Impact of the dead-time correction method on quantitative 177Lu-SPECT (QSPECT) and dosimetry during radiopharmaceutical therapy

Alessandro Desy; Guillaume F. Bouvet; Nancy Lafrenière; Atefeh Zamanian; Philippe Després; Jean-Mathieu Beauregard

doi:10.1186/s40658-022-00484-w

EJNMMI Physics (Aug 2022)

Impact of the dead-time correction method on quantitative 177Lu-SPECT (QSPECT) and dosimetry during radiopharmaceutical therapy

Alessandro Desy,
Guillaume F. Bouvet,
Nancy Lafrenière,
Atefeh Zamanian,
Philippe Després,
Jean-Mathieu Beauregard

Affiliations

Alessandro Desy: Department of Medical Imaging, and Research Centre (Oncology Axis), CHU de Québec – Université Laval
Guillaume F. Bouvet: Department of Medical Imaging, and Research Centre (Oncology Axis), CHU de Québec – Université Laval
Nancy Lafrenière: Department of Medical Imaging, and Research Centre (Oncology Axis), CHU de Québec – Université Laval
Atefeh Zamanian: Department of Medical Imaging, and Research Centre (Oncology Axis), CHU de Québec – Université Laval
Philippe Després: Department of Radiation Oncology, and Research Centre (Oncology Axis), CHU de Québec – Université Laval
Jean-Mathieu Beauregard: Department of Medical Imaging, and Research Centre (Oncology Axis), CHU de Québec – Université Laval

DOI: https://doi.org/10.1186/s40658-022-00484-w
Journal volume & issue: Vol. 9, no. 1
pp. 1 – 12

Abstract

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Abstract Background Dead-time correction is required for accurate quantitative SPECT-based dosimetry in the context of personalised 177Lu radiopharmaceutical therapy. We aimed to evaluate the impact of applying dead-time correction on the reconstructed SPECT image versus on the acquisition projections before reconstruction. Methods Data from 16 SPECT/CT acquisitions of a decaying 177Lu-filled phantom (up to 20.75 GBq) and dual-timepoint SPECT/CT in 14 patients treated with personalised 177Lu peptide receptor radionuclide therapy were analysed. Dead time was determined based on the acquisition wide-spectrum count rate for each projection and averaged for the entire acquisition. Three dead-time correction methods (DTCMs) were used: the per-projection correction, where each projection was individually corrected before reconstruction (DTCM1, the standard of reference), and two per-volume methods using the average dead-time correction factor of the acquisition applied to all projections before reconstruction (DTCM2) or to the SPECT image after reconstruction (DTCM3). Relative differences in quantification were assessed for various volumes of interest (VOIs) on the phantom and patient SPECT images. In patients, the resulting dosimetry estimates for tissues of interest were also compared between DTCMs. Results Both per-volume DTCMs (DTCM2 and DTCM3) were found to be equivalent, with VOI count differences not exceeding 0.8%. When comparing the per-volume post-reconstruction DTCM3 versus the per-projection pre-reconstruction DTCM1, differences in VOI counts and absorbed dose estimates did not exceed 2%, with very few exceptions. The largest absorbed dose deviation was observed for a kidney at 3.5%. Conclusion While per-projection dead-time correction appears ideal for QSPECT, post-reconstruction correction is an acceptable alternative that is more practical to implement in the clinics, and that results in minimal deviations in quantitative accuracy and dosimetry estimates, as compared to the per-projection correction.

Published in EJNMMI Physics

ISSN: 2197-7364 (Online)
Publisher: SpringerOpen
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General): Medical physics. Medical radiology. Nuclear medicine
Website: https://ejnmmiphys.springeropen.com/

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