EBioMedicine (Sep 2021)

Novel theranostic agent for PET imaging and targeted radiopharmaceutical therapy of tumour-infiltrating immune cells in glioma

  • Alexandra Foster,
  • Shubhanchi Nigam,
  • David S Tatum,
  • Itay Raphael,
  • Jide Xu,
  • Rajeev Kumar,
  • Elizabeth Plakseychuk,
  • Joseph D Latoche,
  • Sarah Vincze,
  • Bo Li,
  • Rajan Giri,
  • Lauren H McCarl,
  • Robert Edinger,
  • Murat Ak,
  • Vishal Peddagangireddy,
  • Lesley M Foley,
  • T Kevin Hitchens,
  • Rivka R Colen,
  • Ian F Pollack,
  • Ashok Panigrahy,
  • Darren Magda,
  • Carolyn J Anderson,
  • W Barry Edwards,
  • Gary Kohanbash

Journal volume & issue
Vol. 71
p. 103571

Abstract

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Background: Malignant gliomas are deadly tumours with few therapeutic options. Although immunotherapy may be a promising therapeutic strategy for treating gliomas, a significant barrier is the CD11b+ tumour-associated myeloid cells (TAMCs), a heterogeneous glioma infiltrate comprising up to 40% of a glioma's cellular mass that inhibits anti-tumour T-cell function and promotes tumour progression. A theranostic approach uses a single molecule for targeted radiopharmaceutical therapy (TRT) and diagnostic imaging; however, there are few reports of theranostics targeting the tumour microenvironment. Methods: Utilizing a newly developed bifunctional chelator, Lumi804, an anti-CD11b antibody (αCD11b) was readily labelled with either Zr-89 or Lu-177, yielding functional radiolabelled conjugates for PET, SPECT, and TRT. Findings: 89Zr/177Lu-labeled Lumi804-αCD11b enabled non-invasive imaging of TAMCs in murine gliomas. Additionally, 177Lu-Lumi804-αCD11b treatment reduced TAMC populations in the spleen and tumour and improved the efficacy of checkpoint immunotherapy. Interpretation: 89Zr- and 177Lu-labeled Lumi804-αCD11b may be a promising theranostic pair for monitoring and reducing TAMCs in gliomas to improve immunotherapy responses. Funding: A full list of funding bodies that contributed to this study can be found in the Acknowledgements section.

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