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聚乙二醇化阳离子脂质体可显著增强疫苗诱导的免疫应答:淋巴转运和生物分布的作用。

PEGylated cationic liposomes robustly augment vaccine-induced immune responses: Role of lymphatic trafficking and biodistribution.

机构信息

Key Lab of Health Informatics of Chinese Academy of Sciences, Shenzhen Key Laboratory of Cancer Nanotechnology, Institute of Biomedical and Health Engineering, Shenzhen Institutes of Advance Technology, Chinese Academy of Science, People's Republic of China.

出版信息

J Control Release. 2012 Apr 10;159(1):135-42. doi: 10.1016/j.jconrel.2011.12.017. Epub 2011 Dec 29.


DOI:10.1016/j.jconrel.2011.12.017
PMID:22226776
Abstract

Lymph nodes (LNs) are peripheral lymphoid organs essential for vaccine-induced immune responses. Although cationic liposomes have been documented as a novel adjuvant and vaccine delivery system, whether enhancing LN targeting would improve the efficiency of cationic liposome-formulated vaccines has not been elucidated yet. In the present study we investigated the effect of PEGylation on LN targeting and the immunogenicity of cationic liposome-formulated vaccines. DOTAP cationic liposomes were incorporated with 1 or 5mol% of DSPE-PEG2000 and labeled with near infrared fluorescent dyes. The lymphatic trafficking and biodistribution of different liposomes after subcutaneous (s.c.) injection were recorded using an in-vivo imaging system. The results showed that incorporation of 1mol% DSPE-PEG2000 not only accelerated the drainage of DOTAP liposomes into draining LNs, but also prolonged their LN retention and enhanced liposome uptake by resident antigen-presenting cells. On the other hand, although incorporating 5mol% of DSPE-PEG2000 into DOTAP liposomes enhanced their LN retention and uptake to a lesser extent, it prolonged blood circulation of DOTAP liposomes and increased their splenic accumulation. In addition, PEGylated DOTAP liposomes augmented primary and secondary anti-OVA antibody responses more potently than nonPEGylated DOTAP liposomes did. Hence, incorporating a small amount of DSPE-PEG2000 into DOTAP liposomes not only increased the passive LN targeting of DOTAP-formulated vaccines but also modulated their biodistribution in vivo, which consequently improved the efficiency of cationic liposome-formulated vaccines.

摘要

淋巴结 (LNs) 是疫苗诱导免疫反应所必需的外周淋巴器官。虽然阳离子脂质体已被证明是一种新型佐剂和疫苗递送系统,但增强 LN 靶向是否会提高阳离子脂质体配方疫苗的效率尚未阐明。在本研究中,我们研究了聚乙二醇化对 LN 靶向和阳离子脂质体配方疫苗免疫原性的影响。DOTAP 阳离子脂质体与 1 或 5mol% 的 DSPE-PEG2000 结合,并标记有近红外荧光染料。使用体内成像系统记录不同脂质体在皮下 (s.c.) 注射后的淋巴转运和组织分布。结果表明,1mol% DSPE-PEG2000 的掺入不仅加速了 DOTAP 脂质体进入引流淋巴结的排出,而且延长了它们在淋巴结中的保留时间,并增强了驻留抗原呈递细胞对脂质体的摄取。另一方面,尽管将 5mol% 的 DSPE-PEG2000 掺入 DOTAP 脂质体中在较小程度上增强了它们在淋巴结中的保留和摄取,但它延长了 DOTAP 脂质体的血液循环并增加了它们在脾脏中的积累。此外,PEG 化的 DOTAP 脂质体比非 PEG 化的 DOTAP 脂质体更有效地增强了原发性和次级抗 OVA 抗体反应。因此,将少量的 DSPE-PEG2000 掺入 DOTAP 脂质体中不仅增加了 DOTAP 配方疫苗的被动 LN 靶向,而且还调节了它们在体内的分布,从而提高了阳离子脂质体配方疫苗的效率。

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