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Rationalization of a nanoparticle-based nicotine nanovaccine as an effective next-generation nicotine vaccine: a focus on hapten localization

机译:基于纳米颗粒的尼古丁纳米疫苗作为一种有效的下一代尼古丁疫苗的合理化:对半抗原定位的关注

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摘要

A lipid-polymeric hybrid nanoparticle-based next-generation nicotine nanovaccine was rationalized in this study to combat nicotine addiction. A series of nanovaccines, which had nicotine-haptens localized on carrier protein (LPKN), nanoparticle surface (LPNK), or both (LPNKN), were designed to study the impact of hapten localization on their immunological efficacy. All three nanovaccines were efficiently taken up and processed by dendritic cells. LPNKN induced a significantly higher immunogenicity against nicotine and a significantly lower anti-carrier protein antibody level compared to LPKN and LPNK. Meanwhile, it was found that the anti-nicotine antibodies elicited by LPKN and LPNKN bind nicotine stronger than those elicited by LPKN, and LPNK and LPNKN resulted in a more balanced Th1-Th2 immunity than LPKN. Moreover, LPNKN exhibited the best ability to block nicotine from entering the brain of mice. Collectively, the results demonstrated that the immunological efficacy of the hybrid nanoparticle-based nicotine vaccine could be enhanced by modulating hapten localization, providing a promising strategy to combatting nicotine addiction.
机译:在这项研究中,基于脂质-聚合物杂化纳米颗粒的下一代尼古丁纳米疫苗被合理化以对抗尼古丁成瘾。设计了一系列具有尼古丁半抗原定位在载体蛋白(LPKN),纳米颗粒表面(LPNK)或两者都具有(LPNKN)的纳米疫苗,以研究半抗原定位对其免疫功效的影响。树突状细胞有效吸收并处理了所有三种纳米疫苗。与LPKN和LPNK相比,LPNKN诱导出对尼古丁的显着更高的免疫原性,并显着降低了抗载体蛋白抗体的水平。同时,发现LPKN和LPNKN引起的抗烟碱抗体结合烟碱的强度比LPKN引起的抗尼古丁抗体强,并且LPNK和LPNKN导致的Th1-Th2免疫力比LPKN更平衡。此外,LPNKN具有阻止尼古丁进入小鼠大脑的最佳能力。总的来说,这些结果表明,通过调节半抗原的定位,可以增强基于纳米粒子的混合尼古丁疫苗的免疫学有效性,为对抗尼古丁成瘾提供了有希望的策略。

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