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Interaction between dietary potassium intake and TNF-α rs1800629 genetic polymorphism in gastric cancer risk: a case–control study conducted in Korea

Published online by Cambridge University Press:  09 December 2022

Tao Thi Tran ,
Madhawa Gunathilake ,
Jeonghee Lee ,
Il Ju Choi ,
Young-Il Kim  and
Jeongseon Kim Open the ORCID record for Jeongseon Kim [Opens in a new window]
Tao Thi Tran
Affiliation:
Department of Cancer Control and Population Health, Graduate School of Cancer Science and Policy, Goyang-si, Gyeonggi-do, Republic of Korea
Madhawa Gunathilake
Affiliation:
Department of Cancer Biomedical Science, Graduate School of Cancer Science and Policy, Goyang-si, Gyeonggi-do, Republic of Korea
Jeonghee Lee
Affiliation:
Department of Cancer Biomedical Science, Graduate School of Cancer Science and Policy, Goyang-si, Gyeonggi-do, Republic of Korea
Il Ju Choi
Affiliation:
Center for Gastric Cancer, National Cancer Center Hospital, National Cancer Center, Goyang-si, Gyeonggi-do, Republic of Korea
Young-Il Kim
Affiliation:
Center for Gastric Cancer, National Cancer Center Hospital, National Cancer Center, Goyang-si, Gyeonggi-do, Republic of Korea
Jeongseon Kim*
Affiliation:
Department of Cancer Biomedical Science, Graduate School of Cancer Science and Policy, Goyang-si, Gyeonggi-do, Republic of Korea
*
*Corresponding author: Jeongseon Kim, email jskim@ncc.re.kr
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Abstract

Mineral consumption has been suggested to have an impact on gastric cancer (GC) prevention. However, the protective effect of potassium against gastric carcinogenesis remains inconclusive. The causal link between inflammation and cancer is well established. Notably, potassium intake and potassium channels may play certain roles in regulating the production of TNF-α (TNF-α). We aimed to determine whether dietary potassium intake is related to the risk of GC. We further observed whether this association was modified by TNF-α rs1800629. We designed a case–control study comprising 377 GC cases and 756 controls. Information on dietary potassium intake was collected using a semiquantitative food frequency questionnaire. Genotyping was performed by the Affymetrix Axiom Exom 319 Array platform. Unconditional logistic regression models were used to assess associations. A significantly reduced GC risk was found for those who consumed higher dietary potassium levels (OR = 0·63, 95 % CI = 0·45, 0·89, P for trend = 0·009). In the dominant model, we observed a non-significant association between TNF-α rs1800629 and GC risk (OR = 1·01, 95 % CI = 0·68, 1·49). In females, those who were homozygous for the major allele (G) of rs1800629 with a higher intake of dietary potassium exhibited a decreased risk of GC (OR = 0·40, 95 % CI = 0·20, 0·78, P interaction = 0·041). This finding emphasises the beneficial effect of potassium intake on GC prevention. However, this association could be modified by TNF-α rs1800629 genotypes. A greater protective effect was exhibited for females with GG homozygotes and high potassium intake.

Keywords

PotassiumTNF-α rs1800629Gastric cancerCase–control study
Type
Research Article
Information
British Journal of Nutrition , Volume 130 , Issue 5 , 14 September 2023 , pp. 887 - 894
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Copyright
© The Author(s), 2022. Published by Cambridge University Press on behalf of The Nutrition Society

According to data from 2020, gastric cancer (GC) is responsible for the fifth and fourth greatest incidence and mortality rates worldwide, respectively(Reference Sung, Ferlay and Siegel1). The prevalence rate of GC varies geographically(Reference Katoh and Ishikawa2). The highest incidence rate of GC was recorded in East Asia(Reference Katoh and Ishikawa2,Reference Rahman, Asombang and Ibdah3) . Although South Korea has experienced a decreasing trend in incidence and mortality since 1999(Reference Hong, Won and Lee4), GC remains a significant concern.

Several studies have been conducted to explore various risk factors associated with GC development(Reference Yusefi, Bagheri Lankarani and Bastani5). Although infection with Helicobacter pylori (H. pylori) has been well recognised in relation to GC progression, the role of other risk factors in the aetiology of GC still needs to be determined(6). A healthy diet is indicated to be a key source of important vitamins and minerals, and its importance has drawn much attention in recent years(Reference Richa and Sageena7).

