Gastric ulcer patients are more susceptible to developing gastric cancer compared with concomitant gastric and duodenal ulcer patients

Hong,Jun-Bo; Zuo,Wei; Wang,An-Jiang; Xu,Shan; Tu,Lu‑Xia; Chen,You‑Xiang; Zhu,Xuan; Lu,Nong-Hua

doi:10.3892/ol.2014.2583

Gastric ulcer patients are more susceptible to developing gastric cancer compared with concomitant gastric and duodenal ulcer patients

Authors:
- Jun-Bo Hong
- Wei Zuo
- An-Jiang Wang
- Shan Xu
- Lu‑Xia Tu
- You‑Xiang Chen
- Xuan Zhu
- Nong-Hua Lu
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Affiliations: Department of Gastroenterology, The First Affiliated Hospital of Nanchang University, Nanchang, Jiangxi 330006, P.R. China, Department of Respiratory Medicine, The First Affiliated Hospital of Nanchang University, Nanchang, Jiangxi 330006, P.R. China, Department of Pathology, The First Affiliated Hospital of Nanchang University, Nanchang, Jiangxi 330006, P.R. China
Published online on: October 2, 2014 https://doi.org/10.3892/ol.2014.2583
Pages: 2790-2794

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Abstract

Intestinal metaplasia (IM) and dysplasia are precancerous lesions of gastric cancer (GC); however, the prevalence of IM and dysplasia in patients exhibiting single gastric ulcer (GU) and concomitant gastric and duodenal ulcer (CGDU) varies. In the present study consecutive patients who had undergone esophagogastroduodenal endoscopy were retrospectively screened, and those presenting with GU or CGDU were further evaluated for IM and dysplasia. Patients diagnosed with GC or lymphoma and patients with a history of anti‑Helicobacter pylori, non‑steroidal anti‑inflammatory medicine (NSAIM), H2‑receptor antagonist or proton pump inhibitor therapy, were excluded from the present study. Of the 204,073 consecutively screened cases, 8,855 (4.3%) and 2,397 (1.2%) were diagnosed with GU and CGDU, respectively. A total of 1,722 GU and 233 CGDU patients were excluded; thus, 7,133 and 2,164 cases of GU and CGDU, respectively (n=9,297), were included in the present study. IM and dysplasia were observed in 1,348 (14.5%) and 210 (2.3%) patients, respectively. IM was more frequently identified in GU patients compared with CGDU patients (16.4 vs. 8.3%; odds ratio [OR], 2.158; 95% confidence interval [CI], 1.830‑2.545; χ2=86.932; P<0.001); furthermore, GU patients exhibited significantly more frequent IM compared with CGDU patients at the gastric antrum (14.2 vs. 5.5%; OR, 2.818; 95% CI, 2.199‑3.610; χ2=72.299; P<0.001), gastric incisura (24.0 vs. 14.1%; OR, 1.922; 95% CI, 1.502‑2.432; χ2=30.402; P<0.001) and gastric corpus (12.6 vs. 3.3%; OR, 4.259; 95% CI, 1.030‑17.609; χ2=4.736; P=0.026). Dysplasia was significantly more frequently identified in GU patients compared with CGDU patients (2.7 vs. 0.7%; OR, 4.027; 95% CI, 2.376‑6.823; χ2=31.315; P<0.001), with GU patients exhibiting significantly more severe dysplasia at the gastric antrum (2.4 vs. 0.7%; OR, 3.339; 95% CI, 1.735‑6.425; χ2=14.652; P<0.001) and the gastric incisura (2.9 vs. 0.7%; OR, 4.255; 95% CI, 1.694‑10.689; χ2=11.229; P<0.001). Additionally, mild IM was more frequently identified in GU patients compared with CGDU patients (15.2 vs. 7.1%; OR, 2.353; 95% CI, 1.972‑2.807; χ2=94.798; P<0.001) and dysplasia of a mild (1.7 vs. 0.6%; OR, 2.807; 95% CI, 1.580‑4.987; χ2=13.519; P<0.001) or moderate/severe grade (1.1 vs. 0.09%; OR, 11.642; 95% CI, 2.857‑47.439; χ2=18.896; P<0.001) was more frequent in GU patients compared with CGDU patients. IM and dysplasia were more frequently observed in GU compared with CGDU patients in the present study, which may be associated with an increased probability of developing GC.

