Issue 9, 2024

Automated radiosynthesis and preclinical imaging of a novel [18F]fluorolidocaine analogue via sequential C–H radiolabelling

Abstract

The most prominent myocardial voltage-gated sodium channel, NaV1.5, is a major drug target for treating cardiovascular disease. However, treatment determination and therapeutic development are complicated partly by an inadequate understanding of how the density of SCN5A, the gene that encodes NaV1.5, relates to treatment response and disease prognosis. To address these challenges, imaging agents derived from NaV1.5 blocking therapeutics have been employed in positron emission tomography (PET) imaging to infer how SCN5A expression relates to human disease in vivo. Herein, we describe the preparation of a novel fluorine-18 labelled analogue of lidocaine, a known NaV1.5 inhibitor, and compare this agent to a previously described analogue. Evidence from rodent and non-human primate PET imaging experiments suggests that the imaging utility of these agents may be limited by rapid metabolism and clearance.

Graphical abstract: Automated radiosynthesis and preclinical imaging of a novel [18F]fluorolidocaine analogue via sequential C–H radiolabelling

Supplementary files

Article information

Article type
Research Article
Submitted
23 Apr 2024
Accepted
20 Jul 2024
First published
31 Jul 2024
This article is Open Access
Creative Commons BY license

RSC Med. Chem., 2024,15, 3223-3227

Automated radiosynthesis and preclinical imaging of a novel [18F]fluorolidocaine analogue via sequential C–H radiolabelling

M. Frazier, J. S. Wright, D. M. Raffel, J. Stauff, W. P. Winton, P. J. H. Scott and A. F. Brooks, RSC Med. Chem., 2024, 15, 3223 DOI: 10.1039/D4MD00293H

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