Previous epidemiological studies documented that minerals may have certain roles in GC pathogenesis. For example, sodium consumption has a detrimental effect on GC even with the intake of intermediate levels(Reference Pelucchi, Tramacere and Bertuccio8). A higher haem iron intake was reported to be associated with an elevated GC risk, whereas non-haeme iron was suggested to be a protective factor against GC risk(Reference Tran, Gunathilake and Lee9). A beneficial effect against gastric carcinogenesis was also found for Ca and Mg(Reference Shah, Dai and Zhu10).

Potassium is an essential mineral that is mainly derived from dietary sources such as fruits, vegetables, beans and lentils. The Western diet is a consequence of the global spread of the Western lifestyle, which is characterised by low fruit and vegetable consumption and high processed food consumption. Consequently, there is an imbalance in Na and K intake, where high Na and low K intake have been reported(Reference Weaver11). To date, few studies have been conducted to elucidate the link between low potassium consumption and cancer. Potassium intake was found to be a preventive nutrient for colorectal cancer(Reference Kune, Kune and Watson12,Reference Meng, Sun and Yu13) . Similarly, an appropriate potassium intake served as a protective factor against lung cancer risk(Reference You, Zhang and He14). In contrast, available evidence regarding a protective effect of potassium against other cancers is limited, and GC is no exception. To the best of our knowledge, only one study has been conducted to explore the association of potassium with GC. However, a non-significant association was observed(Reference Pelucchi, Tramacere and Bertuccio8), whereas potassium was suggested to have a preventive effect on GC development by a nutrition survey(Reference Correa, Cuello and Fajardo15). Thus, there is a paucity of evidence related to the relationship of potassium intake with GC risk. In addition to dietary factors such as dietary potassium intake, it is necessary to focus on inflammation-related factors that are strongly related to gastric carcinogenesis.

It has been reported that there are positive correlations between inflammatory cytokines specifically in individuals with H. pylori infection and GC risk(Reference Bockerstett and DiPaolo16). TNF-α is one of the proinflammatory cytokines that stimulates other cytokines and mediates the cytokine cascade causing inflammation(Reference Khan, Mandal and Jawed17). There is a causal association between the production of TNF-α and cancer tumorigenesis(Reference Oshima, Ishikawa and Yoshida18). The regulation of TNF-α production occurs at the level of transcription, and polymorphisms in the TNF-α promoter region are indicated in relation to TNF-α production(Reference Li, Wang and Gu19). The association between TNF-α promoter polymorphisms and GC risk was indicated in a previous meta-analysis(Reference Xu, Kong and Zhao20). One of the TNF-α promoter polymorphisms is the G (guanine) > A (adenine) (rs1800629) SNP located at position -308, which is associated with TNF-α production(Reference Li, Wang and Gu19). In detail, a higher transcriptional activity was observed for the A allele compared to the G allele(Reference Wilson, Symons and McDowell21,Reference Kroeger, Carville and Abraham22) . For example, in comparison with the presence of the G allele at -308 of the TNF-α promoter, the presence of the A allele increased the transcriptional level twofold(Reference Kroeger, Carville and Abraham22). Notably, a previous study emphasised that TNF-α production may be regulated by potassium (K+) and K+ channels by activated human culture-derived macrophages(Reference Qiu, Campbell and Breit23). Furthermore, differences in genetic variants and dietary patterns may account for different GC risks among individuals. Thus, the discrepancy in GC susceptibility may be explained by the interaction between genes and diet(Reference Kim, Cho and Choi24). Based on this biological mechanism, we hypothesised that there may be an interaction between dietary potassium intake and TNF-α rs1800629 in gastric carcinogenesis.

To our knowledge, the potential effect of dietary potassium intake on gastric carcinogenesis has been reported in a few previous studies, and the findings have been ambiguous. Additionally, an interactive effect between potassium intake and TNF-α rs1800629 on gastric carcinogenesis has not been investigated thus far. Therefore, we aimed to examine whether potassium intake is related to GC risk. Moreover, we wanted to observe whether the TNF-α rs1800629 SNP modifies this association.

Materials and methods

Study population

We recruited participants from the National Cancer Center (NCC) Hospital in Korea between March 2011 and December 2014 to conduct a case–control study. The details of participant recruitment are described elsewhere(Reference Kim, Lee and Choi25,Reference Hoang, Lee and Choi26) . Cases were identified as those who were diagnosed with GC within 3 months preceding enrollment, except participants with chronic diseases and who were pregnant or breastfeeding. Subjects without a history of cancer or chronic diseases who visited the Cancer Prevention and Detection Center in NCC for health-screening examinations were identified as controls. We used age (±5 years) and sex to match controls and cases at a ratio of 2:1. A total of 756 controls and 377 cases with available information on genotypes were included for analysis in our study. This study was conducted according to the guidelines laid down in the Declaration of Helsinki, and all procedures involving research study participants were approved by the Institutional Review Board of the National Cancer Center Korea (IRB No. NCC2021–0181). Written informed consent was obtained from all subjects/patients.

