The common variants of E-selectin gene in Graves’ disease

Chen, H; Cui, Bin; Wang, S; Zhao, Zhihui; Sun, Huimin; Gu, Xuejiang; Zhao, Yu; Li, Xiaoying; Ning, Guang

doi:10.1038/sj.gene.6364452

Cited by 13 publications

(17 citation statements)

References 27 publications

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“…The Ser128Arg gene variant, the most commonly reported SELE-gene polymorphism, is associated with a wide variety of disorders, including coronary artery disease, venous thrombosis, ischemic cerebral vascular disease, postoperative myocardial infarction, prognosis of colorectal cancer, restenosis after successful coronary angioplasty, severity of atherosclerotic arterial disease, peripheral arterial occlusive disease, and coronary calcification [8-12]. Common variants of the SELE gene have also been found associated with the susceptibility to either Graves’ disease or hypertension [13-15]. However, the association between SELE SNPs and E-selectin levels has been controversial [15-17], and the association between SELE SNPs and other inflammatory marker levels has not been reported.…”

Section: Introductionmentioning

confidence: 99%

“…Common variants of the SELE gene have also been found associated with the susceptibility to either Graves’ disease or hypertension [13-15]. However, the association between SELE SNPs and E-selectin levels has been controversial [15-17], and the association between SELE SNPs and other inflammatory marker levels has not been reported. This investigation aimed to elucidate the association between SELE SNPs and the plasma levels of sE-selectin and MMP9, in Taiwanese individuals.…”

Section: Introductionmentioning

confidence: 99%

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Association of SELE genotypes/haplotypes with sE-selectin levels in Taiwanese individuals: interactive effect of MMP9 level

Hsu

Teng

et al. 2012

BMC Med Genet

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BackgroundE-selectin is implicated in various inflammatory processes and related disorders. We aimed to investigate the role of SELE-gene genotypes/haplotypes on plasma levels of MMP9 and sE-selectin in Taiwanese individuals.MethodsFive hundred twenty individuals were enrolled. Seven tagging SELE single nucleotide polymorphisms were analyzed.ResultsSELE genotypes were found associated with MMP9 and sE-selectin levels. Multivariate analysis identified that the most significant genetic polymorphism (rs5368 genotype) was independently associated with MMP9 levels (P < 0.001). One haplotype (GGAGAGT) was marginally associated with MMP9 levels (P = 0.0490). One SELE SNP, (rs3917406, P = 0.031) was associated with sE-selectin levels after adjusting for MMP9 and sICAM1 levels. Subgroup and interaction analysis revealed association of SELE SNP rs10800469 with sE-selectin levels only in the highest quartile of MMP9 level (P = 0.002, interaction P = 0.023). Haplotype analysis showed one haplotype (AAAAAGC) borderline associated with sE-selectin level (P = 0.0511).ConclusionSELE genotypes/haplotypes are independently associated with MMP9 and E-selectin levels in Taiwanese individuals. The associations of SELE genotypes/haplotypes with sE-selectin levels are affected by MMP9 levels.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Association of SELE genotypes/haplotypes with sE-selectin levels in Taiwanese individuals: interactive effect of MMP9 level

Hsu

Teng

et al. 2012

BMC Med Genet

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“…To our knowledge only 1 previous study has used similar techniques to identify 6 tagging SNPs [21] and also did not identify A561C as a tagging SNP. Two tagging SNPs identified by HapMap analysis were selected for further study (rs3917417 G2692A and rs3917454 C1901T).…”

Section: Introductionmentioning

confidence: 99%

Low frequency haplotypes of E-selectin polymorphisms G2692A and C1901T give increased protection from coronary artery disease

Gorący

Kaczmarczyk

et al. 2011

Med Sci Monit

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SummaryBackgroundE-selectin polymorphisms are an independent atherosclerosis and coronary artery disease (CAD) risk factor. This study aimed to investigate the link between the C1901T and G2692A E-selectin tagging SNPs and their haplotypes and the extent of coronary artery disease in Polish patients.Material/MethodsFor this study 321 patients were recruited CAD extent by coronary angiography and E selectin gene variant were investigated using HapMap, PCR/RFLP, multivariate logistic regression and haplotype analysis.ResultsFrequency distributions of the C1901T and G2692A polymorphisms were significantly different in CAD patients as compared to control subjects (p=0.037 and p=0.025, respectively). The C1901T polymorphism was found to be an independent genetic predictor of risk of CAD (OR=3.01) in a multivariate model adjusted for classic, environmental risk factors. The A-C and G-T haplotypes showed the strongest significant associations with CAD. The A-C haplotype proved to be significantly more common in controls (haplotype frequency 9.2%) than in CAD (5.7%, p=0.048); the G-T haplotype was not found among control subjects (0.0%) but was found in CAD (1.3%, p=0.0099).ConclusionsAssociations between the C1901T and G2692A E-selectin polymorphisms and CAD in the Polish population were found. Investigated variants correlated with the risk of coronary artery disease development but not with the extent of coronary artery vascular changes. In the haplotype analysis, 2 haplotypes influenced CAD – the A-C haplotype (7%) proved to exert a protective effect against CAD, while the effect of the less frequent G-T haplotype (1%) was associated with significant increase in CAD risk.

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“…[112,113]. Chen H, et al [114,115] reported common L-selectin or E-selectin variants may be associated with susceptibility to Graves' disease in Chinese population. Cytokines, a large group of non-enzymatic proteins, participate in the induction and effector phases of all inflammatory and immune responses, and are therefore likely to play a critical role in the development of autoimmune diseases [116].…”

Section: Hyperthyroidismmentioning

confidence: 99%

The New Perspectives on Genetic Studies of Type 2 Diabetes and Thyroid Diseases

Xu¹,

Bi²,

Cui³

et al. 2013

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Abstract:Recently, genome-wide association studies (GWAS) have led to the discovery of hundreds of susceptibility loci that are associated with complex metabolic diseases, such as type 2 diabetes and hyperthyroidism. The majority of the susceptibility loci are common across different races or populations; while some of them show ethnicity-specific distribution. Though the abundant novel susceptibility loci identified by GWAS have provided insight into biology through the discovery of new genes or pathways that were previously not known, most of them are in introns and the associated variants cumulatively explain only a small fraction of total heritability. Here we reviewed the genetic studies on the metabolic disorders, mainly type 2 diabetes and hyperthyroidism, including candidate genes-based findings and more recently the GWAS discovery; we also included the clinical relevance of these novel loci and the gene-environmental interactions. Finally, we discussed the future direction about the genetic study on the exploring of the pathogenesis of the metabolic diseases.

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The common variants of E-selectin gene in Graves’ disease

Cited by 13 publications

References 27 publications

Association of SELE genotypes/haplotypes with sE-selectin levels in Taiwanese individuals: interactive effect of MMP9 level

Association of SELE genotypes/haplotypes with sE-selectin levels in Taiwanese individuals: interactive effect of MMP9 level

Low frequency haplotypes of E-selectin polymorphisms G2692A and C1901T give increased protection from coronary artery disease

The New Perspectives on Genetic Studies of Type 2 Diabetes and Thyroid Diseases

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