磁性纳米粒子
脂质体
纳米技术
化学
纳米颗粒
小泡
生物物理学
细胞外小泡
膜
纳米尺度
向性
材料科学
细胞外
生物传感器
纳米医学
组织工程
分子生物物理学
光热治疗
混合动力系统
胞外囊泡
脉搏(音乐)
电阻式触摸屏
细胞膜
原子力显微镜
蛋白质工程
磁场
纳米生物技术
作者
Sofia Liz-Basteiro,Marine Sagastuy,Jose E. Perez,Nicolas Ansart,Jean‐Michel Guigner,Christine Ménager,Claire Wilhelm
出处
期刊:Nano Letters
[American Chemical Society]
日期:2026-04-29
卷期号:26 (18): 6190-6200
标识
DOI:10.1021/acs.nanolett.6c01310
摘要
Extracellular vesicles (EVs), liposomes, and magnetic nanoparticles (MNPs) are key nanoplatforms in biomedicine, motivating their integration into hybrid systems. Here, we engineer magnetic EV-liposome hybrids using fusogenic liposomes preloaded with MNPs and establish a multilevel framework to characterize their formation and function. Orthogonal single-particle analyses, including nanoparticle tracking, resistive pulse sensing, high-resolution flow cytometry, and electron microscopy, reveal rapid EV-liposome association into 100-200 nm Janus-like hybrids. Magnetic nanoparticles enable direct visualization of association dynamics by magnetophoresis at ensemble and single-particle levels. Protein assays and Western blotting confirm preservation of EV markers (CD63, CD81, Syntenin-1) and vesicle integrity. Functionally, magnetic guidance enhances hybrid uptake by cancer cells, combining biological tropism with external targeting. This strategy enables controlled engineering of magnetic EV hybrids with preserved identity and multifunctionality, and provides a methodological advance for monitoring nanoscale membrane fusion toward precision theranostics.
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