2. Academic Validation
  3. Preclinical Evaluation of 89Zr-Df-IAB22M2C PET as an Imaging Biomarker for the Development of the GUCY2C-CD3 Bispecific PF-07062119 as a T Cell Engaging Therapy

Preclinical Evaluation of 89Zr-Df-IAB22M2C PET as an Imaging Biomarker for the Development of the GUCY2C-CD3 Bispecific PF-07062119 as a T Cell Engaging Therapy

  • Mol Imaging Biol. 2021 Dec;23(6):941-951. doi: 10.1007/s11307-021-01621-0.
Kevin P Maresca 1 Jianqing Chen 2 Divya Mathur 2 3 Anand Giddabasappa 2 Adam Root 2 4 Jatin Narula 2 Lindsay King 2 David Schaer 2 Jonathan Golas 2 3 Keith Kobylarz 2 Edward Rosfjord 2 5 Edmund Keliher 2 Laigao Chen 2 Sripad Ram 2 Eve H Pickering 2 James S Hardwick 2 Paul A Rejto 2 Amira Hussein 6 Ohad Ilovich 6 Kevin Staton 7 8 Ian Wilson 9 Timothy J McCarthy 2
Affiliations

Affiliations

  • 1 Worldwide Research, Development & Medicine, Pfizer Inc, New York, USA. kevin.maresca@pfizer.com.
  • 2 Worldwide Research, Development & Medicine, Pfizer Inc, New York, USA.
  • 3 Regneron Pharmaceuticals, Tarrytown, NY, USA.
  • 4 Generate Biomedicines, Inc, Cambridge, MA, USA.
  • 5 Black Diamond Therapeutics, New York, NY, USA.
  • 6 Invicro, A Konica Minolta Company, New Haven, USA.
  • 7 Evergreen Theragnostics, Jersey City, NJ, USA.
  • 8 Memorial Sloan Kettering Cancer Center, New York, NY, USA.
  • 9 ImaginAb Inc., Inglewood, CA, USA.
PMID: 34143379 DOI: 10.1007/s11307-021-01621-0
Abstract

Purpose: A sensitive and specific imaging biomarker to monitor immune activation and quantify pharmacodynamic responses would be useful for development of immunomodulating anti-cancer agents. PF-07062119 is a T cell engaging bispecific antibody that binds to CD3 and guanylyl cyclase C, a protein that is over-expressed by colorectal cancers. Here, we used 89Zr-Df-IAB22M2C (89Zr-Df-Crefmirlimab), a human CD8-specific minibody to monitor CD8+ T cell infiltration into tumors by positron emission tomography. We investigated the ability of 89Zr-Df-IAB22M2C to track anti-tumor activity induced by PF-07062119 in a human CRC adoptive transfer mouse model (with injected activated/expanded human T cells), as well as the correlation of tumor radiotracer uptake with CD8+ immunohistochemical staining.

Procedures: NOD SCID gamma mice bearing human CRC LS1034 tumors were treated with four different doses of PF-07062119, or a non-targeted CD3 BsAb control, and imaged with 89Zr-Df-IAB22M2C PET at days 4 and 9. Following PET/CT imaging, mice were euthanized and dissected for ex vivo distribution analysis of 89Zr-Df-IAB22M2C in tissues on days 4 and 9, with additional data collected on day 6 (supplementary). Data were analyzed and reported as standard uptake value and %ID/g for in vivo imaging and ex vivo tissue distribution. In addition, tumor tissues were evaluated by immunohistochemistry for CD8+ T cells.

Results: The results demonstrated substantial mean uptake of 89Zr-Df-IAB22M2C (%ID/g) in PF-07062119-treated tumors, with significant increases in comparison to non-targeted BsAb-treated controls, as well as PF-07062119 dose-dependent responses over time of treatment. A moderate correlation was observed between tumor tissue radioactivity uptake and CD8+ cell density, demonstrating the value of the imaging agent for non-invasive assessment of intra-tumoral CD8+ T cells and the mechanism of action for PF-07062119.

Conclusion: Immune-imaging technologies for quantitative cellular measures would be a valuable biomarker in immunotherapeutic clinical development. We demonstrated a qualification of 89Zr-IAB22M2C PET to evaluate PD responses (mice) to a novel immunotherapeutic.

Keywords

89Zr-IAB22M2C PET imaging; CD8 T cell; GUCY2C bispecific antibody; Immuno-oncology.

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