首页> 外文期刊>Ultrasound in Medicine and Biology >Ultrasound and microbubble-induced intra- and intercellular bioeffects in primary endothelial cells.
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Ultrasound and microbubble-induced intra- and intercellular bioeffects in primary endothelial cells.

机译:超声和微泡诱导的内皮细胞内和细胞间生物效应。

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Recent developments in the field of ultrasound (US) contrast agents have demonstrated that these encapsulated microbubbles can not only be used for diagnostic imaging but may also be employed as therapeutic carriers for localized, targeted drug or gene delivery. The exact mechanisms behind increased uptake of therapeutic compounds by US-exposed microbubbles are still not fully understood. Therefore, we studied the effects of stably oscillating SonoVue microbubbles on relevant parameters of cellular and intercellular permeability, i.e., reactive oxygen species (ROS) homeostasis, calcium permeability, F-actin cytoskeleton, monolayer integrity and cell viability using live-cell fluorescence microscopy. US was applied at 1-MHz, 0.1MPa peak-negative pressure, 0.2% duty cycle and 20Hz pulse repetition frequency to primary endothelial cells. We demonstrated increased membrane permeability for calcium ions, with an important role for H(2)O(2). Catalase, an extracellular H(2)O(2) scavenger, significantly blocked the influx of calcium ions. Further changes in ROS homeostasis involved an increase in intracellular H(2)O(2) levels, protein nitrosylation and a decrease in total endogenous glutathione levels. In addition, an increase in the number of F-actin stress fibers and F-actin cytoskeletal rearrangement were observed. Furthermore, US-exposed microbubbles significantly affected endothelial monolayer integrity, but importantly, disrupted cell-cell interactions were restored within 30min. Finally, cell viability was not affected. In conclusion, these data provide more insight in the interactions between US, microbubbles and endothelial cells, which is important for understanding the mechanisms behind US and microbubble-enhanced uptake of drugs or genes.
机译:超声(US)造影剂领域的最新发展表明,这些封装的微泡不仅可以用于诊断成像,还可以用作局部,靶向药物或基因递送的治疗载体。仍未完全了解暴露于美国的微泡增加治疗性化合物摄取的确切机制。因此,我们使用活细胞荧光显微镜研究了稳定振荡的SonoVue微泡对细胞和细胞间通透性相关参数的影响,即活性氧(ROS)稳态,钙渗透性,F-肌动蛋白细胞骨架,单层完整性和细胞活力。 US以1-MHz,0.1MPa峰值负压,0.2%占空比和20Hz脉冲重复频率应用于原代内皮细胞。我们表现​​出增加的钙离子的膜通透性,对H(2)O(2)具有重要作用。过氧化氢酶,一种细胞外H(2)O(2)清除剂,大大阻止了钙离子的流入。 ROS稳态的进一步变化涉及细胞内H(2)O(2)水平的增加,蛋白质亚硝基化和总内源性谷胱甘肽水平的降低。另外,观察到F-肌动蛋白应激纤维的数量增加和F-肌动蛋白细胞骨架重排。此外,暴露于美国的微泡显着影响内皮单层完整性,但重要的是,被破坏的细胞间相互作用在30分钟内得以恢复。最后,细胞活力不受影响。总之,这些数据为我们提供了更多有关US,微泡与内皮细胞之间相互作用的见解,这对于理解US和微泡增强的药物或基因吸收机制至关重要。

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