Tuning J-Aggregation Behavior of Fused Ring Acceptor Fluorophore within Nanoparticles for NIR-II Excitable Bioimaging with High Brightness.
PubMed
Authors: Wang X, Chen Z, Hu Z, Zhang Y, Zhang X, Yang X, Zhou X, Zhong W, Zhu X, Li X, Xie H, Lam JWY, Sun J, Sun H, Liang Y, Tang BZ
Year
2026
Paper ID
67718
Status
Peer-reviewed
Abstract Read
~2 min
Abstract Words
191
Citations
0
Abstract
Fluorescence imaging in the near-infrared-IIb (NIR-IIb, 1500-1700 nm) window offers high signal-to-background ratios (SBRs). However, the development of bright NIR-IIb fluorophores remains challenging due to the trade-off between long-wavelength absorption and brightness. In this study, we present a molecular design strategy that bypasses this limitation by inducing J-aggregation to redshift the absorption while maintaining an optimized bandgap with a high radiative decay rate. A quinoidal thieno[3,4-]thiophene π-bridge is incorporated to synthesize a fused-ring acceptor fluorophore, CTTIC-4F, affording J-aggregation in encapsulated nanoparticles (NPs) with enhanced brightness. The CTTIC-4F NPs display strongly red-shifted absorption peaked at 1017 nm and an improved fluorescence quantum yield of 0.44% in aqueous solutions, outperforming counterparts with conventional π-bridges. The molecular dynamics simulations indicate compact and spherical aggregates of CTTIC-4F due to strong π-π interactions in aqueous solutions, consistent with J-type packing. imaging demonstrates that the CTTIC-4F NPs achieve a high SBR of 8.26 in vascular imaging and ultrahigh SBRs for lymph system imaging under the 1064 nm laser excitation, enabling high-contrast NIR-IIb lymph system imaging and image-guided resection of tumor-draining sentinel lymph nodes. These results demonstrate the effectiveness of aggregation-regulated molecular design for NIR-IIb fluorophores.
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Fluorescence imaging in the near-infrared-IIb (NIR-IIb, 1500-1700 nm) window offers high signal-to-background ratios (SBRs).
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