Molecular Imaging (Nov 2008)

In Vivo Tumor Targeting by the B-Subunit of Shiga Toxin

  • Thomas Viel,
  • Estelle Dransart,
  • Fariba Nemati,
  • Emilie Henry,
  • Benoit Thézé,
  • Didier Decaudin,
  • Daniel Lewandowski,
  • Raphael Boisgard,
  • Ludger Johannes,
  • Bertrand Tavitian

DOI
https://doi.org/10.2310/7290.2008.00022
Journal volume & issue
Vol. 7

Abstract

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Delivery of drugs to the appropriate target cells would improve efficacy and reduce potential side effects. The nontoxic B-subunit of the intestinal pathogen-produced Shiga toxin (STxB) binds specifically to the glycosphingolipid Gb 3 , overex-pressed in membranes of certain tumor cells, and enters these cells through the retrograde pathway. Therefore, STxB binding to Gb 3 receptors may be useful for cell-specific vectorization or imaging purposes. Here we labeled STxB with a fluorophore to evaluate its potential as an in vivo cell-specific targeting reagent in two different models of human colorectal carcinoma. Fluorescent STxB was administered systemically to xenografted nude mice, and its biodistribution was studied by optical imaging. The use of fluorescent STxB allowed the combination of the macroscopic observations with analyses at the cellular level using confocal microscopy. After administration, the fluorescent STxB was slowly eliminated by renal excretion. However, it accumulated in the tumor area. Furthermore, STxB was demonstrated to enter the Gb 3 -expressing tumoral cells, as well as the epithelial cells of the neovascularization and the monocytes and macrophages surrounding the xenografts.