IgG Subclass-Dependent Pulmonary Antigen Retention during Acute IgG-Dependent Systemic Anaphylaxis in Mice

Biliana Todorova; Ophélie Godon; Eva Conde; Caitlin M. Gillis; Bruno Iannascoli; Odile Richard-Le Goff; Daniel Fiole; Lubka T. Roumenina; Jeanette H.W. Leusen; Andrew J. Murphy; Lynn E. Macdonald; Laurent L. Reber; Friederike Jönsson; Pierre Bruhns

doi:10.4049/jimmunol.2200234

IgG Subclass-Dependent Pulmonary Antigen Retention during Acute IgG-Dependent Systemic Anaphylaxis in Mice

Biliana Todorova, Ophélie Godon, Eva Conde, Caitlin M. Gillis, Bruno Iannascoli, Odile Richard-Le Goff, Daniel Fiole, Lubka T. Roumenina, Jeanette H.W. Leusen, Andrew J. Murphy, Lynn E. Macdonald, Laurent L. Reber, Friederike Jönsson, Pierre Bruhns^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Mouse models of active systemic anaphylaxis rely predominantly on IgG Abs forming IgG-allergen immune complexes that induce IgG receptor-expressing neutrophils and monocytes/macrophages to release potent mediators, leading to systemic effects. Whether anaphylaxis initiates locally or systemically remains unknown. In this study, we aimed at identifying the anatomical location of IgG-allergen immune complexes during anaphylaxis. Active systemic anaphylaxis was induced following immunization with BSA and i.v. challenge with fluorescently labeled BSA. Ag retention across different organs was examined using whole-body fluorescence imaging, comparing immunized and naive animals. Various mouse models and in vivo deletion strategies were employed to determine the contribution of IgG receptors, complement component C1q, myeloid cell types, and anaphylaxis mediators. We found that following challenge, Ag diffused systemically, but specifically accumulated in the lungs of mice sensitized to that Ag, where it formed large Ab-dependent aggregates in the vasculature. Ag retention in the lungs did not rely on IgG receptors, C1q, neutrophils, or macrophages. IgG2a-mediated, but neither IgG1- nor IgG2b-mediated, passive systemic anaphylaxis led to Ag retention in the lung. Neutrophils and monocytes significantly accumulated in the lungs after challenge and captured high amounts of Ag, which led to downmodulation of surface IgG receptors and triggered their activation. Thus, within minutes of systemic injection in sensitized mice, Ag formed aggregates in the lung and liver vasculature, but accumulated specifically and dose-dependently in the lung. Neutrophils and monocytes recruited to the lung captured Ag and became activated. However, Ag aggregation in the lung vasculature was not necessary for anaphylaxis induction.

Original language	English
Pages (from-to)	1243-1251
Number of pages	9
Journal	Journal of immunology (Baltimore, Md. : 1950)
Volume	209
Issue number	7
DOIs	https://doi.org/10.4049/jimmunol.2200234
Publication status	Published - 1 Oct 2022

Keywords

Allergens
Anaphylaxis
Animals
Antigen-Antibody Complex
Complement C1q
Disease Models, Animal
Immunoglobulin G
Lung
Mice
Mice, Inbred C57BL
Receptors, Complement
Receptors, IgG

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10.4049/jimmunol.2200234

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Todorova, B., Godon, O., Conde, E., Gillis, C. M., Iannascoli, B., Richard-Le Goff, O., Fiole, D., Roumenina, L. T., Leusen, J. H. W., Murphy, A. J., Macdonald, L. E., Reber, L. L., Jönsson, F., & Bruhns, P. (2022). IgG Subclass-Dependent Pulmonary Antigen Retention during Acute IgG-Dependent Systemic Anaphylaxis in Mice. Journal of immunology (Baltimore, Md. : 1950), 209(7), 1243-1251. https://doi.org/10.4049/jimmunol.2200234

@article{79e2d38c123c460596c43f8da0042f89,

title = "IgG Subclass-Dependent Pulmonary Antigen Retention during Acute IgG-Dependent Systemic Anaphylaxis in Mice",

abstract = "Mouse models of active systemic anaphylaxis rely predominantly on IgG Abs forming IgG-allergen immune complexes that induce IgG receptor-expressing neutrophils and monocytes/macrophages to release potent mediators, leading to systemic effects. Whether anaphylaxis initiates locally or systemically remains unknown. In this study, we aimed at identifying the anatomical location of IgG-allergen immune complexes during anaphylaxis. Active systemic anaphylaxis was induced following immunization with BSA and i.v. challenge with fluorescently labeled BSA. Ag retention across different organs was examined using whole-body fluorescence imaging, comparing immunized and naive animals. Various mouse models and in vivo deletion strategies were employed to determine the contribution of IgG receptors, complement component C1q, myeloid cell types, and anaphylaxis mediators. We found that following challenge, Ag diffused systemically, but specifically accumulated in the lungs of mice sensitized to that Ag, where it formed large Ab-dependent aggregates in the vasculature. Ag retention in the lungs did not rely on IgG receptors, C1q, neutrophils, or macrophages. IgG2a-mediated, but neither IgG1- nor IgG2b-mediated, passive systemic anaphylaxis led to Ag retention in the lung. Neutrophils and monocytes significantly accumulated in the lungs after challenge and captured high amounts of Ag, which led to downmodulation of surface IgG receptors and triggered their activation. Thus, within minutes of systemic injection in sensitized mice, Ag formed aggregates in the lung and liver vasculature, but accumulated specifically and dose-dependently in the lung. Neutrophils and monocytes recruited to the lung captured Ag and became activated. However, Ag aggregation in the lung vasculature was not necessary for anaphylaxis induction.",

