GENOTYPE ASSOCIATION <i>GSTM1</i> NULL AND GASTRIC CANCER: EVIDENCE-BASED META-ANALYSIS

RIBEIRO, Rívian Xavier; NASCIMENTO, Cícera Isabella Leão Leite; SILVA, Antonio Márcio Teodoro Cordeiro

doi:10.1590/S0004-2803.201700000-14

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Arquivos de Gastroenterologia

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Original Articles • Arq. Gastroenterol. 54 (02) • Apr-Jun 2017 • https://doi.org/10.1590/S0004-2803.201700000-14 copy

GENOTYPE ASSOCIATION GSTM1 NULL AND GASTRIC CANCER: EVIDENCE-BASED META-ANALYSIS

Associação do genótipo nulo GSTM1 e o câncer gástrico: evidências baseadas em meta-análise

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

BACKGROUND

Gastric cancer is the fourth most common cancer in men and the sixth among women, except for non-melanoma skin tumors, in Brazil. Epidemiological evidences reveal the multifactorial etiology of this cancer, highlighting risk factors such as: infection by the bacterium Helicobacter pylori, advanced age, smoking, chronic alcohol abuse, eating habits and genetic polymorphisms. Considering the context of genetic polymorphisms, there is the absence of the GSTM1 gene. The lack of GSTM1 function to detoxify xenobiotics and promote defense against oxidative stress leads to increased DNA damage, promoting gastric carcinogenesis. This process is multifactorial and the development of gastric cancer results from a complex interaction of these variables.

OBJECTIVE

The aim of this study was to investigate the association of GSTM1 null polymorphism in the pathogenesis of gastric cancer.

METHODS

A meta-analysis was conducted from 70 articles collected in SciELO and PubMed databases, between September 2015 and July 2016. In order to evaluate a possible association, we used the odds ratio (OR) and confidence interval of 95% (CI 95%). To assess the heterogeneity of the studies was used the chi-square test. Statistical analysis was performed using the BioEstat^® 5.3.

RESULTS

This study included 70 studies of case-control, including 28,549 individuals, which were assessed for the null polymorphism of the GSTM1 gene, and of which 11,208 (39.26%) were cases and 17,341 (60.74%) were controls. The final analysis showed that the presence of the GSTM1 gene acts as a protective factor against the development of gastric cancer (OR=0.788; 95%CI 0.725-0.857; P<0.0001). Positive statistical association was found in Asia (OR=0.736; 95%CI 0.670-0.809; P<0.0001) and Eurasia (OR=0.671; 95%CI 0.456-0.988; P=0.05). However, statistically significant data was not obtained in Europe (OR=1.033; 95%CI 0.873-1.222; P=0.705) and America (OR=0.866; 95%CI 0.549-1.364; P=0.534). Therefore, the results can not be deduced around the world.

CONCLUSION

This meta-analysis concluded that the presence of the GSTM1 gene is a protector for the emergence of gastric cancer, especially in Asian countries, but this result was not found in Europe and America.

HEADINGS
Stomach neoplasms; Genetic polymorphism; Meta-analysis

Author	Year	Case			Control						CI (95%)
		GSTM1 (+)		GSTM1 (-)		GSTM1 (+)		GSTM1 (-)		OR	Inf.	Sup.	Weight
		n	F (%)	n	F (%)	n	F (%)	n	F (%)	OR	Inf.	Sup.	Weight
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Yadav⁸⁶86. Yadav D, et al. Glutathione-S-transferase M1 and T1 genes and gastric cancer: a case control study in North Indian population. Gene. 2011;487:166-9.	2011	30	73.2	11	26.8	92	70.8	38	29.2	1.104	0.508	2.397	6.389
Jing³⁰30. Jing C, Huang ZJ, Duan YQ, Wang PH, Zhang R, Luo KS, Xiao XR. Glulathione-S-transferases gene polymorphism in prediction of gastric cancer risk by smoking and Helicobacter pylori infection status. Asian Pac J Cancer Prev. 2012;13:3325-8.	2012	170	41.5	240	58.5	203	49.5	207	50.5	0.723	0.549	0.952	50.617
Malakar⁴⁵45. Malakar M, Devi KR, Phukan RK, Kaur T, Deka M, Puia L, et al. Genetic polymorphism of glutathione S-transferases M1 and T1, tobacco habits and risk of stomach cancer in Mizoram. India Asian Pac J Cancer Prev . 2012;13:4725-32.	2012	45	44.1	57	55.9	107	52.5	97	47.5	0.718	0.446	1.155	16.970
Wang⁸²82. Wang WW, Yang WM, Zhang YX, Zhao SY. Research on the relationship of the susceptibility to elderly gastric cancer and GSTM1 gene polymorphism in Hainan. Xian Dai Yu Fang Yi Xue. 2012;39:6273-4.	2012	90	69.8	39	30.2	112	81.2	26	18.8	0.540	0.307	0.949	12.050
Kim³³33. Kim H, Um J, Kim Y. Glutathione S-transferase gene polymorphism in Korean subjects with gastric and colorectal cancer. Oriental Pharmacy and Experimental Medicine. 2012;12:307-12.	2012	41	40.2	61	59.8	76	38.0	124	62.0	1.098	0.676	1.785	16.271
Garcia-Gonzalez¹⁹19. Garcia-Gonzalez MA, Quintero E, Bujanda L, Nicolas D, Benito R, Strunk M, et al. Relevance of GSTM1, GSTT1, and GSTP1 gene polymorphisms to gastric cancer susceptibility and phenotype. Mutagenesis. 2012;27:771-7.	2012	274	49.2	283	50.8	290	52.1	267	47.9	0.892	0.705	1.128	69.682
Eom¹⁶16. Eom SY, Yim DH, Zhang Y, Yun JK, Moon SI, Yun HY, et al. Dietary aflatoxin B1intake, genetic polymorphisms of CYP1A2, CYP2E1, EPHX1, GSTM1, and GSTT1, and gastric cancerrisk in Korean. Cancer Causes Control. 2013;24:1963-72.	2013	214	44.9	263	55.1	217	45.6	259	54.4	0.971	0.753	1.253	59.142
Haholu²⁴24. Haholu A, Berber U, Karagoz B, Tuncel T, Bilgi O, Demirel D. Is there any association of glutathione S-transferase T1 (GSTT1) and glutathione S-transferase M1 (GSTM1) gene polymorphism with gastric cancers? Pol J Pathol. 2013;64:247-52.	2013	24	48.0	26	52.0	32	56.1	25	43.9	0.725	0.341	1.554	6.732
Total		5154	46.0	6054	54.0	8736	50.4	8605	49.6	0.788	0.725	0.857	P<0.0001

Parameters	Number of studies	Heterogeneity			Meta-analysis
Parameters	Number of studies	χ²	gl	P-value	Test	OR	CI (95%)	CI (95%)	P-value
Geral
GSTM1 (+) x GSTM1 (-)	70	154.651	69	<0.0001	DSL	0.788	0.725	0.857	<0.0001
Region
America	5	10.774	4	0.0292	DSL	0.866	0.549	1.364	0.534
Asia	50	99.489	49	<0.0001	DSL	0.736	0.670	0.809	<0.0001
Eurasia	3	0.820	2	0.6637	MH	0.671	0.456	0.988	0.050
Europe	12	22.800	11	0.0189	DSL	1.033	0.873	1.222	0.705

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[1] Correspondence: Antonio Márcio Teodoro Cordeiro Silva. Avenida Universitária, 1440, Setor Leste Universitário, CEP: 74.605-010 - Goiânia, GO, Brasil. E-mail: marciocmed@gmail.com.