Variants at IRX4 as prostate cancer expression quantitative trait loci

Xu, Xianghua; Hussain, Wasay; Vijai, Joseph; Offit, Kenneth; Rubin, Mark A.; Demichelis, Francesca; Klein, Robert J.

doi:10.1038/ejhg.2013.195

Cited by 37 publications

(31 citation statements)

References 53 publications

(58 reference statements)

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“…rs10993994 was associated with NCOA4 in normal tissue with p=5.7x10 −5 , but was null in tumor (p=0.64), consistent with a previous finding (19). We also confirmed other previous findings (20, 21): rs12653946 with IRX4 (in tumor and normal), rs8102476 with PPP1R14A (in tumor and normal), rs6465657 with LMTK2 (in tumor only), and rs5945619 with NUDT10 (in tumor only). However, we did not confirm an association of rs4430796 with HNF1B in normal tissue (p=0.66) (19) or associations with FAM83F (p=0.29), YIF1B (p=0.37) , FAM98C (p=0.17) , FOXP4 (p=0.19) , or TFEB (p=0.78) in tumor tissue (21).…”

Section: Resultssupporting

confidence: 92%

“…In addition to confirming the MSMB and NCOA4 results, NUDT11 was associated with rs5945619 and SLC22A3 was borderline significantly associated with rs9364554 in both tumor and normal tissue; and HNF1B was associated with rs4430796 in normal tissue only (19). Harries et al observed an association between rs6465657 and expression of nearby LMTK2 (20), while Xu et al found a proxy for rs12653946 to be strongly associated with the expression of nearby IRX4 (21). …”

Section: Introductionmentioning

confidence: 99%

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Association of Prostate Cancer Risk Variants with Gene Expression in Normal and Tumor Tissue

Penney

Sinnott

Tyekucheva

et al. 2015

Cancer Epidemiology, Biomarkers &Amp; Prevention

100

102

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Background Numerous germline genetic variants are associated with prostate cancer risk, but their biological role is not well understood. One possibility is that these variants influence gene expression in prostate tissue. We therefore examined the association of prostate cancer risk variants with the expression of genes nearby and genome-wide. Methods We generated mRNA expression data for 20,254 genes with the Affymetrix GeneChip Human Gene 1.0 ST microarray from normal prostate (N=160) and prostate tumor (N=264) tissue from participants of the Physicians’ Health Study and Health Professionals Follow-up Study. With linear models, we tested the association of 39 risk variants with nearby genes and all genes, and the association of each variant with canonical pathways using a global test. Results In addition to confirming previously reported associations, we detected several new significant (p<0.05) associations of variants with the expression of nearby genes including C2orf43, ITGA6, MLPH, CHMP2B, BMPR1B, and MTL5. Genome-wide, four genes (MSMB, NUDT11, NEFM, KLHL33) were significantly associated after accounting for multiple comparisons for each SNP (p<2.5x10−6). Many more genes had a false discovery rate <10%, including SRD5A1 and PSCA, and we observed significant associations with pathways in tumor tissue. Conclusions The risk variants were associated with several genes, including promising prostate cancer candidates and lipid metabolism pathways, suggesting mechanisms for their impact on disease. These genes should be further explored in biological and epidemiological studies. Impact Determining the biological role of these variants can lead to improved understanding of prostate cancer etiology and identify new targets for chemoprevention.

