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通过肽涂层增强光催化二氧化钛纳米颗粒的膜相互作用和抗菌效果。

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

作者信息

Caselli Lucrezia, Parra-Ortiz Elisa, Micciulla Samantha, Skoda Maximilian W A, Häffner Sara Malekkhaiat, Nielsen Emilie Marie, van der Plas Mariena J A, Malmsten Martin

机构信息

Department of Pharmacy, University of Copenhagen, Copenhagen, DK-2100, Denmark.

Department of Physical Chemistry 1, Lund University, Lund, SE-22100, Sweden.

出版信息

Small. 2024 Jul;20(30):e2309496. doi: 10.1002/smll.202309496. Epub 2024 Feb 25.

DOI:10.1002/smll.202309496
PMID:38402437
Abstract

Photocatalytic 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 TiO nanoparticles (NPs) are coated with the AMP LL-37, and ROS generation is found by C-BODIPY to be essentially unaffected after AMP coating. Furthermore, peptide-coated TiO 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 TiO 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 TiO 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.

摘要

光催化纳米颗粒在光照下由于活性氧(ROS)的形成而具有抗菌作用,ROS能够降解细菌膜。然而,ROS也可能降解人类细胞膜并引发毒性。由于抗菌肽(AMPs)可能在人类细胞和细菌之间表现出优异的选择性,因此这些抗菌肽可能为有效地将纳米颗粒“靶向”细菌膜以提高选择性提供机会。为了对此进行研究,将光催化TiO纳米颗粒(NPs)用AMP LL-37进行包被,并且通过C-硼二吡咯发现包被AMP后ROS的产生基本不受影响。此外,肽包被的TiO NPs在紫外线照射1-2小时后仍保持其正ζ电位,表明肽的降解受到充分限制,从而允许肽介导的靶向作用。与此一致,石英晶体微天平测量表明肽包被促进了TiO NPs与膜的结合,对于类细菌阴离子膜和无胆固醇膜尤其如此。结果,对于此类膜,光照期间的膜降解得到强烈促进,但对于类哺乳动物膜则不然。通过中子反射法阐明了这些效应的机制。类似地,LL-37包被促进了TiO NPs对革兰氏阴性菌和革兰氏阳性菌的膜破裂作用,但对人类单核细胞则没有这种作用。这些发现表明,AMP包被可以选择性地增强光催化NPs的抗菌效果。

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