Staging FDG PET-CT changes management in patients with gastric adenocarcinoma who are eligible for radical treatment

The records of patients referred for discussion at the Upper Gastrointestinal Multidisciplinary Team (MDT) meeting at Guy’s and St Thomas’ Hospital NHS Foundation Trust between March 2014 and December 2016 were analysed. All patients with a new diagnosis of biopsy-proven gastric adenocarcinoma were identified. Patients with Siewert Type I or II gastro-oesophageal tumours were excluded from the study; Type III tumours were included. We collected demographic data, tumour characteristics, radiographic and FDG PET-CT scan details, and treatment information from the patients’ electronic record. TNM stage, as per MDT consensus, was recorded both pre- and post-PET-CT scan. The contemporary 7th Edition of the American Joint Committee on Cancer (AJCC) manual of staging criteria was used to further classify staging information [2]. For those patients who subsequently underwent surgical resection the type of resection, number of lymph nodes resected and number of nodes positive for metastatic adenocarcinoma were recorded.

18-FDG-PET-CT scans were performed using the standard clinical oncology protocol at a single high-volume institution with double reporting as standard procedure. Scans were acquired 90 min after intravenous injection of 350 MBq FDG (range 283 MBq to 389 MBq). Images were acquired from skull base to upper thighs with 3 min per bed position using a GE Discovery 710 PET/CT scanner (GE Healthcare, Chicago, USA). A low-dose CT scan (140 kV, 10 mA, 0.5 s rotation time, and 40 mm collimation) was performed at the start of imaging to provide attenuation correction and an anatomical reference. PET images were reconstructed with a time-of-flight ordered subset expectation maximisation algorithm (2 iterations, 24 subsets) with a reconstructed slice thickness of 3.27 mm and pixel size 4.7 mm. FDG PET-CT scan reports were analysed and grouped as follows:

Group 4 includes any positivity that would indicate metastatic disease (and therefore lead to M1 staging), which includes both solid organ and distant lymph node disease [2]. In addition, a record was kept of whether FDG uptake unrelated to the gastric primary was described in the PET-CT report, and whether this then led directly to additional investigations. For quantitative analysis, a single, experienced nuclear medicine physician used a dedicated work-station to analyse FDG PET data for the maximum standardised uptake value (SUV_max).

For each patient who had TNM staging information available both pre- and post-FDG PET-CT, the effect of the additional scan on the staging was grouped as follows:

Group C indicates local nodes identified and involved on FDG PET-CT (i.e. N0 up-staged to N1, N2 or N3) and group D, newly diagnosed metastases (i.e. M0 up-staged to M1).

A total of 330 patients with newly diagnosed, biopsy-proven gastric adenocarcinoma were identified between March 2014 and December 2016. The majority of patients were male (65%, ratio 1.9:1) and median age at diagnosis was 73 years (range, 24–95 years). Histological analysis after endoscopic biopsy showed Lauren classifications consisting of 41% intestinal, 23% diffuse, 11% mixed and 24% not reported. Tumour differentiation at biopsy was 56% poorly differentiated, 33% moderately differentiated 2% well differentiated and 8% not reported. At the time of initial MDT discussion, following endoscopic biopsy and staging CT, 31% patients were found to have metastatic disease. These results are summarised in Table 1.

A total of 105 patients (32%) underwent PET-CT as part of the staging process. Breakdown of the patient and tumour characteristics of this sub-group of patients is also shown in Table 1. FDG PET-CT scans were not performed in the remainder of cases due to findings of metastatic disease on CT 88 (27%), frailty and limited treatment decisions 56 (17%), early/straight to surgery 45 (14%), patient declined 2 (1%) and not documented 34 (9%).

Analysis of FDG PET-CT scan reports showed that 86% of patients had an FDG-avid primary tumour (groups 2–4; 90 of 105 PET-CT scans), with breakdown of distribution as follows: 40 (38%) patients had a positive primary tumour only (group 2), 23 (22%) had positive primary and locoregional lymph nodes (group 3), and 27 (26%) had positive primary and distant metastases (group 4) (Fig. 1). Example images are shown in Fig. 2. The average size of FDG negative tumours was 39.7 mm (range 10–80 mm), i.e. tumours were larger than the resolution of PET-CT. The presence of FDG uptake unrelated to the gastric primary was also recorded and found to be present in 71 (68%) of FDG PET-CT scan reports. Thirteen of 105 (12%) patients required further investigation of incidental findings based on FDG PET-CT results. These included endobronchial ultrasound (EBUS) for upper mediastinal nodes (n = 4), colonoscopy (n = 2), cystoscopy (n = 2), fine needle aspiration of supraclavicular node (n = 1), breast ultrasound (n = 1) and pleural biopsy (n = 1). Incidental uptake typically represented distant inflammatory processes. However, in two cases a synchronous primary tumour was newly identified elsewhere (squamous cell carcinoma of the lung and B cell lymphoma of cervical lymph nodes).

