| Literature DB >> 25365935 |
Wei Zou, Lingshu Yin, Jiajian Shen, Michael N Corradetti, Maura Kirk, Reshma Munbodh, Penny Fang, Salma K Jabbour, Charles B Simone, Ning J Yue, Ramesh Rengan, Boon-Keng Kevin Teo.
Abstract
BACKGROUND: Intensity modulated arc therapy (IMAT) has been widely adopted for Stereotactic Body Radiotherapy (SBRT) for lung cancer. While treatment dose is optimized and calculated on a static Computed Tomography (CT) image, the effect of the interplay between the target and linac multi-leaf collimator (MLC) motion is not well described and may result in deviations between delivered and planned dose. In this study, we investigated the dosimetric consequences of the inter-play effect on target and organs at risk (OAR) by simulating dynamic dose delivery using dynamic CT datasets.Entities:
Mesh:
Year: 2014 PMID: 25365935 PMCID: PMC4243813 DOI: 10.1186/s13014-014-0225-3
Source DB: PubMed Journal: Radiat Oncol ISSN: 1748-717X Impact factor: 3.481
Figure 1Original and partitioned RapidArc plans. a) The original RapidArc plan and corresponding control points indicated by short lines along the arcs. b) A partitioned RapidArc plan with a subset of original control points and interpolated control points associated with one respiratory phase. This partial plan is used to compute the dose delivered to the patient at one respiratory phase.
Figure 2Flow chart of plan partitioning, dose calculation and dose accumulation using 4D CT images. Here “Part. Plan” represents “Partitioned Plan”, “Def. Reg.” represents “Deformable Registration”.
Effect of motion on tumor target dose distribution in fifteen patients
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| PTV V90% | −0.48% (−1.44%, 0.25%) | 0.20% (0.00%,1.89%) | −0.35% (−1.22%, 0.83%) |
| PTV V95% | −0.10% (−1.22%, 1.31%) | 0.12% (0.00%, 1.38%) | −0.26% (−1.06%, 1.97%) |
| PTV V105% | −5.04% (−13.88%, 9.71%) | 1.66% (0.00%, 6.87%) | 2.75% (−5.90%, 4.65%) |
| V_Presp. Iso./V_PTV | −0.15 (−0.31, −0.01) | 0.04 (0.00,0.15) | −0.30 (−0.91, −0.01) |
| V_50% Pres. Iso./V_PTV | −0.14 (−0.68, 0.06) | 0.05 (0.00, 0.24) | −0.32 (−1.63, 0.00) |
| D2cm | −0.22 Gy (−2.20 Gy, 1.70 Gy) | 0.45 Gy (0 Gy, 1.20 Gy) | −1.14 Gy (−4.00 Gy, 0.10 Gy) |
The mean values are cumulative dose differences averaged over all patients. The mean values of the 4D inter-fraction variation are the average of the largest variations among four fractions over all patients.