Data collection

The assessment of dietary intake of participants within 12 months prior to the interview was performed with a 106-item semiquantitative FFQ. The semiquantitative FFQ has been reported to be valid and reliable(Reference Ahn, Kwon and Shim27) and contains nine categories for food consumption frequency and three categories for portion size. Total energy and potassium intake were determined by using a Computer Aided Nutritional analysis program (CAN-PRO 5·0, Korean Nutrition Society). Dietary potassium (mg/d) for each participant was calculated by summing the amount of potassium obtained from consumed foods. Additionally, information on demographics and lifestyle was collected using a self-administered questionnaire.

Genotype identification

Detailed information on the genotyping and quality control steps is mentioned elsewhere(Reference Yang, Park and Lee28,Reference Park, Yang and Lee29) . Briefly, we used peripheral blood to extract genomic DNA. Genotyping was performed using the Affymetrix Axiom Exom 319 Array (Afymetrix Inc.) platform with 318 983 variants. Genotype imputation was performed using the Asian population (n 504) in the 1000 Genome haplotypes phase III integrated variant set release GRch37/hg19 (https://www.1000genomes.org/) as a reference panel. Genetic markers with deviation from Hardy–Weinberg equilibrium P values <1 × 10−10, a minor allele frequency < 0·05, and a low call rate (< 98 %) were discarded. We used SHAPEIT (v2.r837) for phasing and IMPUTE2 (2·3·2) for SNP imputation. After filtering for an INFO score over 0·6, quality control criteria were applied. Finally, TNF-α rs1800629 was selected as a candidate SNP for the analysis of our study.

Statistical analyses

Potassium intake was energy-adjusted using the residual method(Reference Hoang, Lee and Choi26). We used the distribution of controls to classify potassium intake into tertiles. The comparison of general characteristics of cases with controls was performed by using the χ2 test and t test for categorical and continuous variables, respectively. The calculation of OR and 95 % CIs was based on unconditional logistic regression models. The lowest tertile was considered the reference group. Furthermore, we determined the dose–response relationships of intake of dietary potassium in relation to GC risk by using the median value of each tertile of potassium intake to identify a test for trend. We used a dominant model to analyse genetic association. We used tertile categories of potassium intake to examine the impact of the interaction between dietary potassium intake and TNF-α rs1800629 on GC risk. Statistical interaction was determined using a likelihood ratio test of models with and without the interaction term (potassium ×SNP). SAS software (version 9.4, SAS Institute) was used for all statistical analyses, and a two-sided P value less than 0·05 was considered significant.

Results

Demographic characteristics of the study participants

In comparison with healthy individuals, GC patients were more likely to be infected with H. pylori, and a high proportion of patients were current smokers (92·6 % v. 61·4 % and 30·8 % v. 20·4 %, P < 0·001, respectively). Similarly, they exhibited a higher rate of first-degree family history of GC (20·4 % v. 12·6 %, P < 0·001). In contrast, lower proportions of physical activity, level of education, income and occupation were observed in cases than those in controls (36·1 % v. 56·1 %, 23·1 % v. 51·8 %, 23·3 % v. 32·7 % and 17·2 % v. 19·0 %, respectively, P < 0·001). GC cases consumed significantly lower amounts of dietary potassium than controls (P < 0·001) (Table 1).

Table 1. General characteristics of the study participants

* χ2 test for categorical variables and t test for continuous variables were applied.

Mean ± sd was presented for continuous variables.

Potassium intake and GC risk

In comparison with subjects in the low tertile group of potassium intake, subjects in the high tertile group showed a lower GC risk. This significant association was observed in both the univariate model and model adjusted for possible confounders; OR (95 % CI) were 0·56 (0·41, 0·77), P for trend < 0·001 and 0·63 (0·45, 0·89), P for trend = 0·009, respectively. Importantly, the significant inverse associations between dietary potassium intake and GC risk remained for both male (OR = 0·65 (0·42, 0·99), P for trend = 0·042) and female (OR = 0·54 (0·29, 0·99), P for trend = 0·048) populations in the fully adjusted model (Table 2).

Table 2. Association of tertiles of dietary potassium intake with GC risk

GC, gastric cancer.

Model 1: unadjusted model; Model 2: adjusted for age, BMI, first-degree family history of GC, smoking status, alcohol consumption, regular exercise and marital status; Model 3: additionally adjusted for H. pylori infection. In the total subjects, models 2 and 3 were additionally adjusted for sex.

