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Song, J.H.;  Lee, Y.;  Heo, J.;  Son, S.;  Hur, H.;  Han, S. Secondary Primary Cancer after Primary Gastric Cancer. Encyclopedia. Available online: https://encyclopedia.pub/entry/40129 (accessed on 01 July 2024).
Song JH,  Lee Y,  Heo J,  Son S,  Hur H,  Han S. Secondary Primary Cancer after Primary Gastric Cancer. Encyclopedia. Available at: https://encyclopedia.pub/entry/40129. Accessed July 01, 2024.
Song, Jeong Ho, Yeonkyoung Lee, Jaesung Heo, Sang-Yong Son, Hoon Hur, Sang-Uk Han. "Secondary Primary Cancer after Primary Gastric Cancer" Encyclopedia, https://encyclopedia.pub/entry/40129 (accessed July 01, 2024).
Song, J.H.,  Lee, Y.,  Heo, J.,  Son, S.,  Hur, H., & Han, S. (2023, January 12). Secondary Primary Cancer after Primary Gastric Cancer. In Encyclopedia. https://encyclopedia.pub/entry/40129
Song, Jeong Ho, et al. "Secondary Primary Cancer after Primary Gastric Cancer." Encyclopedia. Web. 12 January, 2023.
Secondary Primary Cancer after Primary Gastric Cancer
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This entry is adapted from the peer-reviewed paper 10.3390/cancers14246165

Advances in cancer screening and early detection, as well as improvements in surgical techniques and therapeutics, have contributed to decreasing gastric cancer mortality. The number of gastric cancer survivors continues to rise; however, long-term follow-up has revealed an increase in the risk of post-gastrectomy symptoms or other health problems, such as extra-gastric secondary primary cancer (SPC), in these survivors. The characteristics of SPC are of increasing interest to both treatment providers and gastric cancer survivors.

gastric cancer secondary primary cancer

1. Introduction

Cancer research and advances in cancer treatment modalities have increased the rates of overall survival in cancer patients. After completion of cancer treatment, cancer survivors return to pre-treatment life, but their quality of life is not the same as before treatment. Patients face financial burden, psychological difficulty, work-related problems, and physiological changes in the body after organ resection [1]. Along with providing emotional support and explaining the disease to patients, health care providers should also be aware that secondary primary cancers (SPCs) can develop in cancer survivors.
In gastric cancer, the development of new chemotherapeutic agents and advances in surgical techniques have resulted in more survivors in recent decades [2][3][4][5][6]. In East Asian countries, the advent of national screening programs has resulted in more than half of all gastric cancer patients being diagnosed with early stage tumors, and their 5-year survival rate exceeds 90% [2][7][8]. SPCs affect the long-term survival of cancer survivors, and several national and institutional database studies have been published previously. 

