EJNMMI Research (Jan 2022)

CXCR4 peptide-based fluorescence endoscopy in a mouse model of Barrett’s esophagus

  • Sabrina Marcazzan,
  • Marcos J. Braz Carvalho,
  • Matthias Konrad,
  • Julia Strangmann,
  • Anna Tenditnaya,
  • Theresa Baumeister,
  • Roland M. Schmid,
  • Hans-Jürgen Wester,
  • Vasilis Ntziachristos,
  • Dimitris Gorpas,
  • Timothy C. Wang,
  • Margret Schottelius,
  • Michael Quante

DOI
https://doi.org/10.1186/s13550-021-00875-7
Journal volume & issue
Vol. 12, no. 1
pp. 1 – 11

Abstract

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Abstract Background Near-infrared (NIR) fluorescence imaging has been emerging as a promising strategy to overcome the high number of early esophageal adenocarcinomas missed by white light endoscopy and random biopsy collection. We performed a preclinical assessment of fluorescence imaging and endoscopy using a novel CXCR4-targeted fluorescent peptide ligand in the L2-IL1B mouse model of Barrett’s esophagus. Methods Six L2-IL1B mice with advanced stage of disease (12–16 months old) were injected with the CXCR4-targeted, Sulfo-Cy5-labeled peptide (MK007), and ex vivo wide-field imaging of the whole stomach was performed 4 h after injection. Before ex vivo imaging, fluorescence endoscopy was performed in three L2-IL1B mice (12–14 months old) by a novel imaging system with two L2-IL1B mice used as negative controls. Results Ex vivo imaging and endoscopy in L2-IL1B mice showed that the CXCR4-targeted MK007 accumulated mostly in the dysplastic lesions with a mean target-to-background ratio > 2. The detection of the Sulfo-Cy5 signal in dysplastic lesions and its co-localization with CXCR4 stained cells by confocal microscopy further confirmed the imaging results. Conclusions This preliminary preclinical study shows that CXCR4-targeted fluorescence endoscopy using MK007 can detect dysplastic lesions in a mouse model of Barrett’s esophagus. Further investigations are needed to assess its use in the clinical setting.

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