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Near-infrared fluorescent probe for imaging of pancreatic beta cells.

Bioconjug Chem · 2010

Last updated 2026-05-28

Researchers developed a fluorescent imaging tool that targets GLP-1 receptors on pancreatic beta cells in mice. When injected, the tool clearly highlighted beta cells in the pancreas within 3 minutes, reaching peak visibility at 20 minutes, with a 6:1 contrast ratio compared to surrounding tissue.

AI summary of the abstract below.

JournalBioconjug Chem, 2010
Citations34
Relative citation ratio0.99
NIH percentile50
Molecules

Abstract

The ability to image and ultimately quantitate beta-cell mass in vivo will likely have far reaching implications in the study of diabetes biology, in the monitoring of disease progression or response to treatment, and for drug development. Here, using animal models, we report on the synthesis, characterization, and intravital microscopic imaging properties of a near-infrared fluorescent exendin-4 analogue with specificity for the GLP-1 receptor on beta cells (E4(K12)-Fl). The agent demonstrated subnanomolar EC(50) binding concentrations, with high specificity and binding that could be inhibited by GLP-1R agonists. Following intravenous administration to mice, pancreatic islets were readily distinguishable from exocrine pancreas, achieving target-to-background ratios within the pancreas of 6:1, as measured by intravital microscopy. Serial imaging revealed rapid accumulation kinetics (with initial signal within the islets detectable within 3 min and peak fluorescence within 20 min of injection), making this an ideal agent for in vivo imaging.

Verbatim abstract via PubMed 20583828 ↗