Cha Seongwon, Choi Chan-Bum, Han Tae-Un, Kang Changsoo Paul, Kang Changwon, Bae Sang-Cheol
Korea Advanced Institute of Science and Technology, Daejeon, Republic of Korea.
Arthritis Rheum. 2007 May;56(5):1454-63. doi: 10.1002/art.22570.
Anti-cyclic citrullinated peptide (anti-CCP) antibodies are rheumatoid arthritis (RA)-specific serologic markers. RA susceptibility has been associated with HLA-DRB1 shared epitope (SE) alleles and single-nucleotide polymorphism (SNP) haplotypes in the peptidyl arginine deiminase 4 gene (PADI4). This study was undertaken to determine whether anti-CCP levels are associated with PADI4 haplotypes and/or SE alleles in Korean patients with RA.
Three nonsynonymous SNPs in PADI4 (padi4_89, padi4_90, and padi4_92) and SE alleles were genotyped, and serum anti-CCP levels were measured, in 311 patients with nonerosive or erosive RA. The relationships between anti-CCP levels and PADI4 haplotypes and/or SE alleles were analyzed statistically.
Anti-CCP levels were significantly higher in patients carrying the PADI4 RA risk haplotype than in patients who did not have the risk haplotype, among anti-CCP-positive patients with RA with a disease duration of <or=34 months (P = 0.041), but not among patients with a longer disease duration or among those who had erosive RA versus nonerosive RA. In contrast, the levels were significantly higher in SE carriers than in noncarriers among patients with RA with a disease duration of >or=141 months (P = 0.0037) and among those who had erosive RA (P = 0.000098), but not among patients who had a shorter disease duration or those who had nonerosive RA.
The PADI4 RA risk haplotype is associated with increased anti-CCP levels in RA patients with disease of short duration, and PADI4 may play a role in early RA. In contrast, SE alleles are associated with increased anti-CCP levels in RA patients with very longstanding disease and in patients with erosive RA, suggesting that SE alleles play a role in very late RA.
抗环瓜氨酸肽(anti-CCP)抗体是类风湿关节炎(RA)特异性血清学标志物。RA易感性与HLA-DRB1共享表位(SE)等位基因以及肽基精氨酸脱亚氨酶4基因(PADI4)中的单核苷酸多态性(SNP)单倍型有关。本研究旨在确定韩国RA患者中anti-CCP水平是否与PADI4单倍型和/或SE等位基因相关。
对311例非侵蚀性或侵蚀性RA患者的PADI4中的三个非同义SNP(padi4_89、padi4_90和padi4_92)以及SE等位基因进行基因分型,并检测血清anti-CCP水平。对anti-CCP水平与PADI4单倍型和/或SE等位基因之间的关系进行统计学分析。
在病程<或=34个月的anti-CCP阳性RA患者中,携带PADI4 RA风险单倍型患者的anti-CCP水平显著高于未携带风险单倍型的患者(P = 0.041),但在病程较长的患者中以及侵蚀性RA患者与非侵蚀性RA患者之间无此差异。相反,在病程>或=141个月的RA患者中(P = 0.0037)以及侵蚀性RA患者中(P = 0.000098),SE携带者的anti-CCP水平显著高于非携带者,但在病程较短的患者以及非侵蚀性RA患者中无此差异。
PADI4 RA风险单倍型与病程短的RA患者anti-CCP水平升高相关,且PADI4可能在早期RA中起作用。相反,SE等位基因与病程非常长的RA患者以及侵蚀性RA患者anti-CCP水平升高相关,提示SE等位基因在极晚期RA中起作用。
