¹⁸F-alfatide PET/CT may predict short-term outcome of concurrent chemoradiotherapy in patients with advanced non-small cell lung cancer

Eighteen patients with advanced NSCLC were enrolled in this study (Table 1). There were 14 males and four females with median age of 62 (range: 45–85). All patients had given informed consent to participate in this study, which was approved by the ethics committee of Shandong Cancer Hospital affiliated to Shandong University and met the following inclusion criteria: (1) advanced NSCLC diagnosed by histological and imaging examination such as CT or ¹⁸F-fluorodeoxyglucose (FDG) PET/CT (stage IIIA, IIIB or IV); (2) Karnofsky performance status (KPS) ≥70; (3) had measurable primary tumors according to Response Evaluation Criteria in Solid Tumors (RECIST). All patients were ready to undergo CCRT without undergoing surgery, chemotherapy or radiotherapy for thoracic tumors formerly, and they had the ¹⁸F-alfatide PET/CT scans before CCRT.

Patients were treated with chemoradiotherapy in a concurrent regimen. An intensity-modulated radiotherapy technique (IMRT) or three-dimensional conformal RT (3D-CRT) was delivered to all patients with megavoltage equipment (6 MV). RT was given as the conventionally fractionated regimen, 1.8 to 2.0 Gy for five days per week, and the total dose administered to patients ranged from 56 to 66 Gy (median dose, 60 Gy). RT was planned based on a CT scan performed for planning purposes, the gross tumor volume (GTV) included the primary tumor and involved lymph nodes, and the planning target volume (PTV) included the GTV plus a margin of 1.0–1.5 cm. All patients were treated with two cycles of chemotherapy with a cisplatin/docetaxel or a cisplatin/pemetrexed region during RT and the first cycle of chemotherapy was applied on day 1 of RT. Two to four additional cycles of chemotherapy were needed every 3 weeks after RT.

The simple lyophilized kit for labeling PRGD2 peptide was purchased from Jiangsu Institute of Nuclear Medicine, and the synthesis process was carried out by reference to previous study [13]. The radiochemical purity of the ¹⁸F-alfatide exceeded 95 %, and its specific radioactivity exceeded 37 GBq (1,000 mCi)/μmol. Patients were not requested to fast and to confirm blood glucose levels. After injected with¹⁸F-alfatide (214.38 ± 19.8 MBq) intravenously, they needed to rest for approximately 60 min. Scanning was performed with an integrated in-line PET/CT system (Discovery LS; GE Healthcare). PET images were performed from the head to the thigh, and the spiral CT component was performed with an x-ray tube voltage peak of 140 kV, 80 mA, a 6:1 pitch, a slice thickness of 4.25 mm, and a rotation speed of 0.8 s per rotation. A full-ring dedicated PET scan of the same axial range followed. The patients were in normal shallow respiration during image acquisition. The images were attenuation-corrected with the transmission data from CT. The attenuation-corrected PET images, CT images, and fused PET/CT images, displayed as coronal, sagittal, and transaxial slices, were viewed on a Xeleris workstation (GE Healthcare). The ¹⁸F-alfatide PET/CT scans were performed within 7 days before the start of CCRT.

Two experienced nuclear medicine physicians assessed the ¹⁸F-alfatide PET/CT images visually, referring to PET fusion and CT images, until consensuses were reached. Acquired ¹⁸F-alfatide PET/CT data was transferred into the workstation in the DICOM format. The radiotracer concentration in the regions of interest (ROI) was normalized to the injected dose per kilogram of the patients’ body weight to derive the standardized uptake values (SUVs). The SUVs were calculated according to the following formula: [measured activity concentration (Bq/mL) × body weight (g)]/injected activity (Bq).

PET/CT parameters such as maximum and mean standard uptake values (SUV_max and SUV_mean) and tumor volume (TV_PET) were generated using a vendor-provided automated contouring program. Peak standard uptake values (SUV_peak) were defined as the average SUV in a 1 cm³ sphere surrounding the voxel with the highest activity. We outlined the healthy lung with the position and volume similarly to the primary tumor to obtain the maximal activity of lung background. In addition, the maximal activity of 1 cm³ within the aortic arches and erector spinae were measured. Then the ratios of primary tumor and normal tissues based on SUV_max were calculated, denoted as T/NT (T/NT_lung, T/NT_blood and T/NT_muscle). In addition, tumor volumes were also measured by the CT images of PET/CT images, donated as TV_CT.

Short-term outcome was assessed at 4 weeks after CCRT (56–66 Gy RT and 4–6 cycles of chemotherapy) according to the revised RECIST criteria (v.1.1) using chest CT. According to RECIST criteria, the responders included the patients with an outcome of complete response (CR) or partial response (PR); the patients who had an outcome of stable disease (SD) or progressive disease (PD) were classified as the non-responders.

All statistical tests were performed with SPSS 17.0 and MedCalc 11.0.1.0. Statistical significance was assumed for P values less than 0.05 and all P values were 2-tailed. Eighteen patients were classified as responders and non-responders according to the revised RECIST criteria (v.1.1). Quantitative data for SUV_max, SUV_peak, SUV_mean, TV_PET, TV_CT and T/NT (T/NT_lung, T/NT_blood and T/NT_muscle) were expressed as mean ± standard deviation (SD) or median (interquartile range). Two-sample t tests and Wilcoxon rank-sum tests were used to compare the PET/CT parameters between responders and non-responders. SUV_max, SUV_peak and T/NT and multiple clinical variables such as age, stage, and histopathology were tested by logistic regression analyses to identify the relationships between these variables and the short-term outcomes. Receiver-operating characteristic (ROC) curve analysis was used to achieve the thresholds with the maximum Youden index and determine the diagnostic accuracy of ¹⁸F-alfatide PET/CT parameters in identifying the responders and non-responders.