Impact of RAFT chain transfer agents on the polymeric shell density of magneto-fluorescent nanoparticles and their cellular uptake

Thibaut Blondy; Julien Poly; Camille Linot; Joanna Boucard; Emilie Allard-Vannier; Steven Nedellec; Phillipe Hulin; Céline Hénoumont; Lionel Larbanoix; Robert N. Muller; Sophie Laurent; Eléna Ishow; Christophe Blanquart

doi:10.1039/D1NR06769A

Impact of RAFT chain transfer agents on the polymeric shell density of magneto-fluorescent nanoparticles and their cellular uptake†

Thibaut Blondy,^a Julien Poly,

^b Camille Linot,^a Joanna Boucard,^ac Emilie Allard-Vannier,^d Steven Nedellec,^e Phillipe Hulin,^e Céline Hénoumont,

^f Lionel Larbanoix,^g Robert N. Muller,^f Sophie Laurent,

^fg Eléna Ishow

*^c and Christophe Blanquart

*^a

Author affiliations

* Corresponding authors

^a Nantes Université, Inserm UMR 1307, CNRS UMR 6075, Université d'Angers, CRCI2NA, F-44000 Nantes, France
E-mail: christophe.blanquart@inserm.fr

^b IS2M-UMR CNRS 7361, Université de Haute Alsace, 15 rue Jean Starcky, 68057 Mulhouse, France

^c Nantes Université, CNRS, CEISAM, UMR 6230, F-44000 Nantes, France
E-mail: elena.ishow@univ-nantes.fr

^d EA 6295 ‘Nanomédicaments et Nanosondes’, Université de Tours, Tours, France

^e Nantes Université, INSERM, UMS 016, CNRS, UMS 3556, F-44000 Nantes, France

^f Department of General, Organic, and Biomedical Chemistry, NMR and Molecular Imaging Laboratory, University of Mons-Hainaut, B-7000 Mons, Belgium

^g Center for Microscopy and Molecular Imaging, 8 rue Adrienne Bolland à Gosselies, 6041 Gosselies, Belgium

Abstract

The impact of nanoparticle surface chemistry on cell interactions and especially cell uptake has become evident over the last few years in nanomedicine. Since PEG polymers have proved to be ideal tools for attaining stealthiness and favor escape from the in vivo mononuclear phagocytotic system, the accurate control of their geometry is of primary importance and can be achieved through reversible addition–fragmentation transfer (RAFT) polymerization. In this study, we demonstrate that the residual groups of the chain transfer agents (CTAs) introduced in the main chain exert a significant impact on the cellular internalization of functionalized nanoparticles. High-resolution magic angle spinning ¹H NMR spectroscopy and fluorescence spectroscopy permitted by the magneto-fluorescence properties of nanoassemblies (NAs) revealed the compaction of the PEG comb-like shell incorporating CTAs with a long alkyl chain, without changing the overall surface potential. As a consequence of the capability of alkyl units to self-assemble at the NA surface while hardly contributing more than 0.5% to the total polyelectrolyte weight, denser PEGylated NAs showed notably less internalization in all cells of the tumor microenvironment (tumor cells, macrophages and healthy cells). Interestingly, such differentiated uptake is also observed between pro-inflammatory M1-like and immunosuppressive M2-like macrophages, with the latter more efficiently phagocytizing NAs coated with a less compact PEGylated shell. In contrast, the NA diffusion inside multicellular spheroids, used to mimic solid tumors, appeared to be independent of the NA coating. These results provide a novel effort-saving approach where the sole variation of the chemical nature of CTAs in RAFT PEGylated polymers strikingly modulate the cell uptake of nanoparticles upon the organization of their surface coating and open the pathway toward selectively addressing macrophage populations for cancer immunotherapy.

Nanoscale

Impact of RAFT chain transfer agents on the polymeric shell density of magneto-fluorescent nanoparticles and their cellular uptake†

Abstract

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Impact of RAFT chain transfer agents on the polymeric shell density of magneto-fluorescent nanoparticles and their cellular uptake

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