2. Epidemiology of SPCs

Previous studies on the incidence of SPCs can be divided into two categories according to their scope, namely single institution- and nationwide population-based studies. Single institution-based studies with more than one thousand patients are summarized Table 1 [9][10][11][12][13][14][15][16][17][18][19]. Most studies on SPCs were performed in regions with a high prevalence of gastric cancer. The incidence of SPC in gastric cancer patient survivors varies between 1.0% and 6.6%. Synchronous tumors were defined as those with a time interval between SPC and gastric cancer diagnosis of less than 6 months, and metachronous tumors were defined as those with more than 6 months. The development of SPCs after gastric cancer mainly occurred within 2 years of diagnosis including synchronous tumor [15][17][18].
Table 1. List of single institutional-based studies on the incidence of secondary primary cancer (SPC) after gastric cancer.
Authors Country Publication Year Number of Patients Incidence of SPC Synchronous/
Metachronous		 Common SPCs
Takekuni K et al. [9] Japan 1999 1925 127 (6.6%) N/A Lung, liver, colorectum, esophagus, and pancreas
Dinis-Ribeiro M et al. [10] Portugal 2002 2268 78 (3.4%) 21/57 Colorectum, breast, uterus, urinary tract, and lymphoma
Ikeda Y et al. [11] Japan 2003 2250 95 (4.2%) 48/47 Colorectum, lung, liver, esophagus, and breast
Ikeda Y et al. [12] Japan 2005 1070 54 (5.0%) 0/54 Lung, colorectum, esophagus, breast, and liver
Park YK et al. [13] Korea 2005 2509 65 (2.6%) 17/48 Colorectum, breast, hepatobiliary, esophagus, and uterus
Lee JH et al. [14] Korea 2006 3291 111 (3.4%) 111/0 Colorectum, lung, esophagus, liver, and breast
Molinero M et al. [15] Spain 2006 1170 23 (1.96%) 11/12 Colorectum, multiple myeloma, prostate, lung, and kidney
Ha TK et al. [16] Korea 2007 10,090 96 (1.0%) 96/0 Colorectum, liver, kidney, pancreas and gallbladder
Eom BW et al. [17] Korea 2008 4593 159 (3.4%) 49/110 Colorectum, lung, liver, kidney, and lymphoma
Kim JY et al. [18] Korea 2012 5778 214 (3.70%) 0/214 Colorectum, lung, liver, ovary, and cervix
Kim C et al. [19] Korea 2013 3066 70 (2.5%) 32/38 Colorectum, lung, liver, gallbladder, and head and neck
SPC, secondary primary cancer; N/A, not applicable.
Nationwide population-based studies in Japan, Taiwan, United States of America, Portugal, and Sweden are available and listed in Table 2 [20][21][22][23][24]. The incidence of SPCs in patients with gastric cancer ranges from 4.4% to 5.5%. In most studies, the risk of SPC in patients with gastric cancer was estimated using standardized incidence ratio (SIR), which is defined as the number of observed cancer occurrences divided by the expected number. The expected number of cancers was calculated by multiplying the first primary cancer incidence by the person-years after first primary cancer diagnosis in the general population. The SIR for all SPCs in gastric cancer patients ranges from 0.91 to 1.46. The most common SPC site after gastric cancer is the gastrointestinal tract, such as esophagus, small intestine, and colon. Some studies showed increased incidences of SPCs in thyroid, pancreas, bone and soft tissues, ovaries, bladder, kidney, liver, and intrahepatic bile duct, and non-Hodgkin’s lymphoma. By contrast, the incidence of SPCs in lung, breast and prostate, melanoma, and myeloma decreased after a diagnosis of gastric cancer.
Table 2. List of nationwide population-based studies on the incidence of secondary primary cancer (SPC) after gastric cancer.
Country of Study Publication Year Number of Patients Statistical Significance SPC Site
Japan [20] 2014 174,477 3225 (1.8%) patients had SPC. SIR for all cancers, 1.09.
SIR for esophagus cancer, 1.70
SIR for colorectum cancer, 1.35
Taiwan [21] 2016 47,729 2110 (4.42%) patients had SPC.
SIR for all cancer, 1.46		 SIR for head and neck, 1.34.
SIR for esophagus, 2.16.
SIR for colon and rectum, 1.37.
SIR for bones and soft tissues, 1.95.
SIR for ovaries, 2.89.
SIR for bladder, 1.47.
SIR for kidneys, 1.44.
SIR for non-Hodgkin’s lymphoma, 5.56.
the United States [22] 2016 33,720 1838 (5.45%) patients had SPC with O/E ratio of 1.11. Gastrointestinal O/E ratio, 1.71.
Biliary O/E ratio, 1.30,
Pancreatic O/E ratio, 1.60.
Thyroid O/E ratio 2.00.
Portugal [23] 2017 7427 331 (4.5%) patients had SPC (26.9% synchronous and 73.1% metachronous).
10-year cumulative incidence of SPC, 4.8%
SIR for all cancer, 1.30 (male) and 1.20 (female)		 SIR for esophagus, 4.99 (male) and 8.03 (female).
SIR for small intestine, 11.04 (male) and 13.08 (female).
SIR for colon, 2.42 (male) and 2.58 (female).
SIR for non-Hodgkin’s lymphoma, 2.53 (male).
SIR for liver and intrahepatic bile duct, 5.18 (female).
Sweden [24] 2021 23,137 1042 (4.5%) patients had SPC. SIR for esophagus, 2.15.
SIR for small intestine, 4.12.
SIR for kidney, 1.62.
SPC, secondary primary cancer; O/E, observed/expected; SIR, Standardized incidence ratio.
In both men and women, the incidences of SPCs in the gastrointestinal tract and non-Hodgkin’s lymphoma after diagnosis of gastric cancer were high. In men, the incidence of SPCs were elevated in prostate and bladder, whereas in women, the incidences of SPCs were elevated in bone and soft tissue, ovaries, kidneys, liver and intrahepatic bile ducts. The incidence of SPCs in gastric cancer survivors was higher in men than in women [12][19][21][23].

