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Development of a highly effective combination monoclonal antibody therapy against Herpes simplex virus
by
Kalbermatter, David
, Diebolder, Philipp
, Arndt, Michaela
, Seyfizadeh, Narges
, Ries, Moritz
, Krauss, Jürgen
, Yendrzheyevskiy, Alexandra
, Chami, Mohamed
, Blumenschein, Elisabeth
, Müller, Christian
, Imhof, Thomas
, Moog, Kevin
, Jenner, Leonie
, Engel, Ronja
, Grün, Frank
, Schaller, Torsten
, Eckert, Daniel
in
Analysis
/ Animals
/ Antibodies, Monoclonal - immunology
/ Antibodies, Monoclonal - pharmacology
/ Antibodies, Viral - immunology
/ Antigen-antibody complexes
/ Antigen-presenting cells
/ Antigenic determinants
/ Antigens
/ Antiviral agents
/ Antiviral drugs
/ B cells
/ Binding
/ Biomedical and Life Sciences
/ Biomedicine
/ Biopharmaceutics
/ Cell activation
/ Cell surface
/ Cells
/ Clinical trials
/ Combination therapy
/ Disease
/ Endosomes
/ Epitopes
/ Fab
/ Female
/ Glycoprotein B (gB)
/ Health aspects
/ Herpes simplex
/ Herpes Simplex - drug therapy
/ Herpes Simplex - immunology
/ Herpes Simplex - therapy
/ Herpes simplex virus
/ Herpes simplex virus (HSV)
/ Herpes viruses
/ Herpesvirus 1, Human - drug effects
/ Herpesvirus 1, Human - immunology
/ Herpesvirus 2, Human - drug effects
/ Herpesvirus 2, Human - immunology
/ Humans
/ Immunoglobulin G
/ Immunology
/ Immunotherapy
/ Infection
/ Infections
/ Interferometry
/ Internalization
/ Lymphocytes T
/ Medical research
/ Medicine, Experimental
/ Mice
/ Mice, Inbred BALB C
/ Monoclonal antibodies
/ Mortality
/ Neutralization
/ Phage display
/ Phagocytosis
/ Skin
/ Synergistic effect
/ T cells
/ Therapeutic monoclonal antibody
/ Therapy
/ Vagina
/ Viruses
2024
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Development of a highly effective combination monoclonal antibody therapy against Herpes simplex virus
by
Kalbermatter, David
, Diebolder, Philipp
, Arndt, Michaela
, Seyfizadeh, Narges
, Ries, Moritz
, Krauss, Jürgen
, Yendrzheyevskiy, Alexandra
, Chami, Mohamed
, Blumenschein, Elisabeth
, Müller, Christian
, Imhof, Thomas
, Moog, Kevin
, Jenner, Leonie
, Engel, Ronja
, Grün, Frank
, Schaller, Torsten
, Eckert, Daniel
in
Analysis
/ Animals
/ Antibodies, Monoclonal - immunology
/ Antibodies, Monoclonal - pharmacology
/ Antibodies, Viral - immunology
/ Antigen-antibody complexes
/ Antigen-presenting cells
/ Antigenic determinants
/ Antigens
/ Antiviral agents
/ Antiviral drugs
/ B cells
/ Binding
/ Biomedical and Life Sciences
/ Biomedicine
/ Biopharmaceutics
/ Cell activation
/ Cell surface
/ Cells
/ Clinical trials
/ Combination therapy
/ Disease
/ Endosomes
/ Epitopes
/ Fab
/ Female
/ Glycoprotein B (gB)
/ Health aspects
/ Herpes simplex
/ Herpes Simplex - drug therapy
/ Herpes Simplex - immunology
/ Herpes Simplex - therapy
/ Herpes simplex virus
/ Herpes simplex virus (HSV)
/ Herpes viruses
/ Herpesvirus 1, Human - drug effects
/ Herpesvirus 1, Human - immunology
/ Herpesvirus 2, Human - drug effects
/ Herpesvirus 2, Human - immunology
/ Humans
/ Immunoglobulin G
/ Immunology
/ Immunotherapy
/ Infection
/ Infections
/ Interferometry
/ Internalization
/ Lymphocytes T
/ Medical research
/ Medicine, Experimental
/ Mice
/ Mice, Inbred BALB C
/ Monoclonal antibodies
/ Mortality
/ Neutralization
/ Phage display
/ Phagocytosis
/ Skin
/ Synergistic effect
/ T cells
/ Therapeutic monoclonal antibody
/ Therapy
/ Vagina
/ Viruses
2024
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Development of a highly effective combination monoclonal antibody therapy against Herpes simplex virus
by
Kalbermatter, David
, Diebolder, Philipp
, Arndt, Michaela
, Seyfizadeh, Narges
, Ries, Moritz
, Krauss, Jürgen
, Yendrzheyevskiy, Alexandra
, Chami, Mohamed
, Blumenschein, Elisabeth
, Müller, Christian
, Imhof, Thomas
, Moog, Kevin
, Jenner, Leonie
, Engel, Ronja
, Grün, Frank
, Schaller, Torsten
, Eckert, Daniel
in
Analysis
/ Animals
/ Antibodies, Monoclonal - immunology
/ Antibodies, Monoclonal - pharmacology
/ Antibodies, Viral - immunology
/ Antigen-antibody complexes
/ Antigen-presenting cells
/ Antigenic determinants
/ Antigens
/ Antiviral agents
/ Antiviral drugs
/ B cells
/ Binding
