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Polycarbonate-based ultra-pH sensitive nanoparticles improve therapeutic window

机译:基于聚碳酸酯的超pH敏感纳米粒子改善治疗窗

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Stimuli-sensitive nanomaterials with cooperative response are capable of converting subtle and gradual biological variations into robust outputs to improve the precision of diagnostic or therapeutic outcomes. In this study, we report the design, synthesis and characterization of a series of degradable ultra-pH sensitive (dUPS) polymers that amplify small acidic pH changes to efficacious therapeutic outputs. A hydrolytically active polycarbonate backbone is used to construct the polymer with pH-dependent degradation kinetics. One dUPS polymer, PSC7A, can achieve activation of the stimulator of interferon genes and antigen delivery upon endosomal pH activation, leading to T cell-mediated antitumor immunity. While a non-degradable UPS polymer induces granulomatous inflammation that persists over months at the injection site, degradable PSC7A primes a transient acute inflammatory response followed by polymer degradation and complete tissue healing. The improved therapeutic window of the dUPS polymers opens up opportunities in pH-targeted drug and protein therapy. Stimuli-responsive nanomaterials offer the opportunity to exploit nanoscale cooperativity to improve the precision of diagnostic or therapeutic outcomes. Here, the authors report the design, synthesis and characterization of a series of degradable ultra-pH sensitive polymers that amplify small acidic pH changes to efficacious therapeutic outputs.
机译:具有协同响应的刺激型纳米材料能够将微妙和逐渐的生物变化转化为强大的产出,以提高诊断或治疗结果的精度。在本研究中,我们报告了一系列可降解的超pH敏感(DUPS)聚合物的设计,合成和表征,该聚合物扩增小酸pH变化,以有效的治疗产出。水解活性的聚碳酸酯骨架用于构建具有pH依赖性降解动力学的聚合物。一个杜普聚合物PSC7a可以在内体pH激活时实现干扰素基因的刺激剂和抗原输送,导致T细胞介导的抗肿瘤免疫。虽然不可降解的UPS聚合物诱导颗粒状炎症,但在注射部位持续数月,可降解的PSC7a引发瞬时急性炎症反应,然后是聚合物降解和完全组织愈合。 DUPS聚合物的改进治疗窗口在pH靶向药物和蛋白质疗法中开辟了机会。刺激响应性纳米材料提供了利用纳米级合作的机会,以提高诊断或治疗结果的精确性。在这里,作者报告了一系列可降解的超pH值敏感聚合物的设计,合成和表征,其扩增小酸性pH变化,以有效的治疗输出。

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