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载药纳米胶束将有效载荷递送至淋巴结免疫细胞,并延长移植物存活时间。

Nano-sized drug-loaded micelles deliver payload to lymph node immune cells and prolong allograft survival.

机构信息

Institute of Bioengineering, École Polytechnique Fédérale de Lausanne-EPFL, 1015 Lausanne, Switzerland.

出版信息

J Control Release. 2011 Dec 10;156(2):154-60. doi: 10.1016/j.jconrel.2011.08.009. Epub 2011 Aug 12.

DOI:10.1016/j.jconrel.2011.08.009
PMID:21864593
Abstract

By delivering immunomodulatory drugs in vivo directly to lymph nodes draining an injection site, an opportunity exists to increase drug bioavailability to local immune cells. Importantly, particles smaller than 100 nm are efficiently transported through lymphatic vessels to draining lymph nodes. To investigate whether this approach could be used for local delivery of immunomodulatory drugs, amphiphilic poly(ethylene glycol)-bl-poly(propylene sulfide) (PEG-bl-PPS) block copolymers forming 50 nm micelles were used to encapsulate hydrophobic drugs. Micelle drainage was determined using fluorescent micelles and showed effective targeting of multiple immune cell subsets in lymph nodes. For functional studies of our formulations, two approaches were considered. To evaluate the efficacy of anti-inflammatory drug delivery, dendritic cell activation was shown to be prevented when mice were pretreated with micelles loaded with the glucocorticoid mometasone and then challenged with the TLR9 ligand, CpG. To evaluate whether immunosuppressive drug-loaded micelles were effective in prolonging MHC-mismatched allograft survival, BALB/c mice were treated for 14 consecutive days with drug-loaded micelles following transplantation of allogenic C57BL/6 tail skin. Micelles loaded with a mixture of rapamycin and tacrolimus prolonged allograft survival by 2-fold. Our results indicate that the drug-loaded micelle approach effectively targets the draining lymph nodes and exhibits proper immune regulation.

摘要

通过将免疫调节药物直接递送至注射部位引流的淋巴结中,为增加药物对局部免疫细胞的生物利用度提供了机会。重要的是,小于 100nm 的颗粒可通过淋巴管有效地运输到引流淋巴结。为了研究这种方法是否可用于免疫调节药物的局部递送,采用两亲性聚乙二醇-嵌段-聚(丙烯基硫化物)(PEG-bl-PPS)嵌段共聚物形成 50nm 胶束来包封疏水性药物。使用荧光胶束测定胶束引流,结果显示其可有效地靶向淋巴结中的多种免疫细胞亚群。对于我们制剂的功能研究,考虑了两种方法。为了评估抗炎药物递送的功效,当预先用负载有糖皮质激素倍他米松的胶束处理小鼠,然后用 TLR9 配体 CpG 进行挑战时,发现树突状细胞的激活被阻止。为了评估负载免疫抑制剂的胶束是否可有效延长 MHC 错配同种异体移植物的存活期,在同种异体 C57BL/6 尾巴皮肤移植后,BALB/c 小鼠连续 14 天用负载药物的胶束进行治疗。负载雷帕霉素和他克莫司混合物的胶束使同种异体移植物的存活期延长了 2 倍。我们的结果表明,负载药物的胶束方法可有效地靶向引流淋巴结,并表现出适当的免疫调节作用。

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