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Microbubbles-Assisted Ultrasound Triggers the Release of Extracellular Vesicles

机译:微泡辅助超声触发细胞外囊泡的释放

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Microbubbles-assisted ultrasound (USMB) has shown promise in improving local drug delivery. The formation of transient membrane pores and endocytosis are reported to be enhanced by USMB, and they contribute to cellular drug uptake. Exocytosis also seems to be linked to endocytosis upon USMB treatment. Based on this rationale, we investigated whether USMB triggers exocytosis resulting in the release of extracellular vesicles (EVs). USMB was performed on a monolayer of head-and-neck cancer cells (FaDu) with clinically approved microbubbles and commonly used ultrasound parameters. At 2, 4, and 24 h, cells and EV-containing conditioned media from USMB and control conditions (untreated cells, cells treated with microbubbles and ultrasound only) were harvested. EVs were measured using flow cytometric immuno-magnetic bead capture assay, immunogold electron microscopy, and western blotting. After USMB, levels of CD9 exposing-EVs significantly increased at 2 and 4 h, whereas levels of CD63 exposing-EVs increased at 2 h. At 24 h, EV levels were comparable to control levels. EVs released after USMB displayed a heterogeneous size distribution profile (30–1200 nm). Typical EV markers CD9, CD63, and alix were enriched in EVs released from USMB-treated FaDu cells. In conclusion, USMB treatment triggers exocytosis leading to the release of EVs from FaDu cells.
机译:微气泡辅助超声(USMB)已显示出改善局部药物输送的希望。据报道,USMB可以促进瞬时膜孔的形成和内吞作用,它们有助于细胞吸收药物。在USMB治疗后,胞吐作用似乎也与胞吞作用有关。基于此基本原理,我们调查了USMB是否触发胞吐作用导致细胞外囊泡(EVs)释放。 USMB在具有临床认可的微泡和常用超声参数的单层头颈癌细胞(FaDu)上进行。在第2、4和24小时,收集来自USMB和对照条件(未处理的细胞,仅用微泡处理过的细胞和仅超声处理的细胞)的细胞和含EV的条件培养基。使用流式细胞仪免疫磁珠捕获测定,免疫金电子显微镜和蛋白质印迹法测量电动汽车。在USMB之后,CD9暴露-EV的水平在2和4小时显着增加,而CD63暴露-EV的水平在2小时增加。在24小时时,EV水平与对照组水平相当。 USMB之后发布的电动汽车显示出不同的尺寸分布特征(30–1200 nm)。典型的EV标记CD9,CD63和alix富含从USMB处理过的FaDu细胞释放的EV中。总之,USMB治疗会触发胞吐作用,从而导致FaDu细胞释放EV。

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