Genetic association of PRDM1-ATG5 intergenic region and autophagy with systemic lupus erythematosus in a Chinese population

全基因组关联研究 遗传学 ATG5型 遗传关联 生物 基因分型 基因间区 基因 单核苷酸多态性 候选基因 人口 国际人类基因组单体型图计划 基因型 基因座(遗传学) 医学 基因组 自噬 细胞凋亡 环境卫生
作者
Shu‐Feng Zhou,Xiaolan Lu,Jicheng Lv,Huixia Yang,Lu Xue qin,Ming‐Hui Zhao,Yu‐Feng Su,Zhanguo Li,Hong Zhang
出处
期刊:Annals of the Rheumatic Diseases [BMJ]
卷期号:70 (7): 1330-1337 被引量:224
标识
DOI:10.1136/ard.2010.140111
摘要

Objective

Recent genome-wide association studies suggested the PRDM1-ATG5 gene region as a systemic lupus erythematosus (SLE)-associated locus both in Caucasian and Chinese populations; however, the candidate gene was still obscure and the possible functional significance needed to be determined.

Methods

In this study, by a multistage integrative strategy, the authors first performed a case–control association study involving 1745 individuals in the Chinese population by genotyping nine single nucleotide polymorphisms within this region, and a meta-analysis was conducted. Correlation between associated genotypes and expression levels of messenger RNA in B-cell lines from 210 unrelated HapMap data was examined, and was validated in vitro. To determine the biological significance, a genetic association study was also checked in a pathway-based manner and the significant associations were validated in a second 844 Chinese cohort.

Results

A peak of association was found in the intergenic region (p=0.036–3.26×10−4). Meta-analysis consolidated the association between rs548234 and SLE (OR 1.254, p=1.28×10−16). Significant positive correlations with ATG5 expression were identified, suggesting ATG5 as a candidate gene in the region. Epstein–Barr virus B-cell-based downstream gene expression analysis supported a functional effect of rs548234 and rs6937876, and in-vitro experiments confirmed the regulatory effect of rs6937876 in B-cell populations. Finally, an autophagy pathway-based genetic association study identified ATG7 (p=1.12×10−4) and IRGM (p=0.015) as novel candidate genes, and gene–gene interactions were observed between ATG5, ATG7 and IRGM.

Conclusion

These data may demonstrate that autophagy is involved in the pathogenesis of SLE and imply a common biological pathway in autoimmunity.
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