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妊娠次数及人类白细胞抗原等位基因与类风湿关节炎发病风险的关系

Parity and HLA alleles in risk of rheumatoid arthritis.

作者信息

Guthrie Katherine A, Gammill Hilary S, Madeleine Margaret M, Dugowson Carin E, Nelson J Lee

机构信息

Clinical Research Division, Fred Hutchinson Cancer Research Center; Seattle, WA USA.

出版信息

Chimerism. 2011 Jan;2(1):11-5. doi: 10.4161/chim.2.1.15424.

Abstract

Specific HLA II alleles are associated with rheumatoid arthritis (RA) risk and others with protection. Risk-associated alleles encode similar amino acid sequences from 70 through 74 of HLA-DRβ1 (QKRAA, QRRAA, RRRAA), referred to as the "shared epitope" (SE) and protective alleles encode DERAA at the same location. Fetal-maternal cell exchange results in long-term microchimerism i.e. harboring small numbers of genetically disparate cells. Women with RA who lack the SE were recently found to harbor microchimerism with the SE more often than healthy women. This finding raises the question whether microchimerism with DERAA confers benefit against RA and is underscored by the observation that overall parity reduces RA risk. While there is currently no test for microchimerism with DERAA, we conducted studies to ask whether parity benefits women at risk for RA, either because they have the SE or lack the protective DERAA sequence. HLA genotyping was conducted for 310 RA and 571 healthy women. Parity was associated with reduced RA risk in women aged <45 years (RR 0.53, 95% CI 0.34-0.82) and further analyses examined this group. RA risk reduction with parity was greater among women with the SE than SE-negative women (RR 0.42, 95%CI 0.22-0.79 vs. RR 0.79, 0.38-1.64). Among women without DERAA, RA risk was significantly reduced with parity (RR 0.44, 95% CI 0.26-0.74) but not among DERAA-positive women (RR 0.95 95% CI 0.34-2.65). In summary, results indicate the effect of parity varied according to a woman's HLA-genotype, and women at increased risk of RA benefited most.

摘要

特定的人类白细胞抗原II类等位基因与类风湿性关节炎(RA)风险相关,而其他一些等位基因则具有保护作用。与风险相关的等位基因在HLA-DRβ1的70至74位编码相似的氨基酸序列(QKRAA、QRRAA、RRRAA),称为“共享表位”(SE),而保护性等位基因在相同位置编码DERAA。胎儿-母体细胞交换会导致长期微嵌合体状态,即体内存在少量基因不同的细胞。最近发现,缺乏SE的RA女性比健康女性更常携带具有SE的微嵌合体。这一发现引发了一个问题,即携带DERAA的微嵌合体是否对RA具有保护作用,而总体生育次数会降低RA风险这一观察结果也凸显了这一问题。虽然目前尚无检测携带DERAA微嵌合体的方法,但我们开展了研究,以探究生育次数是否对有RA风险的女性有益,无论她们是具有SE还是缺乏保护性DERAA序列。对310名RA女性和571名健康女性进行了HLA基因分型。生育次数与年龄小于45岁女性的RA风险降低相关(风险比0.53,95%置信区间0.34 - 0.82),进一步分析针对该组人群。有SE的女性生育次数降低RA风险的幅度大于无SE的女性(风险比0.42,95%置信区间0.22 - 0.79 vs.风险比0.79,0.38 - 1.64)。在没有DERAA的女性中,生育次数使RA风险显著降低(风险比0.44,95%置信区间0.26 - 0.74)但在有DERAA的女性中并非如此(风险比0.95,95%置信区间0.34 - 2.65)。总之,结果表明生育次数的影响因女性的HLA基因型而异,RA风险增加的女性受益最大。

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本文引用的文献

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Arthritis Rheum. 2011 Mar;63(3):640-4. doi: 10.1002/art.30160.
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