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Protein corona–mediated targeting of nanocarriers to B cells allows redirection of allergic immune responses - 06/11/18

Doi : 10.1016/j.jaci.2017.08.049 
Limei Shen, PhD a, Stefan Tenzer, PhD b, Wiebke Storck, MSc b, Dominika Hobernik, MSc a, Verena Katherina Raker, PhD a, Karl Fischer, PhD c, Sandra Decker, PhD c, Andrzej Dzionek d, Susanne Krauthäuser, PhD d, Mustafa Diken, PhD e, Alexej Nikolaev f, Joachim Maxeiner, MSc g, Petra Schuster g, Cinja Kappel, MSc a, Admar Verschoor, PhD h, Hansjörg Schild, PhD b, , Stephan Grabbe, MD a, , Matthias Bros, PhD a,
a Department of Dermatology, University of Mainz Medical Center, Mainz, Germany 
b Institute for Immunology, University of Mainz Medical Center, Mainz, Germany 
f Institute for Molecular Medicine, University of Mainz Medical Center, Mainz, Germany 
g Asthma Core Facility, Research Center for Immunotherapy, University of Mainz Medical Center, Mainz, Germany 
c Department of Physical Chemistry, University of Mainz, Mainz, Germany 
d Miltenyi Biotec GmbH, Bergisch Gladbach, Germany 
e TRON-Translational Oncology at the University Medical Center of the Johannes Gutenberg University gGmbH, Mainz, Germany 
h Institute for Systemic Inflammation Research, Universität zu Lübeck, Lübeck, Germany 

Corresponding author: Stephan Grabbe, MD, University Medical Center Mainz, Department of Dermatology, Langenbeckstr 1, Mainz D-55131, Germany.University Medical Center MainzDepartment of DermatologyLangenbeckstr 1MainzD-55131Germany

Abstract

Background

Nanoparticle (NP)–based vaccines are attractive immunotherapy tools because of their capability to codeliver antigen and adjuvant to antigen-presenting cells. Their cellular distribution and serum protein interaction (“protein corona”) after systemic administration and their effect on the functional properties of NPs is poorly understood.

Objectives

We analyzed the relevance of the protein corona on cell type–selective uptake of dextran-coated NPs and determined the outcome of vaccination with NPs that codeliver antigen and adjuvant in disease models of allergy.

Methods

The role of protein corona constituents for cellular binding/uptake of dextran-coated ferrous nanoparticles (DEX-NPs) was analyzed both in vitro and in vivo. DEX-NPs conjugated with the model antigen ovalbumin (OVA) and immunostimulatory CpG-rich oligodeoxynucleotides were administered to monitor the induction of cellular and humoral immune responses. Therapeutic effects of this DEX-NP vaccine in mouse models of OVA-induced anaphylaxis and allergic asthma were assessed.

Results

DEX-NPs triggered lectin-induced complement activation, yielding deposition of activated complement factor 3 on the DEX-NP surface. In the spleen DEX-NPs targeted predominantly B cells through complement receptors 1 and 2. The DEX-NP vaccine elicited much stronger OVA-specific IgG2a production than coadministered soluble OVA plus CpG oligodeoxynucleotides. B-cell binding of the DEX-NP vaccine was critical for IgG2a production. Treatment of OVA-sensitized mice with the DEX-NP vaccine prevented induction of anaphylactic shock and allergic asthma accompanied by IgE inhibition.

Conclusions

Opsonization of lectin-coated NPs by activated complement components results in selective B-cell targeting. The intrinsic B-cell targeting property of lectin-coated NPs can be exploited for treatment of allergic immune responses.

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Key words : Dendritic cells, B cells, complement, antibody, complement factor 3, lectin pathway, IgG2a

Abbreviations used : AIT, APC, BCR, C3, CFSE, CR, DAPI, DC, DEX-NP, FDC, MBL, NP, ODN, OVA, TLR


Plan


 L.S. and S.G. were supported by a grant of the Hoffmann Klose Stiftung. W.S., S.T., and H.S. were supported by Stiftung Rheinland-Pfalz (NANOSCH). L.S., W.S., S.T., H.S., S.G., and M.B. were supported by grants from the DFG (SFB 1066).
 Disclosure of potential conflict of interest: S. Tenzer has received grants from Stiftung Rheinland-Pfalz (NANOSCH) and the German Research Foundation (SFB1066). W. Storck has received grants from Deutsche Forschungsgesellschaft (SFB1066) and Stiftung Rheinland-Pfalz (NANOSCH). S. Krauthauser is employed by Miltenyi Biotec GmbH. Hansjörg Schild has received a grant from the German Research Foundation. S. Grabbe has received grants from the German Research Foundation (SFB1066-B04 and SFB1066-B05), Hoffman-Klose Stiftung, and Stiftung Rheinland-Pfalz; has consultant arrangements with AbbVie, Bristol-Myers-Squibb, Roche, Novartis, MSD, Merck-Serono, and Sanofi-Pasteur-MSD; has provided expert testimony for Guidepoint Global advisors and OnkoZert; has received payment for lectures from Bristol-Myers Squibb, MSD, Roche, MedConcept, Beiersdorf, Loreal, and Novartis; and has received travel support from Bristol-Myers Squibb, AbbVie, MSD, Merck-Serono, Roche, Novartis, and Takeda. M. Bros has received a grant from the German Research Foundation. The rest of the authors declare that they have no relevant conflicts of interest.


© 2018  The Authors. Publié par Elsevier Masson SAS. Tous droits réservés.
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Vol 142 - N° 5

P. 1558-1570 - novembre 2018 Retour au numéro
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