An on‐Demand Oxygen Nano‐vehicle Sensitizing Protein and Nucleic Acid Drug Augment Immunotherapy

加强 核酸 材料科学 药品 免疫疗法 纳米- 纳米技术 药物输送 药理学 生物化学 免疫系统 生物 免疫学 复合材料 语言学 哲学
作者
Sidi Zhang,Xinghui Wang,Xiaojing Chen,Duohuo Shu,Qisheng Lin,Hanbing Zou,Jialin Dong,Bing Wang,Qianyun Tang,Huishan Li,Xiaoxiang Chen,Jun Pu,Bin Gu,Peifeng Liu
出处
期刊:Advanced Materials [Wiley]
标识
DOI:10.1002/adma.202409378
摘要

Hypoxia severely limits the antitumor immunotherapy for breast cancer. Although efforts to alleviate tumor hypoxia and drug delivery using diverse nanostructures achieve promising results, the creation of a versatile controllable oxygen-releasing nano-platform for co-delivery with immunostimulatory molecules remains a persistent challenge. To address this problem, a versatile oxygen controllable releasing vehicle PFOB@F127@PDA (PFPNPs) is developed, which effectively co-delivered either protein drug lactate oxidase (LOX) or nucleic acids drug unmethylated cytosine-phosphate-guanine oligonucleotide (CpG ODNs). Upon photothermal heating, this platform triggered oxygen release, thereby augmenting LOX-mediated lactate detection rates, and improving T cells infiltrating and cytokine expression. Moreover, under an oxygenated tumor microenvironment (TME), PFPNPs co-delivered with CpG ODNs effectively reprogrammed the immunosuppressive TME by repolarizing macrophages to an M1-like phenotype, promoting dendritic cells maturation, and increasing tumor-infiltrating T cells while decreasing the ratio of regulatory T cells (Tregs). Our study demonstrated that this controlled oxygen-releasing platform possessed adaptive drug-loading capabilities to meet varied immunotherapeutic demands in clinical settings.
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