In Vivo Real-Time Pharmaceutical Evaluations of Near-Infrared II Fluorescent Nanomedicine Bound Polyethylene Glycol Ligands for Tumor Photothermal Ablation

纳米医学 体内 聚乙二醇 荧光 光热治疗 材料科学 PEG比率 荧光寿命成像显微镜 纳米颗粒 生物物理学 纳米技术 化学 有机化学 生物技术 经济 物理 生物 量子力学 财务
作者
Shengliang Li,Haoting Chen,Haile Liu,Lu Liu,Yuan Yuan,Cong Mao,Wei Zhang,Xiaodong Zhang,Weisheng Guo,Chun‐Sing Lee,Xing‐Jie Liang
出处
期刊:ACS Nano [American Chemical Society]
卷期号:14 (10): 13681-13690 被引量:44
标识
DOI:10.1021/acsnano.0c05885
摘要

Pharmaceutical evaluations of nanomedicines are of great significance for their further launch into industry and clinic. Near-infrared (NIR) fluorescence imaging plays essential roles in preclinical drug development by providing important insights into the biodistributions of drugs in vivo with deep tissue penetration and high spatiotemporal resolution. However, NIR-II fluorescence imaging has rarely been exploited for in vivo real-time pharmaceutical evaluations of nanomedicine. Herein, we developed a highly emissive NIR-II luminophore to establish a versatile nanoplatform to noninvasively monitor the in vivo metabolism of nanomedicines bound various polyethylene glycol (PEG) ligands in a real-time manner. An alternative D–A–D conjugated oligomer (DTTB) was synthesized to achieve NIR-II emission peaked at ∼1050 nm with high fluorescence QYs of 13.4% and a large absorption coefficient. By anchoring with the DTTB molecule, intrinsically fluorescent micelles were fabricated and bound with PEG ligands at various chain lengths. In vivo NIR-II fluorescence and photoacoustic imaging results revealed that an appropriate PEG chain length could effectively contribute to the longer blood circulation and better tumor targeting. In vivo therapeutic experiments also confirmed the optimized nanomedicines have efficient photothermal elimination of tumors and good biosafety. This work offered an alternative highly fluorescent NIR-II material and demonstrated a promising approach for real-time pharmaceutical evaluation of nanomedicine in vivo.
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