免疫系统
抗原
免疫疗法
癌症免疫疗法
癌症研究
卵清蛋白
黑色素瘤
适体
化学
肽
生物
癌细胞
细胞
细胞生物学
肽核酸
抗原呈递
分子生物学
T细胞
癌症疫苗
癌症
免疫学
表位
核酸
自然杀伤细胞
CD8型
肿瘤抗原
获得性免疫系统
肽疫苗
作者
Yanyu Huang,Cuiqing Huang,Sakshi Pandita,Chon Man Ieong,Yongheng Wang,David Wang,David Wang,Jifeng Chen,Victorio Jauregui Matos,Alessandra Maria Arabelle Beelen,Ya‐Ping Shiau,Shiqi Tang,Junwei Zhao,Qiufang Zong,Menghuan Tang,Zhaoqing Cong,Yuanpei Li,Peter A. Beal,Sheila S. David,Aijun Wang
出处
期刊:Small
[Wiley]
日期:2025-11-07
卷期号:21 (51): e05605-e05605
被引量:1
标识
DOI:10.1002/smll.202505605
摘要
Targeted delivery of antigens and adjuvants to the immune cells without eliciting uncontrolled inflammation is a major challenge in cancer vaccine development. Here, a highly versatile and programmable peptide nucleic acid (PNA)-based vaccine nanoplatform (PVN) is reported to elicit a robust anti-tumor immune response against B16-OVA syngeneic melanoma model. The PVN is built on an 11-mer PNA scaffold, enabling efficient "one-pot" loading of a PNA-modified ovalbumin antigenic peptide (SIINFEKL), CpG adjuvant, and a PNA-derivatized LLP2A ligand (an immune cell and melanoma cell targeting ligand). Super-resolution fluorescence imaging reveals the spatial arrangement of OVA8 within LP10-12[OVA8/CpG/LLP2A], while circular dichroism spectroscopy confirmsparalleled binding of complementary PNA strands in LP11[OVA8/CpG/LLP2A]. LLP2A displayed on PVNs target activated α4β1 integrin expressed by immune and melanoma cells, boosting antigen presentation by dendritic cells and eliciting strong CD8+T cell and natural killer cell responses. This amplified antitumor immune response leads to significant tumor regression and prolonged survival of mice bearing syngeneic B16-OVA melanoma. The modular nature and versatility of PVN allow convenient one-pot assembling of peptide antigens, immunomodulators, immune cell and tumor cell targeting ligands, making it practical for the custom design and preparation of personalized cancer vaccines.
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