Multiplexed In Vivo Imaging Using Size‐Controlled Quantum Dots in the Second Near‐Infrared Window

量子点 材料科学 共轭体系 荧光 聚合物 纳米技术 光电子学 多路复用 荧光寿命成像显微镜 光学 复合材料 电信 计算机科学 物理
作者
Sanghwa Jeong,Yebin Jung,Seoyeon Bok,Yeon‐Mi Ryu,Sumin Lee,Young‐Eun Kim,Jaejung Song,Mi‐Yeon Kim,Sang‐Yeob Kim,G‐One Ahn,Sungjee Kim
出处
期刊:Advanced Healthcare Materials [Wiley]
卷期号:7 (24) 被引量:33
标识
DOI:10.1002/adhm.201800695
摘要

PbS/CdS core/shell quantum dots (QDs) that emit at the second near-infrared (NIR-II, 1000-1700 nm) window are synthesized. The PbS seed size and CdS shell thicknesses are carefully controlled to produce bright and narrow fluorescence that are suitable for multiplexing. A polymer encapsulation yields polymer-encapsulated NIR-II QDs (PQDs), which provides the QDs with long-term fluorescence stability over a week in biological media. Exploiting the simple bioconjugation capability of PQDs, folic acids are conjugated to PQDs that can efficiently label folate receptor overexpressing cell lines. The PQDs afford multiplexed and nearly real-time longitudinal whole-body in vivo imaging. Two NIR-II QD probes are prepared: folic acid-conjugated PQDs (FA-PQDs) emitting at 1280 nm and unconjugated PQDs emitting at 1080 nm. The two PQDs are engineered to have compact and similar hydrodynamic sizes. A mixture of the folic acid-conjugated PQD and unconjugated PQDs is injected intravenously into a tumor-xenografted mouse, and the signals from them are monitored. This NIR-II whole-body imaging with the two PQDs provides precise evaluation of the active ligand-assisted tumor-targeting capability of the FA-PQD probe because the hydrodynamic size control of the two PQDs effectively eliminates effects from the size-dependent accumulations by permeations and retentions in tumors.

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