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Dose painting to combat tumor hypoxia while sparing urethra in prostate IMRT: a biologically based adaptive approach accounting for setup uncertainties and organ motionYin, Lingshu 11 1900 (has links)
Enhanced resistance to radiation could be caused by both chronic hypoxia and acute hypoxic which has been reported in prostate cancer in various studies. Therefore currently used dose prescriptions (70Gy in 35 fractions) for external beam radiation therapy (EBRT) of prostate cancer has been suggested insufficient to provide optimum clinical outcome. In this study, we propose a Biologically Guided Radiation Therapy approach to boost dose in hypoxic prostate tumor regions while sparing the urethra. A previously proposed hypoxia model was modified for prostate cancer and incorporated into treatment plan optimization. The concept of equivalent uniform dose (EUD) was used in the optimization and evaluation of results. CT data from 25 prostate cancer patients who recently received EBRT at the British Columbia Cancer Agency (BCCA) and hypothetical hypoxic regions manually drawn on these CT scans were selected for this study. The results show that our methods could boost dose in target volume to substantially higher levels. EUD of planning target volume increased to more than 80Gy, despite accounting for effects of hypoxia. This increase was achieved with only minor changes in dose in normal tissues, typically less than 5Gy. Notably, urethra sparing was excellent with a EUD around 64Gy. Robustness of the proposed approach is verified against various hypoxic settings. EUD comparison between RT plans in biological guided and conventional approaches using the same RT technique (Volumetric Modulated Arc Therapy) also suggests that biologically guided radiation therapy (BGRT) approach is more suitable for dose painting purposes with the advantage of delivering sufficient dose to hypoxia region in different scenarios and sparing normal tissue better. Furthermore, we also investigated the impact of inter-fraction patient set-up error and intra-fraction organ motion on the high dose gradients achieved with this proposed dose painting method and explored the feasibility of adapting geometrical uncertainties (represented as systematic error and random error) into treatment planning. Image error obtained from EPID images are used to derive systematic uncertainty and random uncertainty. During the geometrical uncertainty adapted optimization, dose matrix in PTV is shifted based on systematic error and convolved with a Gaussian kernel which is pre-calculated using random error. CT sets and organ contours from five patients who enrolled in the previous dose painting
i
study are selected. For each of them, seven plans are generated using cumulated uncertainty data which was collected after every five fractions. We also present the outcome in terms of equivalent uniform dose (EUD). For four of the patients, EUD history of all seven plans suggests using the proposed optimization method with uncertainty data from the first five fractions, it is possible to achieve the same target coverage of static treatment plans (difference in EUD less than 1Gy). Meanwhile, the elimination of PTV margin also leads to a significant dose reduction (more than 15Gy) in rectum. / Science, Faculty of / Physics and Astronomy, Department of / Graduate
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Adult glioma managment with selective biopsy, voxel-wise radiomics, and simultaneous PET/MR imagingEmily Diller (9167027) 30 July 2020 (has links)
Every year more than fourteen-thousand adults in the United States are diagnosed with glioma, the most common malignant tumor of the central nervous system. Gliomas arise from glue like glial cells and present with a range of grade and prognosis. Glioblastoma multiforme (GBM), a grade IV glioma, is the most common glioma subtype and carries dismal prognosis with fewer than one half of patients surviving one year after diagnosis. The standard treatment for GBM is resection followed by a cocktail of chemo and radiation therapy. Unfortunately, complete surgical resection is impossible for GBM, and intra-tumor heterogeneity, a GBM hallmark, negatively impacts chemo and radiation therapy efficacy. This thesis contains six chapters that evaluate advanced imaging and statistical methods that may be used to improve glioma management. Chapter one presents background information to establish the relationship of four subsequent studies with ranging topics on advanced imaging techniques, biopsy sampling, and radiomic analysis. In chapter two, a case report is presented that demonstrates the importance of advanced magnetic resonance imaging (MRI) such as arterial spin labeled (ASL) perfusion sequences. In this case, a patient with a benign cerebral lesion presents with receptive aphasia and of the imaging data acquired, only ASL showed decrease cerebral aphasia. Chapter three describes the impact biopsy selection has on correlation between prognostic and histologic features in 35 patients with GBM. Multiple biopsy selection methods were compared, resulting in a wide range in correlation significance. Chapter four presents different voxel-wise radiomic models in adult glioma patients. From one voxel-wise radiomic model, predicted disease compositions (PDC) were computed in 17 glioma patients and were able to significantly (α = 0.05) predict overall survival, tumor grade, and endothelial proliferation. Chapter five describes the feasibility and hardware constraints of simultaneous PET/MR imaging protocols. A dynamic infusion of fluorodeoxyglucose (FDG) was administered with simultaneous MR imaging including echo planar imaging (EPI) based sequences used for functional MRI (fMRI). Heat from the EPI sequences deposited in the PET detector hardware and resulted in significant hardware failure. Finally, chapter six provides outlook and application to glioma clinical management considering the methods and findings presented in each study.<br>
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Development and Implementation of a GafChromic EBT In-Vivo Personal Dosimetry SystemBugno, Jacob R. 12 November 2008 (has links)
No description available.