keywords = "Allergens, Anaphylaxis, Animals, Antigen-Antibody Complex, Complement C1q, Disease Models, Animal, Immunoglobulin G, Lung, Mice, Mice, Inbred C57BL, Receptors, Complement, Receptors, IgG",

author = "Biliana Todorova and Oph{\'e}lie Godon and Eva Conde and Gillis, {Caitlin M.} and Bruno Iannascoli and {Richard-Le Goff}, Odile and Daniel Fiole and Roumenina, {Lubka T.} and Leusen, {Jeanette H.W.} and Murphy, {Andrew J.} and Macdonald, {Lynn E.} and Reber, {Laurent L.} and Friederike J{\"o}nsson and Pierre Bruhns",

note = "Funding Information: This work was supported by European Research Council (ERC)–Seventh Framework Program Grant ERC-2013-CoG 616050; additional support was provided by the Institut Pasteur and the Institut National de la Sant{\'e} et de la Recherche M{\'e}dicale (INSERM). C.M.G. was supported partly by a stipend from the Pasteur–Paris University International PhD program and by the Institut Carnot Pasteur Maladies Infectieuses. F.J. is an employee of the CNRS. None of the sources of funding has an interest in the subject matter or materials discussed in the submitted manuscript. Funding Information: This work was supported by European Research Council (ERC)-Seventh Framework Program Grant ERC-2013-CoG 616050; additional support was provided by the Institut Pasteur and the Institut National de la Sant{\'e} et de la Recherche M{\'e}dicale (INSERM). C.M.G. was supported partly by a stipend from the Pasteur-Paris University International PhD program and by the Institut Carnot Pasteur Maladies Infectieuses. F.J. is an employee of the CNRS. None of the sources of funding has an interest in the subject matter or materials discussed in the submitted manuscript. We thank D. Sinnaya for administrative help (Institut Pasteur, Paris, France). We also thank Prof. Marina Botto (Imperial College London, London, U.K.) for supplying C1qKO mice. We thank Dr. Gr{\'e}gory Jouvion (Ecole Nationale V{\'e}t{\'e}rinaire d'Alfort, Maisons-Alfort, France) for help with histological analyses. Publisher Copyright: {\textcopyright} 2022 by The American Association of Immunologists, Inc.",

year = "2022",

month = oct,

day = "1",

doi = "10.4049/jimmunol.2200234",

language = "English",

volume = "209",

pages = "1243--1251",

journal = "Journal of immunology (Baltimore, Md. : 1950)",

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publisher = "American Association of Immunologists",

number = "7",

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Todorova, B, Godon, O, Conde, E, Gillis, CM, Iannascoli, B, Richard-Le Goff, O, Fiole, D, Roumenina, LT, Leusen, JHW, Murphy, AJ, Macdonald, LE, Reber, LL, Jönsson, F & Bruhns, P 2022, 'IgG Subclass-Dependent Pulmonary Antigen Retention during Acute IgG-Dependent Systemic Anaphylaxis in Mice', Journal of immunology (Baltimore, Md. : 1950), vol. 209, no. 7, pp. 1243-1251. https://doi.org/10.4049/jimmunol.2200234

TY - JOUR

T1 - IgG Subclass-Dependent Pulmonary Antigen Retention during Acute IgG-Dependent Systemic Anaphylaxis in Mice

AU - Todorova, Biliana

AU - Godon, Ophélie

AU - Conde, Eva

AU - Gillis, Caitlin M.

AU - Iannascoli, Bruno

AU - Richard-Le Goff, Odile

AU - Fiole, Daniel

AU - Roumenina, Lubka T.

AU - Leusen, Jeanette H.W.

AU - Murphy, Andrew J.

AU - Macdonald, Lynn E.

AU - Reber, Laurent L.

