat neovascular eye diseases. Some of these drugs contain Fc fragments (Fc), but it is unknown how their mode of action is influenced by Fc. Therefore, this study investigated the effects of Fc on rat eyes after intravitreal injection. Methods: Eighteen Long-Evans rats were intravitreally injected with sterile, biotin-labeled rat Fc (9.1 μg in 5 μl PBS). For control, 5 μl PBS was injected in another nine rats. Animals were sacrificed between 1 and 3 days (group 1), 7 days (group 2), and 14 days (group 3) after injection. The right eyes were examined by electron microscopy (EM). The left eyes were stained by immunohistochemistry to investigate the distribution of Fc and the presence of macrophages. Results: After 1 day, Fc had penetrated into the anterior chamber and the retina up to the inner nuclear layer, and was located especially in retinal vessels. High numbers of infiltrating cells were present within the vitreous, around the ciliary body, anterior chamber and inside the retina 1-3 days after Fc injection ( p < 0.02 group 1 vs. control). Immunohistochemistry and EM showed that they were macrophages or granulocytes in close association with Fc. Ultrastructurally, there were effects on the blood vessels such as thrombocyte activation and fibrin formation. Conclusions: Biotin labeling is ideal for investigating the distribution of intravitreally injected proteins in ocular tissue. Fc fragments at a dose corresponding to their concentration in standard AMD treatments induced inflammation, and particularly the attraction of immune-competent cells. This may be associated with the risk of inflammation or endophthalmitis after anti-VEGF treatment, and needs further investigation. [ABSTRACT FROM AUTHOR]

Published

2016

23. Screening of Aptamer for Human IgG Fc Fragment by Capillary Electrophoresis-Systematic Evolution of Ligands by Exponential Enrichment

Author

Yuanyu Huang, Feng Qu, Shi-Miao Han, Liping Zhao, Chao Zhu, and Ge Yang

Subjects

Chromatography, Chemistry, Aptamer, 010401 analytical chemistry, 02 engineering and technology, 021001 nanoscience & nanotechnology, 01 natural sciences, Human Immunoglobulin G, Colorimetry (chemical method), 0104 chemical sciences, Analytical Chemistry, Capillary electrophoresis, Fab Fragments, A-DNA, 0210 nano-technology, Systematic evolution of ligands by exponential enrichment, Fc fragment

Abstract

A DNA aptamer screening method for human immunoglobulin G (IgG) Fc fragments was established based on capillary electrophoresis- systematic evolution of ligands by exponential enrichment (CE-SELEX). The purity, charged properties and non-adsorptivity of the samples of IgG, Fc and Fab were analyzed by capillary zone electrophoresis (CZE), and their affinity with ssDNA libraries was compared. The results showed that IgG formed significant complex with the ssDNA libraries, while Fc and Fab fragments exhibited weak affinity with the ssDNA libraries. Therefore, the use of the Fab fragment as the reverse screening target had no significant effect on the sequence except for the specific binding of Fc. The aptamer screening strategy for Fc fragments was designed. Aptamers (Seq Fc1–3) were obtained under optimized incubation conditions (10 mmol/L Na2HPO4-KH2PO4 (pH 7.17), 0.05 mmol/L Mg2+, incubated at 37 °C for 25 min) by three rounds of CE-SELEX, with KD values of 0.071–0.321 μmol/L, and their affinity and specificity were verified by AuNPs colorimetry assay.

Published

2020

24. An Efficient Method for Endotoxin Removal from Snake Antivenoms

Author

Norhan S. Sheraba, Aymen S. Yassin, Magdy A. Amin, Hamdallah Zedan, Mohamed R. Diab, and Yahya Alhamhoom

Subjects

Chromatography, biology, 010405 organic chemistry, Chemistry, 010401 analytical chemistry, Organic Chemistry, Clinical Biochemistry, Antivenom, Product recovery, Ultrafiltration, Serum albumin, Depyrogenation, 01 natural sciences, Biochemistry, 0104 chemical sciences, Analytical Chemistry, Endotoxin removal, biology.protein, Snake antivenom, Fc fragment

Abstract

Parenterally administered snake antivenom immunoglobulins are the only specific treatment for envenoming by snakebites. Endotoxin removal is a necessary part of good manufacturing practice for antivenom products to avoid life-threatening consequences associated with injecting endotoxin-contaminated product. Optimization of pH is an essential factor in endotoxin purification. This study aimed to compare ultrafiltration, ion-exchange chromatography and affinity resin-based chromatography techniques at different pH values to select the depyrogenation method with the highest endotoxin removal efficiency and optimum protein/product recovery. Affinity resin-based chromatography achieved 91.2% protein recovery at acidic pH without detectable endotoxins, while ion-exchange chromatography achieved 74.42% protein recovery at pH 7.5. In contrast, ultrafiltration achieved the lowest protein recovery compared to other chromatography techniques. In addition, ultrafiltration was ineffective in removing serum albumin (~ 42–57 kDa) and low molecular weight (MW) Fc fragments (~ 24–31 kDa). In conclusion, affinity resin-based chromatography has proven to be the most effective endotoxin removal method, while ultrafiltration may not be appropriate for the removal of bacterial LPS from antivenom sera. Moreover, this study demonstrated the existence of an optimum pH for each chromatographic method for the purpose of producing sterile and endotoxin-free snake antivenoms.

Published

2020

25. Construction of a novel plasmid vector expressing GPI anchored Fc fragments that can select transgenic cells by magnetic sorting

Subjects

選択マーカー, Fc フラグメント, cell separation, 磁性ビーズ, 細胞分離, Fc fragment, magnetic beads, selectable marker

Abstract

遺伝子導入実験において、プラスミド導入細胞の選択・分離には、薬剤耐性遺伝子または蛍光タンパク遺伝子をプラスミドに組み込む方法が一般的に利用されている。しかし、これらの方法はネガティブセレクションが不可能なことや、セルソーター等の高価な機器が必要であるといった問題点がある。これらの問題を改善するため、本研究では新たに磁性ビーズにより遺伝子導入細胞を分離するプラスミドを開発した。このプラスミドはFcフラグメントを細胞膜上に発現する選択マーカー遺伝子を所有し、プロテインG感作ビーズを用いて、遺伝子導入細胞を選択することができる。本プラスミドを用いることで、純度95%以上の遺伝子導入細胞が得られた。本システムは簡便性および高価な機器を必要としないことから、遺伝子導入細胞セレクションの新たな方法として有効な選択肢となりうると考えられる。, For the production of transgenic cells, antibiotic resistance or fluorescent protein genes are commonly used as selectable markers. However, the antibiotic resistance gene system is not possible for negative selection and the fluorescent protein system requires special equipment, such as a cell sorter. To overcome such problems, we constructed a new plasmid system for gene expression in mammalian cells that can isolate transgenic cells using protein G conjugated magnetic beads. This plasmid has a selectable marker gene for expressing Fc fragments on the cytoplasmic membrane, which can bind protein G and purify cells expressed Fc fragments through a magnetic technique. This could efficiently enrich transgenic cells at > 95%, as indicated when the purity was assessed by fluorescence-activated cell sorting (FACS). In summary, as this system is very simple and there is no need for expensive equipment, it would be a useful tool for mammalian transformation.