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Dose Modification Factor Analysis of Multi-Lumen Brachytherapy Applicator with Monte Carlo SimulationWilliams, Eric January 2012 (has links)
No description available.
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A Novel Algorithm for the Reconstruction of an Entrance Beam Fluence from Treatment Exit Patient Portal Dosimetry ImagesSperling, Nicholas Niven January 2013 (has links)
No description available.
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In-vivo assessment of trabecular bone structure at the distal radiusGordon, Lane Christopher January 1997 (has links)
<p>Loss of bone mass has long been recognized as a major factor which makes bones brittle and susceptible to fracture. Currently bone mass is measured using a dual energy photon transmission technique, and a fracture risk is derived from comparison with reference normal values. Although the risk of fracture increases as bone mass decreases, variations in trabecular bone architecture can also affect strength. Consequently, trabecular bone architecture is often cited as a factor which might contribute significantly to fracture risk. Currently, estimates of trabecular bone structure are derived from biopsy studies. Such studies are invasive, destructive, cannot be used routinely in patients ar volunteers, and certainly cannot be repeated at the same site to obtain longitudinal measurements. If routine clinical assessments of architecture are to be made, it is necessary to determine which imaging modality best reveals structure in a non-invasive manner. It is also necessary to determine how the competence of the structure can best be expressed quantitatively. This work has examined ways of assessing trabecular bone structure at the distal radius in-vivo to better understand the contribution of architecture to fracture risk. To this end, it proceeded on four major fronts. First, images of sufficient resolution were acquired using a commercial pQCT scanner and a clinical MR imager. Second, the image processing software necessary to segment the imaged trabecular structure was developed. Third, two indices were proposed to quantify the connectivity of the segmented structure. One index was derived from the application of trabecular strut analysis to a skeletonized representation of the bone network. The other quantified the marrow space by deriving a mean hole area and maximum hole area of the bone structure as it appears in two dimensions. The clinical value of these indices was tested by conducting pilot studies which examined the ability of the indices to discriminate a small group of Colles fracture patients from the normal population and to reflect normal age related changes in structure. The proposed structural parameters better discriminated Colles' fracture patients than did measures of bone mineral density. The fourth and last stage of this work examined the proportion of the variance in compressive strength of a group of radius bones that can be accounted for by bone mineral density and bone architecture. In seeking the features that were the most reliable indicators of bone strength, a combination of the mean hole area and maximum hole area had the highest correlation with peak load at fracture. This held true whether these two variables were derived from pQCT or MR images. Therefore, these structural indices may represent a potentially exciting and promising means of discriminating fracture outcomes and monitoring changes in trabecular bone structure.</p> / Thesis / Doctor of Philosophy (PhD)
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Application of a heterogeneous coarse-mesh transport method (COMET) to radiation therapy problemsSatterfield, Megan E. 20 November 2006 (has links)
In recent years, there has been much improvement in radiation therapy delivery systems used in the treatment of cancer; however, in order to fully exploit this enhancement, the computational methodology associated with radiation therapy must improve as well. It is important to accurately determine where the radiation is depositing its energy within the patient. The treatment should allow for the maximal dose at the tumor site, while minimal radiation dose to the surrounding health tissue and structures. In the Computational Reactor and Medical Physics Group here at Georgia Tech, a heterogeneous coarse-mesh transport method (COMET) has been developed for neutron transport to analyze whole-core criticality. COMET decomposes a large, heterogeneous global problem into a set of small fixed source local problems. Response functions, or rather detailed solutions, are obtained for each unique local problem. These response functions are all precomputed and stored in a library. The solution to the global solution is then bound by a linear superposition of the local problems. In this project, COMET is applied for the first time to the transport of photons in human tissues. The parameter of interest in this case is the amount of energy (dose) deposition in tissue. To determine the strengths and weaknesses of the current system, it is important to construct benchmark problems for comparison. This project will encompass a number of benchmarks. The first will involve modeling a simple two-dimensional water phantom. A second benchmark problem involves the use of a heterogeneous phantom composed of different tissues. A third benchmark problem will involve transport through slabs of aluminum, water, and lung tissue. A last, more clinically relevant benchmark problem will involve using the data from a CT scan. For each of these cases the results from COMET will be compared to the computational results obtained from EGSnrc, a Monte Carlo particle transport code. In this study, it was found that generally the results using COMET were comparable with those obtained from the Monte Carlo solutions of EGSnrc. The COMET results were also typically found thousands of times faster than the reference solution.
