Absorbed dose evaluation of Auger electron-emitting radionuclides: impact of input decay spectra on dose point kernels and S-values
Nadia Falzone, Boon Q Lee, Jos\'e M Fern\'andez-Varea, Christiana, Kartsonaki, Andrew E Stuchbery, Tibor Kib\'edi, Katherine A Vallis

TL;DR
This study assesses how different decay data models affect dose calculations for Auger electron-emitting radionuclides, revealing significant differences at nanometer scales that impact biological damage predictions.
Contribution
It introduces the impact of the BrIccEmis decay spectra model on dose point kernels and S-values, highlighting differences from the traditional MIRD-RADTABS data.
Findings
BrIccEmis yields fewer Auger electrons and x-ray photons than MIRD-RADTABS.
Differences in dose point kernels are significant within the first few hundred nanometers.
Larger-scale S-values are not significantly affected by the decay data choice.
Abstract
The aim of this study was to investigate the impact of decay data provided by the newly developed stochastic atomic relaxation model BrIccEmis on dose point kernels (DPKs - radial dose distribution around a unit point source) and S-values (absorbed dose per unit cumulated activity) of 14 Auger electron (AE) emitting radionuclides, namely 67Ga, 80mBr, 89Zr, 90Nb, 99mTc, 111In, 117mSn, 119Sb, 123I, 124I, 125I, 135La, 195mPt and 201Tl. Radiation spectra were based on the nuclear decay data from the medical internal radiation dose (MIRD) RADTABS program and the BrIccEmis code, assuming both an isolated-atom and condensed-phase approach. DPKs were simulated with the PENELOPE Monte Carlo (MC) code using event-by-event electron and photon transport. S-values for concentric spherical cells of various sizes were derived from these DPKS using appropriate geometric reduction factors. The number of…
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