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膜定位磁热疗促进细胞不透探针的细胞内递送。

Membrane-localized magnetic hyperthermia promotes intracellular delivery of cell-impermeant probes.

机构信息

Instituto de Nanociencia y Materiales de Aragón, INMA (CSIC-Universidad de Zaragoza), C/Pedro Cerbuna 12, 50009, Zaragoza, Spain.

Centro de Investigación Biomédica en Red de Bioingeniería, Biomateriales y Nanomedicina (CIBER-BBN), Spain.

出版信息

Nanoscale. 2024 Aug 15;16(32):15176-15195. doi: 10.1039/d4nr01955e.

DOI:10.1039/d4nr01955e
PMID:39052238
Abstract

In this work, we report the disruptive use of membrane-localized magnetic hyperthermia to promote the internalization of cell-impermeant probes. Under an alternating magnetic field, magnetic nanoparticles (MNPs) immobilized on the cell membrane bioorthogonal click chemistry act as nanoheaters and lead to the thermal disruption of the plasma membrane, which can be used for internalization of different types of molecules, such as small fluorescent probes and nucleic acids. Noteworthily, no cell death, oxidative stress and alterations of the cell cycle are detected after the thermal stimulus, although cells are able to sense and respond to the thermal stimulus through the expression of different types of heat shock proteins (HSPs). Finally, we demonstrate the utility of this approach for the transfection of cells with a small interference RNA (siRNA), revealing a similar efficacy to a standard transfection method based on the use of cationic lipid-based reagents (such as Lipofectamine), but with lower cell toxicity. These results open the possibility of developing new procedures for "opening and closing" cellular membranes with minimal disturbance of cellular integrity. This on-demand modification of cell membrane permeability could allow the direct intracellular delivery of biologically relevant (bio)molecules, drugs and nanomaterials, thus overcoming traditional endocytosis pathways and avoiding endosomal entrapment.

摘要

在这项工作中,我们报告了膜定位磁热疗的颠覆性应用,以促进细胞不可渗透探针的内化。在交变磁场下,固定在细胞膜上的磁性纳米粒子(MNPs)通过生物正交点击化学作用作为纳米加热器,导致质膜热破裂,可用于内化不同类型的分子,如小分子荧光探针和核酸。值得注意的是,尽管细胞能够通过表达不同类型的热休克蛋白(HSPs)来感知和响应热刺激,但在热刺激后不会检测到细胞死亡、氧化应激和细胞周期改变。最后,我们证明了这种方法在转染小干扰 RNA(siRNA)方面的实用性,与基于阳离子脂质试剂(如 Lipofectamine)的标准转染方法相比,其效果相似,但细胞毒性较低。这些结果为开发新的方法提供了可能性,即用最小的细胞完整性干扰来“打开和关闭”细胞膜。这种对细胞膜通透性的按需修饰可以允许生物相关(bio)分子、药物和纳米材料的直接细胞内递送,从而克服传统的内吞途径并避免内体捕获。

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