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Recent progress in the engineering of multifunctional colloidal nanoparticles for enhanced photodynamic therapy and bioimaging

机译:增强光动力疗法和生物分析的多功能胶体纳米粒子工程中的最新进展

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This up-to-date review summarizes the design and current fabrication strategies that have been employed in the area of mono- and multifunctional colloidal nanoparticles - nanocarriers well suited for photodynamic therapy (PDT) and diagnostic purposes. Rationally engineered photosensitizer (PS)-loaded nanoparticles may be achieved via either noncovalent (i.e., self-aggregation, interfacial deposition, interfacial polymerization, or core-shell entrapment along with physical adsorption) or covalent (chemical immobilization or conjugation) processes. These PS loading approaches should provide chemical and physical stability to PS payloads. Their hydrophilic surfaces, capable of appreciable surface interactions with biological systems, can be further modified using functional groups (stealth effect) to achieve prolonged circulation in the body after administration and/or grafted by targeting agents (such as ligands, which bind to specific receptors uniquely expressed on the cell surface) or stimuli (e.g, pH, temperature, and light)-responsive moieties to improve their action and targeting efficiency. These attempts may in principle permit efficacious PDT, combination therapies, molecular diagnosis, and in the case of nanotheranostics simultaneous monitoring and treatment. Nanophotosensitizers (nano-PSs) should possess appropriate morphologies, sizes, unimodal distributions and surface processes to be successfully delivered to the place of action after systemic administration and should be accumulated in certain tumors by passive and/or active targeting. Additionally, physically facilitating drug delivery systems emerge as a promising approach to enhancing drug delivery, especially for the non-invasive treatment of deep-seated malignant tissues. Recent advances in nano-PSs are scrutinized, with an emphasis on design principles, via the promising use of colloid chemistry and nanotechnology. (C) 2018 Elsevier B.V. All rights
机译:该最新审查总结了在单核和多功能胶体纳米颗粒 - 纳米载体的面积中使用的设计和当前制造策略 - 纳米载体非常适合于光动力学治疗(PDT)和诊断目的。理性工程光敏剂(PS) - 可以通过非共价(即自聚集,界面沉积,界面聚合或核 - 壳夹在物理吸附)或共价(化学固定化或缀合)过程中来实现纳米颗粒。这些PS加载方法应为PS有效载荷提供化学和物理稳定性。能够使用官能团(隐形效应)进一步修饰其亲水性表面,能够与生物系统相互作用,以通过靶向剂(例如配体与特异性受体结合的配体接枝,在体内延长循环在细胞表面上唯一表达)或刺激(例如,pH,温度和光) - 夸张的部分,以改善其作用和靶向效率。这些尝试可能原则上允许有效的PDT,组合疗法,分子诊断,以及纳米移植的同时监测和治疗。纳米光溶胶(纳米PSS)应具有合适的形态,尺寸,单峰分布和表面过程,以成功地递送到系统施用后的作用,并且应通过被动和/或活性靶向在某些肿瘤中积累。此外,物理促进药物递送系统作为提高药物递送的有希望的方法,特别是对于对深层恶性组织的非侵入性治疗。纳米PSS最近的进展被审查,重点是设计原则,通过有希望使用胶体化学和纳米技术。 (c)2018 Elsevier B.V.所有权利

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