Published

2020

26. Refinement and Neutralization Evaluation of the F(ab’)2 Type of Antivenom against the Deadly Jellyfish Nemopilema nomurai Toxins

Author

Chunlin Yu, Li Pengcheng, Huahua Yu, Li Aoyu, and Li Rongfeng

Subjects

jellyfish, Nemopilema nomurai, antivenom, NnTXs, IgG-AntiNnTXs, F(ab’)2-AntiNnTXs, Male, Jellyfish, Scyphozoa, QH301-705.5, Antivenom, complex mixtures, Catalysis, Neutralization, Article, Antibodies, Inorganic Chemistry, Jellyfish stings, Lethal Dose 50, Immunoglobulin Fab Fragments, Mice, Cnidarian Venoms, Neutralization Tests, biology.animal, Animals, Physical and Theoretical Chemistry, Biology (General), Molecular Biology, QD1-999, Spectroscopy, Antiserum, biology, Antivenins, Organic Chemistry, General Medicine, Virology, eye diseases, Computer Science Applications, Chemistry, Immunoglobulin G, Female, Rabbits, Metalloproteinase activity, Fc fragment

Abstract

Jellyfish stings threaten people’s health and even life in coastal areas worldwide. Nemopilema nomurai is one of the most dangerous jellyfish in the East Asian Marginal Seas, which not only stings hundreds of thousands of people every year but also is assumed to be responsible for most deaths by jellyfish stings in China. However, there is no effective first-aid drug, such as antivenoms, for the treatment of severe stings by N. nomurai to date. In this study, we prepared a N. nomurai antiserum from rabbits using inactivated N. nomurai toxins (NnTXs) and isolated the IgG type of antivenom (IgG-AntiNnTXs) from the antiserum. Subsequently, IgG-AntiNnTXs were refined with multiple optimizations to remove Fc fragments. Finally, the F(ab’)2 type of antivenom (F(ab’)2-AntiNnTXs) was purified using Superdex 200 and protein A columns. The neutralization efficacy of both types of antivenom was analyzed in vitro and in vivo, and the results showed that both IgG and F(ab’)2 types of antivenom have some neutralization effect on the metalloproteinase activity of NnTXs in vitro and could also decrease the mortality of mice in the first 4 h after injection. This study provides some useful information for the development of an effective antivenom for N. nomurai stings in the future.

Published

2021

27. Residue interaction network and molecular dynamics simulation study on the binding of S239D/I332E Fc variant with enhanced affinity to FcγRIIIa receptor.

Author

Jebamani, Petrina, Sriramulu, Dinesh Kumar, and Lee, Sun-Gu

Subjects

*MOLECULAR dynamics, *MOLECULAR interactions, *FC receptors, *ELECTROSTATIC interaction

Abstract

Engineering of Fc has been adapted as an efficient method for enhanced or reduced affinity towards Fc receptors in the development of therapeutic antibodies. S239D/I332E mutation of Fc induces approximately two logs greater affinity to the FcγRIIIa receptor and has been extensively employed in various Fc engineering studies. It is known that the mutation gives rise to the formation of salt bridges between the mutated residues of Fc and FcγRIIIa, but the overall effect of the mutation in the binding interface of the Fc-FcγRIIIa complex is still unclear. In this study, the molecular interactions in the binding interface of mutant Fc and FcγRIIIa were analyzed and compared with those of wild-type Fc binding through residue interaction network (RIN) analysis and molecular dynamics (MD) simulation. RIN analysis identified specific molecular interactions and Hub residues in the interfaces, and their numbers were increased by introducing the mutation, with maintaining most of the molecular interactions in the wild-type complex. MD simulation study revealed that the numbers of stable electrostatic interactions and stable Hub residues in the mutant complex were higher than those in the wild-type complex. The introduced mutations were shown to form further charge-charge attractive interactions in addition to the identified salt bridges without generating any repulsive interactions. These results are expected to provide further structural insight into Fc variants' design based on the S239D/I332E mutation. [Display omitted] • S239D/I332E mutations in Fc showed greater affinity to FcγRIIIa in various experimental studies. • To understand the effect of mutations, RIN analysis and MD simulation were performed. • The results showed that the mutant structure had more stable interactions than the wild-type structure. • Possible new electrostatic interactions can also be induced by the charged mutations. [ABSTRACT FROM AUTHOR]

Published

2023

28. Transient expression of Fc-fused human glycoprotein 130 in Expi293F suspension cells.

Author

Zhao, Xiaozhi, Chen, Wei, Ge, Liyuan, Jiang, Wei, Tang, Bo, Zhang, Qing, Xu, Xiaoyu, Wang, Chong, Cao, Lin, and Guo, Hongqian

Subjects

*INFLAMMATION treatment, *CANCER treatment, *INTERLEUKIN-6, *GLYCOPROTEINS, *GENETIC vectors, *RECOMBINANT proteins, *AFFINITY chromatography, *STAT proteins, *THERAPEUTICS

Abstract

Human glycoprotein 130 (gp130) is a signal-transducing receptor for interleukin 6 (IL-6), whose signaling plays a critical role in chronic inflammation and cancer. The soluble form of gp130 specifically inhibits IL-6 trans-signaling. However, achieving high-level expression of a large glycoprotein such as gp130 is difficult. Here, we designed and constructed one Fc-gp130-pcDNA mammalian expression vector, with the mouse IgG2a Fc fragment added to the N-terminus of human gp130, which greatly increased the secretion of recombinant gp130 protein from Expi293F suspension cells. Recombinant fusion Fc-gp130 was easily and efficiently purified from the supernatant of transfected cells by one-step affinity chromatography. Moreover, Fc-gp130 could automatically form dimers by the disulfide bond. Fc-gp130 was confirmed as a more efficient IL-6 trans-signaling blocker by its higher biological activity against signal transducer and activator of transcription 3 (STAT3). This purified active Fc-gp130 could be used to develop valuable therapeutic agents against inflammatory diseases and cancers. [ABSTRACT FROM AUTHOR]

Published

2016

29. Sweet but dangerous -- the role of immunoglobulin G glycosylation in autoimmunity and inflammation.

Author

Biermann, M. H. C., Griffante, G., Podolska, M. J., Boeltz, S., Strüer, J., Munoz, L. E., Bilyy, R., and Herrmann, M.

