Association between the RAGE (receptor for advanced glycation end-products) -374T/A gene polymorphism and diabetic retinopathy in T2DM

Tao, Dan; Mai, Xuancheng; Zhang, Tiesong; Mei, Yan

doi:10.1590/1806-9282.63.11.971

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ORIGINAL ARTICLE • Rev. Assoc. Med. Bras. 63 (11) • Nov 2017 • https://doi.org/10.1590/1806-9282.63.11.971 copy

Association between the RAGE (receptor for advanced glycation end-products) -374T/A gene polymorphism and diabetic retinopathy in T2DM

Authorship SCIMAGO INSTITUTIONS RANKINGS

Summary

Objective:

Interaction between advanced glycation end-products (AGEs) and receptor for AGEs (RAGE) in cells could affect both extracellular and intracellular structure and function, which plays a pivotal role in diabetic microvascular complications. The results from previous epidemiological studies on the association between RAGE gene -374T/A polymorphism and diabetic retinopathy (DR) risk were inconsistent. Thus, we conducted this meta-analysis to summarize the possible association between RAGE -374T/A polymorphism and DR risk.

Method:

We searched all relevant articles on the association between RAGE -374T/A polymorphism and DR risk from PubMed, Cochrane Library, ScienceDirect, Wanfang, VIP and Chinese National Knowledge Infrastructure (CNKI) web databases up to August 2016. Odds ratio (OR) with 95% confidence interval (CI) were calculated to assess those associations. All analyses were performed using the Review Manager software.

Results:

Nine case-control studies, including 1,705 DR cases and 2,236 controls were enrolled, and the results showed that the A allele of RAGE -374T/A polymorphism was significantly associated with increased DR risk in dominant model (TA/AA vs. TT: OR=1.22, 95CI 1.05-1.41, p=0.006) and heterozygote model (TA vs. TT: OR=1.26, 95CI 1.07-1.47, p=0.005). The subgroup analysis by ethnicity showed that significantly increased DR risk was found in both Asian and Caucasian populations.

Conclusion:

This meta-analysis reveals that the A allele of RAGE -374T/A polymorphism probably increase DR risk.

Keywords:
polymorphism; genetic; diabetic retinopathy; meta-analysis

Study	Country	Ethnicity	Year	Design	Sample source	DM type	Groups	Age, years		Males (%)		DM duration (y)		BMI (kg/m² )		HbA1c (%)
								DR	NDR	DR	NDR	DR	NDR	DR	NDR	DR	NDR
Balasubbu 2010	South India	Asian	2010	Case-control	HB	T2DM	PE1:DR=345; NDR=359 PE2:DR=100; NDR=90	PE1: 57±9 PE2: 57±8	PE1: 59±11 PE2: 58±10	PE1: 70.0 PE2: 56.7	PE1: 58.0 PE2: 57.6	PE1: 14±9 PE2: 14±9	PE1: 12±6 PE2: 14±5	NA	NA	PE1: 6.4±1.6 PE2: 7.6±1.7	PE1: 6.4±1.2 PE2: 7.0± 1.7
Globocnik 2003	Slovenia	Caucasian	2003	Case-control	HB	T2DM	DR=116(PDR=76, NPDR=40); NDR=70	66.1± 8.6	70.0±9.2	44	42.9	18.8±8.7	17.2± 6.9	27.8± 4.5	27.7± 4.4	8.3±1.9	8.2± 1.6
Gu 2014	China,Wuxi	Asian	2014	Case-control	PB	T2DM	DR=92; NDR=93; HC=120	63.60 ± 7.23	61.85 ±9.06	48.9	49.5	NA	NA	24.40 ± 2.98	24.93 ± 3.85	8.78 ±2.11	8.38 ±2.35
Hudson 2001	UK,Leeds	Caucasian	2001	Case-control	HB	T2DM	DR=106; NDR=109; HC=113	NA	NA	NA	NA	NA	NA	NA	NA	NA	NA
Lindholm 2006	Sweden	Caucasian	2006	Case-control	HB	T1DM T2DM	T1DM=867(DR=312); T2DM=2467(DR=278); HC =205	NA	NA	NA	NA	NA	NA	NA	NA	NA	NA
Lindholm 2008	Sweden	Caucasian	2008	Case-control	HB	T1DM T2DM	T1DM=742(DR=315); T2DM=2957(DR=298); HC =206	NA	NA	NA	NA	NA	NA	NA	NA	NA	NA
Ramprasad 2007	South India	Asian	2007	Case-control	HB	T2DM	DR=190(PDR=57,NPD R=133);NDR=189; HC=149	NPDR: 59 ±8; PDR: 59 ±8	63±9	NPDR: 49PDR:70	69	NPDR: 20 ±6; PDR: 20±8	21±5	NA	NA	NPDR: 8.6±1.9 PDR: 8.9±1.7	8.1± 1.6
Santos 2005	Brazil	Caucasian	2005	Case-control	HB	T2DM	PDR⁺=46, PDR^-=126^* * PDR-: without DR plus NPDR.	NA	NA	NA	NA	NA	NA	NA	NA	NA	NA
Z.X.Ng 2012	Malaysia	Asian	2012	Case-control	HB	T2DM	DR=171;NDR=171; HC=235	56.1 ±10.1	59.2 ± 9.6	57.3	58.5	14.8±8.6	10.4± 7.9	26.4± 5.3	27.2± 4.4	9.0±2.1	7.9± 1.8

