Clinicopathological features of alpha-fetoprotein producing early gastric cancer with enteroblastic differentiation

AIM To investigate clinicopathological features of early stage gastric cancer with enteroblastic differentiation (GCED). METHODS We retrospectively investigated data on 6 cases of early stage GCED and 186 cases of early stage conventional gastric cancer (CGC: well or moderately differentiated adenocarcinoma) who underwent endoscopic submucosal dissection or endoscopic mucosal resection from September 2011 to February 2015 in our hospital. GCED was defined as a tumor having a primitive intestine-like structure composed of cuboidal or columnar cells with clear cytoplasm and immunohistochemical positivity for either alpha-fetoprotein, Glypican 3 or SALL4. The following were compared between GCED and CGC: age, gender, location and size of tumor, macroscopic type, ulceration, depth of invasion, lymphatic and venous invasion, positive horizontal and vertical margin, curative resection rate. RESULTS Six cases (5 males, 1 female; mean age 75.7 years; 6 lesions) of early gastric cancer with a GCED component and 186 cases (139 males, 47 females; mean age 72.7 years; 209 lesions) of early stage CGC were investigated. Mean tumor diameters were similar but rates of submucosal invasion, lymphatic invasion, venous invasion, and non-curative resection were higher in GCED than CGC (66.6% vs 11.4%, 33.3% vs 2.3%, 66.6% vs 0.4%, 83.3% vs 11% respectively, P < 0.01). Deep submucosal invasion was not revealed endoscopically or by preoperative biopsy. Histologically, in GCED the superficial mucosal layer was covered with a CGC component. The GCED component tended to exist in the deeper part of the mucosa to the submucosa by lymphatic and/or venous invasion, without severe stromal reaction. In addition, Glypican 3 was the most sensitive marker for GCED (positivity, 83.3%), immunohistochemically. CONCLUSION Even in the early stage GCED has high malignant potential, and preoperative diagnosis is considered difficult. Endoscopists and pathologists should know the clinicopathological features of this highly malignant type of cancer.

[1]  Tsuyoshi Saito,et al.  Clinicopathologic and immunohistochemical characteristics of gastric adenocarcinoma with enteroblastic differentiation: a study of 29 cases , 2016, Gastric Cancer.

[2]  Chen-Ming Hsu,et al.  Clinicopathologial features of gastric hepatoid adenocarcinoma , 2015, Biomedical journal.

[3]  Z. Chang,et al.  Clinicopathological and Prognostic Characteristics of Hepatoid Adenocarcinoma of the Stomach , 2014, Gastroenterology research and practice.

[4]  M. Mori,et al.  Gastrointestinal Obstruction due to Solitary Lymph Node Recurrence of Alpha-Fetoprotein-Producing Gastric Carcinoma with Enteroblastic Differentiation , 2014, Case Reports in Gastroenterology.

[5]  A. Marinis,et al.  Gastric Hepatoid Adenocarcinoma , 2013, Hellenic Journal of Surgery.

[6]  Jun Wu,et al.  Characteristic analysis of α-fetoprotein-producing gastric carcinoma in China , 2013, World Journal of Surgical Oncology.

[7]  F. Tao,et al.  Hepatoid adenocarcinoma of the stomach: a report of three cases. , 2013, World journal of gastroenterology.

[8]  T. Gotoda,et al.  Histologic and Immunohistochemical Analyses of &agr;-Fetoprotein—Producing Cancer of the Stomach , 2012, The American journal of surgical pathology.

[9]  T. Gotoda,et al.  Depth-predicting score for differentiated early gastric cancer , 2011, Gastric Cancer.

[10]  Japanese Gastric Cancer Association Japanese gastric cancer treatment guidelines 2010 (ver. 3) , 2011, Gastric Cancer.

[11]  W. Sheng,et al.  Clinicopathologic features and prognostic factors in alpha‐fetoprotein‐producing gastric cancers: Analysis of 104 cases , 2010, Journal of surgical oncology.

[12]  Tadao Tanaka,et al.  Alpha-fetoprotein (AFP)-producing ovarian tumor in an elderly woman , 2009, International Journal of Clinical Oncology.

[13]  A. Iwasaki,et al.  Alpha-fetoprotein (AFP)-producing adrenocortical carcinoma — Long survival with various therapeutic strategies including a lung resection: Report of a case , 2008, Surgery Today.

[14]  T. Osuga,et al.  Histologic and immunohistochemical studies of alpha-fetoprotein (AFP)-producing gastric carcinoma , 1987, Gastroenterologia Japonica.

[15]  M. Ichinose,et al.  A case of primary lung cancer producing alpha-fetoprotein. , 2004, Canadian respiratory journal.

[16]  H. Tajiri,et al.  Seronegative alpha-fetoprotein-producing early gastric cancer treated with endoscopic mucosal resection and additional surgery. , 2004, Internal medicine.

[17]  S. Kitano,et al.  AFP-Producing Gastric Carcinoma: Multivariate Analysis of Prognostic Factors in 270 Patients , 2003, Oncology.

[18]  D. Hay,et al.  Case Report ALPHA-FETOPROTEIN-PRODUClNG ADENOCARCINOMA OF THE SIGMOID COLON WITH POSSIBLE HEPATOID DIFFERENTIATION , 1995 .

[19]  A. Östör,et al.  Alpha‐fetoprotein‐producing adenocarcinoma of the sigmoid colon with possible hepatoid differentiation , 1995, Pathology.

[20]  A. Mukawa,et al.  Alpha‐fetoprotein–producing gastric carcinoma with enteroblastic differentiation , 1994, Cancer.

[21]  H. Watanabe,et al.  α‐Fetoprotein producing gastric carcinomas: A comparative study of three different subtypes , 1993, Acta pathologica japonica.

[22]  M. Shamoto,et al.  Hepatoid adenocarcinomas of the stomach: An analysis of seven cases , 1986, Cancer.

[23]  Y. Shimosato,et al.  Production of alpha‐fetoprotein, normal serum proteins, and human chorionic gonadotropin in stomach cancer: Histologic and immunohistochemical analyses of 35 cases , 1981, Cancer.

[24]  P. K. Lee,et al.  Carcinoembryonic antigen, alpha‐fetoprotein and carcinoplacental alkaline phosphatase in gastric carcinoma metastatic to the liver , 1977, Cancer.

[25]  H. Nishimura,et al.  Occurrence of alpha-fetoprotein, Regan isoenzyme, and variant alkaline phosphatase in the serum of a patient with gastric cancer. , 1976, Gastroenterology.

[26]  A. Fondimare,et al.  [Existence of alpha feto protein during gastric-origin secondary cancer of the liver]. , 1970, La Presse medicale.

[27]  C G BERGSTRAND,et al.  Demonstration of a new protein fraction in serum from the human fetus. , 1956, Scandinavian journal of clinical and laboratory investigation.