Associations of the TNF-α rs1800629 polymorphism with GC risk

The three genotypes of TNF-α rs1800629 were GG, AG and AA and were in Hardy–Weinberg equilibrium (P = 0·077). A dominant model of the TNF-α rs1800629 SNP was used to examine its association with GC risk. We observed a non-significant association of TNF-α rs1800629 with gastric carcinogenesis. The OR (95 % CI) in the unadjusted and adjusted models were 0·98 (0·68, 1·41) and 1·01 (0·68, 1·49), respectively. Non-significant associations were also observed for both sexes; OR (95 % CI) were 1·19 (0·74, 1·92) and 0·73 (0·36, 1·49) for males and females, respectively (Table 3).

Table 3. TNF rs1800629 genetic polymorphisms and risk of GC in the dominant model

GC, gastric cancer.

Model 1: unadjusted model; Model 2: adjusted for age, BMI, first-degree family history of GC, smoking status, alcohol consumption, regular exercise and marital status; Model 3: additionally adjusted for H. pylori infection. In the total subjects, models 2 and 3 were additionally adjusted for sex.

The interactive effect of the TNF-α rs1800629 polymorphism and potassium intake on gastric carcinogenesis

Table 4 presents the interactive effect of the TNF-α rs1800629 genetic polymorphism and potassium intake on gastric carcinogenesis. High potassium intake was found to be inversely associated with GC risk among subjects who carried the homozygous wild-type allele (GG) regardless of confounding adjustment (Model 3: OR = 0·63 (95 % CI: 0·43, 0·91)). Based on the sex stratification, this preventive effect seemed to be limited to females (OR = 0·40 (95 % CI: 0·20, 0·78)) with a significant interaction (P interaction = 0·041).

Table 4. Interactive effect of the TNF-α rs1800629 polymorphism and potassium intake on gastric carcinogenesis

Model 1: unadjusted model; Model 2: adjusted for age, BMI, first-degree family history of GC, smoking status, alcohol consumption, regular exercise and marital status; Model 3: additionally adjusted for H. pylori infection. In the total subjects, models 2 and 3 were additionally adjusted for sex.

OR, odds ratio; CI, confidence interval.

Discussion

In the present case–control study, we observed a negative association between potassium intake and GC risk. Additionally, TNF-α genetic polymorphism was observed to have an effect modification on this association. In detail, a protective effect of potassium against GC seemed to be greater in subjects who had higher potassium intake and carried the TNF-α rs1800629 homozygous wild-type allele (GG), especially among females.

The effect of a diet high in potassium on cancer prevention was investigated in some previous studies. Existing evidence supports the hypothesis that high potassium intake may contribute to reducing cancer risk. For example, a protective effect of potassium against lung cancer was emphasised in a study of 165 409 participants from the Prostate, Lung, Colorectal and Ovarian Cancer Screening trial and the Women’s Health Initiative(Reference You, Zhang and He14). Another study indicated that high potassium intake may be considered a preventative factor for colorectal cancer occurrence(Reference Kune, Kune and Watson12). The aforementioned association was reinforced by a conclusion drawn from a meta-analysis of twenty-nine studies(Reference Meng, Sun and Yu13).

To date, available evidence indicating the role of potassium in GC prevention is limited. There was only a case–control study conducted to explore the potential effect of potassium on GC risk and found a non-significant association(Reference Pelucchi, Tramacere and Bertuccio8). In contrast, high potassium intake was suggested to have a preventive effect on GC development in our study. This is in agreement with a previous nutrition survey(Reference Correa, Cuello and Fajardo15). Consistent findings were also observed in an in vivo study, which reported that the incidence of GC was reduced significantly due to prolonged oral treatment with potassium(Reference Tatsuta, Iishi and Baba30). The possible biological mechanisms underlying this association may be proposed. First, intracellular ions and potassium can be released into the extracellular fluid by tumour necrosis. T-cell receptor-driven Akt-mTOR phosphorylation and effector programs may be impaired by an increase in intracellular potassium within T cells due to increased extracellular potassium. As a result, T-cell effector function is suppressed. Neoantigens, which are generated and recognised by tumour cells and T cells, respectively, and cancerous cells may be killed by T cells. In addition, T cells may produce chemicals that play a role in the regulation of immunity and protective effects against tumours(Reference You, Zhang and He14). Second, the effect of potassium on GC prevention may be linked to gastric acid secretion. Gastric acid is known to be associated with gastric carcinogenesis(Reference Tatsuta, Iishi and Baba30). It is important to note that potassium ions have a critical role in activating and catalysing gastric H+, K+-ATPase, leading to the secretion of acid(Reference Geibel31). Third, potassium may serve as an anti-tumour agent because it is essential for folding and stabilising G-quadruplexes(Reference Frajese, Benvenuto and Fantini32). Fourth, pancreatic cells need potassium to secrete insulin. As a result, hypokalaemia may lead to impaired insulin secretion and glucose intolerance(Reference Stone, Martyn and Weaver33). A higher risk of diabetes can be attributable to lower potassium intake, which was well recognised in previous studies(Reference Colditz, Manson and Stampfer34,Reference Chatterjee, Colangelo and Yeh35) . Notably, epidemiological studies are robust enough to support the causal link between diabetes and GC occurrence(Reference Lai, Park and Hartge36Reference Tran, Lee and Gunathilake38). Thus, it has been established that diabetes may be a mediator for the link between low potassium intake and increased GC progression.