Subjects

*GLYCOSYLATION, *IMMUNOGLOBULIN G, *AUTOIMMUNITY, *INFLAMMATION treatment, *SYSTEMIC lupus erythematosus treatment

Abstract

Glycosylation is well-known to modulate the functional capabilities of immunoglobulin G (IgG)-mediated cellular and humoral responses. Indeed, highly sialylated and desialylated IgG is endowed with anti- and pro-inflammatory activities, respectively, whereas fully deglycosy-lated IgG is a rather lame duck, with no effector function besides toxin neutralization. Recently, several studies revealed the impact of different glycosylation patterns on the Fc part and Fab fragment of IgG in several autoimmune diseases, including systemic lupus erythematosus (SLE) and rheumatoid arthritis (RA). Here, we provide a synoptic update summarizing the most important aspects of antibody glycosylation, and the current progress in this field. We also discuss the therapeutic options generated by the modification of the glycosylation of IgG in a potential treatment for chronic inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2016

30. The Dual Targeting of FcRn and FcγRs via Monomeric Fc Fragments Results in Strong Inhibition of IgG-Dependent Autoimmune Pathologies

Author

Nicholas C. Masiello, Aurélie Bauduin, Nathalie Fournier, Frederic Dhainaut, Alexander Seifert, Alain Longue, Anais Raia, Michel Nogre, Aurélie Terrier, Anais Engrand, Cécile Beghin, Gilles Dupont, Laetitia Danino, Alexandre Fontayne, Philippe Mondon, Emilie Jacque, Toufik Abache, Dieudonnée Togbe, Falk Nimmerjahn, Carmen Reitinger, Sami Chtourou, Delphine Derache, Wil Stevens, Louis Fauconnier, Céline Monnet, and Christophe De Romeuf

Subjects

Platelet Aggregation, autoantibodies, THP-1 Cells, Autoimmunity, Receptors, Fc, Protein Engineering, Immunoglobulin G, Jurkat Cells, Immunology and Allergy, Receptor, Original Research, Secretory Pathway, biology, immune complex (IC), Chemistry, Cell biology, Antirheumatic Agents, Female, Antibody, Cell activation, Protein Binding, Signal Transduction, medicine.drug_class, Fc gamma receptor (FcγR), Immunology, Fc engineering, autoimmune disease, Complement C5a, Mice, Transgenic, Monoclonal antibody, Binding, Competitive, Immune system, Neonatal Fc receptor, Phagocytosis, medicine, Animals, Humans, ddc:610, Fc fragment, Autoimmune disease, Histocompatibility Antigens Class I, Receptors, IgG, RC581-607, medicine.disease, Arthritis, Experimental, Immunoglobulin Fc Fragments, Mice, Inbred C57BL, FcRn, Kinetics, Mutation, biology.protein, Interleukin-2, Immunologic diseases. Allergy

Abstract

Novel molecules that directly target the neonatal Fc receptor (FcRn) and/or Fc gamma receptors (FcγRs) are emerging as promising treatments for immunoglobulin G (IgG)-dependent autoimmune pathologies. Mutated Fc regions and monoclonal antibodies that target FcRn are currently in clinical development and hold promise for reducing the levels of circulating IgG. Additionally, engineered structures containing multimeric Fc regions allow the dual targeting of FcRn and FcγRs; however, their tolerance needs to first be validated in phase I clinical studies. Here, for the first time, we have developed a modified monomeric recombinant Fc optimized for binding to all FcRns and FcγRs without the drawback of possible tolerance associated with FcγR cross-linking. A rational approach using Fc engineering allowed the selection of LFBD192, an Fc with a combination of six mutations that exhibits improved binding to human FcRn and FcγR as well as mouse FcRn and FcγRIV. The potency of LFBD192 was compared with that of intravenous immunoglobulin (IVIg), an FcRn blocker (Fc-MST-HN), and a trimeric Fc that blocks FcRn and/or immune complex-mediated cell activation through FcγR without triggering an immune reaction in several in vitro tests and validated in three mouse models of autoimmune disease.

Published

2021

31. ПРИМЕНЕНИЕ ТЕХНОЛОГИИ Fc-СЛИЯНИЯ БЕЛКОВ ДЛЯ РАЗРАБОТКИ ВАКЦИН ПРОТИВ ИНФЕКЦИОННЫХ БОЛЕЗНЕЙ ЖИВОТНЫХ И ЧЕЛОВЕКА

Subjects

Tuberculosis, Ebola virus, biology, business.industry, Human immunodeficiency virus (HIV), biology.organism_classification, medicine.disease, medicine.disease_cause, African swine fever virus, Virology, Vaccination, Medicine, General Agricultural and Biological Sciences, business, Fc fragment

Published

2019

32. Adsorption Characteristics of Human Immunoglobulin G on Five New Tetrapeptide Biomimetic Affinity Resins

Author

Dong-Qiang Lin, Shan-Jing Yao, Hong-Yun Zhu, Qi-Lei Zhang, and Sheng-Gang Chen

Subjects

Tetrapeptide, Chemistry, General Chemical Engineering, dBc, 02 engineering and technology, General Chemistry, 010402 general chemistry, 01 natural sciences, Human Immunoglobulin G, Combinatorial chemistry, 0104 chemical sciences, Molecular dynamics, Adsorption, 020401 chemical engineering, Docking (molecular), 0204 chemical engineering, Fc fragment

Abstract

Alternative antibody-binding affinity ligands are expected to support robust time- and cost-effective antibody purification with rapid improvement of upstream productivity and demand on downstream process optimization. Five new tetrapeptide biomimetic affinity ligands (FYRH, HWRH, YHRI, HYRF, and FHRA) were screened by modeling the molecular interaction mechanism between tetrapeptide ligands and the Fc fragment of IgG with molecular dynamics simulation and the flexible docking method, and the corresponding five resins were prepared in this work to evaluate their adsorption characteristics of human immunoglobulin G (hIgG). The results showed that the binding capacities to hIgG of the five resins showed a strong pH-dependency, which was high at pH 7.0–9.0, and extremely low at pH 5.0–6.0, providing a benefit choice to separate hIgG. The dynamic binding capacities (DBC) at 10% breakthrough of five resins could reach up to 28–37 mg/mLgel, and Ac-FYRH-4FF resin showed the best adsorption performance. The eluti...

Published

2019

33. Domain unfolding of monoclonal antibody fragments revealed by non-reducing SDS-PAGE

Author

Andrew B. Norman, Terence L. Kirley, and Kenneth D. Greis

Subjects

Monoclonal antibody, 0301 basic medicine, IPA, isopropanol, Electrophoretic migration, medicine.drug_class, Antibody fragments, Biophysics, Biochemistry, lcsh:Biochemistry, 03 medical and health sciences, h2E2, humanized anti-cocaine monoclonal antibody, medicine, lcsh:QD415-436, mAb, monoclonal antibody, Polyacrylamide gel electrophoresis, lcsh:QH301-705.5, biology, Chemistry, CHO, Chinese Hamster Ovary, MALDI-Tof MS, matrix-assisted laser desorption ionization/time-of-flight mass spectrometry, 3. Good health, 030104 developmental biology, Non-reducing SDS-PAGE, Antibody domain unfolding, lcsh:Biology (General), Antibody analysis, Polyclonal antibodies, Monoclonal, biology.protein, Antibody, Research Article, Fc fragment, Conjugate

Abstract

Monoclonal antibodies and derived fragments are used extensively both experimentally and therapeutically. Thorough characterization of such antibodies is necessary and includes assessment of their thermal and storage stabilities. Thus, assessment of the underlying conformational stabilities of the antibodies is also important. We recently documented that non-reducing SDS-PAGE can be used to assess both monoclonal and polyclonal IgG domain thermal unfolding in SDS. Utilizing this same h2E2 anti-cocaine mAb, in this study we generated and analyzed various mAb antibody fragments to delineate the structural domains of the antibody responsible for the observed discrete bands following various heating protocols and analysis by non-reducing SDS-PAGE. Previously, these domain unfolding transitions and gel bands were hypothesized to stem from known mAb structural domains based on the relative thermal stability of those CH2, CH3, and Fab domains in the absence of SDS, as measured by differential scanning calorimetry. In this study, we generated and analyzed F(ab’)2, Fab, and Fc fragments, as well as a mAb consisting of only heavy chains, and examined the thermally induced domain unfolding in each of these fragments by non-reducing SDS-PAGE. The results were interpreted and integrated to generate an improved model of thermal unfolding for the mAb IgG in SDS. These results and the model presented should be generally applicable to many monoclonal and polyclonal antibodies and allow novel comparisons of conformational stabilities between chemically or genetically modified versions of a given antibody. Such modified antibodies and antibody drug conjugates are commonly utilized and important for experimental and therapeutic applications., Graphical abstract fx1, Highlights • mAb F(ab’)2 fragments exhibit multiple unfolded states in non-reducing SDS-PAGE. • Fab and Fc mAb fragments do not exhibit similar multiple unfolded state bands. • Previous mAb domain unfolding pathway in SDS is revised based on fragment analyses. • A heavy chain only mAb variant is detected and exhibits multiple unfolded states. • These results are likely relevant to analyses of many monoclonal and polyclonal Abs.

