Abstract
Genome-wide association study (GWAS) loci for several immunity-mediated diseases (early onset asthma, inflammatory bowel disease (IBD), primary biliary cholangitis, and rheumatoid arthritis) map to chromosomal region 17q12-q21. The predominant view is that association between 17q12-q21 alleles and increased risk of developing asthma or IBD is due to regulatory variants. ORM sphingolipid biosynthesis regulator (ORMDL3) residing in this region is the most promising gene candidate for explaining association with disease. However, the relationship between 17q12-q21 alleles and disease is complex suggesting contributions from other factors, such as trans-acting genetic and environmental modifiers or circadian rhythms. Circadian rhythms regulate expression levels of thousands of genes and their dysregulation is implicated in the etiology of several common chronic inflammatory diseases. However, their role in the regulation of the 17q12-q21 genes has not been investigated. Moreover, the core clock gene nuclear receptor subfamily 1, group D, member 1 (NR1D1) resides about 200 kb distal to the GWAS region. We hypothesized that circadian rhythms influenced gene expression levels in 17q12-q21 region and conversely, regulatory elements in this region influenced transcription of the core clock gene NR1D1 in cis. To test these hypotheses, we examined the diurnal expression profiles of zona pellucida binding protein 2 (ZPBP2/Zpbp2), gasdermin B (GSDMB), and ORMDL3/Ormdl3 in human and mouse tissues and analyzed the impact of genetic variation in the ZPBP2/Zpbp2 region on NR1D1/Nr1d1 expression. We found that Ormdl3 and Zpbp2 were controlled by the circadian clock in a tissue-specific fashion. We also report that deletion of the Zpbp2 region altered the expression profile of Nr1d1 in lungs and ileum in a time-dependent manner. In liver, the deletion was associated with enhanced expression of Ormdl3. We provide the first evidence that disease-associated genes Zpbp2 and Ormdl3 are regulated by circadian rhythms and the Zpbp2 region influences expression of the core clock gene Nr1d1.
Highlights
Human chromosomal region 17q12-q21 harbors risk alleles for several immunity-mediated diseases, including early onset asthma, inflammatory bowel disease (IBD), primary biliary cholangitis (PBC), and rheumatoid arthritis (RA) [1,2,3,4,5,6,7]
Identification of the gene responsible for the genetic association with disease is complicated by the fact that no polymorphisms that would alter the protein sequence are found in the best gene candidate ORM sphingolipid biosynthesis regulator (ORMDL3) whereas regulatory genetic variants influence expression of at least three protein-coding genes residing in this region, zona pellucida binding protein 2 (ZPBP2), gasdermin B (GSDMB) and ORMDL3, suggesting that transcription of these genes is governed by shared regulatory mechanisms [1, 9, 10]
It has been proposed that loss of CTCC factor (CTCF) site in the ZPBP2 gene resulted in chromatin conformation that favored interaction between the promoters of ORMDL3 and GSDMB and a distant enhancer leading to higher transcription rates [10, 13]
Summary
Human chromosomal region 17q12-q21 harbors risk alleles for several immunity-mediated diseases, including early onset asthma, inflammatory bowel disease (IBD), primary biliary cholangitis (PBC), and rheumatoid arthritis (RA) [1,2,3,4,5,6,7] This suggests that the disease-associated variants (daVs) in this region are likely to have pleiotropic effects and impact a pathway(s) that is critical for the pathogenesis of not one, but several immunity-mediated diseases (reviewed in [8]). The sum of current data suggests a complex relationship between the 17q12-q21 daVs and disease, such as a cumulative effect from variation in expression of several neighboring genes, impact of modifier loci, epigenetic variation, environmental factors, or an association that is time-dependent
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