H. pylori is known to be an aetiology for gastric carcinogenesis. H. pylori and host genetic factors impact the inflammatory response and epithelial cell physiology and increase GC risk(Reference Zheng, Zhang and Zhang39). The TNF-α gene is a major cytokine related to H. pylori infection(Reference Yang, Ko and Cho40). It is reported to be related to chronic inflammation, autoimmunity, tumour progression and metastasis(Reference Cui, Zhang and An41). The role of TNF-α has been indicated to be associated with not only polymorphisms in the genes in relation to regulation of TNF-α production and effect but also polymorphisms in TNF itself(Reference El-Tahan, Ghoneim and El-Mashad42). TNF-α promoter polymorphisms were documented to affect the expression of this gene and are associated with GC susceptibility(Reference Zheng, Zhang and Zhang39). One of the TNF-α promoter polymorphisms is the G (guanine) > A (adenine) (rs1800629) polymorphism, which suggests an impact on the TNF-α level and susceptibility to GC(Reference Li, Wang and Gu19). However, the detrimental effect of TNF-α rs1800629 on GC development is still controversial. It was considered a potential contributor to gastric tumorigenesis and was associated with H. pylori infection in a previous study(Reference Zheng, Zhang and Zhang39). However, a significant association was limited to Caucasians, and a non-significant association was found for East Asians(Reference Li, Wang and Gu19). We found a similar association between TNF-α rs1800629 and GC risk, which is in agreement with a previous study in Korea(Reference Yang, Ko and Cho40).

TNF-α production is associated with cancer progression(Reference Oshima, Ishikawa and Yoshida18). Promoter polymorphisms were indicated in relation to elevated TNF-α production(Reference Li, Wang and Gu19). Macrophages are known to play an important role in immunity and inflammation due to bioactive molecule secretion. A previous study suggested certain roles of K+ and K+ channels in the regulation of TNF-α production by activated human culture-derived macrophages(Reference Qiu, Campbell and Breit23). Thus, we hypothesised that there is an interactive effect of potassium intake with TNF-α rs1800629 on GC carcinogenesis. Our findings suggest a difference in the protective effect of potassium against gastric carcinogenesis according to host genetic factors. A significant effect seems to be observed in those carrying the homozygous wild-type allele of TNF-α rs1800629 (GG). Importantly, a biological interaction between potassium intake and TNF-α rs1800629 was found in our study. Possible mechanisms for the interaction may be explained as follows. Potassium was indicated to regulate TNF-α production. In detail, phorbol myristate acetate-induced cytokine production may be inhibited by the effect of blockade of K+ channels through mechanisms regarding translation or post-translation. This effect is duplicated with an increase in extracellular K+(Reference Qiu, Campbell and Breit23). Additionally, potassium plays a role in TNF-induced apoptosis and gene induction. TNF receptor triggering leads to reduced intracellular spermine, which impacts the activity of potassium channels and intracellular potassium concentrations, enhances the activity of caspases and increases cell death(Reference Penning, Denecker and Vercammen43). Another possible mechanism can be proposed. Potassium cyanate is thought to induce apoptosis in colorectal cancer cell lines. Notably, potassium cyanate is a mediator of TNF-α release in these cells via activation of nuclear factor kappa B(Reference Yang and Chang44). Overall, our study suggests a biological interaction between potassium intake and TNF-α rs1800629. However, a significant interaction was found only for females. Higher expression of inflammatory genes was observed in females than in males due to sex hormones(Reference Klein and Flanagan45). Thus, different eating habits and sex hormones may account for the difference in the interactive effect between males and females(Reference Kim, Lee and Choi46). This interaction should be elucidated in further studies.

