Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III

Using three different Fcγ receptor (FcγR)-deficient mouse strains, we examined the induction of autoimmune hemolytic anemia by each of the four immunoglobulin (Ig)G isotype-switch variants of a 4C8 IgM antierythrocyte autoantibody and its relation to the contributions of the two FcγR, FcγRI, and Fcγ...

Descripción completa

Detalles Bibliográficos
Autores principales: Fossati-Jimack, Liliane, Ioan-Facsinay, Andreea, Reininger, Luc, Chicheportiche, Yves, Watanabe, Norihiko, Saito, Takashi, Hofhuis, Frans M. A., Gessner, J. Engelbert, Schiller, Carsten, Schmidt, Reinhold E., Honjo, Tasuku, Verbeek, J. Sjef, Izui, Shozo
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2000
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2193130/
https://www.ncbi.nlm.nih.gov/pubmed/10770797
_version_ 1782147398238208000
author Fossati-Jimack, Liliane
Ioan-Facsinay, Andreea
Reininger, Luc
Chicheportiche, Yves
Watanabe, Norihiko
Saito, Takashi
Hofhuis, Frans M. A.
Gessner, J. Engelbert
Schiller, Carsten
Schmidt, Reinhold E.
Honjo, Tasuku
Verbeek, J. Sjef
Izui, Shozo
author_facet Fossati-Jimack, Liliane
Ioan-Facsinay, Andreea
Reininger, Luc
Chicheportiche, Yves
Watanabe, Norihiko
Saito, Takashi
Hofhuis, Frans M. A.
Gessner, J. Engelbert
Schiller, Carsten
Schmidt, Reinhold E.
Honjo, Tasuku
Verbeek, J. Sjef
Izui, Shozo
author_sort Fossati-Jimack, Liliane
collection PubMed
description Using three different Fcγ receptor (FcγR)-deficient mouse strains, we examined the induction of autoimmune hemolytic anemia by each of the four immunoglobulin (Ig)G isotype-switch variants of a 4C8 IgM antierythrocyte autoantibody and its relation to the contributions of the two FcγR, FcγRI, and FcγRIII, operative in the phagocytosis of opsonized particles. We found that the four IgG isotypes of this antibody displayed striking differences in pathogenicity, which were related to their respective capacity to interact in vivo with the two phagocytic FcγRs, defined as follows: IgG2a > IgG2b > IgG3/IgG1 for FcγRI, and IgG2a > IgG1 > IgG2b > IgG3 for FcγRIII. Accordingly, the IgG2a autoantibody exhibited the highest pathogenicity, ∼20–100-fold more potent than its IgG1 and IgG2b variants, respectively, while the IgG3 variant, which displays little interaction with these FcγRs, was not pathogenic at all. An unexpected critical role of the low-affinity FcγRIII was revealed by the use of two different IgG2a anti–red blood cell autoantibodies, which displayed a striking preferential utilization of FcγRIII, compared with the high-affinity FcγRI. This demonstration of the respective roles in vivo of four different IgG isotypes, and of two phagocytic FcγRs, in autoimmune hemolytic anemia highlights the major importance of the regulation of IgG isotype responses in autoantibody-mediated pathology and humoral immunity.
format Text
id pubmed-2193130
institution National Center for Biotechnology Information
language English
publishDate 2000
publisher The Rockefeller University Press
record_format MEDLINE/PubMed
spelling pubmed-21931302008-04-16 Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III Fossati-Jimack, Liliane Ioan-Facsinay, Andreea Reininger, Luc Chicheportiche, Yves Watanabe, Norihiko Saito, Takashi Hofhuis, Frans M. A. Gessner, J. Engelbert Schiller, Carsten Schmidt, Reinhold E. Honjo, Tasuku Verbeek, J. Sjef Izui, Shozo J Exp Med Original Article Using three different Fcγ receptor (FcγR)-deficient mouse strains, we examined the induction of autoimmune hemolytic anemia by each of the four immunoglobulin (Ig)G isotype-switch variants of a 4C8 IgM antierythrocyte autoantibody and its relation to the contributions of the two FcγR, FcγRI, and FcγRIII, operative in the phagocytosis of opsonized particles. We found that the four IgG isotypes of this antibody displayed striking differences in pathogenicity, which were related to their respective capacity to interact in vivo with the two phagocytic FcγRs, defined as follows: IgG2a > IgG2b > IgG3/IgG1 for FcγRI, and IgG2a > IgG1 > IgG2b > IgG3 for FcγRIII. Accordingly, the IgG2a autoantibody exhibited the highest pathogenicity, ∼20–100-fold more potent than its IgG1 and IgG2b variants, respectively, while the IgG3 variant, which displays little interaction with these FcγRs, was not pathogenic at all. An unexpected critical role of the low-affinity FcγRIII was revealed by the use of two different IgG2a anti–red blood cell autoantibodies, which displayed a striking preferential utilization of FcγRIII, compared with the high-affinity FcγRI. This demonstration of the respective roles in vivo of four different IgG isotypes, and of two phagocytic FcγRs, in autoimmune hemolytic anemia highlights the major importance of the regulation of IgG isotype responses in autoantibody-mediated pathology and humoral immunity. The Rockefeller University Press 2000-04-17 /pmc/articles/PMC2193130/ /pubmed/10770797 Text en © 2000 The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Original Article
Fossati-Jimack, Liliane
Ioan-Facsinay, Andreea
Reininger, Luc
Chicheportiche, Yves
Watanabe, Norihiko
Saito, Takashi
Hofhuis, Frans M. A.
Gessner, J. Engelbert
Schiller, Carsten
Schmidt, Reinhold E.
Honjo, Tasuku
Verbeek, J. Sjef
Izui, Shozo
Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III
title Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III
title_full Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III
title_fullStr Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III
title_full_unstemmed Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III
title_short Markedly Different Pathogenicity of Four Immunoglobulin G Isotype-Switch Variants of an Antierythrocyte Autoantibody Is Based on Their Capacity to Interact in Vivo with the Low-Affinity Fcγ Receptor III
title_sort markedly different pathogenicity of four immunoglobulin g isotype-switch variants of an antierythrocyte autoantibody is based on their capacity to interact in vivo with the low-affinity fcγ receptor iii
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2193130/
https://www.ncbi.nlm.nih.gov/pubmed/10770797
work_keys_str_mv AT fossatijimackliliane markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT ioanfacsinayandreea markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT reiningerluc markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT chicheporticheyves markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT watanabenorihiko markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT saitotakashi markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT hofhuisfransma markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT gessnerjengelbert markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT schillercarsten markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT schmidtreinholde markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT honjotasuku markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT verbeekjsjef markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii
AT izuishozo markedlydifferentpathogenicityoffourimmunoglobulingisotypeswitchvariantsofanantierythrocyteautoantibodyisbasedontheircapacitytointeractinvivowiththelowaffinityfcgreceptoriii

Ejemplares similares