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An Iterative Approach to Modelling Dosimetric Properties of a Varian MLC


D DiCostanzo

D DiCostanzo1*, (1) Ohio State University, Columbus, OH

Presentations

SU-E-T-111 (Sunday, July 12, 2015) 3:00 PM - 6:00 PM Room: Exhibit Hall


Purpose:
In effort to efficiently and accurately model MLC parameters for use in Varian Eclipse treatment planning system (TPS), an iterative technique for characterizing the dosimetric properties of MLCs has been developed.

Methods:
The initial characterization of the dosimetric leaf gap (DLG) and MLC transmission was performed using varied sizes of moving gaps and transmission measurements through central axis of the radiation beam. These values were determined during the initial data collection. After the initial values were determined and entered into the TPS, two plans were calculated to test the veracity of DLG and transmission independently.

The plan used to determine the DLG has openings of varied sizes which are affected differently by the DLG. A large field uniform fluence that required a MLC carriage shift was used to determine the transmission value independent of DLG. After characterizing the dosimetric properties of the MLC independently, clinical IMRT plans were tested and used to tweak the final values.

Results:
This approach to modelling MLC dosimetric properties was employed for: standard 120 leaf MLC (SDMLC) and 120 leaf high definition MLC (HDMLC). Both types were successfully commissioned, tested, and approved for clinical use on 4 SDMLC machines and 2 HDMLC machines. The pass rate of clinical IMRT plans was 96.9% for 6MV and 98.3% for 10MV for SDMLC and 96.3% for 6MV, 96.5% for 6FFF, and 97.5% for 10FFF for HDMLCs using MapCheck2 with gamma analysis of 2%/2mm and 10% threshold. The final DLG and transmission parameters for 6X were 0.5mm and 0.01, and 1.35mm and 0.02 for HD and SD MLCs respectively.

Conclusion:
This iterative approach of determining dosimetric properties of MLCs is viable for both SDMLC and HDMLC and multiple energies. This approach accurately and efficiently determines the values needed for commissioning MLCs when they are employed for modulated therapies.



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