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Programming the composition of polymer blend particles for controlled immunity towards individual protein antigens

机译:对聚合物共混物颗粒的组成进行编程以控制对单个蛋白质抗原的免疫力

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摘要

In order for a more precise control over the quality and quantity of immune responses stimulated by synthetic particle-based vaccines, it is critical to control the colloidal stability of particles and the release of protein antigens in both extracellular space and intracellular compartments. Different proteins exhibit different sizes, charges and solubilities. This study focused on modulating the release and colloidal stability of proteins with varied isoelectric points. A polymer particle delivery platform made from the blend of three polymers, poly(lactic-coglycolic acid) (PLGA) and two random pH-sensitive copolymers, were developed. Our study demonstrated its programmability with respective to individual proteins. We showed the colloidal stability of particles at neutral environment and the release of each individual protein at different pH environments were dependent on the ratio of two charge polymers. Subsequently, two antigenic proteins, ovalbumin (OVA) and Type 2 Herpes Simplex Virus (HSV-2) glycoprotein D (gD) protein, were incorporated into particles with systematically varied compositions. We demonstrated that the level of in vitro CD8+ T cell and in vivo immune responses were dependent on the ratio of two charged polymers, which correlated well with the release of proteins. This study provided a promising design framework of pH-responsive synthetic vaccines for protein antigens of interest.
机译:为了更精确地控制基于合成颗粒的疫苗刺激的免疫反应的质量和数量,控制颗粒的胶体稳定性以及细胞外空间和细胞内区室中蛋白质抗原的释放至关重要。不同的蛋白质表现出不同的大小,电荷和溶解度。这项研究集中于调节具有不同等电点的蛋白质的释放和胶体稳定性。开发了由三种聚合物(聚乳酸-乙醇酸)(PLGA)和两种无规pH敏感共聚物的混合物制成的聚合物颗粒输送平台。我们的研究证明了其对个别蛋白质的可编程性。我们显示了颗粒在中性环境下的胶体稳定性,每种蛋白质在不同pH环境下的释放取决于两种电荷聚合物的比例。随后,将两种抗原蛋白,卵清蛋白(OVA)和2型单纯疱疹病毒(HSV-2)糖蛋白D(gD)蛋白,掺入系统组成各异的颗粒中。我们证明了体外CD8 + T细胞的水平和体内免疫反应取决于两种带电聚合物的比例,这与蛋白质的释放密切相关。这项研究为目标蛋白抗原的pH响应合成疫苗提供了一个有前途的设计框架。

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