Boosting Membrane Interactions and Antimicrobial Effects of Photocatalytic Titanium Dioxide Nanoparticles by Peptide Coating

Author:

Caselli Lucrezia12,Parra‐Ortiz Elisa13,Micciulla Samantha456,Skoda Maximilian W. A.7,Häffner Sara Malekkhaiat18,Nielsen Emilie Marie1,van der Plas Mariena J.A.1,Malmsten Martin12ORCID

Affiliation:

1. Department of Pharmacy University of Copenhagen Copenhagen DK‐2100 Denmark

2. Department of Physical Chemistry 1 Lund University Lund SE‐22100 Sweden

3. Novonesis Biologiens Vej 2 Lyngby DK‐2800 Kgs Denmark

4. Institut Laue–Langevin CS 20156 Grenoble Cedex 9 38042 France

5. Laboratoire Interdisciplinaire de Physique (LIPhy) Saint Martin d'Hères 38402 France

6. Centre National de la Recherche Scientifique (CNRS) Saint‐Martin‐d'Hères Auvergne‐Rhône‐Alpes France

7. ISIS Pulsed Neutron and Muon Source Rutherford Appleton Laboratory Harwell OX11 0QX UK

8. RISE Research Institutes of Sweden Malvinas väg 3 Stockholm 114 86 Sweden

Abstract

AbstractPhotocatalytic nanoparticles offer antimicrobial effects under illumination due to the formation of reactive oxygen species (ROS), capable of degrading bacterial membranes. ROS may, however, also degrade human cell membranes and trigger toxicity. Since antimicrobial peptides (AMPs) may display excellent selectivity between human cells and bacteria, these may offer opportunities to effectively “target” nanoparticles to bacterial membranes for increased selectivity. Investigating this, photocatalytic TiO2 nanoparticles (NPs) are coated with the AMP LL‐37, and ROS generation is found by C11‐BODIPY to be essentially unaffected after AMP coating. Furthermore, peptide‐coated TiO2 NPs retain their positive ζ‐potential also after 1–2 h of UV illumination, showing peptide degradation to be sufficiently limited to allow peptide‐mediated targeting. In line with this, quartz crystal microbalance measurements show peptide coating to promote membrane binding of TiO2 NPs, particularly so for bacteria‐like anionic and cholesterol‐void membranes. As a result, membrane degradation during illumination is strongly promoted for such membranes, but not so for mammalian‐like membranes. The mechanisms of these effects are elucidated by neutron reflectometry. Analogously, LL‐37 coating promoted membrane rupture by TiO2 NPs for Gram‐negative and Gram‐positive bacteria, but not for human monocytes. These findings demonstrate that AMP coating may selectively boost the antimicrobial effects of photocatalytic NPs.

Funder

ISIS Neutron and Muon Source

Publisher

Wiley

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