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聚乙烯亚胺偶联金纳米粒子作为一种用于体外和体内DNA疫苗递送的高效载体。

Polyethylenimine-Conjugated Au-NPs as an Efficient Vehicle for in vitro and in vivo DNA Vaccine Delivery.

作者信息

Kartouzian Aras, Heiz Alexandra, Shameli Kamyar, Moeini Hassan

机构信息

Catalysis Research Center, School of Natural Sciences, Technical University of Munich, Munich, Germany.

Institute of Virology, School of Medicine, Technical University of Munich, Munich, Germany.

出版信息

Int J Nanomedicine. 2025 Apr 1;20:4021-4034. doi: 10.2147/IJN.S493211. eCollection 2025.

Abstract

PURPOSE

This study aimed to develop green-synthesized gold nanoparticles (Au-NPs) conjugated with polyethyleneimine (PEI) to overcome challenges in intracellular DNA vaccine delivery, focusing on enhancing cellular uptake and immune responses against the human norovirus (HuNoV) GII.4 variants.

METHODS

Au-NPs were synthesized using a citrate-ion-mediated green approach, with size and morphology analyzed via UV-vis spectroscopy and transmission electron microscopy (TEM). Stability was evaluated through zeta potential measurements. PEI conjugation was employed to modify surface charge. After in vitro evaluation of pDNA delivery efficiency and cytotoxicity in HEK293 cells, PEI-coated Au-NPs loaded with a HuNoV GII.4 pDNA vaccine (AuPEI-NPs-pDNA) were assessed for the immune responses in mice.

RESULTS

UV-vis spectroscopy and TEM confirmed successful Au-NP synthesis. Zeta potential shifted from -31.38 mV to -20.60 mV, reflecting stable but slightly reduced colloidal stability with larger sizes. PEI conjugation reversed surface charge to positive, enabling 100% transfection efficacy in HEK293 cells by day two without cytotoxicity. The AuPEI-NPs-pDNA induced significantly higher NoV-specific IgG antibodies and T-cell responses compared to unmodified Au-NPs, highlighting the role of positive charge in enhancing cellular uptake and immune activation. These results underscore PEI-coated Au-NPs as a biocompatible, efficient platform for DNA vaccine delivery.

CONCLUSION

PEI-coated Au-NPs demonstrate exceptional potential as non-toxic, high-efficiency carriers for DNA vaccines, enabling robust humoral and cellular immune responses. This strategy holds promises for advancing gene therapy and combating rapidly evolving pathogens like HuNoV, with broader applications in targeted drug delivery.

摘要

目的

本研究旨在开发与聚乙烯亚胺(PEI)偶联的绿色合成金纳米颗粒(Au-NPs),以克服细胞内DNA疫苗递送中的挑战,重点是增强对人诺如病毒(HuNoV)GII.4变体的细胞摄取和免疫反应。

方法

采用柠檬酸盐离子介导的绿色方法合成Au-NPs,通过紫外-可见光谱和透射电子显微镜(TEM)分析其大小和形态。通过zeta电位测量评估稳定性。采用PEI偶联来修饰表面电荷。在体外评估了pDNA在HEK293细胞中的递送效率和细胞毒性后,对负载HuNoV GII.4 pDNA疫苗的PEI包被的Au-NPs(AuPEI-NPs-pDNA)进行了小鼠免疫反应评估。

结果

紫外-可见光谱和TEM证实了Au-NP的成功合成。zeta电位从-31.38 mV变为-20.60 mV,反映出稳定性良好但尺寸较大时胶体稳定性略有降低。PEI偶联使表面电荷变为正电荷,在第2天实现了HEK293细胞中100%的转染效率且无细胞毒性。与未修饰的Au-NPs相比,AuPEI-NPs-pDNA诱导产生了显著更高的NoV特异性IgG抗体和T细胞反应,突出了正电荷在增强细胞摄取和免疫激活中的作用。这些结果强调了PEI包被的Au-NPs作为DNA疫苗递送的生物相容性高效平台的作用。

结论

PEI包被的Au-NPs作为DNA疫苗的无毒、高效载体具有巨大潜力,能够引发强大的体液和细胞免疫反应。该策略有望推动基因治疗并对抗像HuNoV这样快速进化的病原体,在靶向药物递送中具有更广泛的应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b7c2/11971965/90b13fb3b6c9/IJN-20-4021-g0001.jpg

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