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Secher, T.* ; Bodier-Montagutelli, E.* ; Parent, C.* ; Bouvart, L.* ; Cortes, M.* ; Ferreira, M.A.* ; Macloughlin, R.* ; Ilango, G.* ; Schmid, O. ; Respaud, R.* ; Heuzé-Vourc’h, N.*

Aggregates associated with instability of antibodies during aerosolization induce adverse immunological effects.

Pharmaceutics 14:671 (2022)
Publ. Version/Full Text Research data DOI PMC
Open Access Gold
Creative Commons Lizenzvertrag
Background: Immunogenicity refers to the inherent ability of a molecule to stimulate an immune response. Aggregates are one of the major risk factors for the undesired immunogenicity of therapeutic antibodies (Ab) and may ultimately result in immune-mediated adverse effects. For Ab delivered by inhalation, it is necessary to consider the interaction between aggregates resulting from the instability of the Ab during aerosolization and the lung mucosa. The aim of this study was to determine the impact of aggregates produced during aerosolization of therapeutic Ab on the immune system. Methods: Human and murine immunoglobulin G (IgG) were aerosolized using a clinically-relevant nebulizer and their immunogenic potency was assessed, both in vitro using a standard human monocyte-derived dendritic cell (MoDC) reporter assay and in vivo in immune cells in the airway compartment, lung parenchyma and spleen of healthy C57BL/6 mice after pulmonary administration. Results: IgG aggregates, produced during nebulization, induced a dose-dependent activation of MoDC characterized by the enhanced production of cytokines and expression of co-stimulatory markers. Interestingly, in vivo administration of high amounts of nebulization-mediated IgG aggregates resulted in a profound and sustained local and systemic depletion of immune cells, which was attributable to cell death. This cytotoxic effect was observed when nebulized IgG was administered locally in the airways as compared to a systemic administration but was mitigated by improving IgG stability during nebulization, through the addition of polysorbates to the formulation. Conclusion: Although inhalation delivery represents an attractive alternative route for delivering Ab to treat respiratory infections, our findings indicate that it is critical to prevent IgG aggregation during the nebulization process to avoid pro-inflammatory and cytotoxic effects. The optimization of Ab formulation can mitigate adverse effects induced by nebulization.
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Publication type Article: Journal article
Document type Scientific Article
Corresponding Author
Keywords Aerosol ; Aggregates ; Immunogenicity ; Therapeutic Antibody
ISSN (print) / ISBN 1999-4923
e-ISSN 1999-4923
Journal Pharmaceutics
Quellenangaben Volume: 14, Issue: 3, Pages: , Article Number: 671 Supplement: ,
Publisher MDPI
Non-patent literature Publications
Reviewing status Peer reviewed
Grants Agence Nationale de la Recherche