Am80-lipid nanoparticles serve as an enteric mucosal adjuvant following parenteral immunization with inactivated polio vaccine

佐剂 医学 免疫学 粘膜免疫 免疫 免疫 肠粘膜 免疫系统 粘膜免疫学 体内 接种疫苗 抗原 淋巴 微生物学 脊髓灰质炎灭活疫苗 脊髓灰质炎病毒 淋巴结 粘膜 病毒学 灭活疫苗 抗体 淋巴系统
作者
Behnaz Eshaghi,Erika Yan Wang,Sevinj Mursalova,Timothy A. Forster,Ninaad Lasrado,Jinbi Tian,Dorin Artzi,Stacey Qiaohui Lin,Zongting Wu,Xin Yang,WonTaek Chung,Ilin Sadeghi,Johnny Garcia,Ziqi Chen,Olivia Sheridan,Rishi Das,Alicia Lau,Aki Gurram,Bernardo A. Mainou,Kathryn A.V. Jones
出处
期刊:Science Advances [American Association for the Advancement of Science]
卷期号:12 (23): eaea5433-eaea5433
标识
DOI:10.1126/sciadv.aea5433
摘要

Enteric pathogens are a major contributor to the global disease burden, necessitating vaccines capable of inducing robust gastrointestinal mucosal immunity. Achieving this response is especially challenging with inactivated or subunit vaccines, which lack the ability of live-attenuated formulations to mimic the natural infection process needed to induce strong intestinal mucosal immunity. Specifically, the inactivated polio vaccine (IPV), administered parenterally, elicits strong systemic immunity but fails to induce the mucosal IgA responses required to fully block poliovirus transmission, a critical step toward complete eradication. To address this limitation, we developed a clinically translatable and scalable nanoparticle-based intestinal mucosal adjuvant by encapsulating Am80, a small hydrophobic molecule known to promote intestinal mucosal immunity, within nanoparticles (NPs) designed for lymph node delivery, without requiring antigen modification, encapsulation, or adsorption. Encapsulation in NPs eliminated the need for the use of organic solvents, reduced toxicity, and prevented degradation, while lipid nanoparticles (Am80-LNPs) were engineered for sustained release over 3 to 5 days with high encapsulation efficiency (78 ± 9%). Cy5-labeled Am80-LNPs localized to draining lymph nodes within 6 hours and were retained for up to 72 hours. Coadministration of Am80-LNPs with the licensed IPV-2 in a Wistar rat model significantly boosted IPV-2-specific fecal IgA by 20-fold compared to IPV-2 alone and threefold over free Am80. These findings demonstrate that Am80-LNPs significantly enhance IPV-2-specific mucosal immunity in vivo and suggest their potential as a potent mucosal adjuvant against other enteric pathogens.
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