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将不同类型负载碳酸氢铵的多功能脂质体组合在一起,构建微针阵列作为阴道黏膜疫苗佐剂双重递药系统(VADDS)。

Combining different types of multifunctional liposomes loaded with ammonium bicarbonate to fabricate microneedle arrays as a vaginal mucosal vaccine adjuvant-dual delivery system (VADDS).

机构信息

School of Biological and Medical Engineering, Hefei University of Technology, 193 Tun Brook Road, Hefei, Anhui Province 230009, China.

School of Pharmacy, Anhui Medical University, 81 Plum Hill Road, Hefei, Anhui Province 230032, China.

出版信息

J Control Release. 2017 Jan 28;246:12-29. doi: 10.1016/j.jconrel.2016.12.009. Epub 2016 Dec 13.

DOI:10.1016/j.jconrel.2016.12.009
PMID:27986552
Abstract

To develop effective mucosal vaccines, two types of multifunctional liposomes, the mannosylated lipid A-liposomes (MLLs) with a size of 200nm and the stealth lipid A-liposomes (SLLs) of 50nm, both loaded with a model antigen and NHHCO, were fabricated together into microneedles, forming the proSLL/MLL-constituted microneedle array (proSMMA), which upon rehydration dissolved rapidly recovering the initial MLLs and SLLs. Mice vaccinated with proSMMAs by vaginal mucosa patching other than conventional intradermal administration established robust antigen-specific humoral and cellular immunity at both systemic and mucosal levels, especially, in the reproductive and intestinal ducts. Further exploration demonstrated that the MLLs reconstituted from the administered proSMMAs were mostly taken up by vaginal mucosal dendritic cells, whereas the recovered SLLs trafficked directly to draining lymph nodes wherein to be picked up by macrophages. Moreover, the antigens delivered by either liposomes were also cross-presented for MHC-I displaying by APCs thanks to lysosome escape and ROS (reactive oxygen species) stimulation, both of which occurred when lysosomal acidifying the liposome-released NHHCO into CO and NH/NH to rupture lysosomes by gas expansion and to cause ROS production by excessive ammonia induction, resulting in a mixed Th1/Th2 type response which was also promoted by liposomal lipid A via activation of TLR4. In addition, vaginal vaccination of the engineered HSV2 antigen gD-loaded proSMMAs successfully protected mice from the virus challenge. Thus, the proSMMAs are in fact a vaccine adjuvant-dual delivery system capable of eliciting robust humoral and cellular immunity against the invading pathogens, especially, the sexually transmitted ones.

摘要

为了开发有效的黏膜疫苗,我们制备了两种多功能脂质体,即 200nm 大小的甘露糖基化脂质 A 脂质体(MLLs)和 50nm 的隐形脂质 A 脂质体(SLLs),均负载有模型抗原和 NHHCO,并将它们一起制成微针,形成 proSLL/MLL 构成的微针阵列(proSMMA),当重新水合时,它会迅速溶解,恢复最初的 MLLs 和 SLLs。通过阴道黏膜贴片而非常规皮内给药,用 proSMMAs 接种疫苗的小鼠在全身和黏膜水平上建立了强大的抗原特异性体液和细胞免疫,特别是在生殖和肠道导管中。进一步的探索表明,从给予的 proSMMAs 中重建的 MLLs 主要被阴道黏膜树突状细胞摄取,而回收的 SLLs 则直接运送到引流淋巴结,在那里被巨噬细胞摄取。此外,由于溶酶体逃逸和 ROS(活性氧)刺激,两种脂质体递送的抗原也通过 MHC-I 进行交叉呈递,这是通过将溶酶体酸化释放的 NHHCO 转化为 CO 和 NH/NH 来破坏溶酶体,以及通过过度氨诱导产生 ROS 来实现的,这导致了混合 Th1/Th2 型反应,这种反应也通过脂质体脂质 A 通过激活 TLR4 来促进。此外,工程化 HSV2 抗原 gD 负载的 proSMMAs 的阴道疫苗接种成功地保护了小鼠免受病毒攻击。因此,proSMMAs 实际上是一种疫苗佐剂-双重递药系统,能够引发针对入侵病原体的强大体液和细胞免疫,特别是针对性传播的病原体。

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