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Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies

Mouse immunoglobulins M (IgMs) that recognize human blood group antigens induce haemagglutination and are used worldwide for diagnostic blood typing. Contrary to the current belief that IgGs are too small to simultaneously bind antigens on two different erythrocytes, we obtained agglutinating mouse...

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Autores principales: Klaus, Tomasz, Bzowska, Monika, Kulesza, Małgorzata, Kabat, Agnieszka Martyna, Jemioła-Rzemińska, Małgorzata, Czaplicki, Dominik, Makuch, Krzysztof, Jucha, Jarosław, Karabasz, Alicja, Bereta, Joanna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4971511/
https://www.ncbi.nlm.nih.gov/pubmed/27484487
http://dx.doi.org/10.1038/srep30938
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author Klaus, Tomasz
Bzowska, Monika
Kulesza, Małgorzata
Kabat, Agnieszka Martyna
Jemioła-Rzemińska, Małgorzata
Czaplicki, Dominik
Makuch, Krzysztof
Jucha, Jarosław
Karabasz, Alicja
Bereta, Joanna
author_facet Klaus, Tomasz
Bzowska, Monika
Kulesza, Małgorzata
Kabat, Agnieszka Martyna
Jemioła-Rzemińska, Małgorzata
Czaplicki, Dominik
Makuch, Krzysztof
Jucha, Jarosław
Karabasz, Alicja
Bereta, Joanna
author_sort Klaus, Tomasz
collection PubMed
description Mouse immunoglobulins M (IgMs) that recognize human blood group antigens induce haemagglutination and are used worldwide for diagnostic blood typing. Contrary to the current belief that IgGs are too small to simultaneously bind antigens on two different erythrocytes, we obtained agglutinating mouse IgG3 that recognized antigen B of the human ABO blood group system. Mouse IgG3 is an intriguing isotype that has the ability to form Fc-dependent oligomers. However, F(ab′)(2) fragments of the IgG3 were sufficient to agglutinate type B red blood cells; therefore, IgG3-triggered agglutination did not require oligomerization. Molecular modelling indicated that mouse IgG3 has a larger range of Fab arms than other mouse IgG subclasses and that the unique properties of mouse IgG3 are likely due to the structure of its hinge region. With a focus on applications in diagnostics, we compared the stability of IgG3 and two IgMs in formulated blood typing reagents using an accelerated storage approach and differential scanning calorimetry. IgG3 was much more stable than IgMs. Interestingly, the rapid decrease in IgM activity was caused by aggregation of the molecules and a previously unknown posttranslational proteolytic processing of the μ heavy chain. Our data point to mouse IgG3 as a potent diagnostic tool.
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spelling pubmed-49715112016-08-11 Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies Klaus, Tomasz Bzowska, Monika Kulesza, Małgorzata Kabat, Agnieszka Martyna Jemioła-Rzemińska, Małgorzata Czaplicki, Dominik Makuch, Krzysztof Jucha, Jarosław Karabasz, Alicja Bereta, Joanna Sci Rep Article Mouse immunoglobulins M (IgMs) that recognize human blood group antigens induce haemagglutination and are used worldwide for diagnostic blood typing. Contrary to the current belief that IgGs are too small to simultaneously bind antigens on two different erythrocytes, we obtained agglutinating mouse IgG3 that recognized antigen B of the human ABO blood group system. Mouse IgG3 is an intriguing isotype that has the ability to form Fc-dependent oligomers. However, F(ab′)(2) fragments of the IgG3 were sufficient to agglutinate type B red blood cells; therefore, IgG3-triggered agglutination did not require oligomerization. Molecular modelling indicated that mouse IgG3 has a larger range of Fab arms than other mouse IgG subclasses and that the unique properties of mouse IgG3 are likely due to the structure of its hinge region. With a focus on applications in diagnostics, we compared the stability of IgG3 and two IgMs in formulated blood typing reagents using an accelerated storage approach and differential scanning calorimetry. IgG3 was much more stable than IgMs. Interestingly, the rapid decrease in IgM activity was caused by aggregation of the molecules and a previously unknown posttranslational proteolytic processing of the μ heavy chain. Our data point to mouse IgG3 as a potent diagnostic tool. Nature Publishing Group 2016-08-03 /pmc/articles/PMC4971511/ /pubmed/27484487 http://dx.doi.org/10.1038/srep30938 Text en Copyright © 2016, The Author(s) http://creativecommons.org/licenses/by/4.0/ This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/
spellingShingle Article
Klaus, Tomasz
Bzowska, Monika
Kulesza, Małgorzata
Kabat, Agnieszka Martyna
Jemioła-Rzemińska, Małgorzata
Czaplicki, Dominik
Makuch, Krzysztof
Jucha, Jarosław
Karabasz, Alicja
Bereta, Joanna
Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies
title Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies
title_full Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies
title_fullStr Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies
title_full_unstemmed Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies
title_short Agglutinating mouse IgG3 compares favourably with IgMs in typing of the blood group B antigen: Functionality and stability studies
title_sort agglutinating mouse igg3 compares favourably with igms in typing of the blood group b antigen: functionality and stability studies
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4971511/
https://www.ncbi.nlm.nih.gov/pubmed/27484487
http://dx.doi.org/10.1038/srep30938
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