Bifunctional Janus Particles as Multivalent Synthetic Nanoparticle Antibodies (SNAbs) for Selective Depletion of Target Cells

双功能 杰纳斯 纳米颗粒 杰纳斯粒子 化学 抗体 催化作用 化学工程 生物物理学 纳米技术 组合化学 免疫学 生物 材料科学 生物化学 工程类
作者
Jiaying Liu,Randall Toy,Casey E. Vantucci,Pallab Pradhan,Zijian Zhang,Katie M. Kuo,Kelsey P. Kubelick,Da Huo,Jianguo Wen,Jinhwan Kim,Zhiheng Lyu,Simran Dhal,Alexandra Atalis,Shohini Ghosh-Choudhary,Emily J. Devereaux,James C. Gumbart,Younan Xia,Stanislav Emelianov,Nick J. Willett,Krishnendu Roy
出处
期刊:Nano Letters [American Chemical Society]
卷期号:21 (1): 875-886 被引量:28
标识
DOI:10.1021/acs.nanolett.0c04833
摘要

Monoclonal antibodies (mAb) have had a transformative impact on treating cancers and immune disorders. However, their use is limited by high development time and monetary cost, manufacturing complexities, suboptimal pharmacokinetics, and availability of disease-specific targets. To address some of these challenges, we developed an entirely synthetic, multivalent, Janus nanotherapeutic platform, called Synthetic Nanoparticle Antibodies (SNAbs). SNAbs, with phage-display-identified cell-targeting ligands on one "face" and Fc-mimicking ligands on the opposite "face", were synthesized using a custom, multistep, solid-phase chemistry method. SNAbs efficiently targeted and depleted myeloid-derived immune-suppressor cells (MDSCs) from mouse-tumor and rat-trauma models, ex vivo. Systemic injection of MDSC-targeting SNAbs efficiently depleted circulating MDSCs in a mouse triple-negative breast cancer model, enabling enhanced T cell and Natural Killer cell infiltration into tumors. Our results demonstrate that SNAbs are a versatile and effective functional alternative to mAbs, with advantages of a plug-and-play, cell-free manufacturing process, and high-throughput screening (HTS)-enabled library of potential targeting ligands.

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