AU - Jönsson, Friederike

AU - Bruhns, Pierre

N1 - Funding Information: This work was supported by European Research Council (ERC)–Seventh Framework Program Grant ERC-2013-CoG 616050; additional support was provided by the Institut Pasteur and the Institut National de la Santé et de la Recherche Médicale (INSERM). C.M.G. was supported partly by a stipend from the Pasteur–Paris University International PhD program and by the Institut Carnot Pasteur Maladies Infectieuses. F.J. is an employee of the CNRS. None of the sources of funding has an interest in the subject matter or materials discussed in the submitted manuscript. Funding Information: This work was supported by European Research Council (ERC)-Seventh Framework Program Grant ERC-2013-CoG 616050; additional support was provided by the Institut Pasteur and the Institut National de la Santé et de la Recherche Médicale (INSERM). C.M.G. was supported partly by a stipend from the Pasteur-Paris University International PhD program and by the Institut Carnot Pasteur Maladies Infectieuses. F.J. is an employee of the CNRS. None of the sources of funding has an interest in the subject matter or materials discussed in the submitted manuscript. We thank D. Sinnaya for administrative help (Institut Pasteur, Paris, France). We also thank Prof. Marina Botto (Imperial College London, London, U.K.) for supplying C1qKO mice. We thank Dr. Grégory Jouvion (Ecole Nationale Vétérinaire d'Alfort, Maisons-Alfort, France) for help with histological analyses. Publisher Copyright: © 2022 by The American Association of Immunologists, Inc.

PY - 2022/10/1

Y1 - 2022/10/1

N2 - Mouse models of active systemic anaphylaxis rely predominantly on IgG Abs forming IgG-allergen immune complexes that induce IgG receptor-expressing neutrophils and monocytes/macrophages to release potent mediators, leading to systemic effects. Whether anaphylaxis initiates locally or systemically remains unknown. In this study, we aimed at identifying the anatomical location of IgG-allergen immune complexes during anaphylaxis. Active systemic anaphylaxis was induced following immunization with BSA and i.v. challenge with fluorescently labeled BSA. Ag retention across different organs was examined using whole-body fluorescence imaging, comparing immunized and naive animals. Various mouse models and in vivo deletion strategies were employed to determine the contribution of IgG receptors, complement component C1q, myeloid cell types, and anaphylaxis mediators. We found that following challenge, Ag diffused systemically, but specifically accumulated in the lungs of mice sensitized to that Ag, where it formed large Ab-dependent aggregates in the vasculature. Ag retention in the lungs did not rely on IgG receptors, C1q, neutrophils, or macrophages. IgG2a-mediated, but neither IgG1- nor IgG2b-mediated, passive systemic anaphylaxis led to Ag retention in the lung. Neutrophils and monocytes significantly accumulated in the lungs after challenge and captured high amounts of Ag, which led to downmodulation of surface IgG receptors and triggered their activation. Thus, within minutes of systemic injection in sensitized mice, Ag formed aggregates in the lung and liver vasculature, but accumulated specifically and dose-dependently in the lung. Neutrophils and monocytes recruited to the lung captured Ag and became activated. However, Ag aggregation in the lung vasculature was not necessary for anaphylaxis induction.

AB - Mouse models of active systemic anaphylaxis rely predominantly on IgG Abs forming IgG-allergen immune complexes that induce IgG receptor-expressing neutrophils and monocytes/macrophages to release potent mediators, leading to systemic effects. Whether anaphylaxis initiates locally or systemically remains unknown. In this study, we aimed at identifying the anatomical location of IgG-allergen immune complexes during anaphylaxis. Active systemic anaphylaxis was induced following immunization with BSA and i.v. challenge with fluorescently labeled BSA. Ag retention across different organs was examined using whole-body fluorescence imaging, comparing immunized and naive animals. Various mouse models and in vivo deletion strategies were employed to determine the contribution of IgG receptors, complement component C1q, myeloid cell types, and anaphylaxis mediators. We found that following challenge, Ag diffused systemically, but specifically accumulated in the lungs of mice sensitized to that Ag, where it formed large Ab-dependent aggregates in the vasculature. Ag retention in the lungs did not rely on IgG receptors, C1q, neutrophils, or macrophages. IgG2a-mediated, but neither IgG1- nor IgG2b-mediated, passive systemic anaphylaxis led to Ag retention in the lung. Neutrophils and monocytes significantly accumulated in the lungs after challenge and captured high amounts of Ag, which led to downmodulation of surface IgG receptors and triggered their activation. Thus, within minutes of systemic injection in sensitized mice, Ag formed aggregates in the lung and liver vasculature, but accumulated specifically and dose-dependently in the lung. Neutrophils and monocytes recruited to the lung captured Ag and became activated. However, Ag aggregation in the lung vasculature was not necessary for anaphylaxis induction.

KW - Allergens

KW - Anaphylaxis

KW - Animals

KW - Antigen-Antibody Complex

KW - Complement C1q

KW - Disease Models, Animal

KW - Immunoglobulin G

KW - Lung

KW - Mice

KW - Mice, Inbred C57BL

KW - Receptors, Complement

KW - Receptors, IgG

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U2 - 10.4049/jimmunol.2200234

DO - 10.4049/jimmunol.2200234

M3 - Article

C2 - 36165182

SN - 0022-1767

VL - 209

SP - 1243

EP - 1251

JO - Journal of immunology (Baltimore, Md. : 1950)

JF - Journal of immunology (Baltimore, Md. : 1950)

IS - 7

ER -

IgG Subclass-Dependent Pulmonary Antigen Retention during Acute IgG-Dependent Systemic Anaphylaxis in Mice

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Keywords

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