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首页> 外文期刊>Oncology letters >Sonoporation by low-frequency and low-power ultrasound enhances chemotherapeutic efficacy in prostate cancer cells in vitro
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Sonoporation by low-frequency and low-power ultrasound enhances chemotherapeutic efficacy in prostate cancer cells in vitro

机译:低频和低功率超声进行超声操作可增强体外前列腺癌细胞的化学治疗功效

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Combination therapy is used to optimize anticancer efficacy and reduce the toxicity and side-effects of drugs upon systemic administration. Ultrasound (US) combined with microbubbles (UM) enhances the intracellular uptake of cytotoxic drugs by tumor cells, particularly drug-resistant cells. In the present study, low-frequency and low-energy US (US irradiation conditions: frequency, 21 kHz; power density, 0.113 W/cm2; exposure time, 2 min at a duty cycle of 70%; and valid treatment time, 84 sec) were used in combination with microbubbles (100 μl/ml) to deliver mitoxantrone HCl (MIT) to DU145 cells. The results showed that UM did not change the cell viability in the short- or long-term. However, UM statistically enhanced the therapeutic effects and up to 31.26±3.34% of the cells exposed to UM were permeabilized compared with 9.74±2.55% of cells in the control, when using calcein (MW, 622.53) as a fluorogenic marker. Notably, UM affected the migration capability of the DU145 cells at 6 h post-treatment. In conclusion, the ultrasonic parameters used in the present study enhanced the chemotherapeutic effect and reduced the unwanted side-effects of MIT.
机译:组合疗法可用于优化抗癌功效,并减少全身给药后药物的毒性和副作用。超声(US)与微泡(UM)结合可增强肿瘤细胞(特别是耐药细胞)对细胞毒性药物的细胞内吸收。在本研究中,低频和低能量US(美国照射条件:频率为21 kHz;功率密度为0.113 W / cm2;暴露时间为2%,占空比为70%;有效治疗时间为84 sec)与微泡(100μl/ ml)结合使用,以将米托蒽醌HCl(MIT)递送至DU145细胞。结果表明,UM在短期或长期内均未改变细胞活力。然而,当使用钙黄绿素(MW,622.53)作为荧光标记物时,UM统计学上增强了治疗效果,与对照中的细胞的9.74±2.55%相比,高达31.26±3.34%的UM细胞被透化。值得注意的是,在处理后6小时,UM影响了DU145细胞的迁移能力。总之,本研究中使用的超声参数增强了化疗效果,并减少了MIT的不良副作用。

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