Of the 90 FDG positive primary tumours, those of intestinal subtype were more likely to have FDG-avid lymph nodes (n = 13/44, 30%) or FDG-avid metastases (n = 15/44, 34%) compared with non-intestinal-type tumours (n = 5/46, 11% and n = 9/46, 20%; lymph node and metastasis positivity, respectively; Fig. 3).

Semi-quantitative analysis of FDG-avidity was obtained by measuring the SUV_max of the primary tumour. From this analysis, the primary tumour was found to have a mean SUV_max of 12.0 ± 0.9 (mean ± standard error of the mean (SEM); range, 2.6–41.4). Intestinal-type primary tumours were PET-positive in 93% (41/44) of cases, compared with 36/46 (78%) non-intestinal-type tumours (diffuse, mixed). In the remaining 15 cases, histological subtype was not recorded. In addition, mean SUV_max uptake was significantly higher in tumours of intestinal vs. non-intestinal type tumours (14.1 ± 1.3 vs. 9.0 ± 0.9; mean ± SEM, p = 0.005). Primary tumours that had metastasised also had higher SUV_max values (11.2 ± 1.2 for M0 disease vs. 14.6 ± 1.7 for M0; mean ± SEM; p = 0.052).

TNM stage prior to and following FDG PET-CT was recorded for each patient where this information was available (105 patients) and the impact of the scan on the staging was grouped (see Methods section, above). New information from FDG PET-CT lead to up-staging in 20/105 patients (groups C and D; 19%) by demonstration of previously undetected positive lymph nodes or metastases (Fig. 4). Of those patients who were up-staged, the majority was due to newly detected metastases (group D; 17 patients, 16%). These newly detected occult metastases included distant nodes (8 patients), peritoneal nodules (6 patients), liver metastases (2 patients) and adrenal metastasis (1 patient). Example images from patients with occult metastases are shown in Fig. 5. In 85 patients (groups A and B; 81%), no new information was provided as the FDG PET-CT was either negative or in agreement with the staging after initial MDT discussion (i.e. staging prior to FDG PET-CT).

From a total of 330 patients with newly diagnosed gastric adenocarcinoma, 54 (16%) underwent resectional surgery. Of these patients, 30 had a pre-surgical FDG PET-CT scan to enable comparison of pre-operative regional lymph node FDG-positivity and histological nodal status. Seventeen patients’ nodal status was concordant on FDG PET-CT and histological analysis (Table 2; six FDG and histology positive, 11 FDG and histology negative). Discordance between pre-treatment FDG PET-CT and histological nodal status was seen in 13 patients (Table 2; 4 FDG positive, histology negative, 9 FDG negative, histology positive). Of this discordant group, the majority of those with positive lymph nodes not predicted by PET-CT (i.e. FDG negative, histology positive) were of non-intestinal subtype (78%). In the concordant groups, the mix of intestinal and non-intestinal histological subtypes were evenly distributed. This suggests that nodal positivity is predicted more accurately in intestinal than non-intestinal tumours. These data correspond to an overall sensitivity and specificity of PET-CT nodal detection of 40% and 73%, respectively.

Nineteen of 30 patients underwent neo-adjuvant chemotherapy. Of these, discordance between pre-treatment FDG PET-CT and histological nodal status was seen in seven patients (2 FDG positive, histology negative; 5 FDG negative, histology positive). Four out of five patients in the neo-adjuvant group with positive lymph nodes not predicted by PET-CT were of non-intestinal subtype. Eleven patients proceeded directly to surgery following FDG PET-CT without neo-adjuvant treatment. In two cases, chemotherapy was contraindicated due to gastric outlet obstruction and cardiac comorbidity. In the remaining nine patients, pre-operatively staged as early, six of nine were finally staged as T1/2 (N0–2) and in three cases T3/4 but N0.