Published

2018

34. Antibody glycosylation in autoimmune diseases

Author

Xing Zhou, William M. Ridgway, Weici Zhang, M. Eric Gershwin, Francesca Motta, and Carlo Selmi

Subjects

0301 basic medicine, Glycosylation, Immunology, Lupus, Context (language use), Autoimmunity, Disease, medicine.disease_cause, Inflammatory bowel disease, Autoimmune Disease, Article, Autoimmune Diseases, Arthritis, Rheumatoid, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Immune system, Rheumatoid, medicine, Immunology and Allergy, Lupus Erythematosus, Systemic, Humans, Fc fragment, Antibody, 030203 arthritis & rheumatology, Inflammation, biology, Lupus Erythematosus, business.industry, Arthritis, Inflammatory and immune system, Systemic, medicine.disease, Glycome, 030104 developmental biology, Good Health and Well Being, chemistry, biology.protein, business, Digestive Diseases

Abstract

The glycosylation of the fragment crystallizable (Fc) region of immunoglobulins (Ig) is critical for the modulation of antibody effects on inflammation. Moreover, antibody glycosylation may induce pathologic modifications and ultimately contribute to the development of autoimmune diseases. Thanks to progress in the analysis of glycosylation, more data are available on IgG and its subclass structures in the context of autoimmune diseases. In this review, we focused on the impact of Ig glycosylation in autoimmunity, describing how it modulates the immune response and how glycome profiles can be used as biomarkers of disease activity. The analysis of antibody glycosylation demonstrated specific features in human autoimmune and chronic inflammatory conditions, including rheumatoid arthritis, systemic lupus erythematosus, inflammatory bowel disease and autoimmune liver diseases, among others. Within the same disease, different patterns are associated with disease severity and treatment options. Future research may increase the information available on the distinct glycome profiles and expand their potential role as biomarkers and as targets for treatment, ultimately favoring an individualized approach.

Published

2021

35. Microfluidics as a high-throughput solution for chromatographic process development - The complexity of multimodal chromatography used as a proof of concept

Author

Ana Azevedo, Mariana N. São Pedro, Maria Raquel Aires-Barros, André Nascimento, and Inês F. Pinto

Subjects

chemistry.chemical_classification, Chromatography, Consumables, Process development, Biomolecule, Organic Chemistry, Microfluidics, General Medicine, Ligands, Biochemistry, Biological materials, Analytical Chemistry, High-Throughput Screening Assays, chemistry, Proof of concept, Throughput (business), Fc fragment

Abstract

High-throughput technologies are fundamental to expedite the implementation of novel purification platforms. The possibility of performing process development within short periods of time while saving consumables and biological material are prime features for any high-throughput screening device. In this work, a microfluidic device is evaluated as high-throughput solution for a complete study of chromatographic operation conditions on ten different multimodal resins. The potential of this class of purification solutions is generally hindered by its complexity. Taking this into consideration, the microfluidic platform was herein applied and assessed as a tool for high-throughput applications. The commercially available multimodal ligands were studied for the binding of three antibody-based biomolecules (polyclonal mixture of whole antibodies, Fab and Fc fragments) at different pH and salt conditions, in a total of 450 experiments. The results obtained with the microfluidic device were comparable to a standard 96-well filtering microplate high-throughput tool. Additionally, five of the ten multimodal ligands tested were packed into a bench-scale column to perform a final validation of the microfluidic results obtained. All the data acquired in this work using different screening protocols corroborate each other, showing that microfluidic chromatography is a valuable tool for the fast implementation of a new purification step, particularly, if the goal is to narrow the downstream possibilities by being a first point of decision.

Published

2021

36. Oriented immobilization of antibodies onto sensing platforms - A critical review

Author

Jose M. Guisan, Shipeng Gao, and Javier Rocha-Martín

Subjects

chemistry.chemical_classification, Immunoassay, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Nanotechnology, Biosensing Techniques, Biochemistry, Antibodies, Analytical Chemistry, Immunoglobulin Fc Fragments, chemistry, Covalent bond, Environmental Chemistry, Non-covalent interactions, Biosensor, Antibodies, Immobilized, Spectroscopy, Conjugate, Fc fragment

Abstract

The immunosensor has been proven a versatile tool to detect various analytes, such as food contaminants, pathogenic bacteria, antibiotics and biomarkers related to cancer. To fabricate robust and reproducible immunosensors with high sensitivity, the covalent immobilization of immunoglobulins (IgGs) in a site-specific manner contributes to better performance. Instead of the random IgG orientations result from the direct yet non-selective immobilization techniques, this review for the first time introduces the advances of stepwise yet site-selective conjugation strategies to give better biosensing efficiency. Noncovalently adsorbing IgGs is the first but decisive step to interact specifically with the Fc fragment, then following covalent conjugate can fix this uniform and antigens-favorable orientation irreversibly. In this review, we first categorized this stepwise strategy into two parts based on the different noncovalent interactions, namely adhesive layer-mediated interaction onto homofunctional support and layer-free interaction onto heterofunctional support (which displays several different functionalities on its surface that are capable to interact with IgGs). Further, the influence of ligands characteristics (synthesis strategies, spacer requirements and matrices selection) on the heterofunctional support has also been discussed. Finally, conclusions and future perspectives for the real-world application of stepwise covalent conjugation are discussed. This review provides more insights into the fabrication of high-efficiency immunosensor, and special attention has been devoted to the well-orientation of full-length IgGs onto the sensing platform.

