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A monoclonal antibody with anti-D-like activity in murine immune thrombocytopenia requires Fc domain function for immune thrombocytopenia ameliorative effects

A monoclonal antibody with anti-D-like activity in murine immune thrombocytopenia requires Fc domain function for immune thrombocytopenia ameliorative effects
A monoclonal antibody with anti-D-like activity in murine immune thrombocytopenia requires Fc domain function for immune thrombocytopenia ameliorative effects

BACKGROUND The mechanism of action of anti-D in ameliorating immune thrombocytopenia (ITP) remains unclear. The monoclonal antibody (MoAb) Ter119, which targets murine red blood cells (RBCs), has been shown to mimic the effect of anti-D in improving antibody-mediated murine ITP. The mechanism of Ter119-mediated ITP amelioration, especially the role of the antigen-binding and Fc domains, remains untested. A functional Fc domain is crucial for many therapeutic MoAb activity; therefore, the requirement of Ter119 Fc domain in ITP amelioration is investigated using outbred CD-1 mice.

STUDY DESIGN AND METHODS Ter119 variants, including Ter119 F(ab′)2 fragments, deglycosylated Ter119, and afucosylated Ter119, were generated to test their effect in ameliorating antibody-induced murine ITP. In vivo inhibition of FcγRIII and FcγRIIB was achieved using the Fab fragment of the FcγRIII/FcγRIIB-specific MoAb 2.4G2.

RESULTS Ter119 F(ab′)2 fragments and deglycosylated Ter119 were unable to ameliorate murine ITP or mediate phagocytosis of RBCs by RAW264.7 macrophages in vitro. Inhibition of FcγRIII and FcγRIIB, as well as Ter119 defucosylation, do not affect Ter119-mediated ITP amelioration. CONCLUSION The Fc domain of Ter119, as well as its Fc glycosylation, is required for Ter119-mediated ITP amelioration. Moreover, both Fc and Fc glycosylation are required for Ter119-mediated phagocytosis in vitro. These findings demonstrate the importance of the Fc domain in a therapeutic MoAb with anti-D-like activity.

1537-2995
1501-1511
Yu, Xiaojie
44d52374-eacc-4e23-b7da-c881e6d3a5dd
Menard, Melissa
199dda93-7705-43b9-a96d-3dfcde6a92a0
Seabright, Gemma
09e75998-09b0-465f-a059-c89b07f3b2c3
Crispin, Max
cd980957-0943-4b89-b2b2-710f01f33bc9
Lazarus, Alan H.
eecf3844-9875-4fc1-b9a7-b6d26bcb0758
Yu, Xiaojie
44d52374-eacc-4e23-b7da-c881e6d3a5dd
Menard, Melissa
199dda93-7705-43b9-a96d-3dfcde6a92a0
Seabright, Gemma
09e75998-09b0-465f-a059-c89b07f3b2c3
Crispin, Max
cd980957-0943-4b89-b2b2-710f01f33bc9
Lazarus, Alan H.
eecf3844-9875-4fc1-b9a7-b6d26bcb0758

Yu, Xiaojie, Menard, Melissa, Seabright, Gemma, Crispin, Max and Lazarus, Alan H. (2015) A monoclonal antibody with anti-D-like activity in murine immune thrombocytopenia requires Fc domain function for immune thrombocytopenia ameliorative effects. Transfusion, 55 (6), 1501-1511. (doi:10.1111/trf.13032).

Record type: Article

Abstract

BACKGROUND The mechanism of action of anti-D in ameliorating immune thrombocytopenia (ITP) remains unclear. The monoclonal antibody (MoAb) Ter119, which targets murine red blood cells (RBCs), has been shown to mimic the effect of anti-D in improving antibody-mediated murine ITP. The mechanism of Ter119-mediated ITP amelioration, especially the role of the antigen-binding and Fc domains, remains untested. A functional Fc domain is crucial for many therapeutic MoAb activity; therefore, the requirement of Ter119 Fc domain in ITP amelioration is investigated using outbred CD-1 mice.

STUDY DESIGN AND METHODS Ter119 variants, including Ter119 F(ab′)2 fragments, deglycosylated Ter119, and afucosylated Ter119, were generated to test their effect in ameliorating antibody-induced murine ITP. In vivo inhibition of FcγRIII and FcγRIIB was achieved using the Fab fragment of the FcγRIII/FcγRIIB-specific MoAb 2.4G2.

RESULTS Ter119 F(ab′)2 fragments and deglycosylated Ter119 were unable to ameliorate murine ITP or mediate phagocytosis of RBCs by RAW264.7 macrophages in vitro. Inhibition of FcγRIII and FcγRIIB, as well as Ter119 defucosylation, do not affect Ter119-mediated ITP amelioration. CONCLUSION The Fc domain of Ter119, as well as its Fc glycosylation, is required for Ter119-mediated ITP amelioration. Moreover, both Fc and Fc glycosylation are required for Ter119-mediated phagocytosis in vitro. These findings demonstrate the importance of the Fc domain in a therapeutic MoAb with anti-D-like activity.

Text
2015-A monoclonal antibody with anti-D–like activity in murine immune thrombocytopenia requires Fc domain function for immune thrombocytopenia ameliorative effects
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Accepted/In Press date: 31 December 2014
e-pub ahead of print date: 6 March 2015
Published date: 1 June 2015

Identifiers

Local EPrints ID: 414315
URI: http://eprints.soton.ac.uk/id/eprint/414315
DOI: doi:10.1111/trf.13032
ISSN: 1537-2995
PURE UUID: 7e6c2f59-13e7-418f-b5d9-864d0f8205cb
ORCID for Max Crispin: ORCID iD orcid.org/0000-0002-1072-2694

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Date deposited: 26 Sep 2017 16:30
Last modified: 16 Mar 2024 04:30

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Contributors

Author: Xiaojie Yu
Author: Melissa Menard
Author: Gemma Seabright
Author: Max Crispin ORCID iD
Author: Alan H. Lazarus

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