Normal tissue complication models for clinically relevant acute esophagitis (≥ grade 2) in patients treated with dose differentiated accelerated radiotherapy (DART-bid)

Between January 2004 and December 2011, 166 patients with locally advanced NSCLC (stage II–IIIB, UICC/AJCC 7th ed., 2010) were treated with dose differentiated accelerated radiotherapy, twice daily fractions of 1.8 Gy (DART-bid). Patients were discussed in a tumor board together with pneumologists, radiologists, medical oncologists, thoracic surgeons and radiation oncologists. Until 2008, the planning CT included the volume of the tumor and the lymph nodes but did not routinely cover the whole lung. In this study we only analyze the 66 patients with a total lung scan: 4 stage II, 44 stage IIIA and 18 stage IIIB. 38/66 patients were treated within an observational dose escalation study performed between 01/2004 until 12/2009), the remaining 28 were treated along the same treatment protocol but with improved image guidance in a follow up study [7, 25]. Accrual for the 2^nd study period terminated in December 2014, however, since the 28 patients from this second cohort had a sufficiently long follow up (mean 637 days), they were included in the present toxicity analysis. Overall, the median age was 65 years (range 44–83 years), the median Karnofsky Performance Score (KPS) was 70 (range 50–90). All studies were carried out with the approval of the responsible ethics committee, in accordance with national law and the Helsinki Declaration of 1975 (in its current, revised form). Informed consent was obtained from all patients.

Patients were irradiated with accelerated radiotherapy (1.8 Gy twice daily) delivered with 15-MV photon beams in 3D-target splitting technique [26]. Depending on tumor size (= mean of three perpendicular diameters) patients were allocated to four prescribed-dose groups: <2.5 cm 73.8 Gy, 2.5–4.5 cm 79.2 Gy, 4.5–6 cm 84.6 Gy, >6 cm 90 Gy. For treatment planning, patients were immobilized in a vacuum cradle in supine position. “Slow CTs” (4 s/slice, thickness 7 mm) were acquired. Due to the prolonged acquisition time the GTV appears enlarged on the CT scan, which means that it is actually a “CTV”. A margin of 7 mm was added to the GTV and positive lymph nodes to generate the PTV as described in a previous report [27]. In the diagnostic work up, a PET-CT was obligatory. Delineation of the tumor PTV was done on the post-chemotherapeutic planning CT in the lung window, the chest window was used for the lymph nodes. For treatment related parameters see Table 1. In the first cohort, image guidance was performed with two orthogonal kV images before each fraction, matching central anatomical structures (esophagus, trachea, main stem bronchi). For the second investigational period (starting in 2010), cone-beam-CT based tumor matching was performed (with or without marker fiducials). The following dose constraints were applied: V20-single-lung <50 %, V25-total-lung <30 %, D_max for spinal cord 45 Gy, D_max for esophagus 80 Gy.

Chemotherapy was administered in a sequential mode. All patients received two cycles of platinum based induction chemotherapy before radiotherapy, either with Gemcitabine or Pemetrexed. Antimycotic prophylaxis (Amphotericine B lozengers, 4 times daily) was administered during radiotherapy.

Patients were seen weekly during radiotherapy, 6 weeks after completion of radiotherapy, then quarterly for the first year, every four months during the second and third year, and bi-annually thereafter. AE was documented prospectively, according to RTOG, mild (grade 1), moderate (grade 2), severe (grade 3), life threatening (grade 4), and lethal (grade 5). A patient was scored as having acute esophagitis if the symptoms arose during treatment or within the first 3 months after radiotherapy, thereafter, esophageal toxicity was scored as chronic.

The external surface of the esophagus was contoured on each slice from the lowest edge of the cricoid cartilage to the gastro-esophageal junction. Oral contrast was administered before acquisition of the planning CT scan.

The dose was calculated with collapsed cone (calculation grid: 3 mm) with correction for tissue inhomogeneity (Oncentra Masterplan™ 4.1sp2). For multivariate analysis the following parameters were derived from the dose-volume histogram for each patient: mean esophageal dose (MED), Vx (volume receiving at least dose x) in 2.5 Gy steps from V20 to V70, Dmax, size of the tumor PTV, doses to the tumor, lymph nodes, and elective lymph drainage. A recent review of 18 studies found that the dose range from V20 to V50 including MED was significantly related with AE in most studies [23]. We therefore started our dosimetric analysis at V20. Additionally, the RTOG working group on quantitative analyses of normal tissue effects (QUANTEC) describe a clear trend that V_x with x > 40 Gy correlate with AE [28]. NTCP models were calculated for all dose levels between 0 and 91 Gy, which was the highest dose delivered to a single voxel, in 0.1 Gy steps. The volumes for each step are given as percentages.

NTCP models assign complication probabilities for organs at risk to given, generally inhomogeneous dose distributions. In this study the clinical endpoint, for which the probability of complication was calculated, was AE ≥ grade 2. We compared three models: (1) The Lyman-EUD model [29‐31], which is described by three parameters: the volume-effect parameter n (sometimes also denoted as a = 1/n) of the equivalent uniform dose (EUD), a dose–response steepness parameter m and the dose EUD ₅₀ (usually defined as D ₅₀ ) which leads to 50 % probability of complications. (2) The Lyman-MED model, which is a special case of the Lyman-EUD model, with the parameter n set to 1. (3) The cutoff dose logistic regression model which correlates the volume V _Dc receiving a dose D _c or higher with retrospective toxicity data in terms of a logistic regression (parameters β ₀ and β ₁ ). For the different NTCP modeling approaches we refer to Söhn et al. [32].

Inter-model comparison was performed with the corrected Akaike information criterion (AIC_c). The AIC_c quantifies the tradeoff between the model’s quality of fit (likelihood value, LL) and its complexity (number of model parameters, k) corrected by the number of cases (i.e. patients) N in the dataset: AIC_c = (-2LL + 2 k) + 2*k*(k + 1)/(N-k-1): the smaller the AIC_c value, the more efficient the fit of the model to a given dataset [33].

The biologically equivalent dose (EQD_2,T) was calculated with the linear quadratic formalism including a time factor [34, 35].

The distribution of patient, tumor and treatment characteristics in the dose groups was compared with the non-parametric Kruskal-Wallis-Test. Local and regional control rates as well as OAS were calculated according to the Kaplan-Meier-method. Patients without symptoms (grade 0) or with mild esophagitis (grade 1) were binned in one group, since pre-existing dysphagia is not always easy to differentiate from radiation-induced esophagitis especially in cases with large mediastinal adenopathy. Considering the time to the maximum degree of AE, grade 2 or higher esophagitis was chosen as the statistical endpoint for univariate and multivariate analyses (forward stepwise regression model) to detect potentially predictive factors. We used the software packages Mathematica™ (version 9) for NTCP-modeling and SPSS™ (version 21) for multivariate analyses.