| Literature DB >> 34903859 |
Wei Chen1, Hui Wang1, Nicholas E S Tay2, Vincent A Pistritto2, Kang-Po Li1, Tao Zhang1, Zhanhong Wu1, David A Nicewicz3, Zibo Li4.
Abstract
Positron emission tomography (PET) is a powerful imaging technology that can visualize and measure metabolic processes in vivo and/or obtain unique information about drug candidates. The identification of new and improved molecular probes plays a critical role in PET, but its progress is somewhat limited due to the lack of efficient and simple labelling methods to modify biologically active small molecules and/or drugs. Current methods to radiofluorinate unactivated arenes are still relatively limited, especially in a simple and site-selective way. Here we disclose a method for constructing C-18F bonds through direct halide/18F conversion in electron-rich halo(hetero)arenes. [18F]F- is introduced into a broad spectrum of readily available aryl halide precursors in a site-selective manner under mild photoredox conditions. Notably, our direct 19F/18F exchange method enables rapid PET probe diversification through the preparation and evaluation of an [18F]-labelled O-methyl tyrosine library. This strategy also results in the high-yielding synthesis of the widely used PET agent L-[18F]FDOPA from a readily available L-FDOPA analogue.Entities:
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Year: 2021 PMID: 34903859 DOI: 10.1038/s41557-021-00835-7
Source DB: PubMed Journal: Nat Chem ISSN: 1755-4330 Impact factor: 24.274