/ Biomedical and Life Sciences
/ Biomedicine
/ Biopharmaceutics
/ Cell activation
/ Cell surface
/ Cells
/ Clinical trials
/ Combination therapy
/ Disease
/ Endosomes
/ Epitopes
/ Fab
/ Female
/ Glycoprotein B (gB)
/ Health aspects
/ Herpes simplex
/ Herpes Simplex - drug therapy
/ Herpes Simplex - immunology
/ Herpes Simplex - therapy
/ Herpes simplex virus
/ Herpes simplex virus (HSV)
/ Herpes viruses
/ Herpesvirus 1, Human - drug effects
/ Herpesvirus 1, Human - immunology
/ Herpesvirus 2, Human - drug effects
/ Herpesvirus 2, Human - immunology
/ Humans
/ Immunoglobulin G
/ Immunology
/ Immunotherapy
/ Infection
/ Infections
/ Interferometry
/ Internalization
/ Lymphocytes T
/ Medical research
/ Medicine, Experimental
/ Mice
/ Mice, Inbred BALB C
/ Monoclonal antibodies
/ Mortality
/ Neutralization
/ Phage display
/ Phagocytosis
/ Skin
/ Synergistic effect
/ T cells
/ Therapeutic monoclonal antibody
/ Therapy
/ Vagina
/ Viruses
2024
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Development of a highly effective combination monoclonal antibody therapy against Herpes simplex virus
Journal Article
Development of a highly effective combination monoclonal antibody therapy against Herpes simplex virus
2024
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Overview
Background
Infections with Herpes simplex virus (HSV)-1 or -2 usually present as mild chronic recurrent disease, however in rare cases can result in life-threatening conditions with a large spectrum of pathology. Monoclonal antibody therapy has great potential especially to treat infections with virus resistant to standard therapies. HDIT101, a humanized IgG targeting HSV-1/2 gB was previously investigated in phase 2 clinical trials. The aim of this study was to develop a next-generation therapy by combining different antiviral monoclonal antibodies.
Methods
A lymph-node derived phage display library (LYNDAL) was screened against recombinant gB from Herpes simplex virus (HSV) -1 and HDIT102 scFv was selected for its binding characteristics using bio-layer interferometry. HDIT102 was further developed as fully human IgG and tested alone or in combination with HDIT101, a clinically tested humanized anti-HSV IgG, in vitro and in vivo. T-cell stimulating activities by antigen-presenting cells treated with IgG-HSV immune complexes were analyzed using primary human cells. To determine the epitopes, the cryo-EM structures of HDIT101 or HDIT102 Fab bound to HSV-1F as well as HSV-2G gB protein were solved at resolutions < 3.5 Å.
Results
HDIT102 Fab showed strong binding to HSV-1F gB with Kd of 8.95 × 10
–11
M and to HSV-2G gB with Kd of 3.29 × 10
–11
M. Neutralization of cell-free virus and inhibition of cell-to-cell spread were comparable between HDIT101 and HDIT102. Both antibodies induced internalization of gB from the cell surface into acidic endosomes by binding distinct epitopes in domain I of gB and compete for binding. CryoEM analyses revealed the ability to form heterogenic immune complexes consisting of two HDIT102 and one HDIT101 Fab bound to one gB trimeric molecule. Both antibodies mediated antibody-dependent phagocytosis by antigen presenting cells which stimulated autologous T-cell activation. In vivo, the combination of HDIT101 and HDIT102 demonstrated synergistic effects on survival and clinical outcome in immunocompetent BALB/cOlaHsd mice.
Conclusion
This biochemical and immunological study showcases the potential of an effective combination therapy with two monoclonal anti-gB IgGs for the treatment of HSV-1/2 induced disease conditions.
Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
Subject
/ Animals
/ Antibodies, Monoclonal - immunology
/ Antibodies, Monoclonal - pharmacology
/ Antibodies, Viral - immunology
/ Antigens
/ B cells
/ Binding
/ Biomedical and Life Sciences
/ Cells
/ Disease
/ Epitopes
/ Fab
/ Female
/ Herpes Simplex - drug therapy
/ Herpesvirus 1, Human - drug effects
/ Herpesvirus 1, Human - immunology
/ Herpesvirus 2, Human - drug effects
/ Herpesvirus 2, Human - immunology
/ Humans
/ Mice
/ Skin
/ T cells
/ Therapeutic monoclonal antibody
/ Therapy
/ Vagina
/ Viruses
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