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新型 α-甘露糖功能化聚(β-氨基酯)纳米粒作为 mRNA 疫苗,可增加脾脏中抗原提呈细胞的选择性。

Novel α-mannose-functionalized poly(β-amino ester) nanoparticles as mRNA vaccines with increased antigen presenting cell selectivity in the spleen.

机构信息

Grup d'Enginyeria de Materials (Gemat), Institut Químic de Sarrià (IQS), Universitat Ramon Llull (URL), 08017 Barcelona, Spain.

Laboratoy of Biochemistry, Institut Químic de Sarrià (IQS), Universitat Ramon Llull (URL), 08017 Barcelona, Spain.

出版信息

J Mater Chem B. 2023 Jul 12;11(27):6412-6427. doi: 10.1039/d3tb00607g.

Abstract

mRNA vaccination has emerged as a prominent therapy for the future of medicine. Despite the colossal advance in this technology and worldwide efficacy proof ( COVID vaccines), mRNA carriers still lack cell/tissue specificity, leading to possible side effects, and reduced efficacy among others. Herein we make use of the ubiquitous affinity of antigen-presenting cells (APC)s for glycosides to achieve specific targeting. To achieve this goal, we designed a new generation of α-mannosyl functionalized oligopeptide-terminated poly(β-aminoester). Fine formulation of these polymers with mRNA resulted in nanoparticles decorated with surface-exposed α-mannoses with sizes around 180 nm and positive surface charge. Notably, these particles maintained their properties after freeze-drying and subsequent redispersion. Finally, our mRNA carriers preferentially targeted and transfected APCs and . In conclusion, we demonstrated, at a preclinical level, that the mannose functionalization enables more selective targeting of APCs and, thus, these polymer and nanoparticles are candidates for a new generation of mRNA immunotherapy vaccines.

摘要

mRNA 疫苗已成为医学未来的主要疗法。尽管这项技术取得了巨大进展,并在全球范围内证明了其疗效(COVID 疫苗),但 mRNA 载体仍缺乏细胞/组织特异性,可能导致副作用和疗效降低等问题。在这里,我们利用抗原呈递细胞(APC)对糖苷的普遍亲和力来实现特异性靶向。为此,我们设计了新一代α-甘露糖基功能化的寡肽末端聚(β-氨基酯)。这些聚合物与 mRNA 的精细配方可形成纳米颗粒,表面暴露的α-甘露糖修饰在纳米颗粒表面,粒径约为 180nm,带正电荷。值得注意的是,这些颗粒在冷冻干燥和随后的再分散后仍保持其性质。最后,我们的 mRNA 载体优先靶向和转染 APCs 和 。总之,我们在临床前水平证明,甘露糖功能化能够更有选择性地靶向 APCs,因此,这些聚合物和纳米颗粒是新一代 mRNA 免疫治疗疫苗的候选物。

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