Published

2021

37. Safety, efficacy, and tolerability of efgartigimod in patients with generalised myasthenia gravis (ADAPT): a multicentre, randomised, placebo-controlled, phase 3 trial

Author

Lucy Lam, Jiri Pitha, John Vissing, Laura Fionda, Denis Korobko, Michael Pulley, Tony Vangeneugden, Silvia Bonanno, Nobuhiro Ido, Jerrica Farias, Jafar Shabanpour, James Gilchrist, Girolamo Alfieri, Gyorgyi Szabo, Carlayne E. Jackson, Eduardo Ng, Csilla Rozsa, Hans D. Katzberg, Carlo Antozzi, Aleksandra Golenia, Sayaka Ishida, Temur Margania, Andrzej Szczudlik, Richard J. Barohn, Mari Suzuki., Robert Henegar, Kaoru Sakuma, Evanthia Bernitsas, Elena Lapochka, Yukiko Ozawa, Tomihiro Imai, Debbie Hastings, Antonio Guglietta, Benjamin Frishberg, Elena Antipenko, Vera Bril, Stanislav Vohanka, Isela Hernandez, Ivo Bozovic, Ilona Vergunova, Lorenzo Maggi, Andreas Meisel, Ali Malekniazi, Tahseen Mozaffar, Emmanuelle Salort-Campana, Yasmin Camberos, Jan J.G.M. Verschuuren, Masayuki Masuda, Masanori Takahashi, Yoshihiko Okubo, Marek Smilowski, Yasushi Suzuki, Mary Wagoner, Andrew Heim, David Bors, Chiho Watanabe, Fiammetta Vanoli, Antonio Reia, Zubair Quraishi, Omar Jawdat, Makoto Samukawa, Gregory Sahagian, Gedeonne Margo Jakab, Eiichi Nomura, Samantha Colgan, Cindy Benzel, Ayako Mori, Annabel M. Ruiter, Ratna Bharavaju-Sanka, Roman Shakarishvili, Victoria Cannon, Malkova Nadezhda, Tomas Horak, Anna Kostera-Pruszczyk, Eniko Szabo, Emilien Delmont, Alexander Tsiskaridze, Lubna Daniyal, Vidosava Rakocevic Stojanovic, Szilvia Toth, Siegfried Kohler, Iveta Novakova, Katherine Roath, Kazuna Ikeda, Salma Akhter, Claudia Heibutzki, Martijn R. Tannemaat, Marta Pinkosz, Mads Peter Godtfeldt Stemmerik, Chafic Karam, Irys Caristo, Carolyn Paiz, Josef Bednarik, Monika Frasinska, Stefania Morino, Norianne Pimentel, Kanako Minemoto, Rekha Pillai, Linda Wagemaekers, Annelien De Pue, Irina Poverennova, Katerina Reguliova, Jana Junkerova, Angela Marsili, Anne-Marie Peters, Maren Wyckmans, Michaela Tyblova, Debbie Eggleston, Anne Mette Ostergaard Autzen, Takamichi Sugimoto, Kuldeep Kumar Khatri, Niraja Suresh, Jan De Bleecker, Lea Gerischer, Grazyna Zwolinska, Kevin R Keene, Yosuke Onishi, Francesco Saccà, Zaeem A. Siddiqi, Marjolein Van Heur, Jeffrey Statland, Tatiana Romanova, Diana Dimitrova, Stojan Peric, Tomoko Tsuda, Cathy Bailey, Lubov Urtaeva, Lizzie Zafirakos, Katherine Ruzhansky, Tomoya Kubota, Angela Campanella, Nadezhda Kuznetsova, Sarah Jones, Giovanni Antonini, Hiroyuki Murai, Luca Leonardi, Alan R. Berger, Jonathan Baets, Peter Ulrichts, Said R. Beydoun, Michala Jakubikova, Mamatha Pasnoor, James F. Howard, Leila Darki, Katerina Havelkova, Namita Goyal, Akiyuki Uzawa, Tia Nguyen, Miki Takaki, Matteo Garibaldi, Manisha Kak, Ivonne Turner, Aude-Marie Grapperon, Mageda Horakova, Yuebing Li, Ivana Basta, Lech Szczechowski, Shabber Mannan, Aneta Pasko, Caroline Vinck, Riccardo Giossi, Rudolf Mercelis, Ivana Jurajdova, Lesly Welsh, Małgorzata Bilińska, Marek Halas, Dragana Lavrnic, Kimiaki Utsugisawa, Todd Levine, Erik Velasquez, Daisuke Yamamoto, Constantine Farmakidis, John Anthony Morren, Sarah Hoffman, Manisha Chopra, Shingo Konno, Rita Frangiamore, Kelly Jia, Jana Horakova, Anna Melnikova, Piotr Szczudlik, Ali Habib, Giorgia Puorro, Michael D. Weiss, Robert P. Lisak, Hiroyuki Naito, Shahram Attarian, Hiroko Nakamura, Shin Hisahara, Mazen M. Dimachkie, Genya Watanabe, Duaa Jabari, Ekaterina Bulatova, Angela Genge, Makiko Naito, Melissa Currence, Henning Andersen, Katrien De Mey, Kathy de Koning, Yuen T. So, Chiara Pane, Renato Mantegazza, Rebecca Traub, Manato Yasuda, Amy Visser, Dike Remstedt, Yuka Takematsu, Frauke Stascheit, Ayumi Kamei, Tuan Vu, Tulio E. Bertorini, Ludivine Kouton, Neelam Goyal, Flicia Mada, Nizar Chahin, Mihiro Shimizu, Srikanth Muppidi, and Erina Sugano

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Population, fc fragment, Placebo, Antibodies, Monoclonal, Humanized, law.invention, efgartigimod, myasthenia gravis, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, Double-Blind Method, law, Internal medicine, Activities of Daily Living, Myasthenia Gravis, medicine, Clinical endpoint, Humans, Receptors, Cholinergic, Dosing, Longitudinal Studies, education, Biology, Autoantibodies, education.field_of_study, business.industry, Headache, Antibodies, Monoclonal, Middle Aged, medicine.disease, Myasthenia gravis, 3. Good health, Immunoglobulin Fc Fragments, Clinical trial, Chemistry, 030104 developmental biology, Tolerability, Female, Human medicine, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Background: There is an unmet need for treatment options for generalised myasthenia gravis that are effective, targeted, well tolerated, and can be used in a broad population of patients. We aimed to assess the safety and efficacy of efgartigimod (ARGX-113), a human IgG1 antibody Fc fragment engineered to reduce pathogenic IgG autoantibody levels, in patients with generalised myasthenia gravis. Methods: ADAPT was a randomised, double-blind, placebo-controlled, phase 3 trial done at 56 neuromuscular academic and community centres in 15 countries in North America, Europe, and Japan. Patients aged at least 18 years with generalised myasthenia gravis were eligible to participate in the study, regardless of anti-acetylcholine receptor antibody status, if they had a Myasthenia Gravis Activities of Daily Living (MG-ADL) score of at least 5 (>50% non-ocular), and were on a stable dose of at least one treatment for generalised myasthenia gravis. Patients were randomly assigned by interactive response technology (1:1) to efgartigimod (10 mg/kg) or matching placebo, administered as four infusions per cycle (one infusion per week), repeated as needed depending on clinical response no sooner than 8 weeks after initiation of the previous cycle. Patients, investigators, and clinical site staff were all masked to treatment allocation. The primary endpoint was proportion of acetylcholine receptor antibody-positive patients who were MG-ADL responders (≥2-point MG-ADL improvement sustained for ≥4 weeks) in the first treatment cycle. The primary analysis was done in the modified intention-to-treat population of all acetylcholine receptor antibody-positive patients who had a valid baseline MG-ADL assessment and at least one post-baseline MG-ADL assessment. The safety analysis included all randomly assigned patients who received at least one dose or part dose of efgartigimod or placebo. This trial is registered at ClinicalTrials.gov (NCT03669588); an open-label extension is ongoing (ADAPT+, NCT03770403). Findings: Between Sept 5, 2018, and Nov 26, 2019, 167 patients (84 in the efgartigimod group and 83 in the placebo group) were enrolled, randomly assigned, and treated. 129 (77%) were acetylcholine receptor antibody-positive. Of these patients, more of those in the efgartigimod group were MG-ADL responders (44 [68%] of 65) in cycle 1 than in the placebo group (19 [30%] of 64), with an odds ratio of 4·95 (95% CI 2·21–11·53, p