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1	Danaei G, Vander Hoorn S, Lopez AD, Murray CJ and Ezzati M; Comparative Risk Assessment collaborating group (Cancers). Causes of cancer in the world: comparative risk assessment of nine behavioural and environmental risk factors. Lancet. 366:1784–1793. 2005.
2	Siegel R, Ma J, Zou Z and Jemal A: Cancer statistics, 2014. CA Cancer J Clin. 64:9–29. 2014.
3	Correa P, Haenszel W, Cuello C, Tannenbaum S and Archer M: A model for gastric cancer epidemiology. Lancet. 2:58–60. 1975.
4	de Vries AC, van Grieken NC, Looman CW, Casparie MK, de Vries E, Meijer GA and Kuipers EJ: Gastric cancer risk in patients with premalignant gastric lesions: a nationwide cohort study in the Netherlands. Gastroenterology. 134:945–952. 2008.
5	Uemura N, Okamoto S, Yamamoto S, Matsumura N, Yamaguchi S, Yamakido M, Taniyama K, Sasaki N and Schlemper RJ: Helicobacter pylori infection and the development of gastric cancer. N Engl J Med. 345:784–789. 2001.
6	Naylor GM, Gotoda T, Dixon M, Shimoda T, Gatta L, Owen R, Tompkins D and Axon A: Why does Japan have a high incidence of gastric cancer? Comparison of gastritis between UK and Japanese patients. Gut. 55:1545–1552. 2006.
7	Kim N, Park RY, Cho SI, Lim SH, Lee KH, Lee W, Kang HM, Lee HS, Jung HC and Song IS: Helicobacter pylori infection and development of gastric cancer in Korea: long-term follow-up. J Clin Gastroenterol. 42:448–454. 2008.
8	Clouston AD: Timely topic: Premalignant lesions associated with adenocarcinoma of the upper gastrointestinal tract. Pathology. 33:271–277. 2001.
9	Dinis-Ribeiro M, Areia M, de Vries AC, Marcos-Pinto R, Monteiro-Soares M, O’Connor A, Pereira C, Pimentel-Nunes P, Correia R, Ensari A, et al: European Society of Gastrointestinal Endoscopy; European Helicobacter Study Group; European Society of Pathology; Sociedade Portuguesa de Endoscopia Digestiva: Management of precancerous conditions and lesions in the stomach (MAPS): guideline from the European Society of Gastrointestinal Endoscopy (ESGE), European Helicobacter Study Group (EHSG), European Society of Pathology (ESP), and the Sociedade Portuguesa de Endoscopia Digestiva (SPED). Endoscopy. 44:74–94. 2012.
10	Lv SX, Gan JH, Wang CC, Luo EP, Huang XP, Xie Y and Huang Y: Biopsy from the base of gastric ulcer may find gastric cancer earlier. Med Hypotheses. 76:249–250. 2011.
11	Molloy RM and Sonnenberg A: Relation between gastric cancer and previous peptic ulcer disease. Gut. 40:247–252. 1997.
12	Eidt S and Stolte M: Prevalence of intestinal metaplasia in Helicobacter pylori gastritis. Scand J Gastroenterol. 29:607–610. 1994.
13	Rugge M, Cassaro M, Di Mario F, Leo G, Leandro G, Russo VM, Pennelli G and Farinati F; Interdisciplinary Group on Gastric Epithelial Dysplasia (IGGED). The long term outcome of gastric non-invasive neoplasia. Gut. 52:1111–1116. 2003.
14	Bahmanyar S, Ye W, Dickman PW and Nyrén O: Long-term risk of gastric cancer by subsite in operated and unoperated patients hospitalized for peptic ulcer. Am J Gastroenterol. 102:1185–1191. 2007.
15	Ogura M, Yamaji Y, Hikiba Y, Maeda S, Matsumura M, Okano K, Sassa R, Yoshida H, Kawabe T and Omata M: Gastric cancer among peptic ulcer patients: retrospective, long-term follow-up. Dig Liver Dis. 38:811–814. 2006.
16	Wong BC, Ching CK, Lam SK, Li ZL, Chen BW, Li YN, Liu HJ, Liu JB, Wang BE, Yuan SZ, et al: Differential north to south gastric cancer-duodenal ulcer gradient in China. China Ulcer Study Group. J Gastroenterol Hepatol. 13:1050–1057. 1998.
17	Chen MJ, Wu DC, Ko YC and Chiou YY: Personal history and family history as a predictor of gastric cardiac adenocarcinoma risk: a case-control study in Taiwan. Am J Gastroenterol. 99:1250–1257. 2004.
18	Leung WK, Lin SR, Ching JY, To KF, Ng EK, Chan FK, Lau JY and Sung JJ: Factors predicting progression of gastric intestinal metaplasia: results of a randomised trial on Helicobacter pylori eradication. Gut. 53:1244–1249. 2004.
19	Chang CH, Wu MS, Chang YT, Chang MC, Shun CT, Liu CY and Lin JT: Risk factors for intestinal metaplasia in adult residents of Matzu: a cross-sectional study. J Formos Med Assoc. 101:835–840. 2002.
20	Malfertheiner P, Chan FK and McColl KE: Peptic ulcer disease. Lancet. 374:1449–1461. 2009.
21	Xia HH, Wong BC, Wong KW, Wong SY, Wong WM, Lai KC, Hu WH, Chan CK and Lam SK: Clinical and endoscopic characteristics of non-Helicobacter pylori, non-NSAID duodenal ulcers: a long-term prospective study. Aliment Pharmacol Ther. 15:1875–1882. 2001.
22	Dixon MF, Genta RM, Yardley JH and Correa P: Classification and grading of gastritis. The updated Sydney System International Workshop on the Histopathology of Gastritis, Houston 1994. Am J Surg Pathol. 20:1161–1181. 1996.
23	Yee YK, Wong KW, Hui CK, Chan CK, Chan AO, Lam SK, Fung FM, Hung I and Wong BC: Prevalence and time trend of intestinal metaplasia in Hong Kong. J Gastroenterol Hepatol. 24:896–899. 2009.
24	Ubukata H, Nagata H and Tabuchi T, Konishi S, Kasuga T and Tabuchi T: Why is the coexistence of gastric cancer and duodenal ulcer rare? Examination of factors related to both gastric cancer and duodenal ulcer. Gastric Cancer. 14:4–12. 2011.
25	Misdraji J and Lauwers GY: Gastric epithelial dysplasia. Semin Diagn Pathol. 19:20–30. 2002.
26	Correa P: Clinical implications of recent developments in gastric cancer pathology and epidemiology. Semin Oncol. 12:2–10. 1985.
27	You WC, Li JY, Blot WJ, Chang YS, Jin ML, Gail MH, Zhang L, Liu WD, Ma JL, Hu YR, et al: Evolution of precancerous lesions in a rural Chinese population at high risk of gastric cancer. Int J Cancer. 83:615–619. 1999.