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Association between IL23R and ERAP1 polymorphisms and sacroiliac or spinal MRI inflammation in spondyloarthritis: DESIR cohort data

机译:IL23R与ERAP1多态性与脊椎炎中的酸痛或骶髂骨炎症的关联:DESIR队列数据

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Abstract Background To investigate the association between 12 single nucleotide polymorphisms (SNPs) located on ERAP1 and IL23R with the presence of inflammation on the sacroiliac joint (SIJ) or spinal magnetic resonance imagery (MRI) in an early onset spondyloarthritis (SpA) cohort. Methods All the patients included in the DESIR cohort with an axial SpA and available DNA at baseline were enrolled in this study (n = 645 patients) and underwent a clinical examination, CRP assay, SIJ and spinal MRI scans. Six SNPs located on ERAP1 (rs30187, rs27044, rs27434, rs17482078, rs10050860, rs2287987) and six SNPs located on IL23R (rs1004819, rs10489629, rs1343151, rs2201841, rs10889677, rs11209032) were genotyped. Univariable analyses were performed to test the association between the genotypes and SIJ and spinal MRI inflammation, as well as disease activity based on Bath Ankylosing Spondylitis Disease Activity Index (BASDAI), Ankylosing Spondylitis Disease Activity Score-C-Reactive Protein (ASDAS-CRP) and CRP. Results One SNP located on ERAP1 (rs27434) and haplotype CCT of ERAP1 were associated with SIJ inflammation detected by MRI, but these associations were below the Bonferroni corrected threshold of significance. However, one SNP (rs1004819) located on IL23R was associated with SIJ MRI inflammation (rs1004819: TT 42.3%, CT 40.5%, CC 26.5%, p = 0.0005). This locus was also significantly associated with Spondyloarthritis Research Consortium of Canada scores while no association with another inflammatory parameter such as BASDAI, ASDAS-CRP, CRP or Berlin MRI score was identified in this population. Conclusion One locus of the IL23R gene was associated with SIJ MRI inflammation and might be a marker of more active disease in recent onset SpA. Trial registration clinicaltrials.gov, NCTO 164 8907
机译:抽象背景探讨位于ERAP1和IL23R与炎症对骶髂关节(骶髂关节)或脊髓的磁共振成像(MRI)在早期发病脊椎关节炎(SPA)的队列中存在12个单核苷酸多态性(SNP)之间的关联。方法所有包含在具有轴向SpA和可用的DNA在基线DESIR队列患者在该研究中(N = 645名患者)被纳入并进行了临床检查,CRP测定中,骶髂关节和脊柱的MRI扫描。位于ERAP1(rs30187,rs27044,rs27434,rs17482078,rs10050860,rs2287987)和位于IL23R 6个SNP(rs1004819,rs10489629,rs1343151,rs2201841,rs10889677,rs11209032)的SNP六进行基因分型。进行单变量分析来测试基于Bath强直性脊柱炎疾病活动指数(BASDAI)基因型和SIJ和脊柱MRI炎症之间的关联,以及疾病活动度,强直性脊柱炎疾病活动评分-C反应蛋白(ASDAS-CRP)和CRP。结果的一种SNP位于ERAP1(rs27434)和ERAP1的单倍型与CCT SIJ炎症被关联通过MRI检测到,但这些关联均低于邦弗朗尼校正的意义的阈值。然而,一个SNP(rs1004819)位于IL23R用SIJ MRI炎症(:TT 42.3%,CT 40.5%,26.5 CC%,p值= 0.0005 rs1004819)相关联。该基因还与加拿大分数脊柱关节炎研究协会同时与其它炎症参数如BASDAI,ASDAS-CRP,CRP或柏林MRI得分没有关联在这一人群被确定显著相关。结论IL23R基因的一个位点与骶髂关节MRI炎症有关,并可能会更积极疾病在近期发作的SpA的标志。试验注册clinicaltrials.gov,NCTO 164 8907

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