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Dexamethasone-loaded injectable silk-polyethylene glycol hydrogel alleviates cisplatin-induced ototoxicity

机译:负载地塞米松的可注射丝-聚乙二醇水凝胶可减轻顺铂诱导的耳毒性

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Background: Cisplatin is an extensively used anti-neoplastic agent for the treatment of various solid tumors. However, a high incidence of severe ototoxicity is accompanied by its use in the clinic. Currently, no drugs or therapeutic strategies have been approved for the treatment of cisplatin-induced ototoxicity by the FDA. Purpose: The purpose of this study was to investigate the otoprotective effects of dexamethasone (DEX)-loaded silk-polyethylene hydrogel (DEX-SILK) following round window membrane administration in the cisplatin-induced ototoxicity mouse model. Methods: The morphology, gelation kinetics, viscosity and secondary structure of the DEX-SILK hydrogel were analyzed. DEX concentration in the perilymph was tested at different time points following hydrogel injection on the RWM niche. Cultured cells (HEI-OC1), organ of Corti explants (C57/BL6, P0-2), and cisplatin-induced hearing loss mice model (C57/BL6) were used as in vitro and in vivo models for investigating the otoprotective effects of DEX-SILK hydrogel against cisplatin. Results: Encapsulation of DEX with a loading of 8% (w/v) did not significantly change the silk gelation time, and DEX was evenly distributed in the Silk-PEG hydrogel as visualized by scanning electron microscopy (SEM). The concentration of Silk majorly influenced DEX distribution, morphological characteristics, viscosity, and gelation time. The optimized DEX-SILK hydrogel (8% w/v loading, 15% silk concentration, 10 μl) was administered directly onto the RWM of the guinea pigs. The DEX concentration in the perilymph was maintained above 1 μg/ml for at least 21 days for the DEX-SILK, while it was maintained for less than 6 h in the control sample of free DEX. DEX-SILK (5-60 ng/ml) exhibited significant protective effects against cisplatin-induced cellular ototoxicity and notably reduced the production of reactive oxygen species (ROS). Eventually, pretreatment with DEX-SILK effectively preserved outer hair cells in the cultured organ of Corti explants and demonstrated significant hearing protection at 4, 8, and 16 kHz in the cisplatin-induced hearing loss mice as compared to the effects noted following pretreatment with DEX. Conclusion: These results demonstrated the clinical value of DEX-SILK for the therapy of cisplatin-induced ototoxicity.
机译:背景:顺铂是一种广泛使用的抗肿瘤药物,用于治疗各种实体瘤。然而,严重的耳毒性高发生率伴随着其在临床中的使用。目前,尚未有任何药物或治疗策略被FDA批准用于治疗顺铂诱导的耳毒性。目的:本研究的目的是研究在顺铂诱导的耳毒性小鼠模型中施用圆窗膜后,负载地塞米松(DEX)的丝-聚乙烯水凝胶(DEX-SILK)的耳保护作用。方法:分析了DEX-SILK水凝胶的形貌,凝胶动力学,粘度和二级结构。在RWM生态位上水凝胶注射后,在不同的时间点测试周淋巴中的DEX浓度。将培养的细胞(HEI-OC1),Corti外植体器官(C57 / BL6,P0-2)和顺铂诱导的听力损失小鼠模型(C57 / BL6)用作体外和体内模型,以研究抗顺铂的DEX-SILK水凝胶。结果:以8%(w / v)的载量包封DEX并没有显着改变丝凝胶时间,并且通过扫描电子显微镜(SEM)观察,DEX均匀地分布在Silk-PEG水凝胶中。蚕丝的浓度主要影响DEX的分布,形态特征,粘度和胶凝时间。将优化的DEX-SILK水凝胶(8%w / v负载,15%丝浓度,10μl)直接施用到豚鼠的RWM上。对于DEX-SILK,周淋巴中的DEX浓度至少在1μg/ ml以上保持至少21天,而在游离DEX的对照样品中,DEX浓度保持少于6小时。 DEX-SILK(5-60 ng / ml)对顺铂诱导的细胞耳毒性显示出显着的保护作用,并显着降低了活性氧(ROS)的产生。最终,与使用DEX预处理后所注意到的效果相比,使用DEX-SILK预处理可以有效地在Corti外植体的培养器官中保留外部毛细胞,并在顺铂诱导的听力损失小鼠中在4、8、16 kHz表现出显着的听力保护。 。结论:这些结果证明了DEX-SILK在顺铂诱导的耳毒性治疗中的临床价值。

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