Genetic contrast	Population andsubgroups under analysis	Studies(cases/controls), n (n/n)	OR (95CI)		p value		Q testp value	I 2%
			Fixed model (FEM)	Random model (REM)	Fixed model	Random model
TT vs. TA+AA	All	9(1705/2236)	0.82(0.71-0.94)	0.82(0.70-0.95)	0.006	0.009	0.39	5
	Ethnicity
	Caucasian	6(907/1424)	0.85(0.71-1.01)	0.84(0.68-1.04)	0.06	0.11	0.27	22
	Asian	4(798/812)	0.74(0.57-0.97)	0.74(0.57-0.97)	0.03	0.03	0.45	0
	Case sample size
	< 150	4(423/335)	0.70(0.52-0.95)	0.69(0.44-1.07)	0.02	0.10	0.10	52
	≥ 150	5(1282/1901)	0.86(0.72-1.01)	0.86(0.72-1.01)	0.07	0.07	0.92	0
AA vs. TT+TA	All	7(1254/1768)	0.97(0.71-1.33)	1.26(0.65-2.43)	0.86	0.49	0.01	63
	Ethnicity
	Caucasian	4(801/1315)	0.83(0.59-1.16)	0.85(0.42-1.71)	0.26	0.64	0.03	66
	Asian	3(453/453)	2.92(1.14-7.48)	2.89(1.12-7.44)	0.03	0.03	0.88	0
	Case sample size
	< 150	3(317/226)	1.73(0.91-3.29)	2.45(0.35-17.28)	0.09	0.37	0.005	81
	≥ 150	4(937/1542)	0.80(0.55-1.15)	0.91(0.50-1.64)	0.22	0.75	0.15	44
TA vs. TT	All	8(1502/1993)	1.26(1.07-1.47)	1.26(1.07-1.47)	0.005	0.005	0.81	0
	Ethnicity
	Caucasian	4(737/1202)	1.24(1.03-1.50)	1.24(1.03-1.50)	0.03	0.03	0.82	0
	Asian	4(765/791)	1.29(0.96-1.72)	1.29(0.96-1.72)	0.09	0.09	0.43	0
	Case sample size
	< 150	3(281/212)	1.45(0.98-2.12)	1.44(0.98-2.12)	0.06	0.06	0.47	0
	≥ 150	5(1221/1781)	1.22(1.02-1.45)	1.22(1.02-1.45)	0.03	0.03	0.81	0
AA vs. TT	All	7(784/1164)	1.08(0.79-1.48)	1.39(0.71-2.73)	0.64	0.34	0.01	63
	Ethnicity
	Caucasian	4(466/828)	0.91(0.64-1.29)	0.93(0.45-1.95)	0.60	0.85	0.03	67
	Asian	3(318/336)	3.17(1.23-8.16)	3.14(1.21-8.13)	0.02	0.02	0.87	0
	Case sample size
	< 150	3(200/159)	1.98(1.02-3.84)	2.77(0.37-20.95)	0.04	0.32	0.005	81
	≥ 150	4(584/1005)	0.87(0.60-1.27)	0.96(0.55-1.69)	0.48	0.89	0.19	37
A vs. T	All	8(1599/2127)	1.16(0.97-1.38)	1.19(0.96-1.47)	0.1	0.12	0.26	21
	Ethnicity
	Caucasian	4(801/1315)	1.08(0.88-1.32)	1.11(0.81-1.52)	0.47	0.51	0.12	48
	Asian	4(798/812)	1.43(1.00-2.03)	1.43(1.00-2.03)	0.05	0.05	0.76	0
	Case sample size
	< 150	3(317/226)	1.50(1.00-2.25)	1.59(0.79-3.21)	0.05	0.20	0.06	64
	≥ 150	5(1282/1901)	1.09(0.89-1.32)	1.09(0.89-1.32)	0.41	0.41	0.81	0

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[1] *Correspondence: Kunming University of Science and Technology Kunming – China. Postal code: 650093. taodan1975@163.com