Subcellular S-factors for low-energy electrons: A comparison of Monte Carlo simulations and continuous-slowing-down calculations

Emfietzoglou, Dimitris; Kostarelos, Kostas; Hadjidoukas, Panagiotis E.; Bousis, C.; Fotopoulos, Andreas; Pathak, A. P.; Nikjoo, Hooshang

doi:10.1080/09553000802460180

Cited by 30 publications

(17 citation statements)

References 61 publications

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“…André et al (2014) determined cellular S-values for I-131, I-132, I-133, I-134, I-135 and monoenergetic sources using Geant4-DNA and compared results with other Monte Carlo codes. The Geant4-DNA results were found to be in good agreement with the data obtained using other Monte Carlo codes like CELLDOSE (Champion et al, 2008) (difference up to 8%), MC4V (Emfietzoglou et al, 2008) (difference up to 4%), PENELOPE (Salvat et al, 2008) (difference up to 4%), MCNP (Cai et al, 2010) (difference up to 10%), and EGSnrc (Kawrakow, 2000) (difference up to 7%). Fourie et al (2015) employed Geant4-DNA to calculate S-values in spheres for I-123.…”

Section: Introductionsupporting

confidence: 80%

“…Ftáčniková and Böhm (2000) computed cellular S-values for several Auger emitting radionuclides using the Monte Carlo code ETRACK (Ito, 1987) and reported moderate differences (between À 18% and 21%) against the convolution integral approach. In a more detailed investigation of the validity of the CSDA, Emfietzoglou et al (2008) calculated cellular S-values for monoenergetic sources from 100 eV to 10 keV and water spheres with radius from 5 nm to 1 μm by both the convolution integral method and the Monte Carlo method using their in-house Monte Carlo code MC4 (Emfietzoglou et al, 2000). Significant differences between the two methods were found only when electron penetration depth was comparable to the size of sphere.…”

Section: Introductionmentioning

confidence: 99%

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Calculation of cellular S-values using Geant4-DNA: The effect of cell geometry

Šefl

Incerti

Papamichael

et al. 2015

Applied Radiation and Isotopes

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Section: Introductionsupporting

confidence: 80%

Section: Introductionmentioning

confidence: 99%

Calculation of cellular S-values using Geant4-DNA: The effect of cell geometry

Šefl

Incerti

Papamichael

et al. 2015

Applied Radiation and Isotopes

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“…Therefore, MCNP is capable of modeling the radiation absorbed dose to the cell nucleus (micrometer scale) from Auger electron-emitting radiotherapeutic agents that are not intimately associated with DNA. To model the dose to DNA at the nanometer scale for DNA-binding radiotherapeutics such as 125 I-iododeoxyuridine, a detailed history Monte Carlo code that follows the transport of electrons down to 100 eV would be necessary (27). Other methods, such as the inner shell ionization model, have been proposed (28).…”

Section: Discussionmentioning

confidence: 99%

Cellular Dosimetry of ¹¹¹In Using Monte Carlo N-Particle Computer Code: Comparison with Analytic Methods and Correlation with In Vitro Cytotoxicity

Cai

Pignol²,

Chan³

et al. 2010

J Nucl Med

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Our objective was to compare Monte Carlo N-particle (MCNP) self-and cross-doses from 111 In to the nucleus of breast cancer cells with doses calculated by reported analytic methods (Goddu et al. and Farragi et al.). A further objective was to determine whether the MCNP-predicted surviving fraction (SF) of breast cancer cells exposed in vitro to 111 In-labeled diethylenetriaminepentaacetic acid human epidermal growth factor ( 111 In-DTPAhEGF) could accurately predict the experimentally determined values. The MCNP-predicted SF for monolayer MDA-MB-468, MDA-MB-231, and MCF-7 cells agreed with the experimental data (relative error of 3.1%, 21.0%, and 1.7%). The single-cell and cell cluster models were less accurate in predicting the SF. For MDA-MB-468 cells, relative error was 8.1% using the singlecell model and 254% to 267% using the cell cluster model. Individual cell-line dimensions had large effects on S values and were needed to estimate doses and SF accurately. Conclusion: MCNP simulation compared well with the reported analytic methods in the calculation of subcellular S values for single cells and cell clusters. Application of a monolayer model was most accurate in predicting the SF of breast cancer cells exposed in vitro to 111 In-DTPA-hEGF.