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Numerical benchmarking of a coarse-mesh transport (COMET) method for medical physics applicationsBlackburn, Megan Satterfield 02 July 2009 (has links)
Radiation therapy has become a very import method for treating cancer patients. Thus, it is extremely important to accurately determine the location of energy deposition during these treatments, maximizing dose to the tumor region and minimizing it to healthy tissue. A Coarse-Mesh Transport Method (COMET) has been developed at the Georgia Institute of Technology in the Computational Reactor and Medical Physics Group for use very successfully with neutron transport to analyze whole-core criticality. COMET works by decomposing a large, heterogeneous system into a set of smaller fixed source problems. For each unique local problem that exists, a solution is obtained that we call a response function. These response functions are pre-computed and stored in a library for future use. The overall solution to the global problem can then be found by a linear superposition of these local problems. This method has now been extended to the transport of photons and electrons for use in medical physics problems to determine energy deposition from radiation therapy treatments. The main goal of this work was to develop benchmarks for testing in order to evaluate the COMET code to determine its strengths and weaknesses for these medical physics applications. For response function calculations, Legendre polynomial expansions are necessary for space, angle, polar angle, and azimuthal angle. An initial sensitivity study was done to determine the best orders for future testing. After the expansion orders were found, three simple benchmarks were tested: a water phantom, a simplified lung phantom, and a non-clinical slab phantom. Three more clinically relevant problems were developed from patient CT scans. Different coarse-mesh sizes and incident energies were tested. The COMET solutions for each case were compared to a reference solution obtained by pure Monte Carlo results from EGSnrc. In most cases, the COMET solutions produced reasonably good agreement with the COMET solutions. It was found that better results were obtained for lower energy incident photon beams as well as for larger mesh sizes. Recommendations were made for future development of COMET and the numerical benchmarks.
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Effects of linear energy transfer and hypoxia on radiation-induced immunogenicity through STINGDEVIN Andrew MILES (8770328) 28 April 2020 (has links)
<div>
<div>
<p>Purpose: Preclinical studies have demonstrated that cancer cells may produce innate immune
signals such as type-I interferons following radiation damage, which derives from activation
of the cGAS-STING pathway following detection of cytosolic dsDNA. Limited studies have
explored how these mechanisms vary from the conditions of the radiation exposure. High-
linear energy transfer (LET) radiation induces more DNA double-strand breaks (DSB) per
dose than low-LET radiation, thus is expected to be more immunogenic. However, DNA
damage in hypoxic cells is more probable to undergo chemical repair due to limitations in
oxygen fixation, thus is expected to be more immunosuppressive. Our goal is to study and
model the dose response characteristics of IFNβ and Trex1 in vitro following exposure of
radiations with varying LET and to develop techniques for further study in vivo.<br></p><p><br></p>
<p>Methods: Reference data from Vanpouille-Box (2017) on STING dose response was applied
to develop empirical models of cytosolic dsDNA and Trex1 regulation as a function of dose
and quantity of DNA DSB, the latter of which is dependent on particle LET and oxygenation
and is calculated using Monte Carlo Damage Simulation (MCDS) software. These models
were used as preliminary data to guide in vitro experiments using Merkel cell carcinoma
cells. The dose response of pro-inflammatory IFNβ and exonuclease Trex1, an anti-inflammatory suppressor of cGAS-STING, was measured post-irradiation. MCDS was again
used to model fast neutron relative biological effectiveness for DSB induction (RBEDSB) and
compared to laboratory measurements of the RBE for IFNβ production (RBEIFNβ). RBEIFNβ
models were applied to radiation transport simulations to quantify the potential secretion of
IFNβ in representative clinical beams. To enable intra-tumor radiation targeting of tumor
hypoxia, mice were seeded with syngeneic tumors and imaged longitudinally with PCT-
spectroscopy to determine local variations hemoglobin concentration (Hb) and oxygen
saturation (SaO2) over time. Hypoxia classification was based on SaO2 levels in voxels
containing hemoglobin relative to a “hypoxia threshold” of SaO2 < 0.2.</p><p><br></p>
