4D in vivo dose verification for real-time tumor tracking treatments using EPID dosimetry.

The use of sophisticated techniques such as gating and tracking treatments requires additional quality assurance to mitigate increased patient risks. To address this need, we have developed and validated an in vivo method of dose delivery verification for real-time aperture tracking techniques, using an electronic portal imaging device (EPID)-based, on-treatment patient dose reconstruction and a dynamic anthropomorphic phantom. Using 4DCT scan of the phantom, ten individual treatment plans were created, 1 for each of the 10 separate phases of the respiratory cycle. The 10 MLC apertures were combined into a single dynamic intensity-modulated radiation therapy (IMRT) plan that tracked the tumor motion. The tumor motion and linac delivery were synchronized using an RPM system (Varian Medical Systems) in gating mode with a custom breathing trace. On-treatment EPID frames were captured using a data-acquisition computer with a dedicated frame-grabber. Our in-house EPID-based in vivo dose reconstruction model was modified to reconstruct the 4D accumulated dose distribution for a dynamic MLC (DMLC) tracking plan using the 10-phase 4DCT dataset. Dose estimation accuracy was assessed for the DMLC tracking plan and a single-phase (50% phase) static tumor plan, represented a static field test to verify baseline accuracy. The 3%/3 mm chi-comparison between the EPID-based dose reconstruction for the static tumor delivery and the TPS dose calculation for the static plan resulted in 100% pass rate for planning target volume (PTV) voxels while the mean percentage dose difference was 0.6%. Comparing the EPID-based dose reconstruction for the DMLC tracking to the TPS calculation for the static plan gave a 3%/3 mm chi pass rate of 99.3% for PTV voxels and a mean percentage dose difference of 1.1%. While further work is required to assess the accuracy of this approach in more clinically relevant situations, we have established clinical feasibility and baseline accuracy of using the transmission EPID-based, in vivo patient dose verification for MLC-tracking treatments.

Aftabi S ，Sasaki D ，VanBeek T ，Pistorius S ，McCurdy B ... -  《-》

Toward real-time verification for MLC tracking treatments using time-resolved EPID imaging.

In multileaf collimator (MLC) tracking, the MLC positions from the original treatment plan are continuously modified to account for intrafraction tumor motion. As the treatment is adapted in real time, there is additional risk of delivery errors which cannot be detected using traditional pretreatment dose verification. The purpose of this work is to develop a system for real-time geometric verification of MLC tracking treatments using an electronic portal imaging device (EPID). MLC tracking was utilized during volumetric modulated arc therapy (VMAT). During these deliveries, treatment beam images were taken at 9.57 frames per second using an EPID and frame grabber computer. MLC positions were extracted from each image frame and used to assess delivery accuracy using three geometric measures: the location, size, and shape of the radiation field. The EPID-measured field location was compared to the tumor motion measured by implanted electromagnetic markers. The size and shape of the beam were compared to the size and shape from the original treatment plan, respectively. This technique was validated by simulating errors in phantom test deliveries and by comparison between EPID measurements and treatment log files. The method was applied offline to images acquired during the LIGHT Stereotactic Ablative Body Radiotherapy (SABR) clinical trial, where MLC tracking was performed for 17 lung cancer patients. The EPID-based verification results were subsequently compared to post-treatment dose reconstruction. Simulated field location errors were detected during phantom validation tests with an uncertainty of 0.28 mm (parallel to MLC motion) and 0.38 mm (perpendicular), expressed as a root-mean-square error (RMSError ). For simulated field size errors, the RMSError was 0.47 cm2 and field shape changes were detected for random errors with standard deviation ≥ 2.5 mm. For clinical lung SABR deliveries, field location errors of 1.6 mm (parallel MLC motion) and 4.9 mm (perpendicular) were measured (expressed as a full-width-half-maximum). The mean and standard deviation of the errors in field size and shape were 0.0 ± 0.3 cm2 and 0.3 ± 0.1 (expressed as a translation-invariant normalized RMS). No correlation was observed between geometric errors during each treatment fraction and dosimetric errors in the reconstructed dose to the target volume for this cohort of patients. A system for real-time delivery verification has been developed for MLC tracking using time-resolved EPID imaging. The technique has been tested offline in phantom-based deliveries and clinical patient deliveries and was used to independently verify the geometric accuracy of the MLC during MLC tracking radiotherapy.

Zwan BJ ，Caillet V ，Booth JT ，Colvill E ，Fuangrod T ，O'Brien R ，Briggs A ，O'Connor DJ ，Keall PJ ，Greer PB ... -  《-》

Frame average optimization of cine-mode EPID images used for routine clinical in vivo patient dose verification of VMAT deliveries.

McCowan PM ，McCurdy BM 《-》

Validation of a method for in vivo 3D dose reconstruction for IMRT and VMAT treatments using on-treatment EPID images and a model-based forward-calculation algorithm.

Van Uytven E ，Van Beek T ，McCowan PM ，Chytyk-Praznik K ，Greer PB ，McCurdy BM ... -  《-》

Clinical experience with EPID dosimetry for prostate IMRT pre-treatment dose verification.

McDermott LN ，Wendling M ，van Asselen B ，Stroom J ，Sonke JJ ，van Herk M ，Mijnheer BJ ... -  《MEDICAL PHYSICS》