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Safety and photochemotherapeutic application of poly(γ-glutamic acid)-based biopolymeric nanoparticle

机译:聚(γ-谷氨酸)基生物聚合物纳米粒子的安全性和光化学疗法应用

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摘要

The safety of nanomaterials, a crucial consideration for clinical translation, is enhanced by using building blocks that are biologically nontoxic. Here, we used poly(γ-glutamic acid) (γ-PGA) and dopamine as building blocks of polymeric nanomaterials for carrying hydrophobic anticancer drugs. The introduction of phenylalanine onto γ-PGA enabled the resulting amphiphilic derivative of γ-PGA acid to self-assemble in the presence of the anticancer drug paclitaxel (PTX) to form PTX-encapsulated micelles. The surfaces of PTX-loaded micelles were then coated with polymerized dopamine (PDA). The PDA-coated, amphiphilic γ-PGA-based micelles (AM) carrying PTX (PDA/AM/P) exerted near-infrared-responsive photothermal effects. Near-infrared irradiation of cancer cells treated with PDA/AM/P nanoparticles produced a greater anticancer effect than that observed in other treatment groups, indicating a synergistic effect. Intravenous administration of PDA/AM/P completely ablated tumors and prevented their recurrence. Notably, the in vivo safety profile of PDA/AM/P nanoparticles allowed PTX to be delivered at a 3.6-fold higher dose than was possible with PTX solubilized in surfactant, and circumvented the side effects of the surfactant. These results support the multifunctional potential of PDA/AM for the delivery of various hydrophobic drugs and imaging dyes for safe translation of nanomaterials into the clinic.
机译:纳米材料的安全性(作为临床翻译的关键考虑因素)通过使用生物无毒的结构单元得以增强。在这里,我们使用聚(γ-谷氨酸)(γ-PGA)和多巴胺作为携带疏水性抗癌药物的聚合物纳米材料的基础。在抗癌药紫杉醇(PTX)存在下,将苯丙氨酸引入γ-PGA可使所得的γ-PGA酸两亲衍生物自组装,从而形成PTX封装的胶束。然后将负载有PTX的胶束的表面涂上聚合的多巴胺(PDA)。带有PTX(PDA / AM / P)的PDA涂层,两亲基于γ-PGA的胶束(AM)发挥了近红外响应的光热效应。用PDA / AM / P纳米颗粒处理的癌细胞的近红外辐射产生的抗癌作用比其他治疗组更强,表明具有协同作用。静脉内施用PDA / AM / P可完全消融肿瘤并防止其复发。值得注意的是,与溶解在表面活性剂中的PTX相比,PDA / AM / P纳米粒子的体内安全性使PTX可以以3.6倍的高剂量给药,并避免了表面活性剂的副作用。这些结果支持了PDA / AM在输送各种疏水性药物和显像染料方面的多功能潜力,从而可以将纳米材料安全地翻译到临床中。

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