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    Prognostic prediction in gastric cancer patients without serosal invasion: comparative study between UICC 7thedition and JCGS 13thedition N-classification systems

    2014-03-21 02:56:07
    Chinese Journal of Cancer Research 2014年5期

    Department of General Surgery, The First Affliated Hospital, Dalian Medical University, Dalian 116011, China

    *These authors contributed equally to this work.

    Correspondence to: Xiang Hu, MD. Department of General Surgery, The First Affliated Hospital, Dalian Medical University, No. 222 Zhongshan Road, Dalian 116011, China. Email: caoliang913@163.com.

    Prognostic prediction in gastric cancer patients without serosal invasion: comparative study between UICC 7thedition and JCGS 13thedition N-classification systems

    Xiang Hu*, Liang Cao*, Yi Yu

    Department of General Surgery, The First Affliated Hospital, Dalian Medical University, Dalian 116011, China

    *These authors contributed equally to this work.

    Correspondence to: Xiang Hu, MD. Department of General Surgery, The First Affliated Hospital, Dalian Medical University, No. 222 Zhongshan Road, Dalian 116011, China. Email: caoliang913@163.com.

    Objective:T-stage and N-stage have been proven to be the most important factors infuencing survival in gastric cancer patients, and have been accepted for use in the Japanese Classifcation of Gastric Carcinoma (JCGC) and the Union International Cancer Control (UICC-TNM) staging systems. The purpose of this study was to compare the prognostic values of the different N classifcation systems in gastric cancer patients without serosal invasion.

    Methods:We retrospectively compared the clinicopathological results of 1,115 patients with primary gastric cancer who underwent curative gastric resection.

    Results:Serosal invasion was identifed in 212 of 1,115 patients (19.0%), and it was associated with lymph node metastasis according to the JCGC13th(P<0.001) and TNM7th(P<0.001) systems. The 5-year survival rate for the serosal invasion-negative patients (78.2%) was significantly higher than that for the serosal invasion-positive patients (31.1%) (P<0.001). Multivariate Cox regression survival analysis showed that depth of invasion (P=0.013), 13thJCGC PN stage (P<0.001), and 7thTNM PN stage (P<0.001) were independent prognostic factors for serosal invasion-negative gastric cancer patients.

    Conclusions:The prognosis of gastric cancer patients with serosal invasion is very poor. Both the 13thJCGC and 7thTNM N-staging systems were able to accurately estimate the prognosis of gastric cancer patients, but the 7thTNM system was simpler and easier to use.

    Gastric cancer; serosal invasion; depth of invasion; lymph node metastasis

    View this article at:http://dx.doi.org/10.3978/j.issn.1000-9604.2014.10.09

    Introduction

    There are currently two main staging systems for gastric cancer, the Japanese Classification of Gastric Carcinoma (JCGC) and the Union International Cancer Control (UICC-TNM), which defne disease stage mainly according to tumor stage (T-stage) and lymph node stage (N-stage). Many studies have shown that N-stage and T-stage are the two most important factors for assessing the extent of disease, determining prognosis, and providing guidance for therapeutic strategies in gastric cancer patients (1-5).

    The prognosis of gastric cancer patients with serosal invasion is very poor. Even after radical resection of primary tumors, approximately 20% of these patients die due to recurrence (4-6). Peritoneal dissemination represents the most common type of recurrence (5). Peritoneal metastasis is known to be the most common non-curative factor, and serosal invasion is a critical predisposing factor for peritoneal metastasis in advanced gastric cancer (7). The main mechanism underlying peritoneal metastasis is thought to involve free cancer cells that are exfoliated from tumor cells in the gastric serosa, and the frequency of peritoneal metastasis therefore increases once tumor cellspenetrate the serosa (8,9).

    Table 1 Clinicopathological factors according to serosal invasion

    Lymph node involvement is the most important independent prognostic factor for gastric cancer (2-4). The JCGC (13thedition) N-classification system is based on the sites of involved lymph nodes, whereas the new TNM (7thedition) N-staging system is based on the number of metastatic lymph nodes (10,11). The purpose of this study was to compare N-classification systems (TNM 7thed. vs. JCGC 13thed.) and to evaluate the prognostic value of the N-number of the TNM 7thed. We also analyzed the effect of serosal invasion on prognosis and attempted to clarify the impact of lymph node metastasis on prognosis in gastric cancer patients.