3. Biology of SPCs

Several risk factors for gastric cancer have been documented, namely Helicobacter pylori infection, male sex, old age, low socioeconomic status, smoking, alcohol consumption, salted food intake, preserved food, genetic factors, and familial predisposition [25]. These factors often overlap with risk factors for other cancers.
Consumption of preserved foods increases the risk of gastric cancer, hepatocellular carcinoma, nasopharyngeal carcinoma breast cancer, and prostate cancer [26][27][28][29][30][31]. By contrast, low intake of vegetables is known to lead to gastric cancer, lung cancer, hepatocellular carcinoma, and nasopharyngeal cancer [25][32][33][34]. Smoking is the major risk factor for cancers at several sites, such as stomach, oropharynx, larynx, esophagus, and lung [25][35][36][37][38][39]. In a previous study, seven out of nine patients (77.7%) with SPCs after gastric cancer consumed tobacco [40]. A synergy between smoking and alcohol consumption was also identified as contributing to carcinogenesis [41][42].
Chemo/radiotherapy has been proposed to contribute to the development of SPCs. Treatments for the first malignancy may contribute to the development of SPCs by causing damage to specific regions of DNA, chromosomal rearrangements, or chromosome loss [43][44]. Some genetic factors have been found to be associated with the development of gastric and other cancers. Microsatellite instability is closely associated with gastric and sporadic colorectal carcinoma [45][46][47]. Lynch syndrome, an autosomal dominant inherited cancer predisposition syndrome, is a risk factor for tumors of gastric, colorectal, small bowel, gallbladder, and biliary tract, and is also associated with microsatellite instability [48][49][50]. In addition, several hereditary diseases, such as Li-Fraumeni syndrome, breast-ovarian cancer syndrome, multiple endocrine neoplasia, Peutz-Jegher syndrome, and Cowden syndrome, increase the risk of gastric and other cancers [40][51].

4. Predisposing Factors for SPCs

A Taiwanese population-based study employing multivariate logistic regression analysis demonstrated that age over 70 years, male sex, and comorbidities, such as diabetes mellitus, chronic obstructive pulmonary disease, and liver cirrhosis are risk factors for developing SPCs [21]. Several single institution-based studies found several risk factors for developing SPCs after gastric cancer, such as age over 60 years, differentiated histology, earlier stage gastric cancer, and multiplicity of lesions [14][19].

5. Prognosis of Patients with SPCs

The long-term outcomes of gastric cancer patients with SPCs have not been reported by national population-based studies. However, several single-institutional retrospective studies have reported the long-term survival outcomes of gastric cancer patients with SPCs. In a Korean study, the 5-year overall survival rate according to gastric cancer stage regardless of SPC site was as follows; 61% for stage I, 39% for stage II, 30% for stage III, and 0% for stage IV [16]. In studies comparing the survival outcomes of patients with and without SPCs, the 5-year survival rates of patients with SPCs were statistically poorer than those of patients without SPCs [18][19]. In addition, the 5-year survival rate of patients without SPCs was 76.5%, that of patients with metachronous SPC was 67.5%, and that of patients with synchronous SPC was 34.1%, which were statistically significant (p < 0.001 for metachronous SPC vs. no SPC and p < 0.001 for synchronous SPC vs. no SPC). In a Japanese study analyzing 10-year survival rates, the survival rate of patients with metachronous SPC was higher than that of patients without SPC or with synchronous SPC (75.2% for metachronous SPC; 69.3% for no SPC; and 40.1% for synchronous; p < 0.01) [11]. The 5-year survival of metachronous SPC patients was significantly superior to that of synchronous SPC patients in a Korean retrospective study (77.9% for metachronous SPC and 55.2% for synchronous SPC; p = 0.002) [17]. However, in a Spanish study, no significant differences in survival rates were found between patients with synchronous and those with metachronous SPC [15].

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Subjects: Gastroenterology & Hepatology
Contributors MDPI registered users' name will be linked to their SciProfiles pages. To register with us, please refer to https://encyclopedia.pub/register :
Jeong Ho Song
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Yeonkyoung Lee
,
Jaesung Heo
,
Sang-Yong Son
,
Hoon Hur
,
Sang-Uk Han
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Entry Collection: Gastrointestinal Disease
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Update Date: 13 Jan 2023
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