This study is one of few studies aiming to determine the protective effect of high potassium intake on the progression of GC. Importantly, our study represents the first attempt to demonstrate an impact of an interactive effect between potassium intake and genetic polymorphisms in proinflammatory genes on GC risk. Additionally, we used a validated and reliable semiquantitative FFQ to collect information on nutrient intake. Information on general characteristics, especially possible confounders, was collected by trained personnel. As a consequence, the quality of our data was relatively higher. Although the associations for subtypes of GC were not assessed in our study due to the limited number of cases, cases in our study well reflect the trend in Asia, where the majority of cases are non-cardia GC(6). Furthermore, the statistical power of genotype associations may be affected by the small number of variant allele carriers. Although we tried to tackle case–control study-related limitations, selection bias and recall bias may occur. Finally, although there would be a possibility to have effect from other genes, except TNF-α, that might be helpful in reaching an effective conclusion. However, we did not consider the effect from other probable genes or combinations of genes in our current study.

In conclusion, our study emphasised a protective effect of high potassium intake against GC carcinogenesis. Additionally, we drew a concept regarding an interaction between dietary potassium intake and TNF-α rs1800629. In detail, the preventative effect of potassium depended on the individual’s genetic background. A greater effect seems to be exhibited for TNF-α rs1800629 homozygous wild-type allele carriers, especially females. This evidence suggests that we should consider individual genotypes to develop strategies for GC prevention.

Acknowledgements

This work was supported by International Cooperation & Education Program (NCCRI NCCI 52 210–52 211, 2020) of National Cancer Center, Korea and grants from National Cancer Center, Korea (1 910 330) and National Research Foundation of Korea (2021R1A2C2008439).

Formal analysis, T. T. T., J. L.; Preparation of original draft, T. T. T.; Writing review and editing, M. G., J. K.; Data curation, I. J. C., Y-I. K., J. K.; Investigation, I. J. C. and Y-I. K.; Methodology, I. J. C., Y-I. K. and J. K.; Funding acquisition, J. K.; Project administration, J. K.; Supervision, J. K. All authors have critically reviewed and approved the final version of the manuscript submitted for publication.

The authors declare that they have no conflicts of interests.