    Materials and methods

    Clinical samples

    A total of 1,115 patients with primary gastric cancer who underwent curative gastric resection with D2 lymphadenectomy at The First Affiliated Hospital of Dalian Medical University between January 2000 and January 2008 were included in this study (Table 1). The surgical procedure was defined as curative resection (R0, absence of residual tumor as determined both macroscopically and microscopically). All of the patients provided written, informed consent to participate based on a document approved by our institutional ethics committee. None of the patients received preoperative adjuvant therapy. To reduce any effects directly related to surgery, patients whose preoperative examination revealed distant metastasis or those who died within 6 months after surgical resection were excluded from this study. All surgical resections were performed by a single experienced surgical team. All clinicopathologic variables were classified according to the JCGC (13thed.) and TNM (7thed.). The clinicopathologic data and long-term survival of the two groups were analyzed retrospectively. The follow-up period was calculated from the date of surgery until January 2013, and all patients were followed up for at least 5 years after surgery. The mean follow-up period was 71 months (range of 13-142 months). The follow-up data were obtained from census registry certifcates and outpatient records. Only cancer-related deaths were considered in survival analysis in this study.

    Follow-up evaluation consisted of assessments of patient history, physical examination, laboratory tests, including tumor marker tests (carcinoembryonic antigen, alphafetoprotein, carbohydrate antigen 12-5 and carbohydrate antigen 19-9), chest radiography, endoscopy, computed tomography (CT), and bone scintigraphy. These assessments were repeated every 6 months until the third postoperative year, and then every year thereafter for at least 5 years. Magnetic resonance imaging, CT of the brain or chest, and positron emission tomography were performed only when indicated.

    Statistical analysis

    Group differences were statistically analyzed using the χ2test and t-test. Cumulative survival curves were constructed by the Kaplan-Meier method, and the differences betweenthe curves were analyzed by the log-rank test. Multivariate analysis was based on the Cox regression model (the N-stages according to the JCGC13thand TNM7thsystems were analyzed separately). Statistical procedures were performed using SPSS version 15.0 (SPSS Inc., Chicago, IL, USA). P<0.05 was considered statistically signifcant.

    Table 2 Lymph node metastasis according to depth of invasion (%)

    Figure 1 Five-year survival rate according to serosal invasion (P<0.001).

    Results

    The clinicopathologic features of the patients with and without serosal invasion are shown in Table 1. Serosal invasion was identifed in 212 of 1,115 patients (19.0%), and it was significantly associated with lymph node metastasis according to the JCGC13th(P<0.001) and TNM7th(P<0.001) systems. However, age, gender, tumor location, tumor size, Borrmann type and histological type did not significantly differ (Table 1).

    Figure 2 Five-year survival rate according to depth of invasion (P<0.001). M, mucosa; SM, submucosa; MP, muscularis propria; SS, subserosa; SE, serosa; SI, adjacent structures.

    The TNM N-stages were equally divided within the T subgroups similar to the JCGC N-stages. As shown in Table 2, 416 patients (37.3%) were classifed as pN0. According to the JCGC 13th edition, the N+ cases were subclassifed as follows: 394 (35.3%) pN1, 229 (20.5%) pN2, and 76 (6.8%) pN3. According to the TNM 7thedition, the same cases were divided as follows: 372 (33.4%) pN1, 162 (14.5%) pN2, and 165 (14.8%) pN3.

    The 5-year survival rate of the serosal invasion-negative patients (78.2%) was significantly higher than that of the serosal invasion-positive patients (31.1%) (P<0.001) (Figure 1). According to the T-stages, the 5-year survival rates were as follows: mucosa (M)-stage 94.4%, submucosa (SM)-stage 86.9%, muscularis propria (MP)-stage 76.3%, subserosa (SS)-stage 64.6%, and serosa and adjacent structures (SE + SI)-stage 31.1% (Figure 2). According to the JCGC (13thed.) system, the 5-year survival rates were as follows: N0-stage 86.5%, N1-stage 74.9%, and N2-stage 47.2%, and N3-stage 11.8% (P<0.001) (Figure 3). The TNM (7thed.) system revealed that the 5-year survival rates were as follows: N0-stage 86.5%, N1-stage 80.9%, N2-stage 53.1%, N3a-stage 20.0%, and N3b-stage 9.2% (P<0.001) (Figure 4).

    Figure 3 Five-year survival rate according to lymph node metastasis (JCGC13th) (P<0.001).

    Figure 4 Five-year survival rate according to lymph node metastasis (TNM7th) (P<0.001).

    Univariate survival analysis indicated that the statistically signifcant prognostic factors affecting 5-year survival rate were tumor size (P=0.024), depth of invasion (P<0.001), the 13thJCGC PN stage (P<0.001), and the 7thTNM PN stage (P<0.001) (Table 3).

