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Lattice Distortion in Hollow Multi‐shelled Structures for Efficient Visible Light CO2 Reduction with SnS2/SnO2 Junction

DOI:10.1002/ange.201912069 期刊:Angewandte Chemie 出版年份:2019 更新时间:2025-09-19 17:13:59
摘要: When nanoparticles interact with cellular or organelle membranes, the coating ligands are known to affect the integrity of the membranes, which regulate cell death and inflammation. However, the molecular mechanisms of this modulation remain unresolved. Here, we use synchrotron X-ray liquid surface scattering and molecular dynamics simulations to study interface structures between phospholipids and gold nanorods (AuNRs) coated by surfactant and polyelectrolyte. These ligands are two types of widely used surface modification with different self-assembled structures and stabilities on the surface of nanoparticles. We reveal distinct mechanisms of the ligand stability in disrupting membrane integrity. We find that the cationic surfactant ligand cetyltrimethylammonium bromide detaches from the AuNRs and inserts into phospholipids, resulting in reduced membrane thickness by compressing the phospholipids the cationic polyelectrolyte ligand poly- ligand. Conversely, (diallyldimethylammonium chloride) is more stable on AuNRs; although it adsorbs onto the membrane, it does not cause much impairment. The distinct coating ligand interactions with phospholipids are further verified by cellular responses including impaired lysosomal membranes and triggered inflammatory effects in macrophages. Together, the quantitative analysis of interface structures elucidates key bio?nano interactions and highlights the importance of surface ligand stability for safety and rational design of nanoparticles.
作者: Xiaochun Wu,Ruhong Zhou,Leili Zhang,Yuliang Zhao,Peiyu Quan,Serena H. Chen,Yu-Feng Li,Binhua Lin,Wei Bu,Xiaoming Jiang,Liming Wang,Junguang Wu,Chunying Chen
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Investigating the molecular mechanisms of how coating ligands on nanoparticles affect the integrity of cellular or organelle membranes, and how these interactions regulate cell death and inflammation.

The study reveals that the stability of coating ligands on nanoparticles significantly affects their interaction with biological membranes, influencing membrane integrity, cytotoxicity, and inflammatory responses. Cationic surfactant ligands (CTAB) are less stable and can insert into membranes, reducing thickness and causing damage, whereas polyelectrolyte ligands (PDC) are more stable and cause minimal impairment. These findings highlight the importance of surface ligand stability for the safety and rational design of nanoparticles.

The study focuses on model systems (AuNRs with specific coatings and SOPC monolayers/bilayers), which may not fully represent the complexity of biological membranes in vivo. The physical structures of the monolayer and bilayer of SOPC differ, which might affect the generalizability of the findings.

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