Colocalization of Gene Expression and DNA Methylation with Genetic Risk Variants Supports Functional Roles of MUC5B and DSP in Idiopathic Pulmonary Fibrosis

被引:20
|
作者
Borie, Raphael [1 ]
Cardwell, Jonathan [2 ]
Konigsberg, Iain R. [2 ]
Moore, Camille M. [3 ,4 ]
Zhang, Weiming [3 ]
Sasse, Sarah K. [5 ]
Gally, Fabienne [2 ,6 ]
Dobrinskikh, Evgenia [2 ,7 ]
Walts, Avram [2 ]
Powers, Julie [2 ]
Brancato, Janna [2 ]
Rojas, Mauricio [8 ]
Wolters, Paul J. [9 ]
Brown, Kevin K. [5 ]
Blackwell, Timothy S. [10 ]
Nakanishi, Tomoko [11 ]
Richards, J. Brent [11 ]
Gerber, Anthony N. [2 ,5 ,6 ]
Fingerlin, Tasha E. [3 ,4 ,6 ]
Sachs, Norman [12 ]
Pulit, Sara L. [13 ]
Zappala, Zachary [13 ]
Schwartz, David A. [2 ,14 ]
Yang, Ivana V. [2 ,15 ]
机构
[1] Univ Paris Diderot, Paris, France
[2] Univ Colorado Anschutz Med Campus, Dept Med, Aurora, CO USA
[3] Univ Colorado Anschutz Med Campus, Dept Pediat, Aurora, CO USA
[4] Univ Colorado Anschutz Med Campus, Dept Microbiol & Immunol, Aurora, CO USA
[5] Colorado Sch Publ Hlth, Dept Biostat & Bioinformat, Aurora, CO USA
[6] Colorado Sch Publ Hlth, Dept Epidemiol, Aurora, CO USA
[7] Natl Jewish Hlth, Ctr Genes Environm & Hlth, Denver, CO USA
[8] Natl Jewish Hlth, Dept Med, Denver, CO USA
[9] Natl Jewish Hlth, Dept Immunol & Genom Med, Denver, CO USA
[10] Ohio State Univ, Ohio State Coll Med, Dept Internal Med, Columbus, OH USA
[11] Univ Calif San Francisco, Dept Med, San Francisco, CA USA
[12] Vanderbilt Univ, Med Ctr, Dept Med, Nashville, TN USA
[13] McGill Univ, Dept Human Genet, Lady Davis Inst, Jewish Gen Hosp, Montreal, PQ, Canada
[14] Vertex Pharmaceut, Cell Biol, San Diego, CA USA
[15] Vertex Pharmaceut, Computat Genom, Boston, MA USA
关键词
pulmonary fibrosis; functional genomics; common genetic variant; transcriptome; epigenome; INTERSTITIAL LUNG-DISEASE; GENOME-WIDE ASSOCIATION; PROMOTER POLYMORPHISM; DESMOPLAKIN CAUSES; DISTAL AIRWAYS; SUSCEPTIBILITY; MUTATIONS; PNEUMONITIS; LOCI; COHORT;
D O I
10.1164/rccm.202110-2308OC
中图分类号
R4 [临床医学];
学科分类号
1002 ; 100602 ;
摘要
Rationale: Common genetic variants have been associated with idiopathic pulmonary fibrosis (IPF). Objectives: To determine functional relevance of the 10 IPF-associated common genetic variants we previously identified. Methods: We performed expression quantitative trait loci (eQTL) and methylation quantitative trait loci (mQTL) mapping, followed by co-localization of eQTL and mQTL with genetic association signals and functional validation by luciferase reporter assays. Illumina multi-ethnic genotyping arrays, mRNA sequencing, and Illumina 850k methylation arrays were performed on lung tissue of participants with IPF (234 RNA and 345 DNA samples) and non-diseased controls (188 RNA and 202 DNA samples). Measurements and Main Results: Focusing on genetic variants within 10 IPF-associated genetic loci, we identified 27 eQTLs in controls and 24 eQTLs in cases (false-discovery-rate-adjusted P<0.05). Among these signals, we identified associations of lead variants rs35705950 with expression of MUC5B and rs2076295 with expression of DSP in both cases and controls. mQTL analysis identified CpGs in gene bodies of MUC5B (cg17589883) and DSP (cg08964675) associated with the lead variants in these two loci. We also demonstrated strong co-localization of eQTL/mQTL and genetic signal in MUC5B (rs35705950) and DSP (rs2076295). Functional validation of the mQTL in MUC5B using luciferase reporter assays demonstrates that the CpG resides within a putative internal repressor element. Conclusions: We have established a relationship of the common IPF genetic risk variants rs35705950 and rs2076295 with respective changes in MUC5B and DSP expression and methylation. These results provide additional evidence that both MUC5B and DSP are involved in the etiology of IPF.
引用
收藏
页码:1259 / 1270
页数:12
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