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ENCAPSULATION-FREE CONTROLLED PROTEIN RELEASE SYSTEM

机译:无胶囊控制的蛋白质释放系统

摘要

The present disclosure provides a delivery system for controlled protein release without encapsulation. Identical, burst-free, extended release profiles for three different protein therapeutics were obtained with and without encapsulation in PLGA nanoparticles embedded within a hydrogel. Using both positively and negatively charged proteins, it was shown that short-range electrostatic interactions between the proteins and the PLGA nanoparticles are the underlying mechanism for controlled release. Moreover, tunable release was demonstrated by modifying nanoparticle concentration, nanoparticle size, or environmental pH. Additionally, the utility of this system was demonstrated in vivo for BDNF delivery in a rat model of stroke. These new insights obviate the need for encapsulation and offer promising, translatable strategies for more effective delivery of therapeutic biomolecules.
机译:本公开提供了用于无需包封的受控蛋白质释放的递送系统。在有和没有封装在嵌入水凝胶内的PLGA纳米颗粒中的情况下,获得了三种不同蛋白质治疗药物的相同,无破裂,延长释放曲线。使用带正电和带负电的蛋白质,结果表明,蛋白质与PLGA纳米粒子之间的短程静电相互作用是控制释放的基本机制。此外,通过改变纳米粒子的浓度,纳米粒子的大小或环境pH值可以证明可调释。另外,该系统的实用性在中风的大鼠模型中体内证明了BDNF的递送。这些新见解消除了对封装的需求,并提供了有希望的,可翻译的策略,以更有效地递送治疗性生物分子。

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