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Biodistribution of vaccines comprised of hydrophobically-modified poly(γ-glutamic acid) nanoparticles and antigen proteins using fluorescence imaging

机译:使用荧光成像技术对由疏水修饰的聚(γ-谷氨酸)纳米颗粒和抗原蛋白组成的疫苗进行生物分配

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Fluorophores-modified nanoparticles comprised of poly(γ-glutamic acid)-phenylalanine (γ-PGA-Phe-633) and ovalbumin (OVA-750) termed NPs-633/OVA-750 were prepared to assess their biodistribution using an in vivo fluorescence imager. Dynamic light scattering measurements indicated that NPs-633/OVA-750 were about 200 nm in diameter. The release of encapsulated OVA from NPs-633 in PBS was negligible (~10%) for a week. When subcutaneously injected, the localization period of OVA-750-encapsulated into NPs-633 at the site of injection (SOI) was much longer than that of free OVA-750, but was shorter as compared to a mixture with aluminum hydroxide. The NPs-633 disappeared at the SOI and major organs within 1 month after administration. Moreover, intravenously and intraperitoneally administered NPs-633 were mainly observed at the liver, and there was more rapid clearance from all organs as compared with non-biodegradable NPs. These fast clearance and degradation characteristics of γ-PGA-Phe NPs will be important not only for avoiding undesired adverse effects, but also for inducing a strong vaccine effect.
机译:制备了由聚(γ-谷氨酸)-苯丙氨酸(γ-PGA-Phe-633)和卵清蛋白(OVA-750)组成的被称为NPs-633 / OVA-750的荧光团修饰的纳米颗粒,以利用体内荧光评估其生物分布成像仪。动态光散射测量表明,NPs-633 / OVA-750的直径约为200 nm。在PBS中从NPs-633释放出包封的OVA可以忽略不计(约10%)。皮下注射时,在注射位点(SOI)封装到NPs-633中的OVA-750的定位时间比游离的OVA-750的定位时间长得多,但比与氢氧化铝的混合物短。给药后1个月内,NPs-633在SOI和主要器官消失。而且,主要在肝脏观察到静脉内和腹膜内施用的NPs-633,并且与不可生物降解的NPs相比,其从所有器官的清除更快。 γ-PGA-PheNP的这些快速清除和降解特性不仅对于避免不良副作用,而且对于诱导强烈的疫苗作用都是重要的。

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