Association of the GNAS1 T393C polymorphism with tumor stage and survival in gastric cancer

doi:10.3748/wjg.15.6061

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World Journal of Gastroenterology

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1007-9327

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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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World J Gastroenterol. Dec 28, 2009; 15(48): 6061-6067
Published online Dec 28, 2009. doi: 10.3748/wjg.15.6061

Table 1 Allele frequencies and genotype distribution of GNAS1 T393C polymorphism in 122 gastric cancer patients and in the reference group (n = 820) n (%)

T393C	Patients (n = 122)			Reference group (n = 820)			χ²	P	Odds ratio	95% CI
Allele	C 135 (55.3)		T 109 (44.7)	C 873 (53.2)		T 767 (46.7)	0.38	0.54	0.92	0.70-1.20
Genotype	CC 39 (32.0)	CT 57 (46.7)	TT 26 (21.3)	CC 235 (28.7)	CT 403 (49.1)	TT 182 (22.2)	0.37	0.54	0.92

Table 2 Clinicopathological characteristics of 122 patients with gastric cancer n (%)

	All	T393C genotypes			P
	All	CC	CT	TT	P
n (%)	122 (100)	39 (32)	57 (46.7)	26 (21.3)
Gender
Male	78 (63.9)	25 (32.1)	34 (43.6)	19 (24.4)
Female	44 (36.1)	14 (31.8)	23 (52.3)	7 (15.9)	0.274
WHO
Papillary/Tubular/Mucinous	76 (62.3)	23 (30.3)	34 (44.7)	19 (25)
Signet-ring cancer	38 (31.1)	12 (31.6)	19 (50)	7 (18.4)
Other	8 (6.6)	4 (50)	4 (50)	0	0.340
Differentiation
Well/Moderate (G1-G2)	42 (34.4)	12 (28.6)	22 (52.4)	8 (19)
Poor (G3-G4)	80 (65.6)	27 (33.8)	35 (43.8)	18 (22.5)	0.805
Laurén
Intestinal	52 (42.6)	16 (30.8)	25 (48.1)	11 (21.2)
Diffuse	55 (45.1)	17 (30.9)	29 (52.7)	9 (16.4)
Mixed	15 (12.3)	6 (40)	3 (20)	6 (40)	0.171
Ming
Expanding	47 (38.5)	14 (29.8)	24 (51.1)	9 (19.1)
Infiltrative	75 (61.5)	25 (33.3)	33 (44)	17 (22.7)	0.620
pT-category
T1	30 (24.6)	7 (23.3)	13 (43.3)	10 (33.3)
T2	44 (36.1)	12 (27.3)	22 (50)	10 (22.7)
T3	38 (31.1)	14 (36.8)	18 (47.4)	6 (15.8)
T4	10 (8.2)	6 (60)	4 (40)	0	0.110
pN-category
N0	49 (40.2)	11 (22.4)	24 (49)	14 (28.6)
N1	34 (27.9)	13 (38.2)	13 (38.2)	8 (23.5)
N2	14 (11.5)	6 (42.9)	6 (42.9)	2 (14.3)
N3	25 (20.5)	9 (36)	14 (56)	2 (8)	0.196
pM-category
M0	99 (81.1)	30 (30.3)	45 (45.5)	24 (24.2)
M1	23 (18.9)	9 (39.1)	12 (52.2)	2 (8.7)	0.101
R-category
R0	118 (96.7)	38 (32.5)	54 (46.2)	25 (21.4)
R1/R2	4 (3.3)	1 (25)	2 (50)	1 (25)	0.950
UICC stage
Ia	26 (21.3)	5 (19.2)	11 (42.3)	10 (38.5)
Ib	22 (18)	7 (31.8)	12 (54.5)	3 (13.6)
II	18 (14.8)	4 (22.2)	7 (38.9)	7 (38.9)
IIIa	11 (9)	4 (36.4)	5 (45.5)	2 (18.2)
IIIb	4 (3.3)	2 (50)	2 (50)	0
IV	41 (33.6)	17 (41.5)	20 (48.8)	4 (9.8)	0.023

P values are given for dichotomization between C+ (CC+CT) and C- (TT) genotypes.