    Multivariate Cox regression survival analysis revealed that depth of invasion (P=0.013), the 13thJCGC PN stage (P<0.001), and the 7thTNM PN stage (P<0.001) were meaningful independent prognostic factors for the serosal invasion-negative gastric cancer patients (Table 4).

    Discussion

    Cancer staging systems are the most important tools for treatment planning in oncology and for assessing patient prognosis. The JCGC system defnes N stage by the site of lymph node metastasis relative to the primary tumor (10). The UICC (5thed., 1997) system is based on the number of metastatic lymph nodes (12). Before the 5thedition was published, N classifcation of gastric cancer was based on the anatomic locations of metastatic lymph nodes (13). Cancer staging systems should be simple, reproducible, and possess prognostic relevance. The 13thJCGC N-classification system, which is frequently used worldwide, is based on the extent of lymphatic metastasis and anatomic location, but this system is complicated and not always applicable. Many studies have reported that the UICC N staging system, which is based on the number of metastatic lymph nodes, is superior to that of the JCGC in terms of feasibility, objectivity, reproducibility and accuracy of prognostic prediction (14,15). Thus, the new 14thJCGC and 7thTNM staging systems are both based on the number metastatic lymph nodes and are considered to be better prognostic determinants than the former Japanese system (9,16).

    T-stage and N-stage have been proven to be the most important factors influencing survival in gastric cancer patients, and they are included in the JCGC and UICC systems (9,16). N stage is the most important survival predictor for gastric cancer. To date, three main N-stage classifcations have shown utility in predicting prognosis of gastric cancer patients worldwide, including classifcations based on the number of positive nodes, on the location of positive nodes, and on the ratio between metastatic and examined nodes (16-18).

    In this study, we found 394 (35.3%) pN1, 229 (20.5%) pN2, and 76 (6.8%) pN3 cases according to the JCGC 13thed. According to the TNM 7thed., the same cases were divided as follows: 372 (33.4%) pN1, 162 (14.5%) pN2, and 165 (14.8%) pN3. The 13thJCGC revealed the following 5-year survival rates: N0-stage 86.5%, N1-stage 74.9%, N2-stage 47.2%, and N3-stage 11.8% (P<0.001). The 7thTNM system indicated the following 5-year survival rates: N0-stage 86.5%, N1-stage 80.9%, N2-stage 53.1%, N3astage 20.0%, and N3b-stage 9.2% (P<0.001). Therefore, our results suggest that both the 13thJCGC N staging system and the 7thTNM N staging system can accurately estimate prognosis of gastric cancer patients but that the 7thTNM N staging system is simpler and easier to use.

    Table 3 Univariate analysis of 5-year survival rates gastric cancer patients

    Table 4 Independent prognostic factors in multivariate survival analysis of gastric cancer patients

    Many studies have reported that the 5-year survival rate of gastric cancer patients with serosal invasion is very poor (4,5,7). When gastric carcinomas have invaded the serosa or surrounding organs and tissues, curative resection may be diffcult, and it is not associated with a good prognosis (19-21). In this study, out of all of the gastric cancer patients who underwent curative gastric resection with D2 lymphadenectomy, the 5-year survival rate for the serosal invasion-negative patients (78.2%) was signifcantly higher than that of the serosal invasion-positive patients (31.1%) (P<0.001). The 5-year survival rates were as follows: M-stage 94.4%, SM-stage 86.9%, MP-stage 76.3%, SS-stage 64.6%, and SE + SI-stage 31.1%. Univariate survival analysis revealed that the depth of invasion was a significant prognostic factor affecting the 5-year survival rate (P<0.001).

    Conclusions

    In conclusion, the prognosis of gastric cancer patients with serosal invasion is very poor. Both the 13thJCGC N staging system and the 7thTNM N staging system are able to accurately estimate the prognosis of gastric cancer patients, but the 7thTNM system is simpler and easier to use.

    Acknowledgements

    Disclosure: The authors declare no confict of interest.

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    Cite this article as:Hu X, Cao L, Yu Y. Prognostic prediction in gastric cancer patients without serosal invasion: comparative study between UICC 7thedition and JCGS 13thedition N-classification systems. Chin J Cancer Res 2014;26(5):596-601. doi: 10.3978/j.issn.1000-9604.2014.10.09

    10.3978/j.issn.1000-9604.2014.10.09

    Submitted May 23, 2014. Accepted for publication Oct 09, 2014.

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