Kalyankuppam Selvaraj, Jothybasu
Modelling the effect of geometric uncertainties, clonogen
distribution and IMRT interplay effect on tumour control probability.
Doctor of Philosophy thesis, University of Liverpool.
![[img]](https://livrepository.liverpool.ac.uk/style/images/fileicons/application_pdf.png) |
PDF (PhD Thesis Final)
ThesisPhD_JothybasuSelvaraj_Revised.pdf - Submitted version Access to this file is embargoed until Unspecified. Available under License Creative Commons Attribution Non-commercial No Derivatives. Download (9MB) |
|
PDF
Kalyankuppam_SelvarajJot_Sep2013_17533.pdf - Author Accepted Manuscript Available under License Creative Commons Attribution No Derivatives. Download (9MB) |
Abstract
Geometric uncertainties are inevitable in radiotherapy. These uncertainties in tumour position are classi�fied as systematic (�) and random (�) errors. To account for these uncertainties, a margin is added to the clinical target volume (CTV) to create the planning target volume (PTV). The size of the PTV is critical for obtaining an optimal treatment plan. Dose-based (i.e., physical) margin recipes as a function of systematic and random errors based on coverage probability of a certain level of dose (90% or 95% of the prescription dose) have been published and widely used. However, with a TCP-based margin it is possible to consider fractionation and the radiobiological characteristics, especially the dose-response slope (50) of the tumour. Studies have shown that the density of the clonogens decrease from the boundary of the gross tumour volume (GTV). In such a scenario, dose that is lower than in the GTV should be suffi�cient to eradicate these clonogens. Thus a smaller PTV margin with a gradual dose fall off� can be used if the clonogen density in the GTV-CTV region is found to be lower than in GTV. Studies have reported tiny tumour islets outside the CTV region. These tiny tumour islets can be eradicated in some cases by the incidental dose outside the PTV due to the nature of the photon beam irradiation, but if they are not in the beam path the treatment outcome is compromised. In this thesis, a Monte Carlo approach is used to simulate the e�ect of geometric uncertainties, number of fractions and dose-response slope (gamma50) using the `enhanced Marsden' TCP model on the treatment outcome. Systematic and random errors were drawn from a pseudo-random number generator.The dose variations caused by tumour displacements due to geometric uncertainties in the CTV are accumulated each fraction on a voxel-by-voxel basis. Required margins for � 1% mean population TCP (TCPpop) for four-�field (4F) brick and a highly conformal spherical dose distribution for varying number of fractions, di�fferent 50 and di�fferent combinations of � and � are investigated. It is found that TCP-based margins are considerably smaller than dose-based recipes in most cases except for tumours with a steep dose-response slope (high 50) and a small number of fractions for both 4F and spherical dose distributions. For smaller geometric uncertainties (systematic,random� = �=1 mm) margins can be close to zero for the 4F technique due to high incidental dose outside the PTV. It is evident from the analyses that margins depend on the number of fractions, 50, the degree of dose conformality in addition to � and �. Ideally margins should be anisotropic and individualized, taking into account 50, number of fractions, and the dose distribution, as well as estimates of � and �. No single \recipe" can adequately account for all these variables.Using an exponential clonogen distribution in the GTV-CTV region, possible PTV margin reduction is demonstrated. Moreover, the e�ect of extra-CTV tumour islets is studied using a prostate IMRT plan. The islets were randomly distributed around the CTV with in a radius of 3 cm to represent di�erent patients. The doses were rescaled up to 102 Gy to obtain the dose-response curve (DRC). Interestingly, the obtained DRC showed a biphasic response where 100% TCP could not be achieved just by escalating the dose. Another potential problem encountered in intensity-modulated radiotherapy (IMRT) is the problems caused by the `interplay' e�ect between the respiration-induced tumour motion and the multileaf collimator (MLC) leaves movement during treatment. Several dosimetric studies in the literature have shown that `interplay' eff�ects blur the dose distribution by producing `hot' and `cold' dose inside the tumour. Most of these studies were done in a phantom with ion chambers or �lms, which provide only 1D or 2D dose information. If 3D dose information is available, a TCP based analysis would provide a direct estimate of interplay on the clinical outcome. In this thesis, an in-house developed dose model enabled us to calculate the 3D time-resolved dose contribution to each voxel in the target volume considering the change in segment shapes and position of the target volume. Using the model, delivered dose is accumulated in a voxel-by-voxel basis inclusive of tumour motion over the course of treatment. The eff�ect of interplay on dose and TCP is studied for conventionally and hypofractionated treatments using DICOM datasets. Moreover, the e�ect of dose rate on interplay is also studied for single-fraction treatments. Simulations were repeated several times to obtain mean population TCP (TCPpop) for each plan. The average variation observed in mean dose to the target volumes were
| Item Type: | Thesis (Doctor of Philosophy) |
|---|---|
| Additional Information: | Date: 2013-09 (completed) |
| Uncontrolled Keywords: | TCP modelling, Geometric uncertainties in radiotherapy, interplay effect in IMRT, Clonogen distribution in CTV, TCP loss, Monte Carlo simulation of geometric uncertainties |
| Subjects: | ?? RC0254 ?? |
| Divisions: | Faculty of Health and Life Sciences |
| Depositing User: | Symplectic Admin |
| Date Deposited: | 04 Aug 2014 06:44 |
| Last Modified: | 16 Dec 2022 04:41 |
| DOI: | 10.17638/00017533 |
| Supervisors: |
|
| URI: | https://livrepository.liverpool.ac.uk/id/eprint/17533 |
Dimensions
Dimensions
