Preclinical assessment of IRDye800CW‐labeled gastrin‐releasing peptide receptor‐targeting peptide for near infrared‐II imaging of brain malignancies

Author:

Zhang Yuan12,Wang Li3,Zhang Chengkai12,Zhang Jingjing456,Yuan Linhao12,Jin Shucheng12,Zhou Wenjianlong12,Guan Xiudong12,Kang Peng12,Zhang Chuanbao12,Tian Jie789,Chen Xiaoyuan456,Li Deling12,Jia Wang12ORCID

Affiliation:

1. Department of Neurosurgery, Beijing Tiantan Hospital Capital Medical University Beijing China

2. Beijing Neurosurgical Institute Beijing China

3. Jiangsu Xinrui Pharmaceutical Co., Ltd. Nantong China

4. Departments of Diagnostic Radiology, Surgery, Chemical and Biomolecular Engineering, and Biomedical Engineering, Yong Loo Lin School of Medicine and Faculty of Engineering National University of Singapore Singapore Singapore

5. Clinical Imaging Research Centre, Centre for Translational Medicine, Yong Loo Lin School of Medicine National University of Singapore Singapore Singapore

6. Nanomedicine Translational Research Program, NUS Center for Nanomedicine, Yong Loo Lin School of Medicine National University of Singapore Singapore Singapore

7. CAS Key Laboratory of Molecular Imaging, Beijing Key Laboratory of Molecular Imaging, The State Key Laboratory of Management and Control for Complex Systems Institute of Automation, Chinese Academy of Sciences Beijing China

8. School of Artificial Intelligence University of Chinese Academy of Sciences Beijing China

9. Beijing Advanced Innovation Center for Big Data‐Based Precision Medicine, School of Medicine Beihang University Beijing China

Abstract

AbstractWe aimed to develop a new biocompatible gastrin‐releasing peptide receptor (GRPR) targeted optical probe, IRDye800‐RM26, for fluorescence image‐guided surgery (FGS) of brain malignancies in near‐infrared window II (NIR‐II) imaging. We developed a novel GRPR targeting probe using a nine‐amino‐acid bombesin antagonist analog RM26 combined with IRDye800CW, and explored the fluorescent probe according to optical properties. Fluorescence imaging characterization in NIR‐I/II region was performed in vitro and in vivo. Following simulated NIR‐II image‐guided surgery, we obtained time‐fluorescent intensity curves and time‐signal and background ratio curves. Further, we used histological sections of brain from tumor‐beating mice model to compare imaging specificity between 5‐aminolevulinic acid (5‐ALA) and IRDye800‐RM26, and evaluated biodistribution and biocompatibility. IRDye800‐RM26 had broad emission ranging from 800 to 1200 nm, showing considerable fluorescent intensity in NIR‐II region. High‐resolution NIR‐II imaging of IRDye800‐RM26 can enhance the advantages of NIR‐I imaging. Dynamic and real time fluorescence imaging in NIR‐II region showed that the probe can be used to treat brain malignancies in mice between 12 and 24 h post injection. Its specificity in targeting glioblastoma was superior to 5‐ALA. Biodistribution analysis indicated IRDye800‐RM26 excretion in the kidney and liver. Histological and blood test analyses did not reveal acute severe toxicities in mice treated with effective dose (40 μg) of the probe for NIR‐II imaging. Because of the considerable fluorescent intensity in NIR‐II region and high spatial resolution, biocompatible and excretable IRDye800‐RM26 holds great potentials for FGS, and is essential for translation into human use.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biotechnology

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