Published

2020

38. SLC-Her-2/neu-p53-FC融合基因重组腺病毒真核表达载体对荷黑色素瘤小鼠的免疫治疗效果

Author

王慰敏, 孙文欣, 钱海利, 王海娟, 张叔人, and 林 晨

Abstract

Objective To amplify and purify the recombinant adenovirus with fused gene of SLC, Her-2/neu, p53 and Fc fragment (SLC-HP-Fc) and test its immunotherapeutic effect on mice bearing melanoma. Methods The adenovirus was given to the C57BL/6 mice model bearing melanoma to test its anti-tumor effect. Results By LDH assay, we found the cytolysis activity of mice spleen lymphocytes from the mice treated with high dosage of AdEasyTM-SLC-HP-Fc by intramuscular injection was higher than that of the spleen lymphocytes of the mice from other groups. Conclusion The fused gene transmission by the adenovirus vector is feasible. And the eukaryotic expression of the recombinant adenovirus AdEasyTM-SLC-HP-Fc, especially with high dosage by intramuscular injection, can delay tumor emergence and inhibit tumor growth. [ABSTRACT FROM AUTHOR]

Published

2014

39. Relations between macro- and microstability of C2 domains of human IgG2 and their biological activity: 2. Calculation of thermodynamic functions that characterize the domain stability.

Author

Tishchenko, V.

Subjects

*IMMUNOGLOBULIN G, *THERMAL stability, *MICROCALORIMETRY, *THERMODYNAMIC functions, *PROTEIN analysis, *ENTROPY, *ENTHALPY

Abstract

Thermodynamic parameters of stabilization of the native structure of C2 domains in human myeloma second subclass LOM and SIN immunoglobulins and their hFc fragments, which we obtained for the first time, were determined using the method of scanning microcalorimetry. The decrease in thermal stability and energy of stabilization of the native structure of the domains in intact proteins in the physiological range of temperatures (20-37°C) correlated mainly with the entropy factor. [ABSTRACT FROM AUTHOR]

Published

2014

40. Intravenous immunoglobulin preparation prevents the production of pro-inflammatory cytokines by modulating NFκB and MAPKs pathways in the human monocytic THP-1 cells stimulated with procalcitonin.

Author

Murakami, Kazuki, Suzuki, Chiaki, Fujii, Akihiro, Kobayashi, Fujio, Nakano, Atsushi, and Kamizono, Akihito

Subjects

*IMMUNOGLOBULINS, *CYTOKINES, *NF-kappa B, *TUMOR necrosis factors, *INTERLEUKIN-6, *ENZYME-linked immunosorbent assay

Abstract

Objective: In the previous investigations, we showed that intravenous immunoglobulin (IVIG) prevented cytokine release in procalcitonin (PCT)-stimulated monocytic cells. The aim of the present study was to investigate the underlying mechanisms of inhibition of IVIG on cytokine production in PCT-stimulated THP-1 cells. Methods: THP-1 cells treated with phorbol myristate acetate were stimulated with PCT. The protein levels of pro-inflammatory cytokines [tumor necrosis factor-α (TNF-α), interleukin-6 (IL-6), and high-mobility group box 1 (HMGB1)] in the culture supernatants were determined using enzyme-linked immunosorbent assay kits. The mRNA level of TNF-α was determined by reverse transcription-polymerase chain reaction. The phosphorylations of nuclear factor kappa B (NFκB) and the mitogen-activated protein kinases (MAPKs) were determined by Western blotting. Results: IVIG reduced mRNA expression and protein production of TNF-α in PCT-stimulated THP-1 cells. Not only IVIG but also both the Fc fragment and the F(ab') fragment inhibited PCT-induced TNF-α, IL-6, and HMGB1 production. Furthermore, IVIG and its fragments suppressed PCT-induced phosphorylations of NFκB, p38 MAPK, and c-Jun N-terminal kinase. Conclusions: Our results indicate that IVIG prevents PCT-induced cytokine production mediated by not only the Fab region but also the Fc region. The activity of IVIG and its fragments might be regulated by inhibiting NFκB and MAPKs pathways in THP-1 cells. [ABSTRACT FROM AUTHOR]

Published

2014

41. In vivo pharmacokinetic enhancement of monomeric Fc and monovalent bispecific designs through structural guidance

Author

Herren Wu, Kimberly M Cook, Sonia Dragulin-Otto, Nydia Van Dyk, Melissa Damschroder, Vaheh Oganesyan, Lu Shan, Martin J Borrok, Nantaporn Haskins, Ronit Mazor, Yu Jiang, Kim Rosenthal, and William F Dall'Acqua

Subjects

QH301-705.5, Medicine (miscellaneous), Mice, Transgenic, Receptors, Fc, Protein Engineering, General Biochemistry, Genetics and Molecular Biology, Article, chemistry.chemical_compound, Mice, In vivo, Animals, Humans, Biology (General), Receptor, X-ray crystallography, Protein therapeutics, biology, Molecular medicine, Chemistry, Histocompatibility Antigens Class I, Fusion protein, Immunoglobulin Fc Fragments, Fc fusion, Monomer, biology.protein, Biophysics, Antibody, General Agricultural and Biological Sciences, Fc fragment, Half-Life

Abstract

In a biologic therapeutic landscape that requires versatility in targeting specificity, valency and half-life modulation, the monomeric Fc fusion platform holds exciting potential for the creation of a class of monovalent protein therapeutics that includes fusion proteins and bispecific targeting molecules. Here we report a structure-guided approach to engineer monomeric Fc molecules to adapt multiple versions of half-life extension modifications. Co-crystal structures of these monomeric Fc variants with Fc neonatal receptor (FcRn) shed light into the binding interactions that could serve as a guide for engineering the half-life of antibody Fc fragments. These engineered monomeric Fc molecules also enabled the generation of a novel monovalent bispecific molecular design, which translated the FcRn binding enhancement to improvement of in vivo serum half-life., Lu Shan et al. present a structure-guided approach to engineer a monovalent form of the fragment crystallizable (Fc) region of an IgG4 antibody to adapt multiple versions of half-life extension modifications and bispecific targeting. Additionally, they report co-crystal structures of the variants bound to the Fc neonatal receptor that allow insights into the binding interactions.