<p>Results: Based on analysis of published data, our preliminary models of cytosolic DNA and
Trex1 dose responses demonstrate dose enhancements from high-LET radiation, such as that
at the distal edge of a Bragg peak, and suppression from cellular hypoxia. This manifests as
an RBE-dependent ‘shift’ in STING response. Laboratory measurements in MCC13 cells
show peak IFNβ production at 6.1 Gy following fast neutron irradiation and 14.5 Gy
following x-rays (RBEIFNβ = 2.4). However, IFNβ signal amplitudes were not significantly
different between these radiation types. Trex1 signal increased linearly with dose, with
fourfold higher upregulation per dose for fast neutrons. Modeling of RBE in clinical beams
suggests that ion sources may induce spatially localized IFNβ near their end of range, which
is potentially advantageous for initiation of tumor-specific immune activity. Uncharged
sources stimulate IFNβ more uniformly with depth. Longitudinal PCT-S scanning is able to localize and distinguish chronic and acute hypoxia in vivo. Changes in the hypoxic
classification from tumor growth and following anti-angiogenic therapy are distinguishable.<br> </p><p>
</p><div>
<div>
<div>
<p>Conclusion: Radiation-induced immunogenicity can be induced differentially based on
radiation quality and is expected to be affected by cellular oxygenation. High-LET radiation,
such as fast neutrons, drives greater IFNβ innate immune response per dose than low-LET
radiation, such as x-rays, which may enhance abscopal effects when used in combination
with immune-stimulating agents. However, anti-inflammatory signaling is greater per dose
for fast neutrons, and it remains unclear if high-LET radiations are therapeutically
advantageous over low-LET radiation for pro-inflammatory tumor signaling. High
resolution in vivo imaging of tumor hypoxia is feasible with photoacoustic techniques, which
can potentially be leveraged to study selective immunogenicity enhancement of the hypoxic
niche following radiation therapy. <br></p>
</div>
</div>
</div>
<p> </p>
</div></div>
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Characterization of a New D-D Neutron Generator System for Neutron Activation of Manganese in Bone In-VivoElizabeth Helen Jaye (12463536) 27 April 2022 (has links)
<p>Neutron Activation Analysis (NAA) is a non-invasive method for assessing the qualitative and quantitative elemental composition of a sample. One application of this technique is in-vivo quantification of specific elements in the human body. An important element in terms of human exposure assessment is Manganese (Mn). Mn is the fourth most usedindustrial metal and can be an inhalation exposure hazard specifically for welders. Over exposure to Mn can lead to neurological degeneration issues similar to Parkinson’s disease. It has been found that bone is a good biomarker for Mnas Mn is deposited in the bone and remains for long periods of time,allowing for an assay to reveal long term exposure information. The method of using NAA to quantify levels of Mn in-vivo using the bones in the human hand is being explored in this work.The NAA system used, involves a deuterium-deuterium neutron generator and an N-type High Purity Germanium Detector. It is critical to have the performance of the entire system characterized using phantoms and cadaver bones before the system can be used for in-vivo measurements. The goal of this work is to determine the neutron yield of the generator system, the neutron and photon dose received by a sample, the detection limit of Mn with this system, and to evaluate the Mn detection capability of the systemusing cadaver bones from occupationally exposed Mn miners. The parameters were determined through a combination of simulation with Monte Carlo N-Particle Code (MCNP), experiments using Mn doped bone phantoms and cadaver bones, and various dosimetry tools such as TLDs and EPDs. The neutron yieldfor the D-D 109M generator wasestimated to be2.24E+09+/-2.15E+07neutrons per secondfor this work. The Mn detection limit for the system was estimatedto be 0.442 ppm. The equivalent dose received by the sampleduring the standard 10-minute irradiation was estimated to be 8.45 +/-2.05rem. The results found for the human cadaver bones weremixed. It was found that the system was able to successfully detect Mn incadaver bones. Unexpectedly, however, three of the samples showed little to no Ca signal.In addition, significant amounts of soft tissue and bone marrow exist in the samples.Thereforethe Mn concentration in the bones was not able to be accurately estimated. A relative metric of Mn concentration was used instead and showed a slight positive increase from the unexposed to exposed samples but was not statistically significant.</p>
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