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Ultrasound-induced reactive oxygen species generation and mitochondria-specific damage by sonodynamic agent/metal ion-doped mesoporous silica

机译:超声诱导的反应性氧物种产生和线粒体特异性损伤的声学试剂/金属离子掺杂的介孔二氧化硅

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Designing tumor microenvironment (TME)-specific active nanoparticles with minimum side effects for synergistic cancer therapy has become a hot topic in the recent decades. Aiming at further enhancing the therapeutic efficacy, an in situ-induced mitochondrial dysfunction is a very promising strategy. To achieve these goals, a nano-sono-chemodynamic agent denoted as TPP-Cu@HMS, which integrated hematoporphyrin monomethyl ether (HMME), mPEG-NHS, triphenylphosphonium (TPP)-decorated mesoporous silica (MS) and coordinatively bound Cu2+ ions for mitochondria-specific sonodynamic-chemodynamic therapy (SDT-CDT) of cancer, was designed. Upon the ultrasound (US) treatment, TPP-Cu@HMS can specifically target mitochondria and in situ generate O-1(2) against cancer cells. Specifically, to overcome the short lifespan of O-1(2), the released Cu2+ ions from TPP-Cu@HMS could act as a Fenton-like agent to convert endogenous H2O2 to center dot OH in the acidic environment of cancer cells, disrupt the mitochondrial membrane potential and lead to mitochondrial disintegration, which could systematically enhance the therapeutic efficiency of SDT. Therefore, we highlight the current strategy as a promising prospect for cancer therapy.
机译:设计肿瘤微环境(TME)特异性活性纳米颗粒,对协同癌症治疗的最小副作用已成为近几十年来的热门话题。旨在进一步提高治疗效果,原位诱导的线粒体功能障碍是一种非常有前途的策略。为了实现这些目标,纳米超声化学动力学剂表示为TPP-Cu @ HMS,其整合血液卟啉单甲基醚(HMME),MPEG-NHS,三苯基鏻(TPP) - 研磨的中孔二氧化硅(MS)和协调地结合的Cu 2 +离子设计了癌症的线粒体特异性奏效性 - 化学动力学治疗(SDT-CDT)。在超声(US)处理后,TPP-Cu @ HMS可以特异性地靶向线粒体,并且原位产生癌细胞的O-1(2)。具体而言,为了克服O-1(2)的短寿命,来自TPP-Cu的释放的Cu2 +离子可以用作Fenton样剂以将内源性H 2 O 2转化为Center Dot OH在癌细胞的酸性环境中,破坏线粒体膜电位导致线粒体崩解,可以系统地提高SDT的治疗效率。因此,我们突出了目前的策略作为癌症治疗的有希望的前景。

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    《RSC Advances》 |2019年第68期|共8页
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  • 正文语种 eng
  • 中图分类 化学;
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