Motion effect on OAR dose distribution in fifteen patients
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| −0.03 Gy (−0.40 Gy, 0.20 Gy) | −0.05 Gy (0.00 Gy, 0.40 Gy) | −0.03 Gy (−0.30 Gy, 0.50 Gy) |
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| 0.00 Gy (−0.16 Gy, 0.17 Gy) | 0.02 Gy (0.00 Gy, 0.05 Gy) | 0.03 Gy (−0.12 Gy, 0.24 Gy) |
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| 0.01 Gy (−0.12 Gy, 0.14 Gy) | 0.02 Gy (0.00 Gy, 0.06 Gy) | 0.03 Gy (−0.13 Gy, 0.18 Gy) |
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| −0.22 Gy (−1.30 Gy, 0.30 Gy) | −0.19 Gy (0.00 Gy, 0.80 Gy) | −0.37 Gy(−2.60 Gy, 0.30 Gy) |
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| −0.06 Gy (−0.83 Gy, 1.37 Gy) | 0.07 Gy (0.01 Gy, 0.21 Gy) | −0.16 Gy (−0.89 Gy, 0.30 Gy) |
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| −0.51 Gy (−2.00 Gy, 0.90 Gy) | 0.27 Gy (0.00 Gy, 0.80 Gy) | −0.63 Gy (−2.5 Gy, 0.90 Gy) |
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| −0.18 Gy (−0.69 Gy, 0.92 Gy) | 0.08 Gy (0.00 Gy, 0.23 Gy) | −0.38 Gy (−1.54 Gy, 0.33 Gy) |
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| −0.52 Gy (−1.80 Gy, 6.00 Gy) | 0.19 Gy (0.00 Gy, 0.40 Gy) | 0.39 Gy (−1.10 Gy, 2.00 Gy) |
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| −0.12 Gy (−2.44 Gy, 2.66 Gy) | 0.04 Gy (0.00 Gy, 0.13 Gy) | −0.03 Gy (−1.05 Gy, 0.63 Gy) |
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| 0.04 Gy (−2.10 Gy, 1.40 Gy) | 0.03 Gy (0.00 Gy, 0.40 Gy) | 0.13 Gy (0.00 Gy, 1.00 Gy) |
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| −0.01 Gy (−0.42 Gy, 0.19 Gy) | 0.03 Gy (0.00 Gy, 0.37 Gy) | 0.01 Gy (−0.08 Gy, 0.14 Gy) |
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| 0.25 Gy (−2.00 Gy, 4.90 Gy) | 0.37 Gy (0.00 Gy, 1.20 Gy) | 0.75 Gy (−2.00 Gy, 7.80 Gy) |
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| −0.42 Gy (−4.10 Gy, 2.98 Gy) | 0.08 Gy (0.00 Gy, 0.25 Gy) | 0.30 Gy (−0.40 Gy, 1.59 Gy) |
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| −0.58 Gy (−3.00 Gy, 1.50 Gy) | 0.29 Gy (0.00 Gy, 1.20 Gy) | −0.54 Gy (−1.50 Gy, 0.60 Gy) |
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| −0.19 Gy (−1.58 Gy, 4.64 Gy) | 0.10 Gy (0.01 Gy, 0.32 Gy) | −0.33 Gy (−0.99 Gy, 0.44 Gy) |
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| 0.02% (−0.87%, 0.66%) | 0.02% (0.00%, 0.14%) | −0.08% (−0.41% 0.15%) |
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| −0.03 Gy (−0.23 Gy, 0.64 Gy) | 0.01 Gy (0.00 Gy, 0.09 Gy) | 0.03 Gy (−0.13 Gy, 0.74 Gy) |
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| −0.03 Gy (−0.18 Gy, 0.16 Gy) | 0.00 Gy (0.00 Gy, 0.02 Gy) | 0.03 Gy (−0.09 Gy, 0.46 Gy) |
The mean value are cumulative dose differences averaged over all patients. The mean values of the 4D inter-fraction variation are the average values of the largest variations among four fractions over all patients.
Figure 3The DVH comparison of the fractional dose for all four fractions when motion was considered. Very limited differences in dose distributions were observed from the DVHs of four fractions.
Figure 4Histogram representations of the motion effect. a) and b) Inter-fraction interplay effect: the voxel histogram of the largest dose differences in PTV volume and GTV volume among all four fractions for three patients; c) and d) difference in cumulative 4D dose with and without motion: histogram of dose differences in the PTV and GTV due to motion. The bars represent the percentage of the voxels in the PTV or GTV with dose differences in 0.2 Gy bins.
Figure 5Axial and coronal views of the dose difference with and without motion of three patients. The colored contours denote the GTV (magenta), PTV (black), PTV + 2 cm (red) and body (blue). The color overlay of the dose difference range from −5.0 Gy to 5.0 Gy.
Figure 6Verification plot to show that the planned MLC leaf positions at the control points correspond to the actual MLC leaf motion during delivery. These data correspond to MLC leaf 32 of bank A.