Multi‐institutional investigation into the robustness of intra‐cranial multi‐target stereotactic radiosurgery plans to delivery errors

Author:

May Lauren1,Hardcastle Nicholas12,Hernandez Victor3,Saez Jordi4,Rosenfeld Anatoly1,Poder Joel156

Affiliation:

1. Centre for Medical and Radiation Physics University of Wollongong North Wollongong NSW Australia

2. Physical Sciences Peter MacCallum Cancer Centre Melbourne VIC Australia

3. Department of Medical Physics, Hospital Universitari Sant Joan de Reus IISPV Tarragona Spain

4. Department of Radiation Oncology Hospital Clínic de Barcelona Barcelona Spain

5. St George Cancer Care Centre St George Hospital Kogarah NSW Australia

6. School of Physics University of Sydney Camperdown NSW Australia

Abstract

AbstractBackgroundThe use of modulated techniques for intra‐cranial stereotactic radiosurgery (SRS) results in highly modulated fields with small apertures, which may be susceptible to uncertainties in the delivery device.PurposeThis study aimed to quantify the impact of simulated delivery errors on treatment plan dosimetry and how this is affected by treatment planning system (TPS), plan geometry, delivery technique, and plan complexity. A beam modelling error was also included as context to the dose uncertainties due to treatment delivery errors.MethodsDelivery errors were assessed for multiple‐target brain SRS plans obtained through the Trans‐Tasman Radiation Oncology Group (TROG) international treatment planning challenge (2018). The challenge dataset consisted of five intra‐cranial targets, each with a prescription of 20 Gy. Of the final dataset of 54 plans, 51 were created using the volumetric modulated arc therapy (VMAT) technique and three used intensity modulated arc therapy (IMRT). Thirty‐five plans were from the Varian Eclipse TPS, 17 from Elekta Monaco TPS, and one plan each from RayStation and Philips Pinnacle TPS. The errors introduced included: monitor unit calibration errors, multi‐leaf collimator (MLC) bank offset, single MLC leaf offset, couch rotations, and collimator rotations. Dosimetric leaf gap (DLG) error was also included as a beam modelling error. Dose to targets was assessed via dose covering 98% of planning target volume (PTV) (D98%), dose covering 2% of PTV (D2%), and dose covering 99% of gross tumor volume (GTV) (D99%). Dose to organs at risk (OARs) was assessed using the volume of normal brain receiving 12 Gy (V12Gy), mean dose to normal brain, and maximum dose covering 0.03cc brainstem (D0.03cc). Plan complexity was also assessed via edge metric, modulation complexity score (MCS), mean MLC gap, mean MLC speed, and plan modulation (PM).ResultsPTV D98% showed high robustness on average to most errors with the exception of a bank shift of 1.0 mm and large rotational errors ≥1.0° for either the couch or collimator. However, in some cases, errors close to or within generally accepted machine tolerances resulted in clinically relevant impacts. The greatest impact upon normal brain V12Gy, mean dose to normal brain, and D0.03cc brainstem was found for DLG error in alignment with other recent studies. All delivery errors had on average a minimal impact across these parameters. Comparing plans from the Monaco TPS and the Eclipse TPS, showed a lesser increase to V12Gy, mean dose to normal brain, and D0.03cc brainstem for Monaco plans (p < 0.01) when DLG error was simulated. Monaco plans also correlated to lower plan complexity. Using Spearman's correlation coefficient (r) a strong negative correlation (r ≤ −0.8) was found between the mean MLC gap and dose to OARs for DLG errors.ConclusionsReducing MLC complexity and using larger mean MLC gaps is recommended to improve plan robustness and reduce sensitivity to delivery and modelling errors. For cases in which the calculated dose distribution or dose indices are close to the clinically acceptable limits, this is especially important.

Publisher

Wiley

Subject

General Medicine

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