Membrane Interactions of Virus-like Mesoporous Silica Nanoparticles

介孔二氧化硅 纳米颗粒 脂质双层 中子反射计 生物物理学 材料科学 双层 纳米技术 化学 介孔材料 化学工程 小角中子散射 中子散射 生物化学 散射 生物 光学 物理 工程类 催化作用
作者
Sara Malekkhaiat Häffner,Elisa Parra‐Ortiz,Kathryn L. Browning,Elin Jørgensen,Maximilian W. A. Skoda,Costanza Montis,Xiaomin Li,Debora Berti,Dongyuan Zhao,Martin Malmsten
出处
期刊:ACS Nano [American Chemical Society]
卷期号:15 (4): 6787-6800 被引量:107
标识
DOI:10.1021/acsnano.0c10378
摘要

In the present study, we investigated lipid membrane interactions of silica nanoparticles as carriers for the antimicrobial peptide LL-37 (LLGDFFRKSKEKIGKEFKRIVQRIKDFLRNLVPRTES). In doing so, smooth mesoporous nanoparticles were compared to virus-like mesoporous nanoparticles, characterized by a "spiky" external surface, as well as to nonporous silica nanoparticles. For this, we employed a combination of neutron reflectometry, ellipsometry, dynamic light scattering, and ζ-potential measurements for studies of bacteria-mimicking bilayers formed by palmitoyloleoylphosphatidylcholine/palmitoyloleoylphosphatidylglycerol. The results show that nanoparticle topography strongly influences membrane binding and destabilization. We found that virus-like particles are able to destabilize such lipid membranes, whereas the corresponding smooth silica nanoparticles are not. This effect of particle spikes becomes further accentuated after loading of such particles with LL-37. Thus, peptide-loaded virus-like nanoparticles displayed more pronounced membrane disruption than either peptide-loaded smooth nanoparticles or free LL-37. The structural basis of this was clarified by neutron reflectometry, demonstrating that the virus-like nanoparticles induce trans-membrane defects and promote incorporation of LL-37 throughout both bilayer leaflets. The relevance of such effects of particle spikes for bacterial membrane rupture was further demonstrated by confocal microscopy and live/dead assays on Escherichia coli bacteria. Taken together, these findings demonstrate that topography influences the interaction of nanoparticles with bacteria-mimicking lipid bilayers, both in the absence and presence of antimicrobial peptides, as well as with bacteria. The results also identify virus-like mesoporous nanoparticles as being of interest in the design of nanoparticles as delivery systems for antimicrobial peptides.
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