Synergetic Enhancing Effects between Platinum Nanosensitizers and Clinically Approved Stabilizing Ligands in Proton Therapy, Causing High‐Yield Double‐Strand Breaks of Plasmid DNA at Relevant Dose

Author:

Zwiehoff Sandra1,Hensel Astrid2,Rishmawi Ramin1,Shakibaei Parisa1,Behrends Carina34,Hommel Katrin2,Bäumer Christian345,Knauer Shirley Karin2,Timmermann Beate456,Rehbock Christoph1,Barcikowski Stephan1ORCID

Affiliation:

1. Faculty of Chemistry University of Duisburg‐Essen, Technical Chemistry I and Center for Nanointegration Duisburg-Essen (CENIDE) 45141 Essen Germany

2. Faculty of Biology University of Duisburg‐Essen, Molecular Biology I 45141 Essen Germany

3. Department of Physics TU Dortmund University 44227 Dortmund Germany

4. West German Proton Therapy Centre Essen (WPE), West German Cancer Centre (WTZ), University Hospital Essen 45147 Essen Germany

5. German Cancer Consortium (DKTK) 69120 Heidelberg Germany

6. Department of Particle Therapy, Faculty of Medicine University of Duisburg-Essen, University Hospital Essen 45147 Essen Germany

Abstract

Proton therapy is used to eradicate tumors in sensitive areas by targeted delivery of energy. Its effectiveness can be amplified using nanoparticles (NPs) as sensitizers, due to the production of reactive oxygen species at the NP's catalytically active surface, causing the cleavage of DNA. However, the impact of stabilizing macromolecular ligands capping the particles, needed for nanosensitizer dispersion in physiological fluids, is underexplored. Herein, ligand‐free colloidal platinum NPs (PtNPs) fabricated by scalable laser synthesis in liquids are used, which allows studying particle and ligand effects separately. PtNPs are incubated with stabilizing concentrations of the clinically approved ligands albumin, Tween, and polyethylene glycol, and irradiated with proton beams at clinically relevant doses (2 and 5 Gy). At these doses, plasmid DNA cleavage larger than 55% of clustered DNA damage is achieved. Bovine serum albumin, Tween, and polyethylene glycol on the NP surface work as double‐strand breaks (DSB) enhancers and synergetic effects occur even at low and clinically relevant particle concentrations and irradiation doses. Here, DSB enhancement by ligand‐capped PtNP even exceeds the sum of the individual ligand and particle effects. The presented fundamental correlations provide selection rules for nanosensitizer design in proton therapy.

Publisher

Wiley

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