Targeted interleukin-2 enhances the in vivo anti-cancer activity of Pluvicto™.

Eur J Nucl Med Mol Imaging

R&D Department, Philochem AG, Libernstrasse 3, CH-8112, Otelfingen, ZH, Switzerland.

Published: July 2024

AI Article Synopsis

  • - Pluvicto™ is a recently approved treatment for metastatic castration-resistant prostate cancer, but its effectiveness is limited due to uptake in salivary glands and kidneys, which restricts dose escalation.
  • - Researchers developed a new PSMA-expressing model to study the effectiveness of Pluvicto™ combined with L19-IL2, and found that this combination achieved curative responses in animal tests while being well tolerated.
  • - The study concluded that L19-IL2 enhances the immune response when used with low radioactive doses of Pluvicto™, suggesting a promising direction for future clinical trials.

Article Abstract

Purpose: Pluvicto™ ([Lu]Lu-PSMA-617), a radioligand therapeutic targeting prostate-specific membrane antigen (PSMA), has been recently approved for the treatment of metastatic castration-resistant prostate cancer (mCRPR). The drug suffers from salivary gland and kidney uptake that prevents its dose escalation to potentially curative doses. In this work, we sought to potentiate the in vivo anti-cancer activity of Pluvicto™ by combining it with L19-IL2, a clinical-stage investigational medicinal product based on tumor-targeted interleukin-2.

Methods: We established a new PSMA-expressing model (HT-1080.hPSMA) and validated it using a fluoresceine analogue of PSMA-617 (compound 1). The HT-1080.hPSMA model was used to study the saturation and tumor retention of Pluvicto™ (compound 2) and to run combination therapy studies with L19-IL2. To complement our understanding of the mechanism of action of this novel combination, we conducted proteomics experiments on tumor samples after therapy with Pluvicto™ alone or in combination with the immunocytokine.

Results: High, selective, and long-lived tumor uptake was observed for Pluvicto™ (2) in the novel HT-1080.hPSMA model. Therapy studies in HT-1080.hPSMA tumor-bearing mice revealed that the combination of Pluvicto™ (2) plus L19-IL2 mediated curative and durable responses in all animals. Potent in vivo anti-cancer activity was observed solely for the combination modality, at doses that were well tolerated by treated animals. Proteomics studies indicated that L19-IL2 boosts the activation of the immune system in animals pre-treated with Pluvicto™.

Conclusion: The therapeutic efficacy of Pluvicto™ at low radioactive doses can be effectively enhanced by the combination with L19-IL2. Our findings warrant further clinical exploration of this novel combination modality.

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Source
http://dx.doi.org/10.1007/s00259-024-06705-xDOI Listing

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