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Journal of Nuclear Medicine

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OtherClinical Investigations (Human)

Quantification of PD-L1 expression with [18F]BMS-986192 PET/CT in patients with advanced stage non-small-cell lung cancer

Marc Huisman, Anna-Larissa Niemeijer, Bert Windhorst, Robert Schuit, David Leung, Wendy Hayes, Alex Poot, Idris Bahce, Teodora Radonic, Daniela Oprea-Lager, Otto Hoekstra, Erik Thunnissen, Harry Hendrikse, Egbert Smit, Joop De Langen and Ronald Boellaard
Journal of Nuclear Medicine February 2020, jnumed.119.240895; DOI: https://doi.org/10.2967/jnumed.119.240895
Marc Huisman
1 VU University Medical Center, Netherlands;
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Anna-Larissa Niemeijer
1 VU University Medical Center, Netherlands;
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Bert Windhorst
1 VU University Medical Center, Netherlands;
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Robert Schuit
1 VU University Medical Center, Netherlands;
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David Leung
2 Bristol-Myers Squibb Research and Development;
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Wendy Hayes
2 Bristol-Myers Squibb Research and Development;
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Alex Poot
1 VU University Medical Center, Netherlands;
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Idris Bahce
1 VU University Medical Center, Netherlands;
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Teodora Radonic
1 VU University Medical Center, Netherlands;
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Daniela Oprea-Lager
1 VU University Medical Center, Netherlands;
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Otto Hoekstra
1 VU University Medical Center, Netherlands;
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Erik Thunnissen
1 VU University Medical Center, Netherlands;
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Harry Hendrikse
1 VU University Medical Center, Netherlands;
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Egbert Smit
3 Netherlands Cancer Institute
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Joop De Langen
3 Netherlands Cancer Institute
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Ronald Boellaard
1 VU University Medical Center, Netherlands;
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Abstract

The aim of this work was to quantify the uptake of [18F]BMS-986192, a PD-L1 adnectin PET tracer, in patients with non-small-cell lung cancer (NSCLC). To this end, plasma input kinetic modeling of dynamic tumor uptake data with online arterial blood sampling was performed. In addition, the accuracy of simplified uptake metrics such as standardized uptake value (SUV) was investigated. Methods: Data from a study with [18F]BMS-986192 in patients with advanced stage NSCLC eligible for nivolumab treatment were used if a dynamic scan was available and lesions were present in the field of view of the dynamic scan. After injection of [18F]BMS-986192, a 60-minutes dynamic PET-CT scan was started, followed by a 30-min whole body PET-CT scan. Continuous arterial and discrete arterial and venous blood sampling were performed to determine a plasma input function. Tumor time activity curves were fitted by several plasma input kinetic models. Simplified uptake parameters included tumor to blood ratio as well as several SUV measures. Results: Twenty two tumors in nine patients were analyzed. The arterial plasma input single-tissue reversible compartment model with fitted blood volume fraction seems to be the most preferred model as it best fitted 11 out of 18 tumor time activity curves. The distribution volume VT ranged from 0.4 to 4.8 mL·cm-3. Similar values were obtained with an image derived input function. From the simplified measures, SUV normalized for body weight (SUVBW) at 50 and 67 minutes post injection correlated best with VT, with an R2 > 0.9. Conclusion: A single tissue reversible model can be used for the quantification of tumor uptake of the PD-L1 PET tracer [18F]BMS-986192. SUVBW at 60 minutes post injection, normalized for body weight, is an accurate simplified parameter for uptake assessment of baseline studies. In order to assess its predictive value for response evaluation during PD-(L)1 immune checkpoint inhibition further validation of SUV against VT based on an image derived input function is recommended.

  • Molecular Imaging
  • PET/CT
  • Radiotracer Tissue Kinetics
  • PD-L1 expression
  • PET-CT
  • immune checkpoint inhibitors
  • kinetic modeling
  • Copyright © 2020 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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Quantification of PD-L1 expression with [18F]BMS-986192 PET/CT in patients with advanced stage non-small-cell lung cancer
Marc Huisman, Anna-Larissa Niemeijer, Bert Windhorst, Robert Schuit, David Leung, Wendy Hayes, Alex Poot, Idris Bahce, Teodora Radonic, Daniela Oprea-Lager, Otto Hoekstra, Erik Thunnissen, Harry Hendrikse, Egbert Smit, Joop De Langen, Ronald Boellaard
Journal of Nuclear Medicine Feb 2020, jnumed.119.240895; DOI: 10.2967/jnumed.119.240895

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Quantification of PD-L1 expression with [18F]BMS-986192 PET/CT in patients with advanced stage non-small-cell lung cancer
Marc Huisman, Anna-Larissa Niemeijer, Bert Windhorst, Robert Schuit, David Leung, Wendy Hayes, Alex Poot, Idris Bahce, Teodora Radonic, Daniela Oprea-Lager, Otto Hoekstra, Erik Thunnissen, Harry Hendrikse, Egbert Smit, Joop De Langen, Ronald Boellaard
Journal of Nuclear Medicine Feb 2020, jnumed.119.240895; DOI: 10.2967/jnumed.119.240895
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Keywords

  • Molecular imaging
  • PET/CT
  • radiotracer tissue kinetics
  • PD-L1 expression
  • PET-CT
  • immune checkpoint inhibitors
  • kinetic modeling
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