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首页> 外文期刊>European journal of pharmaceutics and biopharmaceutics: official journal of Arbeitsgemeinschaft fuer Pharmazeutische Verfahrenstechnik e.V >Development of PLGA nanoparticle loaded dissolving microneedles and comparison with hollow microneedles in intradermal vaccine delivery
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Development of PLGA nanoparticle loaded dissolving microneedles and comparison with hollow microneedles in intradermal vaccine delivery

机译:PLGA纳米粒子的研制溶解溶解微针及其在皮内疫苗递送中的空心微针比较

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摘要

Skin is an attractive but also very challenging immunisation site for particulate subunit vaccines. The aim of this study was to develop hyaluronan (HA)-based dissolving microneedles (MNs) loaded with PLGA nanoparticles (NPs) co-encapsulating ovalbumin (OVA) and poly(I:C) for intradermal immunisation. The NP:HA ratio used for the preparation of dissolving MNs appeared to be critical for the quality of MNs and their dissolution in ex vivo human skin. Asymmetrical flow field-flow fractionation and dynamic light scattering were used to analyse the NPs released from the MNs in vitro. Successful release of the NPs depended on the drying conditions during MN preparation. The delivered antigen dose from dissolving MNs in mice was determined to be 1 mu g OVA, in NPs or as free antigen, by using near-infrared fluorescence imaging. Finally, the immunogenicity of the NPs after administration of dissolving MNs (NP:HA weight ratio 1:4) was compared with that of hollow MN-delivered NPs in mice. Immunization with free antigen in dissolving MNs resulted in equally strong immune responses compared to delivery by hollow MNs. However, humoral and cellular immune responses evoked by NP-loaded dissolving MNs were inferior to those elicited by NPs delivered through a hollow MN. In conclusion, we identified several critical formulation parameters for the further development of NP-loaded dissolving MNs.
机译:皮肤是一种有吸引力的,但对于颗粒亚基疫苗的免疫部位也是非常挑战性的。本研究的目的是开发透明质酸(HA)的溶解微针(MNS),该溶解用PLGA纳米颗粒(NPS)共同包封的卵磷酸酯(OVA)和聚(I:C)用于皮内免疫。用于制备溶解MNS的NP:HA比对于MNS的质量和它们在离体人体皮肤中的溶解至关重要。不对称流场 - 流动分级和动态光散射用于分析在体外从MNS释放的NPS。成功释放NPS在Mn制备期间依赖于干燥条件。通过使用近红外荧光成像,将递送的抗原剂量从小鼠中溶解在小鼠中,在NPS或作为游离抗原中的1μgova。最后,将NPS在施用溶解MNS(NP:HA重量比1:4)后的NPS与小鼠中的中空Mn递送的NPS进行比较的免疫原性。与通过中空MN的递送相比,用游离抗原免疫抗原导致同样强烈的免疫应答。然而,通过NP溶解的MNS引起的体温和细胞免疫应答差不等于通过中空Mn递送的NPS引起的那些。总之,我们确定了几种关键配方参数,用于进一步发展NP溶解MNS。

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