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系统性硬化症是一种主要与免疫调节和炎症基因相关的复杂疾病。

Systemic Sclerosis is a Complex Disease Associated Mainly with Immune Regulatory and Inflammatory Genes.

作者信息

Jin Jingxiao, Chou Chou, Lima Maria, Zhou Danielle, Zhou Xiaodong

机构信息

University of Texas Medical School at Houston, USA ; Duke University, USA.

University of Texas Medical School at Houston, USA.

出版信息

Open Rheumatol J. 2014 Sep 29;8:29-42. doi: 10.2174/1874312901408010029. eCollection 2014.

Abstract

Systemic sclerosis (SSc) is a fibrotic and autoimmune disease characterized clinically by skin and internal organ fibrosis and vascular damage, and serologically by the presence of circulating autoantibodies. Although etiopathogenesis is not yet well understood, the results of numerous genetic association studies support genetic contributions as an important factor to SSc. In this paper, the major genes of SSc are reviewed. The most recent genome-wide association studies (GWAS) are taken into account along with robust candidate gene studies. The literature search was performed on genetic association studies of SSc in PubMed between January 2000 and March 2014 while eligible studies generally had over 600 total participants with replication. A few genetic association studies with related functional changes in SSc patients were also included. A total of forty seven genes or specific genetic regions were reported to be associated with SSc, although some are controversial. These genes include HLA genes, STAT4, CD247, TBX21, PTPN22, TNFSF4, IL23R, IL2RA, IL-21, SCHIP1/IL12A, CD226, BANK1, C8orf13-BLK, PLD4, TLR-2, NLRP1, ATG5, IRF5, IRF8, TNFAIP3, IRAK1, NFKB1, TNIP1, FAS, MIF, HGF, OPN, IL-6, CXCL8, CCR6, CTGF, ITGAM, CAV1, MECP2, SOX5, JAZF1, DNASEIL3, XRCC1, XRCC4, PXK, CSK, GRB10, NOTCH4, RHOB, KIAA0319, PSD3 and PSOR1C1. These genes encode proteins mainly involved in immune regulation and inflammation, and some of them function in transcription, kinase activity, DNA cleavage and repair. The discovery of various SSc-associated genes is important in understanding the genetics of SSc and potential pathogenesis that contribute to the development of this disease.

摘要

系统性硬化症(SSc)是一种纤维化自身免疫性疾病,临床特征为皮肤和内脏器官纤维化以及血管损伤,血清学特征为循环自身抗体的存在。尽管其发病机制尚未完全明确,但众多基因关联研究结果支持遗传因素是SSc的一个重要致病因素。本文对SSc的主要相关基因进行综述。纳入了最新的全基因组关联研究(GWAS)以及可靠的候选基因研究。检索了2000年1月至2014年3月期间PubMed上关于SSc基因关联研究的文献,纳入的研究一般总参与者超过600例且有重复验证。还纳入了一些关于SSc患者相关功能变化的基因关联研究。共报道了47个与SSc相关的基因或特定基因区域,尽管其中一些存在争议。这些基因包括HLA基因、STAT4、CD247、TBX21、PTPN22、TNFSF4、IL23R、IL2RA、IL - 21、SCHIP1/IL12A、CD226、BANK1、C8orf13 - BLK、PLD4、TLR - 2、NLRP1、ATG5、IRF5、IRF8、TNFAIP3、IRAK1、NFKB1、TNIP1、FAS、MIF、HGF、OPN、IL - 6、CXCL8、CCR6、CTGF、ITGAM、CAV1、MECP2、SOX5、JAZF1、DNASEIL3、XRCC1、XRCC4、PXK、CSK、GRB10、NOTCH4、RHOB、KIAA0319、PSD3和PSOR1C1。这些基因编码的蛋白质主要参与免疫调节和炎症反应,其中一些在转录、激酶活性、DNA切割和修复中发挥作用。发现各种与SSc相关的基因对于理解SSc的遗传学以及导致该疾病发生发展的潜在发病机制具有重要意义。

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