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Research ArticleBasic Science Investigation

Diels–Alder Reaction for Tumor Pretargeting: In Vivo Chemistry Can Boost Tumor Radiation Dose Compared with Directly Labeled Antibody

Raffaella Rossin, Tilman Läppchen, Sandra M. van den Bosch, Richard Laforest and Marc S. Robillard
Journal of Nuclear Medicine October 2013, jnumed.113.123745; DOI: https://doi.org/10.2967/jnumed.113.123745
Raffaella Rossin
1Department of Minimally Invasive Healthcare, Philips Research, Eindhoven, The Netherlands; and
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Tilman Läppchen
1Department of Minimally Invasive Healthcare, Philips Research, Eindhoven, The Netherlands; and
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Sandra M. van den Bosch
1Department of Minimally Invasive Healthcare, Philips Research, Eindhoven, The Netherlands; and
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Richard Laforest
2Division of Radiological Sciences, Washington University School of Medicine, St. Louis, Missouri
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Marc S. Robillard
1Department of Minimally Invasive Healthcare, Philips Research, Eindhoven, The Netherlands; and
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Abstract

Current pretargeting systems use noncovalent biologic interactions, which are prone to immunogenicity. We previously developed a novel approach based on the bioorthogonal reaction between a radiolabeled tetrazine and an antibody-conjugated trans-cyclooctene (TCO). However, the tumor-to-blood ratio was low due to reaction with freely circulating antibody-TCO. Methods: Here we developed 2 tetrazine-functionalized clearing agents that enable rapid reaction with and removal of a TCO-tagged antibody (CC49) from blood. Next, we incorporated this approach into an optimized pretargeting protocol in LS174T-bearing mice. Then we compared the pretargeted 177Lu-labeled tetrazine with 177Lu-labeled CC49. The biodistribution data were used for mouse and human dosimetry calculations. Results: The use of a clearing agent led to a doubling of the tetrazine tumor uptake and a 125-fold improvement of the tumor-to-blood ratio at 3 h after tetrazine injection. Mouse dosimetry suggested that this should allow for an 8-fold higher tumor dose than is possible with nonpretargeted radioimmunotherapy. Also, humans treated with CC49-TCO–pretargeted 177Lu-tetrazine would receive a dose to nontarget tissues 1 to 2 orders of magnitude lower than with directly labeled CC49. Conclusion: The in vivo performance of chemical pretargeting falls within the range of results obtained for the clinically validated pretargeting approaches in mice, with the advantage of potentially allowing for fractionated radiotherapy as a result of a lower likelihood of immunogenicity. These findings demonstrate that biologic pretargeting concepts can be translated to rapid bioorthogonal chemical approaches with retained potential.

  • Diels-Alder
  • pretargeting
  • clearing agent
  • 177Lu
  • dosimetry

Footnotes

  • Published online ▪▪▪.

  • © 2013 by the Society of Nuclear Medicine and Molecular Imaging, Inc.
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Journal of Nuclear Medicine: 66 (5)
Journal of Nuclear Medicine
Vol. 66, Issue 5
May 1, 2025
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Diels–Alder Reaction for Tumor Pretargeting: In Vivo Chemistry Can Boost Tumor Radiation Dose Compared with Directly Labeled Antibody
Raffaella Rossin, Tilman Läppchen, Sandra M. van den Bosch, Richard Laforest, Marc S. Robillard
Journal of Nuclear Medicine Oct 2013, jnumed.113.123745; DOI: 10.2967/jnumed.113.123745

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Diels–Alder Reaction for Tumor Pretargeting: In Vivo Chemistry Can Boost Tumor Radiation Dose Compared with Directly Labeled Antibody
Raffaella Rossin, Tilman Läppchen, Sandra M. van den Bosch, Richard Laforest, Marc S. Robillard
Journal of Nuclear Medicine Oct 2013, jnumed.113.123745; DOI: 10.2967/jnumed.113.123745
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Keywords

  • Diels-Alder
  • pretargeting
  • clearing agent
  • 177Lu
  • dosimetry
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