Published

2020

42. Use of IHF-QD Microscopic Analysis for the Detection of Food Allergenic Components: Peanuts and Wheat Protein

Author

Dani Dordevic, Marie Bartlová, Martin Hostovský, Bohuslava Tremlová, Zdeňka Javůrková, Matej Pospiech, Ludmila Kalčáková, and Hana Běhalová

Subjects

fluorophore, Health (social science), Fluorophore, quantum dots, Plant Science, lcsh:Chemical technology, medicine.disease_cause, 01 natural sciences, Health Professions (miscellaneous), Microbiology, Article, chemistry.chemical_compound, 0404 agricultural biotechnology, Allergen, Ara h1, medicine, lcsh:TP1-1185, Food allergens, Chromatography, biology, Chemistry, 010401 analytical chemistry, food and beverages, 04 agricultural and veterinary sciences, 040401 food science, Primary and secondary antibodies, 0104 chemical sciences, biology.protein, Microscopic imaging, gliadin, Gliadin, QD conjugates, Food Science, Fc fragment, allergen

Abstract

The aim of the study was to analytically evaluate quantum dots in immunohistofluorescence (IHF-QD) microscopic imaging as detectors of food allergens&mdash, peanut and wheat. The experiment was designed as two in silico experiments or simulations: (a) models of pastry samples were prepared with the addition of allergenic components (peanut and wheat protein components) and without the addition of allergenic components, and (b) positive and negative commercial samples underwent food allergen detection. The samples from both simulations were tested by the ELISA and IHF-QD microscopic methods. The primary antibodies (secondary antibodies to a rabbit Fc fragment with labeled CdSe/ZnS QD) were labelled at 525, 585, and 655 nm emissions. The use of quantum dots (QDs) has expanded to many science areas and they are also finding use in food allergen detection, as shown in the study. The study indicated that differences between the ELISA and IHF-QD microscopic methods were not observable among experimentally produced pastry samples with and without allergenic components, although differences were observed among commercial samples. The important value of the study is certainly the differences found in the application of different QD conjugates (525, 585, and 655). The highest contrast was found in the application of 585 QD conjugates that can serve for the possible quantification of present food allergens&mdash, peanuts and wheat. The study clearly emphasized that QD can be used for the qualitative detection of food allergens and can represent a reliable analytical method for food allergen detection in different food matrixes.

Published

2020

43. Computational Design of Antiangiogenic Peptibody by Fusing Human IgG1 Fc Fragment and HRH Peptide: Structural Modeling, Energetic Analysis, and Dynamics Simulation of Its Binding Potency to VEGF Receptor

Author

Lin Ning, Zhengya Bai, Shasha Hou, Zhongyan Li, Peng Zhou, Jian Huang, and Bifang He

Subjects

PbHRH, Vascular Endothelial Growth Factor A, 0301 basic medicine, Recombinant Fusion Proteins, VEGF receptors, Molecular Sequence Data, Peptide, Receptors, Fc, Computational biology, Molecular Dynamics Simulation, Applied Microbiology and Biotechnology, VEGFR, 03 medical and health sciences, Romiplostim, peptibody, Humans, Computational design, Amino Acid Sequence, Binding site, Receptor, Molecular Biology, Ecology, Evolution, Behavior and Systematics, chemistry.chemical_classification, HRH peptide, Free state, biology, Chemistry, Computational Biology, Biological activity, Cell Biology, VEGF, Immunoglobulin Fc Fragments, 030104 developmental biology, Thrombopoietin, Immunoglobulin G, biology.protein, antiangiogenesis, Research Paper, Protein Binding, Developmental Biology, Fc fragment

Abstract

Peptibodies represent a new class of biological therapeutics with combination of peptide activity and antibody-like properties. Previously, we discovered a novel peptide HRH that exhibited a dose-dependent angiogenesis-suppressing effect by targeting vascular endothelial growth factor receptors (VEGFRs). Here, we computationally designed an antiangiogenic peptibody, termed as PbHRH, by fusing the HRH peptide to human IgG1 Fc fragment using the first approved peptibody drug Romiplostim as template. The biologically active peptide of Romiplostim is similar with HRH peptide; both of them have close sequence lengths and can fold into a α-helical conformation in free state. Molecular dynamics simulations revealed that the HRH functional domain is highly flexible, which is functionally independent of Fc fragment in the designed PbHRH peptibody. Subsequently, the intermolecular interactions between VEGFR-1 domain 2 (D2) and PbHRH were predicted, clustered and refined into three representatives. Conformational analysis and energetic evaluation unraveled that the PbHRH can adopt multiple binding modes to block the native VEGF-A binding site of VEGFR-1 D2 with its HRH functional domain, although the binding effectiveness of HRH segments in peptibody context seems to be moderately decreased relative to that of free HRH peptide. Overall, it is suggested that integrating HRH peptide into PbHRH peptibody does not promote the direct intermolecular interaction between VEGFR-1 D2 and HRH. Instead, the peptibody may indirectly help to improve the pharmacokinetic profile and bioavailability of HRH.

Published

2018

44. Fc Fragment

Author

Gooch, Jan W. and Gooch, Jan W., editor

Published

2011

45. Destabilization of C2 domains in intact IgG2 is accompanied by reduced ability to inhibit complement system factor C1.

Author

Timchenko, M. and Tischenko, V.

Subjects

*IMMUNOGLOBULIN G, *MYELOMA proteins, *PROTEOLYSIS, *FLUORESCENCE spectroscopy, *TUMOR proteins, *PROTEIN metabolism

Abstract

Fc fragments (hFc) of human myeloma IgG2 proteins LOM and SIN having core hinge (Cys-Cys-Val-Glu-Cys-Pro-Pro-Cys) were first obtained by a modified proteolytic procedure. The thermostability of C2 domains inside of standard Fc, hFc fragments, and intact IgG2 LOM and SIN was studied by fluorescence spectroscopy. It was found that C2 domains of intact IgG2 are destabilized. The destabilization is accompanied by reduced ability of IgG2 to inhibit the activation of complement system by classical pathway. This could be due to the decrease in the affinity of C2 domains to factor C1q. [ABSTRACT FROM AUTHOR]

Published

2013

46. Oriented immobilized anti-hIgG via Fc fragment-imprinted PHEMA cryogel for IgG purification.

Author

Bereli, Nilay, Ertürk, Gizem, Tümer, M.Aşkın, Say, Rıdvan, and Denizli, Adil

Abstract

ABSTRACT Antibodies are used in many applications, especially as diagnostic and therapeutic agents. Among the various techniques used for the purification of antibodies, immunoaffinity chromatography is by far the most common. For this purpose, oriented immobilization of antibodies is an important step for the efficiency of purification step. In this study, Fc fragment-imprinted poly(hydroxyethyl methacrylate) cryogel (MIP) was prepared for the oriented immobilization of anti-hIgG for IgG purification from human plasma. Non-imprinted poly(hydroxyethyl methacrylate) cryogel (NIP) was also prepared for random immobilization of anti-hIgG to compare the adsorption capacities of oriented (MIP/anti-hIgG) and random (NIP/anti-hIgG) cryogel columns. The amount of immobilized anti-hIgG was 19.8 mg/g for the NIP column and 23.7 mg/g for the MIP column. Although the amount of immobilized anti-hIgG was almost the same for the NIP and MIP columns, IgG adsorption capacity was found to be three times higher than the NIP/anti-hIgG column (29.7 mg/g) for the MIP/anti-hIgG column (86.9 mg/g). Higher IgG adsorption capacity was observed from human plasma (up to 106.4 mg/g) with the MIP/anti-hIgG cryogel column. Adsorbed IgG was eluted using 1.0 m NaCl with a purity of 96.7%. The results obtained here are very encouraging and showed the usability of MIP/anti-hIgG cryogel prepared via imprinting of Fc fragments as an alternative to conventional immunoaffinity techniques for IgG purification. Copyright © 2012 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2013

