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Development of a leucine-rich repeat-containing protein 15-targeted radio-immunotheranostic approach to deplete pro-tumorigenic mechanisms and immunotherapy resistance

  • Claire M. Storey
  • , Mohamed Altai
  • , Katharina Lückerath
  • , Wahed Zedan
  • , Henan Zhu
  • , Lara Breuer
  • , Marija Trajkovic-Arsic
  • , Julie Park
  • , Abbie Hasson
  • , Jens Siveke
  • , Diane Abou
  • , Haley Marks
  • , Enna Ulmert
  • , Alexander Ridley
  • , Marcella Safi
  • , Urpo Lamminmäki
  • , Constance Yuen
  • , Susanne Geres
  • , Liqun Mao
  • , Michael Cheng
  • Sumit K. Subudhi, Bilal A. Siddiqui, Noah Federman, Johannes Czernin, Ken Herrmann, Laurent Bentolila, Xia Yang, Thomas G. Graeber, Robert Damoiseaux, Daniel Thorek, David Ulmert

Research output: Contribution to journalArticlepeer-review

Abstract

Leucine-rich repeat containing 15 (LRRC15) has emerged as an attractive biomarker and target for cancer therapy. Transforming growth factor-β (TGFβ) induces the expression of this plasma membrane protein specifically in aggressive and treatment resistant tumor cells derived from mesenchymal stem cells, with minimal expression observed in non-neoplastic tissues. We have developed a humanized monoclonal antibody, DUNP19, that specifically binds with high affinity to a phylogenetically conserved LRRC15 epitope and is rapidly internalized upon LRRC15 binding. In multiple subcutaneous and orthotopic tumor xenograft mouse models, Lutetium-177 labeled DUNP19 ([177Lu]Lu-DUNP19) enabled non-invasive imaging and molecularly precise radiotherapy to LRRC15-expressing cancer cells and murine cancer-associated fibroblasts, effectively halting tumor progression and prolonging survival with minimal toxicity. Transcriptomic analyses of [177Lu]Lu-DUNP19-treated tumors reveal a loss of pro-tumorigenic mechanisms, including a previously reported TGFβ-induced LRRC15+ signature associated with immunotherapy resistance. In a syngeneic tumor model, administration of [177Lu]Lu-DUNP19 significantly potentiated checkpoint-blockade therapy, yielding durable complete responses. Together, these results demonstrate that radio-theranostic targeting of LRRC15 with DUNP19 is a compelling precision medicine platform for image-guided diagnosis, eradication, and reprogramming of LRRC15+ tumor tissue that drives immuno-resistance and disease aggressiveness in a wide range of currently untreatable malignancies.

Original languageEnglish (US)
Article number319
JournalSignal Transduction and Targeted Therapy
Volume10
Issue number1
DOIs
StatePublished - Dec 2025

ASJC Scopus subject areas

  • Genetics
  • Cancer Research

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