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“…This tool, however, has several limitations related mainly to simplified biological assumptions (e.g., spherical cell geometry lacking a physical membrane, unit density, and uniform activity distributions) and a semi-analytical radiation transport model adopting the continuous-slowing-down approximation (CSDA), thus neglecting electron straggling and secondary electrons. Indeed, other authors made use of pre-calculated Dose Point Kernels [6,7] or direct Monte Carlo radiation transport [8][9][10], pointing out the discrepancy with MIRDcell, specifically for the low energy range of electrons [11]. Moreover, it was demonstrated that asymmetries in the geometry [12,13], as well as non-concentric cell and nucleus morphology [14] significantly impact the absorbed dose to the nucleus.…”

Section: Introductionmentioning

confidence: 99%

Cellular dosimetry of [177Lu]Lu-DOTA-[Tyr3]octreotate radionuclide therapy: the impact of modeling assumptions on the correlation with in vitro cytotoxicity

et al. 2020

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Background: Survival and linear-quadratic model fitting parameters implemented in treatment planning for targeted radionuclide therapy depend on accurate cellular dosimetry. Therefore, we have built a refined cellular dosimetry model for [ 177 Lu]Lu-DOTA-[Tyr 3 ]octreotate (177 Lu-DOTATATE) in vitro experiments, accounting for specific cell morphologies and sub-cellular radioactivity distributions. Methods: Time activity curves were measured and modeled for medium, membrane-bound, and internalized activity fractions over 6 days. Clonogenic survival assays were performed at various added activities (0.1-2.5 MBq/ml). 3D microscopy images (stained for cytoplasm, nucleus, and Golgi) were used as reference for developing polygonal meshes (PM) in 3DsMax to accurately render the cellular and organelle geometry. Absorbed doses to the nucleus per decay (S values) were calculated for 3 cellular morphologies: spheres (MIRDcell), truncated cone-shaped constructive solid geometry (CSG within MCNP6.1), and realistic PM models, using Geant4-10.03. The geometrical setup of the clonogenic survival assays was modeled, including dynamic changes in proliferation, proximity variations, and cell death. The absorbed dose to the nucleus by the radioactive source cell (self-dose) and surrounding source cells (cross-dose) was calculated applying the MIRD formalism. Finally, the correlation between absorbed dose and survival fraction was fitted using a linear dose-response curve (high α/β or fast sub-lethal damage repair half-life) for different assumptions, related to cellular shape and localization of the internalized fraction of activity. Results: The cross-dose, depending on cell proximity and colony formation, is a minor (15%) contributor to the total absorbed dose. Cellular volume (inverse exponential trend), shape modeling (up to 65%), and internalized source localization (up to + 149% comparing cytoplasm to Golgi) significantly influence the self-dose to nucleus. The absorbed dose delivered to the nucleus during a clonogenic survival assay is 3-fold higher with MIRDcell compared to the polygonal mesh structures. Our cellular dosimetry model indicates that 177 Lu-DOTATATE treatment might be more effective than suggested by average spherical cell dosimetry, predicting a lower absorbed dose for the same cellular survival. Dose-rate effects and heterogeneous dose delivery might account for differences in dose-response compared to x-ray irradiation.

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Subcellular S-factors for low-energy electrons: A comparison of Monte Carlo simulations and continuous-slowing-down calculations

Abstract: The use of the CSDA methodology may be unsuitable for the sub-micron scale where a more realistic description of electron transport becomes important.

Cited by 30 publications

References 61 publications

Calculation of cellular S-values using Geant4-DNA: The effect of cell geometry

Calculation of cellular S-values using Geant4-DNA: The effect of cell geometry

Cellular Dosimetry of ¹¹¹In Using Monte Carlo N-Particle Computer Code: Comparison with Analytic Methods and Correlation with In Vitro Cytotoxicity

Cellular dosimetry of [177Lu]Lu-DOTA-[Tyr3]octreotate radionuclide therapy: the impact of modeling assumptions on the correlation with in vitro cytotoxicity

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Subcellular S-factors for low-energy electrons: A comparison of Monte Carlo simulations and continuous-slowing-down calculations

Abstract: The use of the CSDA methodology may be unsuitable for the sub-micron scale where a more realistic description of electron transport becomes important.

Cited by 30 publications

References 61 publications

Calculation of cellular S-values using Geant4-DNA: The effect of cell geometry

Calculation of cellular S-values using Geant4-DNA: The effect of cell geometry

Cellular Dosimetry of 111In Using Monte Carlo N-Particle Computer Code: Comparison with Analytic Methods and Correlation with In Vitro Cytotoxicity

Cellular dosimetry of [177Lu]Lu-DOTA-[Tyr3]octreotate radionuclide therapy: the impact of modeling assumptions on the correlation with in vitro cytotoxicity

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Cellular Dosimetry of ¹¹¹In Using Monte Carlo N-Particle Computer Code: Comparison with Analytic Methods and Correlation with In Vitro Cytotoxicity