Assessing the dosimetric consequence of inter-fractional setup shifts on helical tomotherapy plans with independent dose calculation

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Abstract

This work studied on dosimetric impact due to inter-fractional uncertainties for one hundred patients from five different treatment sites (30 prostate, 26 head & neck, 18 lung, 17 pelvis, and 9 brain patients) for Tomotherapy modality. Daily setup shifts were quantified and grouped into systematic (mean daily setup shifts) and random shifts (fraction based shifts with corresponding systematic shift subtraction). Both systematic and random shifts were incorporated into in-house independent point dose calculation software, MU-Tomo, to separately evaluate the systematic and random dosimetric variations. Systematic dosimetric variations showed large dose deviation, with the largest difference at -10.02% compared to the planned dose and 3% standard deviation. Mean random dosimetric variations showed relatively small dose deviation with the largest at -5.65% compared to the planned dose and 1.9% standard deviation. Furthermore, different treatment sites were sorted into the head & neck and brain group, and the body group including lung, pelvis, and prostate cancers. According to ANOVA analyses, random dosimetric variations were found significantly different between patients treated at the same treatment site, while systematic dosimetric variations were significantly different between the head & neck and brain group and the body group. No significant differences were discovered among specific patients for systematic dosimetric variations, and no significant differences were observed within each of the two groups for random dosimetric variations. Dosimetric consequences are not significantly correlated with treatment fraction number according to the Pearson correlation analysis. By comparing doses without any shift against those with the random shift, overall dosimetric impacts to each patient were found to be very small with the mean value -0.0053% and standard deviation of 1.11%. Ninety-nine percentage of the averaged variation results were within 3.5%. This implies that overall dosimetric impact from random variations is small; instead, dosimetric impact is more affected by systematic shifts. © 2010 He W, et al.

Figures

  • Figure 1: The MU-Tomo second check software working platform.
  • Table 1: Mean systematic shifts with standard deviation (SD) for dif ferent treatment sites. Positive and negative signs denote the coor dinate directions of Tomotherapy system.
  • Table 2: Mean standard deviations (mean SD), min, and max of random shifts for patients from different treatment sites.
  • Table 3: MU-Tomo calculated dose differences compared with planned doses information. Dose information for each group of patients is summarized here with the mean value, standard deviation (SD), maximum and minimum dose deviation.
  • Figure 2: Both plots show the independent dose calculation result from 100 helical tomotherapy patient plans with MU-Tomo. (a) Second check results without shifts (non-shift dose differences). (b) Dose difference consequences with systematic inter-fraction setup shifts.
  • Figure 3: Mean random variation of dosimetric consequences with standard deviations for each patient over its treatment fractions. Dose dif ferences were calculated with MU-Tomo with random shifts. Dosimetric consequences are shown in the following plots for (a) prostate patients, (b) head & neck patients, (c) lung patients, (d) pelvis patients, and (e) brain patients.
  • Table 4: Treatment site specif c random dosimetric difference result compared to the planned dose. Daily setup shifts were corrected by subtracting the systematic shifts.
  • Figure 4: Benchmarked dose dif ferences show the overall dosimetric impact after systematic correction for each of the hundred patients. The benchmarked dose dif ference is de f ned by subtracting the non-shift (reference) dose difference from the mean random dose difference.

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CITATION STYLE

APA

He, W., Luis, A. V. Q., Dzintars, E., Papanikolaou, N., & Shi, C. (2010). Assessing the dosimetric consequence of inter-fractional setup shifts on helical tomotherapy plans with independent dose calculation. Journal of Cancer Science and Therapy, 2(5), 136–144. https://doi.org/10.4172/1948-5956.1000039

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