Hapten/Myristoyl Functionalized Poly(propyleneimine) Dendrimers as Potent Cell Surface Recruiters of Antibodies for Mediating Innate Immune Killing

Author:

Uvyn Annemiek1,Vleugels Marle Elisabeth Jacqueline2ORCID,de Waal Bas2,Hamouda Ahmed Emad Ibrahim34,Dhiman Shikha2,Louage Benoit1,Albertazzi Lorenzo2,Laoui Damya34,Meijer E. W.25,De Geest Bruno G.1ORCID

Affiliation:

1. Department of Pharmaceutics Ghent University Ghent 9000 Belgium

2. Department of Biomedical Engineering Institute for Complex Molecular Systems Eindhoven University of Technology MB 5600 P.O. Box 513 Eindhoven The Netherlands

3. Laboratory of Dendritic Cell Biology and Cancer Immunotherapy VIB Center for Inflammation Research Brussels 1050 Belgium

4. Laboratory of Cellular and Molecular Immunology Vrije Universiteit Brussel Brussels 1050 Belgium

5. School of Chemistry, RNA Institute University of new South Wales Sydney NSW 1050 Australia

Abstract

AbstractRecruiting endogenous antibodies to the surface of cancer cells using antibody‐recruiting molecules has the potential to unleash innate immune effector killing mechanisms against antibody‐bound cancer cells. The affinity of endogenous antibodies is relatively low, and many currently explored antibody‐recruiting strategies rely on targeting over‐expressed receptors, which have not yet been identified in most solid tumors. Here, both challenges are addressed by functionalizing poly(propyleneimine) (PPI) dendrimers with both multiple dinitrophenyl (DNP) motifs, as anti‐hapten antibody‐recruiting motifs, and myristoyl motifs, as universal phospholipid cell membrane anchoring motifs, to recruit anti‐hapten antibodies to cell surfaces. By exploiting the multivalency of the ligand exposure on the dendrimer scaffold, it is demonstrated that dendrimers featuring ten myristoyl and six DNP motifs exhibit the highest antibody‐recruiting capacity in vitro. Furthermore, it is shown that treating cancer cells with these dendrimers in vitro marks them for phagocytosis by macrophages in the presence of anti‐hapten antibodies. As a proof‐of‐concept, it is shown that intratumoral injection of these dendrimers in vivo in tumor‐bearing mice results in the recruitment of anti‐DNP antibodies to the cell surface in the tumor microenvironment. These findings highlight the potential of dendrimers as a promising class of novel antibody‐recruiting molecules for use in cancer immunotherapy.

Funder

Fonds Wetenschappelijk Onderzoek

European Research Council

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials,General Materials Science

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