Associations of <i><scp>FUT2</scp></i> and <i><scp>FUT3</scp></i> gene polymorphisms with <scp>C</scp>rohn's disease in <scp>C</scp>hinese patients

Hu, Dingyuan; Shao, Xiao-xiao; Xu, Chunyan; Xia, Shenglong; Yu, Liqin; Jiang, Lijia; Jin, Jie; Lin, Xiuqing; Jiang, Yi

doi:10.1111/jgh.12599

Cited by 21 publications

(15 citation statements)

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“…In a large cohort of 316 Chinese participants, we performed accurate genotyping and a combined analysis of nine SNPs reported previously in the fucosyltransferase genes . False‐negative reactions are often produced in Lewis blood typing due to weak hemagglutination reactions, which in the main is accounted for by adsorption of glycolipids and by erythrocyte levels .…”

Section: Discussionmentioning

confidence: 99%

“…Cooperation of the two fucosyltransferases ultimately regulates the expression of the histo‐blood group antigens, including CA19‐9 (sLe a ), in body fluids and on the surface of epithelial cells. A single nucleotide polymorphism (SNP) of FUT3 and FUT2 is prevalent in multiple populations and dramatically determines the fucosyltransferase activities . Distribution of the FUT3 / FUT2 genotypes exhibits ethnic heterogeneity and is strongly associated with a wide range of human diseases .…”

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confidence: 99%

“…However, Lewis‐positive individuals (the Le / Le and Le / le genotypes) are divided into three Lewis‐secretor phenotypes according to distinct Secretor genotypes as follows: (a) Le (a−b+) secretors with the Se / Se or Se / se genotype; (b) Le (a+b−) non‐secretors with the se / se genotype; and (c) Le (a+b+) partial secretors having homozygosity for the weak Secretor allele . Nucleotide substitutions inactivating the FUT2 / 3 genes have been found within various populations, and the phenotypes have been determined by the ethnic group‐specific genotypes . Both genotypes of Lewis and Secretor are crucial for an individual's phenotype formation, and the serum CA19‐9 value will directly reflect the differences among individuals.…”

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confidence: 99%

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Distribution of Lewis and Secretor polymorphisms and corresponding CA19‐9 antigen expression in a Chinese population

Guo

Luo

et al. 2017

FEBS Open Bio

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The Lewis (FUT3) and Secretor (FUT2) genes, corresponding to secretion of Lewis ABO (H) histo‐blood group antigen CA19‐9, are highly polymorphic with differences between populations. In this study, the FUT3 and FUT2 genes in 316 Chinese participants were sequenced to detect polymorphisms, and the associated CA19‐9 antigen secretion was also measured. In total, 14 genotypes of FUT3 and 10 genotypes of FUT2 were verified. Le/Le, Le/le59,508 and Le/le59 were the main genotypes of FUT3 with frequencies of 53.2%, 10.7% and 3.5%, respectively. Se/Se, Se/se385 and se385/se385 were the main genotypes of FUT2, with frequencies of 21.4%, 18.6% and 16.2%, respectively. The alleles le1067 and le508 were found extensively in the Chinese population, and the frequency of allele se385 was shown to be higher than previously reported. Phenotype analysis revealed that 9.8% of individuals were the Lewis‐negative type and 22.5% were the secretor‐negative type. Combined phenotypes showed that 3.2% of participants were of ‘double‐negative’ phenotype (le, se) and 19.3% were of single dominant non‐secretor phenotype (Le, se). Serum Lewis antigen CA19‐9 levels were significantly different between subgroups and consistent with the defined phenotype. Our study revealed the unique distribution of Lewis and Secretor polymorphisms in a large Chinese population, and decoded the combined genotypes of the two CA19‐9‐related genes.

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Section: Discussionmentioning

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Distribution of Lewis and Secretor polymorphisms and corresponding CA19‐9 antigen expression in a Chinese population

Guo

Luo

et al. 2017

FEBS Open Bio

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“…Interestingly, the non-secretor phenotype, characterized by a null variant in another FUT gene, FUT2 , and the resulting absence of ABH antigens in the mucosa in homozygotes for the null allele, influences the composition and diversity of the microbiome in the human intestinal tract (Wacklin et al 2011; Rausch et al 2011). Moreover, variants in both FUT2 and FUT3 have been shown in GWAS to increase susceptibility to diseases associated with both mucosal surface pathobiology and microbiome composition, such as cystic fibrosis (Taylor-Cousar et al 2009), Crohn’s disease (Hu et al 2014) and ulcerative colitis (Hu et al 2016). Our study extends a role for fucosyltransferases to the nasal mucosal surface, and further implicates host genetic influences on bacterial diversity at this site.…”

Section: Discussionmentioning

confidence: 99%

Host genetic variation in mucosal immunity pathways influences the upper airway microbiome

Gilad

Nicolae

Pinto

et al. 2016

Preprint

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“…We found significant associations of rs601338 with disease in Turks ( P =6.51×10 −9 ) and in Iranians ( P =1.65x10 −5 ), and also significant association of rs1047781 in Japanese ( P =6.50×10 −4 , Supplementary Table 15). These non-secretor genotypes are also associated with Crohn’s disease risk 26,27 and with the gut microbiome composition 28,29 . The non-secretor phenotype has also been associated with increased predisposition to or resistance to different infectious agents 30–32 .…”

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Dense genotyping of immune-related loci implicates host responses to microbial exposure in Behçet's disease susceptibility

et al. 2017

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We analyzed 1,900 Turkish Behçet’s disease cases and 1,779 controls genotyped with the Immunochip. The most significantly associated single nucleotide polymorphism (SNP) was rs1050502, a tag SNP for HLA-B*51. In the Turkish discovery set, we identified three novel loci, IL1A-IL1B, IRF8, and CEBPB-PTPN1, with genome-wide significance (P<5×10−8) by direct genotyping, and ADO-EGR2 by imputation. ADO-EGR2, IRF8, and CEBPB-PTPN1 replicated by genotyping 969 Iranian cases and 826 controls. Imputed data in 608 Japanese cases and 737 controls replicated ADO-EGR2 and IRF8 and meta-analysis additionally identified RIPK2 and LACC1. The disease-associated allele of rs4402765, the lead marker of the IL1A-IL1B locus, was associated with both decreased interleukin-1α and increased interleukin-1β production. ABO non-secretor genotypes of two ancestry-specific FUT2 SNPs showed strong disease association (P=5.89×10−15). Our findings extend shared susceptibility genes with Crohn’s disease and leprosy, and implicate mucosal factors and the innate immune response to microbial exposure in Behçet’s disease susceptibility.

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Associations of FUT2 and FUT3 gene polymorphisms with Crohn's disease in Chinese patients

Abstract: Our study strongly implicates the polymorphic locus of FUT2 (rs1047781) in CD susceptibility in Chinese population. Mutations of FUT3 (rs28362459) and (rs3745635) might influence the lesion locations in CD patients.

Cited by 21 publications

References 50 publications

Distribution of Lewis and Secretor polymorphisms and corresponding CA19‐9 antigen expression in a Chinese population

Distribution of Lewis and Secretor polymorphisms and corresponding CA19‐9 antigen expression in a Chinese population

Host genetic variation in mucosal immunity pathways influences the upper airway microbiome

Dense genotyping of immune-related loci implicates host responses to microbial exposure in Behçet's disease susceptibility

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