Proinflammatory effects of bare and PEGylated ORMOSIL-, PLGA- and SUV-NPs on monocytes and PMNs and their modulation by f-MLP

Author:

Segat Daniela1,Tavano Regina2,Donini Marta3,Selvestrel Francesco4,Rio-Echevarria Iria4,Rojnik Matija5,Kocbek Petra5,Kos Janko5,Iratni Selma6,Sheglmann Dietrich6,Mancin Fabrizio4,Dusi Stefano3,Papini Emanuele7

Affiliation:

1. Centro di Ricerca Interdipartimentale per le Biotecnologie Innovative, Università di Padova, via U. Bassi 58/B, I-35131, Padova, Italy and Dipartimento di Biologia, Università di Padova, via U. Bassi 58/B, I-35131, Padova, Italy

2. Centro di Ricerca Interdipartimentale per le Biotecnologie Innovative, Università di Padova, via U. Bassi 58/B, I-35131, Padova, Italy and Dipartimento di Scienze Biomediche Sperimentali, Università di Padova, via U. Bassi 58/B, I-35131, Padova, Italy

3. Dipartimento di Patologia e Diagnostica, Università di Verona, Strada Le Grazie 8, I-37134, Verona, Italy

4. Dipartimento di Scienze Chimiche, Università di Padova, via Marzolo 1, I -35131 Padova, Italy

5. Department of Pharmaceutical Biology, Faculty of Pharmacy, University of Ljubijana, Askerceva 7, 1000 Ljubijana, Slovenia

6. Research & Development Biolitec AG, Winzerlaer Strasse 2, D-07745, Jena, Germany

7. Centro di Ricerca Interdipartimentale per le Biotecnologie Innovative, Università di Padova, via U. Bassi 58/B, I-35131, Padova, Italy and Dipartimento di Scienze Biomediche Sperimentali, Università di Padova, via U. Bassi 58/B, I-35131, Padova, Italy.

Abstract

Aims: We wanted to test the proinflammatory effects of vinyltriethoxysilane-based organically modified silica nanoparticles (ORMOSIL-NPs) in vitro on blood leukocytes. Materials & Methods: Cell selectivity, cytokines/chemokines and O2 - production were analyzed using nonpolyethylene glycol (PEG)ylated and PEGylated ORMOSIL-NPs, poly(lactic-co-glycolic acid) (PLGA)-NPs and small unilamellar vesicles (SUV)-NPs. Results: ORMOSIL-NPs mostly bound to monocytes while other NPs to all leukocyte types similarly. Cell capture of PEGylated-NPs decreased strongly (ORMOSIL), moderately (PLGA) and weakly (SUV). Bare ORMOSIL-NPs effectively stimulated the production of IL-1β/IL-6/TNF-α/IL-8 by monocytes and of IL-8 by polymorphonuclear leukocytes (PMNs). NP PEGylation inhibited such effects only partially. Formyl-methionine-leucine phenylalanine (f-MLP) further increased the release of cytokines/chemokines by monocytes/PMNs primed with bare and PEGylated ORMOSIL-NPs. PEGylated SUV-NPs, bare and PEGylated ORMOSIL- and PLGA-NPs sensitize PMNs and monocytes to secrete O2 - upon f-MLP stimulation. Conclusion: ORMOSIL-NPs are preferentially captured by circulating monocytes but stimulate both monocytes and PMNs per se or by sensitizing them to another agonist (f-MLP). PEG-coating confers stealth effects but does not completely eliminate leukocyte activation. Safe nanomedical applications require the evaluation of both intrinsic and cooperative proinflammatory potential of NPs.

Publisher

Future Medicine Ltd

Subject

Development,General Materials Science,Biomedical Engineering,Medicine (miscellaneous),Bioengineering

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