Appearances of screen-detected versus symptomatic colorectal cancers at CT colonography

CTC images depicting CRC derived from two sources: prospective collection via two paired, randomized trials (the Special Interest Group in Gastrointestinal and Abdominal Radiology [SIGGAR] trials); and retrospective collection from a national CRC screening program (the English Bowel Cancer Screening Programme, EBCSP). Ethical permission was granted for use of CTC data for future research in the randomized trials and waived by the Joint Research Office of the chief investigator for the screening datasets. Patients in the randomized studies gave written informed consent.

The RCTs required full bowel purgation for CTC, multidetector acquisition at ≥2.5 mm collimation and dual patient positioning. Oral fecal tagging agents were discretionary, as was the use of intravenous contrast. The EBCSP requires multidetector-row CTC at slice thickness of 1–3 mm and dual positioning. Fecal tagging, antispasmodics, and the use of carbon dioxide were recommended at program inception and mandated since 2012. Intravenous contrast is generally discouraged unless there is a specific requirement for detailed extracolonic evaluation. Detailed acquisition parameters are provided in Supplementary Table 1.

Two radiologists (AAP, seven years experience of CTC) and (FP, two years experience) reviewed the CTC images independently. Each radiologist used the prone and supine images (with multiplanar reformatting and endoluminal views when needed) to record: (a) tumour morphology; either non-polypoid or polypoid; (b) for polypoid lesions, their sub-type using the Paris classification [21]: sessile, pedunculated, semi-pedunculated or flat (<2.5 mm height); (c) for non-polypoid lesions, whether they were annular (≥90 % of the colonic circumference) or non-annular; (d) presence/absence of luminal stenosis (≥50 % diameter reduction versus the immediately distal colonic segment); (e) tumour dimensions (maximum multiplanar long axis and orthogonal short axis for polypoid lesions; long axis and tumour thickness for non-polypoid tumours); (f) radiological T stage, using the TNM 7th edition [22]; (g) for T3 and T4 lesions, extramural depth of spread (EMD) beyond the muscularis propria; (h) presence/absence of radiologically-involved lymph nodes; (i) presence/absence of vascular invasion; (j) subjective image quality using a combined assessment of bowel cleansing and distension (1 = good, 2 = moderate or 3 = poor); (k) use of fecal tagging; and (l) subjective conspicuity of the tumour on a 100-point scale (1 = “barely visible”; 100 = “immediately obvious”). We followed the criteria of Burton et al. when determining lymph node involvement and vascular invasion [23] (nodal involvement=at least one node ≥1 cm in short axis, or a cluster of ≥3 nodes within the tumour local vascular pedicle; vascular invasion=nodular enlargement of colic veins).

Tumour segmental location was extracted from either SIGGAR trial or EBCSP records and confirmed from the images by both radiologists. Differences between radiologists regarding tumour morphology, T stage, EMD, nodal status, and vascular invasion were resolved by face-to-face discussion with images available, although we also recorded each radiologists’ original opinion for assessment of interobserver agreement. Since TNM stage does not always influence pre-operative treatment decisions, we also coded all tumours as either good-prognosis or poor-prognosis tumours, which is both reproducible and important when considering the administration of neoadjuvant therapy [24‐26]. Specifically, tumours of either T1, T2, or T3 stage with <5 mm of EMD are regarded as having a good prognosis, whereas T4 and T3 tumours with either (a) radiologically-involved lymph nodes or (b) ≥5 mm of EMD are viewed as having a poor prognosis [25, 26].

Since radiologist opinions are inherently subjective, we generated objective measures of tumour location, ease of detection, and volume. To achieve this, AAP recorded (a) workstation-derived distance along the colonic centerline from the anorectal junction to the distal edge of the tumour; (b) presence/absence of at least one CAD mark within 5 mm of the tumour in any direction; (c) the total number of CAD marks for each patient; and (d) tumour volume, calculated by manually outlining the tumour on each slice and using the workstation’s volume calculation function. The CAD package used was iCAD (Nashua, New Hampshire) version 1.4.1.

Data were collated using Microsoft Excel 2011 (Microsoft, Redmond, WA) and analyzed with R version 3.0.1. Since three patients had more than one tumour, analysis was on a per-patient basis for patient-level variables (e.g., scan quality, demographics) and on a per-lesion basis for tumour-level variables (e.g., dimensions, conspicuity).

Patient age and subjective image quality (averaged between readers) were compared between symptomatic and screening groups with the Mann-Whitney-Wilcoxon test. Patient sex and use of fecal tagging were compared using chi-squared and Fisher exact tests, respectively. To determine imaging features that differed significantly between symptomatic and screen-detected tumours after adjustment for age and sex, we applied multivariable regressions using linear, binary logistic, multinominal, or ordered logistic regression as appropriate. Tumour dimensions, volumes, and conspicuity scores were log-transformed to approximate normality prior to modeling. We used case origin (i.e., symptomatic vs screening) as the explanatory variable and patient age and sex as covariates. Image quality was added as a covariate for analysis of subjective conspicuity.

Agreement between radiologists’ initial independent reads for tumour stage, nodal stage, and presence of vascular invasion was calculated using quadratic weighted kappa for tumour stage and unweighted kappa for nodal and vascular stage. Probability values of <0.05 were taken as statistically significant.