Choice of immobilization of stereotactic body radiotherapy in lung tumor patient by BMI

The present study was approved by the Ethics Committee and Institutional Review Board of Zhejiang Cancer Hospital (belongs to Zhejiang Cancer Hospital; the committee’s reference Number: IRB-2018-153(Ke)). The medical records of NSCLC patients, who underwent SBRT in Zhejiang Cancer Hospital from January 2012 to September 2015 were reviewed. The inclusion criteria stated that the patients with early-stage (T1-T2N0M0) NSCLC lung cancer or oligometastatic lung cancer (IVa stage) were eligible for participation in this study. NSCLC (including carcinoma, adenocarcinoma, large cell carcinoma, and mixed cell carcinoma) in all patients was confirmed by histology. However, patients with several tumors in the lung were excluded from the analysis.

Patients were immobilized by TMPs (Klarity Medical Products, Newark, NJ, USA) or VCSs (Klarity Medical Products, Newark, NJ, USA) [13]. The patients were positioned in the immobilization device with the arms placed above the head. In the simulation, free breathing and 4D-CT (Philips Brilliance CT Big Bore, USA) were undertaken. The scan encompassed the upper margin of the second cervical spine up to the lower margin of the second lumbar spine with 3–5 mm layer thickness. The inhalation and exhalation correlated datasets were identified and transferred to the treatment planning system (RayStation Launcher 4.5.1, RaySearch Laboratories AB, Sweden or Philips Pinnacle 9.2 treatment planning system, Amsterdam, The Netherlands) for delineation of the gross tumor volume (GTV). The time phase interval of respiration in 4D-CT scanning was 10% with 10 images of the respiratory time phase on each layer. Furthermore, lung window and mediastinal window were compared. The GTV was contoured phase-by-phase referring to the result of chest CT or PET/CT. No margin was applied to the GTV to generate the clinical target volume (CTV). The GTV inhale and GTV exhale were fused to generate the internal tumor volume (ITV). The planning target volume (PTV) expanded 5–8 mm in every direction based on the ITV range. Moreover, organs at risk (OAR) including spinal cord, bilateral lungs, trachea, chest wall, brachial plexus, heart, and esophagus were contoured. The conformality and dose limits of normal tissues were set according to RTOG0236 [14]. The treatment requirements for large lesions (maximum cross-sectional diameter > 4 cm) or adjacent vital organs were satisfied by reducing the dose in each fraction and increasing the number of fractions. In the treatment, 80% iso-dose line was used as the prescribed dose to cover 95% PTV, and 100% iso-dose line was used to cover 100% ITV. The fraction dose was 5–15Gy. Patients received 4–10 SBRT fractions (mean = 5) by 6MV X-ray in 6–14 fields using the coplanar technique IMRT or volumetric modulated arc therapy (VMAT) (ElektaSynergy™, Stockholm, Sweden) or Varian Trilogy-SN5387 linear accelerator (Varian Medical Systems Inc., Palo Alto, CA, USA).

For initial treatment, the patients were set up to isocenter with in-room lasers and skin tattoos. Then, CBCT scanning was conducted in a 360° standard rotation mode. First, a rigid registration of the bony anatomy was performed to assess rotation, initiating the patient re-setup by therapists if a ± 3° rotational tolerance was exceeded. The manual registration of the ITV contour was performed with respect to patient’s tumor and soft-tissue target after the rotational parameters were measured within the tolerance limits. The data on the shifts were obtained from On Bio-rad Imager 1.6 system (Varian Medical Systems Inc., Baden, Switzerland), and cross-sectional, sagittal, and coronal CT images were obtained by analysis and reconstruction (automatic registration function equipped with OBI 1.6 software). The grayscale registration was conducted on areas including the tumor, the surrounding tissue, and vital organs at risk. The shifts from the first couch were adjusted accordingly. The tolerance of CBCT for treatment at our institute was 5, 5, and 5 mm in left-right, AP, and CC directions, respectively. Those exceeding these limits required verification of CBCT when the shift was adjusted. The couch position from the first fraction treatment was used as the couch position for the other fractions. Subsequently, the treatment was performed, post-treatment CBCT scanning was conducted after the treatment, and intrafraction setup errors data were obtained.