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Section: Resultssupporting

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Association of Prostate Cancer Risk Variants with Gene Expression in Normal and Tumor Tissue

Penney

Sinnott

Tyekucheva

et al. 2015

Cancer Epidemiology, Biomarkers &Amp; Prevention

100

102

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“…Over-expression of IRX4 significantly increased invasion relative to controls in all conditions examined and IRX4 had high relative expression in a subset of basal-like breast cancers (Figures 5,6). IRX4 is a homeobox transcription factor involved in cardiogenesis, marking a ventricular-specific progenitor cell (Nelson et al, 2016) and is also associated with prostate cancer risk (Xu et al, 2014). SNX29 belongs to the sorting nexin protein family that function in endosomal sorting and signalling (Marat and Haucke, 2016).…”

Section: Novel Twist and Snail Functional Targets Influence Invasion mentioning

confidence: 99%

Functionally Coherent Transcription Factor Target Networks Illuminate Control of Epithelial Remodelling

et al. 2018

Preprint

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Cell identity is governed by gene expression, regulated by Transcription Factor (TF) binding at cisregulatory modules. We developed the NetNC software to decode the relationship between TF binding and the regulation of cognate target genes in cell decision-making; demonstrated on nine datasets for the Snail and Twist TFs, and also modENCODE 'HOT' regions. Results illuminated conserved molecular networks controlling development and disease, with implications for precision medicine. Predicted 'neutral' TF binding accounted for the majority (50% to ≥80%) of candidate target genes from statistically significant peaks and HOT regions had high functional coherence.Expression of orthologous functional TF targets discriminated breast cancer molecular subtypes and predicted novel tumour biology. We identified new gene functions and network modules including crosstalk with notch signalling and regulation of chromatin organisation, evidencing networks that reshape Waddington's landscape during epithelial remodelling. Predicted invasion roles were validated using a tractable cell model, supporting our computational approach.

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“…Multiple studies have shown that PrCa-and other disease-associated variants are enriched near variants that correlate with gene expression levels [9][10][11][12][13] . In fact, recent approaches have integrated expression quantitative trait loci (eQTLs) with GWAS to implicate several plausible genes for PrCa risk (e.g., IRX4, MSMB, NCOA4, NUDT11 and SLC22A3) 5; [14][15][16][17][18][19][20][21] . While overlapping eQTLs and GWAS is powerful, the high prevalence of eQTLs 22 coupled with linkage disequilibrium (LD) renders it difficult to distinguish the true susceptibility gene from spurious co-localization at the same locus 23 .…”

Section: Introductionmentioning

confidence: 99%

Large-scale transcriptome-wide association study identifies new prostate cancer risk regions

Mancuso

Gayther

Gusev

et al. 2018

Preprint

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Although genome-wide association studies (GWAS) for prostate cancer (PrCa) have identified more than 100 risk regions, most of the risk genes at these regions remain largely unknown.Here, we integrate the largest PrCa GWAS (N=142,392) with gene expression measured in 45 tissues (N=4,458), including normal and tumor prostate, to perform a multi-tissue transcriptomewide association study (TWAS) for PrCa. We identify 235 genes at 87 independent 1Mb regions . CC-BY-NC-ND 4.0 International license It is made available under a (which was not peer-reviewed) is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity.The copyright holder for this preprint . http://dx.doi.org/10.1101/345736 doi: bioRxiv preprint first posted online Jun. 14, 2018; associated with PrCa risk, 9 of which are regions with no genome-wide significant SNP within 2Mb. 24 genes are significant in TWAS only for alternative splicing models in prostate tumor thus supporting the hypothesis of splicing driving risk for continued oncogenesis. Finally, we use a Bayesian probabilistic approach to estimate credible sets of genes containing the causal gene at pre-defined level; this reduced the list of 235 associations to 120 genes in the 90% credible set. Overall, our findings highlight the power of integrating expression with PrCa GWAS to identify novel risk loci and prioritize putative causal genes at known risk loci.

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Variants at IRX4 as prostate cancer expression quantitative trait loci

Cited by 37 publications

References 53 publications

Association of Prostate Cancer Risk Variants with Gene Expression in Normal and Tumor Tissue

Association of Prostate Cancer Risk Variants with Gene Expression in Normal and Tumor Tissue

Functionally Coherent Transcription Factor Target Networks Illuminate Control of Epithelial Remodelling

Large-scale transcriptome-wide association study identifies new prostate cancer risk regions

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