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首页> 外文期刊>ACS applied materials & interfaces >Reduction/Oxidation-Responsive Hierarchical Nanoparticles with Self-Driven Degradability for Enhanced Tumor Penetration and Precise Chemotherapy
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Reduction/Oxidation-Responsive Hierarchical Nanoparticles with Self-Driven Degradability for Enhanced Tumor Penetration and Precise Chemotherapy

机译:减少/氧化反应性分层纳米颗粒,具有自驱动可降解性,可增强肿瘤渗透和精确化疗

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摘要

Deep tumor penetration, long blood circulation, rapid drug release, and sufficient stability are the most concerning dilemmas of nano-drug-delivery systems for efficient chemotherapy. Herein, we develop reduction/oxidation-responsive hierarchical nanoparticles co-encapsulating paclitaxel (PTX) and pH-stimulated hyaluronidase (pSH) to surmount the sequential biological barriers for precise cancer therapy. Poly(ethylene glycol) diamine (PEG-dia) is applied to collaboratively cross-link the shell of nanoparticles self-assembled by a hyaluronic acid-stearic acid conjugate linked via a disulfide bond (HA-SS-SA, HSS) to fabricate the hierarchical nanoparticles (PHSS). The PTX and pSH coloaded hierarchical nanoparticles (PTX/pSH-PHSS) enhance the stability in normal physiological conditions and accelerate drug release at tumorous pH, and highly reductive or oxidative environments. Functionalized with PEG and HA, the hierarchical nanoparticles preferentially prolong the circulation time, accumulate at the tumor site, and enter MDA-MB-231 cells via CD44-mediated endocytosis. Within the acidic tumor micro-environment, pSH would be partially reactivated to decompose the dense tumor extracellular matrix for deep tumor penetration. Interestingly, PTX/pSH-PHSS could be degraded apace by the completely activated pSH within endo/lysosomes and the intracellular redox micro-environment to facilitate drug release to produce the highest tumor inhibition (93.71%) in breast cancer models.
机译:深肿瘤渗透,长血液循环,快速释放,充分稳定性是纳米药物输送系统最有效化疗的困境。在此,我们开发还原/氧化响应性分层纳米颗粒共同包封的紫杉醇(PTX)和pH刺激的透明质酸酶(PSH)以超越序贯生物屏障,用于精确癌症治疗。将聚(乙二醇)二胺(PEG-DIA)应用于通过通过二硫键(HA-SS-SA,HSS)连接的透明质酸 - 硬脂酸缀合物通过二硫键(HA-SS-SA,HSS)来协作交联链接纳米颗粒的壳体。分层纳米粒子(pHS)。 PTX和PSH加冕的分层纳米颗粒(PTX / PHSS)增强了正常生理条件下的稳定性,并在肿瘤pH下加速药物释放,以及高度还原或氧化环境。用PEG和HA官能化,分层纳米粒子优先延长循环时间,在肿瘤部位积聚,并通过CD44介导的内吞作用进入MDA-MB-231细胞。在酸性肿瘤微环境中,PSH将部分重新激活以分解致密肿瘤细胞外基质进行深肿瘤渗透。有趣的是,PTX / PSH-PHS可以通过Endo /溶酶体内的完全活化的PSH降解APACE和细胞内氧化还原微环境,以促进药物释放,以产生乳腺癌模型中的最高肿瘤抑制(93.71%)。

著录项

  • 来源
    《ACS applied materials & interfaces》 |2020年第16期|共19页
  • 作者单位

    China Pharmaceut Univ Dept Pharmaceut State Key Lab Nat Med Nanjing 210009 Peoples R China;

    China Pharmaceut Univ Dept Pharmaceut State Key Lab Nat Med Nanjing 210009 Peoples R China;

    China Pharmaceut Univ Dept Pharmaceut State Key Lab Nat Med Nanjing 210009 Peoples R China;

    China Pharmaceut Univ Dept Pharmaceut State Key Lab Nat Med Nanjing 210009 Peoples R China;

    China Pharmaceut Univ Dept Pharmaceut State Key Lab Nat Med Nanjing 210009 Peoples R China;

    China Pharmaceut Univ Ctr New Drug Safety Evaluat &

    Res Nanjing 210009 Peoples R China;

    Univ Manitoba Fac Pharm Winnipeg MB R3E 0T5 Canada;

    China Pharmaceut Univ Ctr New Drug Safety Evaluat &

    Res Nanjing 210009 Peoples R China;

    China Pharmaceut Univ Dept Pharmaceut State Key Lab Nat Med Nanjing 210009 Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学工业;
  • 关键词

    dual redox-response; deep tumor penetration; hyaluronidase; tumor micro-environment; cancer therapy;

    机译:双氧化还原响应;深肿瘤渗透;透明质酸酶;肿瘤微环境;癌症治疗;

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