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Peptidoglycan-Targeted [ 18 F]3,3,3-Trifluoro-d-alanine Tracer for Imaging Bacterial Infection

Title: Peptidoglycan-Targeted [ 18 F]3,3,3-Trifluoro-d-alanine Tracer for Imaging Bacterial Infection
Authors: Sorlin AM; Lopez-Alvarez M; Biboy J; Gray J; Rabbitt SJ; Rahim JU; Lee SH; Bobba KN; Blecha J; Parker MF; Flavell RR; Engel J; Ohliger M; Vollmer W; Wilson DM
Source: JACS Au, 2023
Publisher Information: American Chemical Society
Publication Year: 2023
Collection: Newcastle University Library ePrints Service
Description: © 2024 The Authors. Published by American Chemical Society. Imaging is increasingly used to detect and monitor bacterial infection. Both anatomic (X-rays, computed tomography, ultrasound, and MRI) and nuclear medicine ([111In]-WBC SPECT, [18F]FDG PET) techniques are used in clinical practice but lack specificity for the causative microorganisms themselves. To meet this challenge, many groups have developed imaging methods that target pathogen-specific metabolism, including PET tracers integrated into the bacterial cell wall. We have previously reported the d-amino acid derived PET radiotracers d-methyl-[11C]-methionine, d-[3-11C]-alanine, and d-[3-11C]-alanine-d-alanine, which showed robust bacterial accumulation in vitro and in vivo. Given the clinical importance of radionuclide half-life, in the current study, we developed [18F]3,3,3-trifluoro-d-alanine (d-[18F]-CF3-ala), a fluorine-18 labeled tracer. We tested the hypothesis that d-[18F]-CF3-ala would be incorporated into bacterial peptidoglycan given its structural similarity to d-alanine itself. NMR analysis showed that the fluorine-19 parent amino acid d-[19F]-CF3-ala was stable in human and mouse serum. d-[19F]-CF3-ala was also a poor substrate for d-amino acid oxidase, the enzyme largely responsible for mammalian d-amino acid metabolism and a likely contributor to background signals using d-amino acid derived PET tracers. In addition, d-[19F]-CF3-ala showed robust incorporation into Escherichia coli peptidoglycan, as detected by HPLC/mass spectrometry. Based on these promising results, we developed a radiosynthesis of d-[18F]-CF3-ala via displacement of a bromo-precursor with [18F]fluoride followed by chiral stationary phase HPLC. Unexpectedly, the accumulation of d-[18F]-CF3-ala by bacteria in vitro was highest for Gram-negative pathogens in particular E. coli. In a murine model of acute bacterial infection, d-[18F]-CF3-ala could distinguish live from heat-killed E. coli, with low background signals. These results indicate the viability of ...
Document Type: article in journal/newspaper
File Description: application/pdf
Language: unknown
Relation: https://eprints.ncl.ac.uk/297670; https://eprints.ncl.ac.uk/fulltext.aspx?url=297670/305D8241-D3C3-429D-B123-2D302848CE51.pdf&pub_id=297670
Availability: https://eprints.ncl.ac.uk/297670
Rights: https://creativecommons.org/licenses/by/4.0/
Accession Number: edsbas.82715ED8
Database: BASE