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首页> 外文期刊>Biomaterials >Drug releasing behavior of hybrid micelles containing polypeptide triblock copolymer.
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Drug releasing behavior of hybrid micelles containing polypeptide triblock copolymer.

机译:含有多肽三嵌段共聚物的杂化胶束的药物释放行为。

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We report a new type of hybrid polymeric micelles for drug delivery applications. These micelles consist of PLGA (PLGA: poly(l-glutamic acid)) and PEG (PEG: polyethylene glycol) mixed corona chains. In acidic condition, PLGA undergoes a transformation from water-soluble random coils to water-insoluble alpha-helix, leading to microphase separation in micelle coronas and formation of PEG channels. These channels connect the inner core and the outer milieu, accelerating the diffusion of drugs from micelles. The micelles were prepared through a co-micellization of PLGA-b-PPO-b-PLGA (PPO: poly(propylene oxide)) and PEG-b-PPO in water. During the self-assembly, the PPO blocks of both block copolymers aggregated into cores that were surrounded by mixed corona chains of PLGA and PEG blocks. We confirmed this structure by using a number of characterization techniques including nuclear magnetic resonance spectroscopy, zeta potential, circular dichroism, and dynamic light scattering. We also performed molecular dynamics (MD) simulations to verify the models of the hybrid micelle structure. One advantage of the hybrid micelles as drug carriers is their tunable release rate without sacrificing colloidal stability. The rate can be tuned by either micelle structures such as the composition of the mixture or external parameters such as pH.
机译:我们报告了一种新型的混合高分子胶束,用于药物输送应用。这些胶束由PLGA(PLGA:聚(1-谷氨酸))和PEG(PEG:聚乙二醇)混合电晕链组成。在酸性条件下,PLGA经历了从水溶性无规卷曲到水不溶性α螺旋的转变,导致胶束电晕中的微相分离和PEG通道的形成。这些通道连接内核和外部环境,从而加速了药物从微团的扩散。通过将PLGA-b-PPO-b-PLGA(PPO:聚环氧丙烷)和PEG-b-PPO在水中共同胶束化来制备胶束。在自组装过程中,两种嵌段共聚物的PPO嵌段聚集成核,并被PLGA和PEG嵌段的混合电晕链包围。我们通过使用许多表征技术,包括核磁共振波谱,ζ电位,圆二色性和动态光散射,确认了这种结构。我们还进行了分子动力学(MD)模拟,以验证混合胶束结构的模型。杂化胶束作为药物载体的优点之一是其可调节的释放速率而不会牺牲胶体稳定性。可以通过胶束结构(例如混合物的组成)或外部参数(例如pH)来调整速率。

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