References

Sung, H, Ferlay, J, Siegel, RL, et al. (2021) Global cancer statistics 2020: GLOBOCAN estimates of incidence and mortality worldwide for 36 cancers in 185 countries. CA Cancer J Clin 71, 209249.CrossRefGoogle ScholarPubMed
Katoh, H & Ishikawa, S (2021) Lifestyles, genetics, and future perspectives on gastric cancer in East Asian populations. J Hum Genet 66, 887899.10.1038/s10038-021-00960-8CrossRefGoogle ScholarPubMed
Rahman, R, Asombang, AW & Ibdah, JA (2014) Characteristics of gastric cancer in Asia. World J Gastroenterol 20, 44834490.CrossRefGoogle ScholarPubMed
Hong, S, Won, YJ, Lee, JJ, et al. (2021) Cancer statistics in Korea: incidence, mortality, survival, and prevalence in 2018. Cancer Res Treat 53, 301315.CrossRefGoogle ScholarPubMed
Yusefi, AR, Bagheri Lankarani, K, Bastani, P, et al. (2018) Risk factors for gastric cancer: a systematic review. Asian Pac J Cancer Prev 19, 591603.Google ScholarPubMed
World Cancer Research Fund/American Institute for Cancer Research (2018) Report, C. U. P. E. Diet, Nutrition, Physical Activity and Stomach Cancer. https://www.wcrf.org/diet-and-cancer/ (accessed May 2022).Google Scholar
Richa, SN & Sageena, G (2022) Dietary factors associated with gastric cancer – a review. Transl Med Commun 7, 7.CrossRefGoogle Scholar
Pelucchi, C, Tramacere, I, Bertuccio, P, et al. (2009) Dietary intake of selected micronutrients and gastric cancer risk: an Italian case-control study. Ann Oncol 20, 160165.CrossRefGoogle ScholarPubMed
Tran, TT, Gunathilake, M, Lee, J, et al. (2021) The associations of dietary iron intake and the Transferrin Receptor (TFRC) rs9846149 polymorphism with the risk of gastric cancer: a case-control study conducted in Korea. Nutrients 13, 2600.CrossRefGoogle ScholarPubMed
Shah, SC, Dai, Q, Zhu, X, et al. (2020) Associations between calcium and magnesium intake and the risk of incident gastric cancer: a prospective cohort analysis of the National Institutes of Health-American Association of Retired Persons (NIH-AARP) Diet and Health Study. Int J Cancer 146, 29993010.CrossRefGoogle ScholarPubMed
Weaver, CM (2013) Potassium and health. Adv Nutr 4, 368s377s.10.3945/an.112.003533CrossRefGoogle ScholarPubMed
Kune, GA, Kune, S & Watson, LF (1989) Dietary sodium and potassium intake and colorectal cancer risk. Nutr Cancer 12, 351359.10.1080/01635588909514036CrossRefGoogle ScholarPubMed
Meng, Y, Sun, J, Yu, J, et al. (2019) Dietary intakes of calcium, iron, magnesium, and potassium elements and the risk of colorectal cancer: a meta-analysis. Biol Trace Elem Res 189, 325335.CrossRefGoogle ScholarPubMed
You, D, Zhang, M, He, W, et al. (2021) Association between dietary sodium, potassium intake and lung cancer risk: evidence from the prostate, lung, colorectal and ovarian cancer screening trial and the Women’s Health Initiative. Transl Lung Can Res 10, 4556.CrossRefGoogle ScholarPubMed
Correa, P, Cuello, C, Fajardo, LF, et al. (1983) Diet and gastric cancer: nutrition survey in a high-risk area. J Natl Cancer Inst 70, 673678.Google Scholar
Bockerstett, KA & DiPaolo, RJ (2017) Regulation of gastric carcinogenesis by inflammatory cytokines. Cell Mol Gastroenterol Hepatol 4, 4753.CrossRefGoogle ScholarPubMed
Khan, S, Mandal, RK, Jawed, A, et al. (2016) TNF-α -308 G > A (rs1800629) polymorphism is associated with Celiac disease: a meta-analysis of 11 case-control studies. Sci Rep 6, 32677.CrossRefGoogle Scholar
Oshima, H, Ishikawa, T, Yoshida, GJ, et al. (2014) TNF-α/TNFR1 signaling promotes gastric tumorigenesis through induction of Noxo1 and Gna14 in tumor cells. Oncogene 33, 38203829.10.1038/onc.2013.356CrossRefGoogle ScholarPubMed
Li, M, Wang, Y & Gu, Y (2014) Quantitative assessment of the influence of tumor necrosis factorα polymorphism with gastritis and gastric cancer risk. Tumour Biol 35, 14951502.10.1007/s13277-013-1206-0CrossRefGoogle Scholar
Xu, T, Kong, Z & Zhao, H (2018) Relationship between tumor necrosis factor-α rs361525 polymorphism and gastric cancer risk: a meta-analysis. Front Physiol 9, 469.CrossRefGoogle ScholarPubMed
Wilson, AG, Symons, JA, McDowell, TL, et al. (1997) Effects of a polymorphism in the human tumor necrosis factorα promoter on transcriptional activation. Proc Natl Acad Sci USA 94, 31953199.10.1073/pnas.94.7.3195CrossRefGoogle Scholar
Kroeger, KM, Carville, KS & Abraham, LJ (1997) The -308 tumor necrosis factor- α promoter polymorphism effects transcription. Mol Immunol 34, 391399.CrossRefGoogle ScholarPubMed
Qiu, MR, Campbell, TJ & Breit, SN (2002) A potassium ion channel is involved in cytokine production by activated human macrophages. Clin Exp Immunol 130, 6774.CrossRefGoogle ScholarPubMed
Kim, J, Cho, YA, Choi, WJ, et al. (2014) Gene–diet interactions in gastric cancer risk: a systematic review. World journal of gastroenterology. World J Gastroenterol 20, 96009610.10.3748/wjg.v20.i28.9600CrossRefGoogle Scholar
