| Literature DB >> 29682821 |
Weizhi Wang1,2, Zhuoran Ma2, Shoujun Zhu2, Hao Wan2, Jingying Yue2, Huilong Ma3, Rui Ma3, Qinglai Yang3, Zihua Wang1,4, Qian Li4, Yixia Qian1, Chunyan Yue1, Yuehua Wang1, Linyang Fan1, Yeteng Zhong2, Ying Zhou2, Hongpeng Gao2, Junshan Ruan2, Zhiyuan Hu1,5,6, Yongye Liang3, Hongjie Dai2.
Abstract
In vivo molecular imaging of tumors targeting a specific cancer cell marker is a promising strategy for cancer diagnosis and imaging guided surgery and therapy. While targeted imaging often relies on antibody-modified probes, peptides can afford targeting probes with small sizes, high penetrating ability, and rapid excretion. Recently, in vivo fluorescence imaging in the second near-infrared window (NIR-II, 1000-1700 nm) shows promise in reaching sub-centimeter depth with microscale resolution. Here, a novel peptide (named CP) conjugated NIR-II fluorescent probe is reported for molecular tumor imaging targeting a tumor stem cell biomarker CD133. The click chemistry derived peptide-dye (CP-IRT dye) probe afforded efficient in vivo tumor targeting in mice with a high tumor-to-normal tissue signal ratio (T/NT > 8). Importantly, the CP-IRT probes are rapidly renal excreted (≈87% excretion within 6 h), in stark contrast to accumulation in the liver for typical antibody-dye probes. Further, with NIR-II emitting CP-IRT probes, urethra of mice can be imaged fluorescently for the first time noninvasively through intact tissue. The NIR-II fluorescent, CD133 targeting imaging probes are potentially useful for human use in the clinic for cancer diagnosis and therapy.Entities:
Keywords: molecular imaging; peptide probe; renal-excretion; second near-infrared window; tumor targeting
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Year: 2018 PMID: 29682821 PMCID: PMC6485425 DOI: 10.1002/adma.201800106
Source DB: PubMed Journal: Adv Mater ISSN: 0935-9648 Impact factor: 30.849