47. A C-terminal interdomain disulfide bond significantly stabilizes the Fc fragment of IgG

Author

Wozniak-Knopp, Gordana and Rüker, Florian

Subjects

*DISULFIDES, *CHEMICAL bonds, *IMMUNOGLOBULIN G, *BINDING sites, *SPECTRUM analysis, *TEMPERATURE effect

Abstract

Abstract: We describe the stabilization of human IgG1 Fc by an engineered interdomain disulfide bond at the C-terminal end of the molecule. Covalently interconnecting the C-termini of the CH3 domains led to an increase of the melting temperatures by 5.6 and 9.1°C respectively as compared to CH3 domains in the context of the wild-type Fc. Combined with a recently described additional intradomain disulfide bond, both novel disulfide bonds led to an increase of the Tm by about 18.1°C to 100.7°C. The interdomain disulfide bond had no impact on the thermal stability of the CH2 domain. Far- and near-UV CD spectroscopy showed very similar overall CD profiles, indicating that secondary and tertiary structure of the Fc was not negatively affected. When introduced into an Fc fragment that had been engineered to bind to Her2/neu via a novel antigen binding site located at the C-terminus of the CH3 domain, the novel inter- and intra-domain bonds also brought about a significant increase in thermostability. Using them in combination, the Tm of the CH3 domain was raised by 18°C and thus restored to the Tm of the wild-type CH3 domain. Importantly, antigen binding of the modified Fc was not affected by the engineered disulfide bonds. [Copyright &y& Elsevier]

Published

2012

48. Correlation between CD16a binding and immuno effector functionality of an antigen specific immunoglobulin Fc fragment (Fcab)

Author

Kainer, Manuela, Antes, Bernhard, Wiederkum, Susanne, Wozniak-Knopp, Gordana, Bauer, Anton, Rüker, Florian, and Woisetschläger, Max

Subjects

*STATISTICAL correlation, *IMMUNOASSAY, *GENETIC mutation, *PROTEIN binding, *CELL membranes, *RECOMBINANT proteins

Abstract

Abstract: Antigen binding immunoglobulin Fc fragments (Fcab) are generated by engineering loop regions in the CH3 domain of human IgG1 Fc. Variants of an Fcab specific for Her-2 were designed to display either enhanced (S239D:A330L:I332E) or diminished (L234A:L235A) binding affinities to the Fc receptor CD16a based on mutations described previously. The two mutant Fcab proteins demonstrated the expected modulation of CD16a binding. Interaction with recombinant or cell surface expressed Her-2 was unaffected in both mutants compared to the parental Fcab. Binding affinities for CD16a correlated with the ADCC-potencies of the Fcab variants. Additional studies indicated that the L234A:L235A variant Fcab had equivalent structural features as the unmodified Fcab since their DSC profiles were similar and antigen binding after re-folding upon partial heat denaturation had not changed. Introduction of the S239D:A330L:I332E mutations resulted in a significant reduction of the CH2 domain melting temperature, a moderate decrease of the thermal transition of the CH3 domain and lower antigen binding after thermal stress compared to the parental Fcab. We conclude that the known correlation between CD16a binding affinity and ADCC potency is also valid in Fcab proteins and that antigen specific Fcab molecules can be further engineered for fine tuning of immuno effector functions. [Copyright &y& Elsevier]

Published

2012

49. Effect of zinc on human IgG1 and its FcγR interactions

Author

Sibéril, Sophie, Ménez, Renée, Jorieux, Sylvie, de Romeuf, Christophe, Bourel, Dominique, Fridman, Wolf-Herman, Ducancel, Frédéric, Stura, Enrico A., and Teillaud, Jean-Luc

Subjects

*ZINC, *IMMUNOGLOBULIN G, *FC receptors, *ETHYLENEDIAMINETETRAACETIC acid, *CRYSTALLOGRAPHY, *GENETIC mutation

Abstract

Abstract: In the present study, we show that histidines 310 and 435 at the CH2–CH3 interface of the Fc portion of human IgG1 can coordinate a Zn2+ and participate in the control of the CH2–CH2 interdomain opening. Structures obtained in the absence of Zn2+ have a reduced interdomain gap that likely hamper FcγR binding. This closed conformation of the Fc is stabilized by inter-CH2 domain sugar contacts. Zinc appears to counteract the sugar mediated constriction, suggesting that zinc could be an important control factor in IgG1/FcγR interactions. The results of binding studies performed in the presence of EDTA on FcγR expressing cells supports this hypothesis. When a mutated Fc fragment, in which histidines 310 and 435 have been substituted by lysines (Fc H/K), was compared with the wild-type Fc in crystallographic studies, we found that the mutations leave the interface unaltered but have a long-range effect on the CH2 interdomain separation. Moreover, these substitutions have a differential effect on the binding of IgG1 to Fcγ receptors and their functions. Interaction with the inhibitory FcγRIIB is strongly perturbed by the mutations and mutant IgG1 H/K only weakly engages this receptor. By contrast, higher affinity FcγR are mostly unaffected. [Copyright &y& Elsevier]

Published

2012

50. Fab fragments imprinted SPR biosensor for real-time human immunoglobulin G detection

Author

Ertürk, Gizem, Uzun, Lokman, Tümer, M. Aşkın, Say, Rıdvan, and Denizli, Adil

Subjects

*IMPRINTED polymers, *BIOSENSORS, *IMMUNOGLOBULIN G, *SURFACE plasmon resonance, *MOLECULAR imprinting, *POLYMERIZATION, *MONOMERS, *HYDROGEN-ion concentration

Abstract

Abstract: Fab fragments imprinted surface plasmon resonance (SPR) chip was prepared for the real-time detection of human immunoglobulin G (IgG). In order to attach polymerization precursor on SPR chip, the SPR chip surface was modified with allyl mercaptan. Fab fragments of the IgG molecules were prepared by papain digestion procedure and collected by fast protein liquid chromatography (FPLC) system using Hi-Trap_r Protein A FF column. The collected Fab fragments were complexed with histidine containing specific monomer, N-methacryloyl-l-histidine methyl ester (MAH). Molecular imprinted polymeric nanofilm was prepared on SPR chip in the presence of ethylene glycol dimethacrylate and 2-hydroxyethylmethacrylate. The template molecules, Fab fragments, were removed from the polymeric nanofilm using 1M NaCl solution (pH: 7.4, phosphate buffer system). The molecular imprinted SPR chip was characterized by contact angle, atomic force microscopy and Fourier transform infrared spectroscopy. By the real-time IgG detection studies carried out using aqueous IgG solutions in different concentrations, the kinetics and isotherm parameters of the molecular imprinted SPR chip–IgG system were calculated. To show selectivity and specificity of the molecular imprinted SPR chip, competitive kinetic analyses were performed using bovine serum albumin (BSA), IgG, Fab and Fc fragments in singular and competitive manner. As last step, IgG detection studies from human plasma were performed and the measured IgG concentrations were well matched with the results determined by enzyme-linked immunosorbent assay (ELISA). The results obtained with the molecular imprinted SPR chip were well fitted to Langmuir isotherm and the detection limit was found as 56ng/mL. In the light of the results, we can conclude that the proposed molecular imprinted SPR chip can detect IgG molecules from both aqueous solutions and complex natural samples. [Copyright &y& Elsevier]

Published

2011