4.7 Article

Enabling AIEgens close assembly in tumor-overexpressed protein cluster for boosted image-guided cancer surgery

Journal

SCIENCE CHINA-CHEMISTRY
Volume 63, Issue 11, Pages 1694-1702

Publisher

SCIENCE PRESS
DOI: 10.1007/s11426-020-9829-x

Keywords

aggregation-induced emission luminogen; fluorescent probe; self-assembling peptide; fluorescence image-guided cancer surgery; tumor-to-normal tissue ratio

Funding

  1. Tianjin Technical Expert Project [19JCTPJC41200]
  2. National Natural Science Foundation of China [51873150, 31770974]
  3. National Key Research and Development Program of China [2017YFE0132200]

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Development of efficient fluorescent probes that can realize precise fluorescence image-guided cancer surgery (FIGCS) with extremely high tumor-to-normal tissue (T/NT) ratio is urgently desirable. Herein, we report the design and synthesis of an aggregation-induced emission (AIE)-active, peptide-based fluorescence turn-on probe MPA-Ph-R-FFGYSAYPDSVPMMS (MPA-Ph-R-FFGYSA for short), which consists of a new near-infrared emissive AIE luminogen (AIEgen) MPA-Ph-R, a self-assembling peptide sequence FFG, and an active targeting peptide YSAYPDSVPMMS that can selectively bind to EphA2 protein cluster overexpressed in many cancers. As compared to the control probe MPA-Ph-R-YSA without FFG, MPA-Ph-R-FFGYSA exhibits much higher fluorescent brightness and sensitivity in both cellular and in vivo studies on EphA2 cluster detection/imaging, as FFG is beneficial to closer assembly of AIEgens in EphA2 cluster, leading to more effective restriction of the intramolecular motion of AIEgen. In vivo studies demonstrate that MPA-Ph-R-FFGYSA is a safe bioprobe and gives excellent performance in FIGCS with a rather high T/NT ratio of similar to 13.4 upon intravenous administration into peritoneal carcinomatosis-bearing mice. This study provides a new strategy of utilizing the close assembly of tumor microenvironment-responsive AIE probes for boost FIGCS.

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