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The Intrinsic Biological Identities of Iron Oxide Nanoparticles and Their Coatings: Unexplored Territory for Combinatorial Therapies

机译:氧化铁纳米粒子及其涂层的内在生物学性质:组合疗法的未开发领域

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摘要

Over the last 20 years, iron oxide nanoparticles (IONPs) have been the subject of increasing investigation due to their potential use as theranostic agents. Their unique physical properties (physical identity), ample possibilities for surface modifications (synthetic identity), and the complex dynamics of their interaction with biological systems (biological identity) make IONPs a unique and fruitful resource for developing magnetic field-based therapeutic and diagnostic approaches to the treatment of diseases such as cancer. Like all nanomaterials, IONPs also interact with different cell types in vivo, a characteristic that ultimately determines their activity over the short and long term. Cells of the mononuclear phagocytic system (macrophages), dendritic cells (DCs), and endothelial cells (ECs) are engaged in the bulk of IONP encounters in the organism, and also determine IONP biodistribution. Therefore, the biological effects that IONPs trigger in these cells (biological identity) are of utmost importance to better understand and refine the efficacy of IONP-based theranostics. In the present review, which is focused on anti-cancer therapy, we discuss recent findings on the biological identities of IONPs, particularly as concerns their interactions with myeloid, endothelial, and tumor cells. Furthermore, we thoroughly discuss current understandings of the basic molecular mechanisms and complex interactions that govern IONP biological identity, and how these traits could be used as a stepping stone for future research.
机译:在过去的20年中,由于它们的潜在用途作为其潜在用途,氧化铁纳米颗粒(IONP)是提高调查的主题。它们独特的物理性质(物理身份),表面修改的充分可能性(合成标识)以及它们与生物系统相互作用的复杂动态(生物身份)使IONPS成为开发基于磁场的治疗和诊断方法的独特和富有成效的资源治疗癌症等疾病。与所有纳米材料一样,IONPS也与体内不同的细胞类型相互作用,这是最终在短期和长期内决定其活动的特征。单核吞噬系统(巨噬细胞),树突细胞(DCS)和内皮细胞(ECS)的细胞接通在生物体中的大部分IONP遇到,并且还确定IONP生物分布。因此,对离子触发在这些细胞(生物身份)中的生物学效应是最重要的,以更好地理解和优化基于IONP的Theranostics的疗效。在本综述中,其重点是抗癌治疗,我们讨论了最近对IONP的生物学身份的发现,特别是与髓样,内皮和肿瘤细胞相互作用。此外,我们彻底讨论了目前对基本分子机制的谅解和控制IONP生物标识的复杂相互作用,以及这些特征如何作为未来研究的踏脚石。

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