Practical problems of measuring depth of submucosal invasion in T1 colorectal carcinomas

In the present study, we analyzed T1 CRCs that were resected at Showa University Northern Yokohama Hospital in Japan from April 2001 to December 2013. A total of 21,060 colorectal neoplasms, excluding advanced carcinomas, had been resected endoscopically or surgically. Of these, 902 were T1 CRCs. To evaluate precise pathological diagnoses and LNM outcomes, we excluded lesions from 334 patients, including 279 patients who underwent only endoscopic resection, 20 who had synchronous advanced CRCs, one with familial adenomatous polyposis, three with Lynch syndromes, one with inflammatory bowel disease, and 30 whose specimens were impossible to evaluate pathologically in detail because of damage or loss (Fig. 1). In total, 568 patients with T1 CRC were included in this study, of whom 295 underwent surgical resection and lymph node dissection as first-line treatment, and 273 underwent first-line endoscopic resection followed by additional surgery with lymph node dissection. None of the patients received preoperative radiotherapy or neoadjuvant chemotherapy. We found each patient’s age, sex, and tumor location from their hospital records. For the morphological classification, we divided the lesions into three types: flat elevated type (0–IIa or laterally spreading tumor [LST]) [13]; protruded type (0–Is, Isp, or Ip); and depressed type (0–IIc, IIc + IIa, IIa + IIc, Is + IIc, or Ip + IIc); Fig. 2 [34, 35].

All resected specimens were immediately fixed in 10 % buffered formalin solution, observed with a focus on pit pattern using a stereomicroscope, and dissected at the point where the deepest invasion area could be exposed on the cut end surface. The other histological specimens were subsequently dissected into parallel 2- to 3-mm-thick sections and stained with hematoxylin and eosin (H&E). An experienced pathologist (S.H.) examined all the specimens histologically. Histologic grade was diagnosed based on the World Health Organization Classification of Tumors [36] and the current JSCCR guidelines. Unfavorable histological types were poorly differentiated adenocarcinoma (Por) or mucinous carcinoma (Muc) at any part of the lesion; favorable histological types were well or moderately differentiated adenocarcinoma. Double staining with H&E and Victoria blue (Muto Pure Chemicals Co., Ltd., Tokyo, Japan) was used to diagnose vascular infiltration. Lymphatic infiltration and status of muscularis mucosae were evaluated using H&E staining and immunostaining with D2-40 antibody (Dako North America Inc., Carpinteria, CA, USA) and desmin antibody (Dako North America Inc.), respectively. Tumor budding was defined as a cancer cell nest consisting of 1 or ˂5 cells that had infiltrated the interstitium at the invasive margin of the cancer. After selecting the field where budding was the most intensive, buddings were counted in a 0.785-mm² field as observed through an objective lens. Depending on the number of buddings, budding grade was scored as Grade 1: 0–4; Grade 2: 5–9; and Grade 3: ≥10 [8, 16, 37]. Grades 2–3 were defined as tumor budding positive.

We measured SID according to the clinical guidelines of the JSCCR [5, 16]. SID can be measured in two ways (Fig. 3). When it was possible to identify or estimate the location of the muscularis mucosae, we measured the SID directly from the line of the muscularis mucosae (method A; Fig. 3a). When the line of the muscularis mucosae was not easily identified because of carcinoma invasion, we measured the SID from the surface layer of the lesion (method B; Fig. 3b).

The lesions were divided into two groups: those with SID <1000 μm and those with SID ≥1000 μm. Between the two groups, we compared incidences of clinicopathological factors: age, sex, tumor location, tumor morphology, tumor size, method of measurement, mean SID, histologic type, lymphatic infiltration, vascular infiltration, tumor budding, and LNM. Mean SID and the LNM rates were calculated for each morphological type. We also assessed correlations between histologic type, lymphatic infiltration, vascular infiltration, tumor budding, and LNM, and SID by depth (0–999 μm, 1000–1999 μm, 2000–2999 μm, 3000–3999 μm, 4000–4999 μm, 5000–5999 μm, 6000–6999 μm, 7000–7999 μm, and ≧8000 μm,). Finally, in lesions with SID ≥1000 μm, we examined correlations between LNM and histologic type, lymphatic infiltration, vascular infiltration, and tumor budding.

Data are presented as the mean ± standard deviation. Differences were analyzed using the χ ² test, Fisher’s exact test, Student’s t test, or Ryan multiple comparison as necessary. Statistical significance was defined as a P < 0.05. All statistical analyses were performed using R version 2.10.0. (http://​www.​r-project.​org).

The ethics committee of our hospital approved the study protocol (approval number; 1408–01). Informed consent was obtained from all patients before endoscopy or surgery. This study was registered in the University Hospital Medical Network Clinical Trials Registry (UMIN R000017608). A summary of this study was presented at the United European Gastroenterology Week, Vienna, Austria on October 21, 2014 (oral presentation).