Abstract

BackgroundMultiple post-treatment dosimetry methods are currently under investigation for Yttrium-90 (^{90}hbox {Y}) radioembolization. Within each methodology, a variety of dosimetric inputs exists that affect the final dose estimates. Understanding their effects is essential to facilitating proper dose analysis and crucial in the eventual standardization of radioembolization dosimetry. The purpose of this study is to investigate the dose differences due to different self-calibrations and mass density assignments in the non-compartmental and local deposition methods. A practical mean correction method was introduced that permits dosimetry in images where the quality is compromised by patient motion and partial volume effects.MethodsTwenty-one patients underwent ^{90}hbox {Y} radioembolization and were imaged with SPECT/CT. Five different self-calibrations (FOV, Body, OAR, Liverlung, and Liver) were implemented and dosimetrically compared. The non-compartmental and local deposition method were used to perform dosimetry based on either nominal- or CT calibration-based mass densities. A mean correction method was derived assuming homogeneous densities. Cumulative dose volume histograms, linear regressions, boxplots, and Bland Altman plots were utilized for analysis.ResultsUp to 270% weighted dose difference was found between self-calibrations with mean dose differences up to 50 Gy in the liver and 23 Gy in the lungs. Between the local deposition and non-compartmental methods, the liver and lung had dose differences within 0.71 Gy and 20 Gy, respectively. The local deposition method’s nominal and CT calibration-based mass density implementations dosimetric metrics were within 1.4% in the liver and 24% in the lungs. The mean lung doses calculated with the CT method were shown to be inflated. The mean correction method demonstrated that the corrected mean doses were greater by up to sim 5 Gy in the liver and lower by up to sim 12 Gy in the lungs.ConclusionsThe OAR calibration may be utilized as a potentially more accurate and precise self-calibration. The non-compartmental method was found more comparable to the local deposition method in organs that were more homogeneous in mass densities. Due to the potential for inflated lung mean doses, the non-compartmental and local deposition method implemented with nominal mass densities is recommended for more consistent dosimetric results. If patient motion and partial volume effects are present in the liver, our practical correction method will calculate more representative doses in images suboptimal for dosimetry.

Highlights

  • Multiple post-treatment dosimetry methods are currently under investigation for Yttrium-90 ( 90Y ) radioembolization

  • The dosimetric methodologies clinically suggested are the partition and the non-compartmental models [1, 2]. These models are based on the Medical Internal Radiation Dose (MIRD) schema and apply two gross assumptions; (1) the injected microsphere sources distribute uniformly within entire regions of interest (ROI), which may include an entire organ and (2) the administered activity is contained entirely within the liver and lungs [2]

  • The nominal methods utilize contours drawn on CT and overlaid to the original SPECT images, which may result in organ volume errors

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Summary

Introduction

Multiple post-treatment dosimetry methods are currently under investigation for Yttrium-90 ( 90Y ) radioembolization. A variety of dosimetric inputs exists that affect the final dose estimates Understanding their effects is essential to facilitating proper dose analysis and crucial in the eventual standardization of radioembolization dosimetry. The non-compartmental and local deposition method were used to perform dosimetry based on either nominal- or CT calibration-based mass densities. The dosimetric methodologies clinically suggested are the partition and the non-compartmental models [1, 2] These models are based on the Medical Internal Radiation Dose (MIRD) schema and apply two gross assumptions; (1) the injected microsphere sources distribute uniformly within entire regions of interest (ROI), which may include an entire organ and (2) the administered activity is contained entirely within the liver and lungs [2]. Quantitative SPECT/CT images enable patient-specific treatment planning and subsequent dose verification

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