The Different Strategies for the Radiolabeling of [211At]-Astatinated Radiopharmaceuticals

Author:

Gao Jie12,Li Mei1,Yin Jingjing1,Liu Mengya12,Wang Hongliang3,Du Jin24ORCID,Li Jianguo1

Affiliation:

1. China Institute for Radiation Protection, National Atomic Energy Agency Nuclear Technology (Nonclinical Evaluation of Radiopharmaceuticals) Research and Development Center, CNNC Key Laboratory on Radiotoxicology and Radiopharmaceutical Preclinical Evaluation, Taiyuan 030006, China

2. China Institute of Atomic Energy, Beijing 102413, China

3. First Hospital of Shanxi Medical University, Taiyuan 030001, China

4. China Isotope & Radiation Corporation, Beijing 100089, China

Abstract

Astatine-211 (211At) has emerged as a promising radionuclide for targeted alpha therapy of cancer by virtue of its favorable nuclear properties. However, the limited in vivo stability of 211At-labeled radiopharmaceuticals remains a major challenge. This review provides a comprehensive overview of the current strategies for 211At radiolabeling, including nucleophilic and electrophilic substitution reactions, as well as the recent advances in the development of novel bifunctional coupling agents and labeling approaches to enhance the stability of 211At-labeled compounds. The preclinical and clinical applications of 211At-labeled radiopharmaceuticals, including small molecules, peptides, and antibodies, are also discussed. Looking forward, the identification of new molecular targets, the optimization of 211At production and quality control methods, and the continued evaluation of 211At-labeled radiopharmaceuticals in preclinical and clinical settings will be the key to realizing the full potential of 211At-based targeted alpha therapy. With the growing interest and investment in this field, 211At-labeled radiopharmaceuticals are poised to play an increasingly important role in future cancer treatment.

Funder

Nuclear Energy Development Program of China

Natural Science Foundational of Shanxi Province

Publisher

MDPI AG

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