The 687 CBCT scans were collected from a cohort of 121 patients. In total, 60 patients received IMRT, while 61 patients received VMAT. Subsequently, 26 patients received 12.5Gy × 4 fractions, 91 received 10Gy × 5 fractions, 1 received 7.5Gy × 8 fractions, 2 received 7Gy × 10 fractions, and 1 received 6Gy × 10 fractions. The interfraction setup errors of patients are shown in Table 1.

As shown in Table 1, no correlation was established in the maximum interfraction setup errors in any direction irrespective of the factors such as the age, educational status, lesion location (left upper lobe, left lower lobe, right upper lobe, right middle lobe, right lower lobe), patients from rural or urban areas, body mass index (BMI), Karnofsky performance status (KPS), and methods of immobilization.

Thus, the setup errors in the ML, CC, and AP directions were less than a specific value, otherwise, CBCT necessitates verification. For example, if the CBCT required verification when the setup error was > 5 mm, then that in the ML, CC, and AP directions satisfying the initial CBCT< 6 mm were 95.3, 89.5, and 91.4%, respectively. The setup error < 6 mm in any direction was potentially 78.6%, while 21.4% was the probability of the necessity of CBCT verification (Fig. 1).

The patients were divided into two groups: BMI < 24 and BMI ≥ 24. The effects of different ways of immobilization on the interfraction setup errors after grouping were compared and the probability of CBCT verification was calculated. In the group with BMI ≥ 24, the setup error in the ML direction immobilized by TMP was 1.4 ± 1.2 mm, which was lower than that of VCS (2.4 ± 2.0 mm) (P < 0.001). The setup errors in the CC and AP directions immobilized by TMP were 2.0 ± 1.9 mm and 2.4 ± 1.4 mm, respectively, which did not differ significantly as compared to those by VCS (2.0 ± 1.9 mm in the CC direction, P = 0.917; 2.6 ± 2.1 mm in the AP direction, P = 0.546; Fig. 2).

In the group with BMI < 24, the interfraction setup error in the CC direction immobilized by VCS was 2.2 ± 2.2 mm, which was significantly lower as compared to the TMP (2.9 ± 2.3 mm; P = 0.001). However, the interfraction setup error in the AP direction immobilized by TPM was 1.8 ± 1.8 mm, which was significantly lower as compared to that by VCS (2.3 ± 2.0 mm; P = 0.006). Furthermore, no significant difference was observed in the ML direction between TMP and VCS (1.8 ± 1.4 mm in the CC direction vs. 2.1 ± 1.8 mm in the AP direction; P = 0.098; Fig. 3).

Furthermore, the acceptable setup errors in each direction did not exceed a specific value, or else, CBCT would require verification. The correlation between acceptable errors and rate in the ML, CC, and AP direction immobilized by VCS or TMP is shown (Fig. 4).

A total of 126 CBCT scans from 29 patients before and after radiotherapy were collected. The relative displacements before and after the treatment were 0.9 ± 1.0 mm in the ML direction, 1.1 ± 1.5 mm in the CC direction, and 1.2 ± 1.2 mm in the AP direction. The required expansions of PTV are listed (Table 2) according to different recipes. A total of 22 patients in the cohort used TMP, and the displacements during the treatment were 0.9 ± 1.0 mm in the ML direction, 1.1 ± 1.3 mm in the CC direction, and 1.2 ± 1.2 mm in the AP direction. On the other hand, 7 patients used VCS, and displacements were 1.3 ± 1.3 mm in the ML direction, 1.6 ± 2.2 mm in the CC direction, and 1.6 ± 1.3 mm in the AP direction. However, no significant difference was noted in all relative displacements of patients when different ways of immobilization were employed during the treatment (all P > 0.05).