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Free radical-mediated targeting and immobilization of coupled payloads

机译:自由基介导的耦合有效载荷的靶向和固定化

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Targeted drug delivery is a promising approach to enhance the accumulation of therapies in diseased tissues while limiting off-site effects. Ligand-receptor interactions are traditionally identified to deliver therapies, and although specific, this can be costly and often suffers from limited sensitivity. An emerging approach is to target intermediary species that modulate disease progression. Here, we propose novel methods of targeting therapies by using native free radicals as a homing signal. Elevated concentrations of free radicals are a characteristic comorbidity of many different diseases. In polymer chemistry, free radicals are frequently used to initiate crosslinking reactions. We proposed that free radicals elevated in injury sites are capable of inducing crosslinking of acrylate groups on polymer chains. Coupling payloads to the polymer then allow for specific targeting of therapies to areas with elevated free radicals. We demonstrate in vitro proof-of-principle of this approach. Reactive oxygen species (ROS) initiated crosslinking of acrylated PEGs, which immobilized a fluorescent payload within tissue mimics. The cross-linking efficiency and immobilization potential varied with the polymer chain length, suggesting that a tuneable platform can be achieved. Together these results provide promising proof-of-concept for using free radicals to specifically target and sustain nearly endless payloads to disease sites.
机译:有针对性的药物递送是一种有希望的方法,可以增强患病组织中疗法的积累,同时限制缺失的效果。传统上鉴定配体 - 受体相互作用以提供疗法,虽然具体,但这可能是昂贵的并且通常存在有限的灵敏度。一种新兴的方法是靶向调节疾病进展的中介物种。这里,我们通过使用本机自由基作为归位信号提出了靶向治疗的新方法。升高的自由基浓度是许多不同疾病的特征化合并症。在聚合物化学中,通常使用自由基来引发交联反应。我们提出损伤部位升高的自由基能够在聚合物链中诱导丙烯酸酯基团的交联。将有效载荷耦合到聚合物,然后允许对具有升高自由基的区域进行特定靶向疗法。我们展示了这种方法的体外证明原理。反应性氧物质(ROS)引发了丙烯酸粘合剂的交联,其将荧光有效载荷固定在组织模拟中。交联效率和固定电位随聚合物链长而变化,表明可以实现可调平台。这些结果共同提供了有希望的概念证据,用于使用自由基特异性靶向并维持几乎无数的有效载荷。

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