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类风湿性关节炎基因-基因交互作用研究进展

孙庆庆 张伟 张莉娜 邬秀娣 岑晗

孙庆庆, 张伟, 张莉娜, 邬秀娣, 岑晗. 类风湿性关节炎基因-基因交互作用研究进展[J]. 中华疾病控制杂志, 2019, 23(7): 871-876, 880. doi: 10.16462/j.cnki.zhjbkz.2019.07.025
引用本文: 孙庆庆, 张伟, 张莉娜, 邬秀娣, 岑晗. 类风湿性关节炎基因-基因交互作用研究进展[J]. 中华疾病控制杂志, 2019, 23(7): 871-876, 880. doi: 10.16462/j.cnki.zhjbkz.2019.07.025
SUN Qing-qing, ZHANG Wei, ZHANG Li-na, WU Xiu-di, CEN Han. A review of gene-gene interaction studies in rheumatoid arthritis[J]. CHINESE JOURNAL OF DISEASE CONTROL & PREVENTION, 2019, 23(7): 871-876, 880. doi: 10.16462/j.cnki.zhjbkz.2019.07.025
Citation: SUN Qing-qing, ZHANG Wei, ZHANG Li-na, WU Xiu-di, CEN Han. A review of gene-gene interaction studies in rheumatoid arthritis[J]. CHINESE JOURNAL OF DISEASE CONTROL & PREVENTION, 2019, 23(7): 871-876, 880. doi: 10.16462/j.cnki.zhjbkz.2019.07.025

类风湿性关节炎基因-基因交互作用研究进展

doi: 10.16462/j.cnki.zhjbkz.2019.07.025
基金项目: 

国家自然科学基金 81602921

详细信息
    通讯作者:

    岑晗, E-mail: cenhan@nbu.edu.cn

  • 中图分类号: R593.22

A review of gene-gene interaction studies in rheumatoid arthritis

Funds: 

National Natural Science Foundation of China 81602921

More Information
  • 摘要: 迄今为止,大样本遗传关联研究尤其是全基因组关联研究(genome-wide association study,GWAS)发现并且确认了大量与类风湿性关节炎(rheumatoid arthritis,RA)遗传易感性相关的基因/区域,但是这些已经发现的遗传因素尚不足以完全解释RA的遗传度,而基因-基因交互作用是尚未被发现的遗传度的重要组成部分。实际上,基因间交互作用研究一直是RA遗传流行病学研究的一个重要方向,这类研究为深入认识RA的遗传基础和发病生物学机制提供了重要线索,也为RA发病风险预测和疾病预防提供了科学参考依据。本文将对RA基因-基因交互作用研究进展进行综述,从而为今后开展相关研究提供参考。
  • 表  1  RA中功能相关基因之间的交互作用研究

    Table  1.   Studies of the interaction between functionally related genes in RA

    第一作者 发表时间(年) 人种 基因 研究结果
    Martínez A[35] 2006 西班牙人 NFκB1与FCRL3 NFκB1-94ins/del ATTG位点杂合子而非纯合子者中发现FCRL3-169位点与RA相关。
    Julià A[36] 2007 西班牙人 IL6与IL4I1 多因子降维法分析发现IL6 rs1800797位点与IL4I1 rs1290754位点之间存在交互作用(验证样本准确度为0.60;OR=2.23,95% CI:1.51~3.28;P < 0.02)。
    McKinney C[37] 2008 新西兰人和英国人 CCL3L1与CCR5 同时携带CCL3L1至少3个拷贝数与CCR5△32纯合子者发病风险高,但是未做相加模型交互作用的假设检验。
    Marinou I[38] 2009 英国人 SELSIL1β、IL6、TNF IL1β -511基因型为AA而非GA/GG者中SELS-105A等位基因在显性遗传模型下与RA发病相关,且层间异质性检验有统计学意义。未发现SELSIL6、TNF间存在交互作用。
    Assmann G[39] 2009 德国人 MDM2与p53 MDM2 SNP309位点与p53 P72R位点存在相乘模型交互作用。
    Marinou I[40] 2008 英国人 IL-4、IL-4R与IL-13 IL-4R Q551R位点的A等位基因在显性遗传模型下与RA的关联强度在携带IL-13-1112位点不同基因型(TT/CT/CC)的个体中存在统计学差异,然而经过校正后无统计学差异。
    Kawasaki A[41] 2010 日本人 TNFAIP3与TNIP1 未发现TNFAIP3 rs2230926位点与TNIP1 rs7708392位点之间存在相乘模型交互作用。
    Perdigones N[42] 2010 西班牙人 TNFRSF14与TNFRSF6B 第一阶段研究、第二阶段研究及合并研究均发现在TNFRSF6B rs4809330位点基因型为GG而非GA/AA者中TNFRSF14 rs668486位点G等位基因与RA发病有关,且层间异质性检验有统计学意义。
    Deshmukh HA[43] 2011 哥伦比亚人 MMEL1、CD244、KIAA1109、
    ADAD1、CDK6、C8orf13-BLK
    PHF19-TRAF1、TRAF1-C5、
    DKFZKIF5ASH2B3、
    C12orf30、CLEC16AITGAM
    CD226与CD40
    MMEL1 rs3890745位点与C80rf13-BLK rs13277113位点存在相乘模型交互作用。
    Génin E[44] 2013 法国人、日本人和西班牙人 BANK1与BLK 在欧洲人群RA中BANK1 rs3733197位点与BLK rs13277113位点存在相乘模型交互作用;在西班牙人群及欧洲人群中,BANK1 rs3733197位点G等位基因仅在BLK rs13277113位点基因型为GG者中与RA有关;多因子降维法发现在欧洲人群而非日本人群RA中BANK1 rs3733197位点与BLK rs13277113位点存在交互作用。
    Kim K[45] 2013 韩国人 IRF5与STAT4 IRF5 rs77571059位点与STAT4 rs16833215位点存在相乘模型交互作用。
    Lee SH[46] 2014 韩国人 CTLA4、CD28、CD40、CD40LGCD86 多因子降维法分析发现CD40LG -3458 T>G与CD86 -3479 T>G之间存在交互作用。
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  • 收稿日期:  2018-12-06
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