Kim, JH, Lee, J, Choi, IJ, et al. (2018) Dietary carotenoids intake and the risk of gastric cancer:a case-control study in Korea. Nutrients 10, 1031.CrossRefGoogle ScholarPubMed
Hoang, BV, Lee, J, Choi, IJ, et al. (2016) Effect of dietary vitamin C on gastric cancer risk in the Korean population. World J Gastroenterol 22, 62576267.CrossRefGoogle ScholarPubMed
Ahn, Y, Kwon, E, Shim, JE, et al. (2007) Validation and reproducibility of food frequency questionnaire for Korean genome epidemiologic study. Eur J Clin Nutr 61, 14351441.CrossRefGoogle ScholarPubMed
Yang, S, Park, Y, Lee, J, et al. (2017) Effects of soy product intake and interleukin genetic polymorphisms on early gastric cancer risk in Korea: a case-control study. Cancer Res Treat 49, 10441056.CrossRefGoogle ScholarPubMed
Park, B, Yang, S, Lee, J, et al. (2019) Genome-wide association of genetic variation in the PSCA Gene with gastric cancer susceptibility in a Korean population. Cancer Res Treat 51, 748757.10.4143/crt.2018.162CrossRefGoogle Scholar
Tatsuta, M, Iishi, H, Baba, M, et al. (1991) Protective effect by potassium chloride against gastric carcinogenesis induced by N-methyl-N'-nitro-N-nitrosoguanidine in spontaneously hypertensive rats. Jpn J Cancer Res 82, 280285.CrossRefGoogle ScholarPubMed
Geibel, JP (2005) Role of potassium in acid secretion. World J Gastroenterol 11, 52595265.10.3748/wjg.v11.i34.5259CrossRefGoogle ScholarPubMed
Frajese, GV, Benvenuto, M, Fantini, M, et al. (2016) Potassium increases the antitumor effects of ascorbic acid in breast cancer cell lines in vitro . Oncol Lett 11, 42244234.10.3892/ol.2016.4506CrossRefGoogle ScholarPubMed
Stone, MS, Martyn, L & Weaver, CM (2016). Potassium intake, bioavailability, hypertension, and glucose control. Nutrients 8, 444.10.3390/nu8070444CrossRefGoogle ScholarPubMed
Colditz, GA, Manson, JE, Stampfer, MJ, et al. (1992) Diet and risk of clinical diabetes in women. Am J Clin Nutr 55, 10181023.CrossRefGoogle ScholarPubMed
Chatterjee, R, Colangelo, LA, Yeh, HC, et al. (2012) Potassium intake and risk of incident type 2 diabetes mellitus: the coronary artery risk development in young adults (CARDIA) study. Diabetologia 55, 12951303.10.1007/s00125-012-2487-3CrossRefGoogle ScholarPubMed
Lai, GY, Park, Y, Hartge, P, et al. (2013) The association between self-reported diabetes and cancer incidence in the NIH-AARP Diet and Health study. J Clin Endocrinol Metab 98, E497502.10.1210/jc.2012-3335CrossRefGoogle ScholarPubMed
Lindkvist, B, Almquist, M, Bjørge, T, et al. (2013) Prospective cohort study of metabolic risk factors and gastric adenocarcinoma risk in the Metabolic Syndrome and Cancer Project (Me-Can). Cancer Causes Control 24, 107116.CrossRefGoogle ScholarPubMed
Tran, TT, Lee, J, Gunathilake, M, et al. (2022) Influence of fasting glucose level on gastric cancer incidence in a prospective cohort study. Cancer Epidemiol Biomarkers Prev 31, 254261.10.1158/1055-9965.EPI-21-0670CrossRefGoogle ScholarPubMed
Zheng, W, Zhang, S, Zhang, S, et al. (2017) The relationship between tumor necrosis factor-α polymorphisms and gastric cancer risk: an updated meta-analysis. Biomed Rep 7, 133142.10.3892/br.2017.934CrossRefGoogle ScholarPubMed
Yang, JJ, Ko, KP, Cho, LY, et al. (2009) The role of TNF genetic variants and the interaction with cigarette smoking for gastric cancer risk: a nested case-control study. BMC Cancer 9, 238.CrossRefGoogle Scholar
Cui, X, Zhang, H, An, Cao, et al. (2020) Cytokine TNF-α promotes invasion and metastasis of gastric cancer by down-regulating Pentraxin3. J Cancer 11, 18001807.10.7150/jca.39562CrossRefGoogle ScholarPubMed
El-Tahan, RR, Ghoneim, AM & El-Mashad, N (2016) TNF-α gene polymorphisms and expression. SpringerPlus 5, 1508.CrossRefGoogle ScholarPubMed
Penning, LC, Denecker, G, Vercammen, D, et al. (2000) A role for potassium in TNF-induced apoptosis and gene-induction in human and rodent tumour cell lines. Cytokine 12, 747750.CrossRefGoogle ScholarPubMed
Yang, EJ & Chang, JH (2014) TNF-α regulates potassium cyanate-induced apoptosis via NF-κB activation in HCT 116 cells. Biomed Sci 20, 3238.Google Scholar
Klein, SL & Flanagan, KL (2016). Sex differences in immune responses. Nat Rev Immunol 16, 626638.10.1038/nri.2016.90CrossRefGoogle ScholarPubMed
Kim, J, Lee, J, Choi, IJ, et al. (2020) TNF genetic polymorphism (rs1799964) may modify the effect of the dietary inflammatory index on gastric cancer in a case-control study. Sci Rep 10, 14590.CrossRefGoogle ScholarPubMed
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Table 1. General characteristics of the study participants

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Table 2. Association of tertiles of dietary potassium intake with GC risk

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Table 3. TNF rs1800629 genetic polymorphisms and risk of GC in the dominant model

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Table 4. Interactive effect of the TNF-α rs1800629 polymorphism and potassium intake on gastric carcinogenesis