Table 3 Univariate and multivariate survival analysis of 122 gastric cancer patients

Covariate	n	Univariate analysis			Multivariate analysis
Covariate	n	P value	5-yr-SR (%)	SE (±%)	P value	HR	95% CI
pT-category		< 0.001			< 0.001
pT1	30		85.4	6.8		1
pT2	44		44.5	7.8	< 0.001	6.212	2.31-16.70
pT3	38		5.4	3.7	< 0.001	13.026	4.44-38.23
pT4	10		33.3	15.7	0.001	7.838	2.24-27.46
pN-category		< 0.001			0.549
pN0	49		61.6	7.4		1
pN1	34		47.1	8.6	0.226	0.663	0.34-1.29
pN2	14		16.9	10.9	0.986	0.993	0.43-2.27
pN3	25		8.0	5.4	0.814	0.905	0.40-2.07
T393C SNP		0.043			0.333
CC/CT	96		36.7	5.1		1
TT	26		56.9	10.4		0.712	0.36-1.42
pM-category		< 0.001			0.027
M0	99		48.1	5.2		1
M1	23		9.2	6.2		2.087	1.09-4.01
R-category		< 0.001			0.022
R0	118		42.3	4.7		1
R+	4		0	0		3.128	1.18-8.27

SNP: Single nucleotide polymorphism; 5-yr-SR: 5-yr-survival; HR: Hazard ratio.

Table 4 Summary of the effect of the GNAS1 T393C polymorphism on various carcinomas

Cancer type	Yr	n	Effect	Benefit (survival)
Gastric cancer	2009	122	The present study demonstrates a significant survival benefit for the TT genotype with a 5-yr-survival rate of 56.9% vs the CC/CT group with a 5-yr-survival rate of only 36.7% (P = 0.043)	TT-genotype
Squamous cell cancer of larynx[15]	2008	157	Survival was significantly dependent on the T393C genotype in advanced American Joint Committee on Cancer (AJCC) stages (III-IV) with higher 5-yr survival rates for TT, followed by TC and CC (P = 0.0437)	TT-genotype
Oro- and hypo-pharyngeal squamous cell carcinoma[16]	2008	202	C homozygous patients displayed a higher risk for disease progression than T homozygous patients (P = 0.019) and a higher risk for death (P = 0.015). In multivariate analysis, besides cancer stage and tumor localization, the T393C polymorphism was an independent prognostic factor for disease progression and death	TT-genotype
Clear cell renal cell carcinoma[11]	2006	150	Tumor progression, development of metastasis and tumor-related death was significantly associated with the T393C polymorphism. In multivariate analysis CC patients were at highest risk for progression or tumor-related death compared with T-allele carriers (P = 0.018)	TT-genotype
Chronic lymphocytic leukemia[17]	2006	144	Median progression-free survival was significantly higher for T-allele carriers (P = 0.007). In multivariate analysis, the T393C polymorphism kept its prognostic independence (P = 0.01) besides of ZAP-70 (P = 0.005) and Binet stage (P < 0.001). Regarding overall survival, CC genotypes were significantly at highest risk for death compared to T-alleles both in univariate (P < 0.001) and multivariate analysis (P = 0.002)	TT-genotype
Bladder cancer[10]	2005	254	Progression-free survival (P = 0.011), metastasis-free survival (P = 0.001) and cancer-specific survival (P = 0.014) were significantly increased in TT genotypes compared with CC genotypes. In multivariate analysis, the T393C polymorphism kept its prognostic independence	TT-genotype
Sporadic colorectal cancer[12]	2005	151	In UICC stages I to II, the 5-yr survival rate was significantly (P = 0.009) higher in TT genotypes (88%) compared with TC (71%) and CC genotypes (50%). In multivariate analysis, the T393C polymorphism was also an independent prognostic factor. No significant effect could be seen for UICC stages III to IV	TT-genotype
Cholangio-carcinoma[14]	2007	87	Disease-specific overall survival was significantly dependent on the T393C genotype (P = 0.02), with TT genotypes showing reduced survival compared to patients carrying at least one C allele. In multivariate analysis (TT/C+) the T393C genotype kept its prognostic independence (P = 0.04)	CC-genotype
Breast carcinoma[13]	2007	279	Overall survival was significantly (P = 0.033) associated with the T393C polymorphism with lowest survival rates for the TT-genotype and highest survival rate for the CC-genotype. In multivariate analysis, the TT-genotype still had a significant survival benefit compared to the CC genotype (P = 0.045)	CC-genotype
Esophageal cancer[28]	2009	51	T393C polymorphism was significantly associated with tumor response to Cisplatin/5-FU-based radiochemotherapy. 63% of the T allele carriers had a minor histopathologic response (MiHR) with more than 10% residual vital tumor cells in resection specimens. For the CC genotype MiHR was seen only in 20%. In binary logistic regression analysis, the T393C genotype kept its independence (P < 0.05)	CC-genotype

Citation: Alakus H, Mönig SP, Warnecke-Eberz U, Alakus G, Winde G, Drebber U, Schmitz KJ, Schmid KW, Riemann K, Siffert W, Bollschweiler E, Hölscher AH, Metzger R. Association of the GNAS1 T393C polymorphism with tumor stage and survival in gastric cancer. World J Gastroenterol 2009; 15(48): 6061-6067
URL: https://www.wjgnet.com/1007-9327/full/v15/i48/6061.htm
DOI: https://dx.doi.org/10.3748/wjg.15.6061