Tumor‐Associated Immune‐Cell‐Mediated Tumor‐Targeting Mechanism with NIR‐II Fluorescence Imaging

材料科学 自体荧光 癌症研究 生物物理学 肺癌 光学成像 免疫系统 癌细胞 医学 荧光 病理 癌症 内科学 免疫学 生物 光学 物理
作者
Homan Kang,Md Shamim,Xiaoran Yin,Eeswar Adluru,Takeshi Fukuda,Shinya Yokomizo,Hyejin Chang,Seung Hun Park,Yanan Cui,Austin J. Moy,Satoshi Kashiwagi,Maged Henary,Hak Soo Choi
出处
期刊:Advanced Materials [Wiley]
卷期号:34 (8): e2106500-e2106500 被引量:74
标识
DOI:10.1002/adma.202106500
摘要

Abstract The strategy of structure‐inherent tumor targeting (SITT) with cyanine‐based fluorophores is receiving more attention because no chemical conjugation of targeting moieties is required. However, the targeting mechanism behind SITT has not yet been well explained. Here, it is demonstrated that heptamethine‐cyanine‐based fluorophores possess not only targetability of tumor microenvironments without the need for additional targeting ligands but also second near‐infrared spectral window (NIR‐II) imaging capabilities, i.e., minimum scattering and ultralow autofluorescence. The new SITT mechanism suggests that bone‐marrow‐derived and/or tissue‐resident/tumor‐associated immune cells can be a principal target for cancer detection due to their abundance in tumoral tissues. Among the tested, SH1 provides ubiquitous tumor targetability and a high tumor‐to‐background ratio (TBR) ranging from 9.5 to 47 in pancreatic, breast, and lung cancer mouse models upon a single bolus intravenous injection. Furthermore, SH1 can be used to detect small cancerous tissues smaller than 2 mm in diameter in orthotopic lung cancer models. Thus, SH1 could be a promising cancer‐targeting agent and have a bright future for intraoperative optical imaging and image‐guided cancer surgery.
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