Functional characterization of the 12p12.1 renal cancer-susceptibility locus implicates BHLHE41

Bigot, Pierre; Colli, Leandro M.; Machiela, Mitchell J.; Jessop, Lea; Myers, Timothy A.; Carrouget, J.; Wagner, Sarah; Roberson, David A.; Eymerit, Caroline; Henrion, Didier; Chanock, Stephen J.

doi:10.1038/ncomms12098

Cited by 31 publications

(28 citation statements)

References 51 publications

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“…Motivated by the prioritization of HIF1a/HIF2a binding sites, we searched for SNPs in the RCC GWAS that overlapped asQTL peaks and HIF1a/HIF2a active sites (or sites that disrupted known HIF motifs, see Methods) and identified a total of 8 SNPs where the GWAS association was significant after Bonferroni correction: 3/8 loci were identified or connected to target genes or enhancers from asQTLs in this study: DPF3, SCARB1 , and GRAMD4; another 4/8 loci were previously linked to HIF binding and/or experimentally supported: EPAS1 (HIF2a), CCND1, BHLHE41 40 , and MYC 41 ( Figure 3b,c, Supplementary Table S14 ) and the remaining SNP was in an intron of the RBPMS gene but could not be connected to a target. In total, asQTLs were observed at all four loci previously implicated through HIF binding and highlighted three novel gene targets at four loci without previous experimental follow-up.…”

Section: Resultsmentioning

confidence: 81%

Allelic imbalance reveals widespread germline-somatic regulatory differences and prioritizes risk loci in Renal Cell Carcinoma

Gusev

Spisák

Fay

et al. 2019

Preprint

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Determining the function of non-coding regulatory variants in cancer is a key challenge transcriptional biology. We investigated genetic (germline and somatic) determinants of regulatory mechanisms in renal cell carcinoma (RCC) using H3K27ac ChIP-seq data in 10 matched tumor/normal samples and RNA-seq data from 496/66 tumor/normal samples from The Cancer Genome Atlas (TCGA). Unsupervised clustering of H3K27ac activity cleanly separated tumor from normal individuals, highlighting extensive epigenetic reprogramming during transformation. We developed a novel method to test each chromatin feature for evidence of an allele-specific quantitative trait locus (asQTL) and evaluate tumor/normal differences in allele-specificity (d-asQTLs) while modelling local structural variation and read overdispersion. At an FDR of 5%, we identified 1,356 unique asQTL chromatin peaks in normal tissues; 2,868 in tumors; and 1,054 d-asQTLs (primarily imbalanced in tumor). The d-asQTL peaks were significantly enriched for RCC genome-wide association study (GWAS) heritability (32x, P=1.8×10−3), more so than any other functional feature including all H3K27ac peaks (12x), super-enhancers (5x), and asQTL genes (4x). Intersection of asQTLs with RCC GWAS loci identified putative functional features for 6/17 known loci including tumor-specific activity at SCARB1, a cholesterol metabolism mediator, which has recently been implicated in RCC progression. We validated the asQTL variant through CRISPR interference (CRISPRi) and demonstrated a concomitant allelic effect on the overlapping enhancer and on downstream SCARB1 expression. Knockdowns of master transcription factors (TFs) involved in the hypoxia pathway altered the expression of SCARB1 in a kidney cancer cell line, consistent with a variant-TF interaction. Genome-wide, d-asQTLs were significantly enriched for tumor-specific binding of hypoxic transcription factors, implicating a more general mechanism for polygenic germline-somatic interaction.

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Section: Resultsmentioning

confidence: 81%

Allelic imbalance reveals widespread germline-somatic regulatory differences and prioritizes risk loci in Renal Cell Carcinoma

Gusev

Spisák

Fay

et al. 2019

Preprint

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“…The 2p21 locus maps to EPAS1 , a gene encoding the HIF-2α subunit 55 whereas the biological effects underlying the 11q13.3 locus seems to be attributable to changes in the regulation of CCND1 (encoding cyclin D1, which is involved in cell cycle regulation) 59 . The locus 12p11.23 probably maps to changes in BHLHE41 (encoding basic helix-loop-helix family member e41, which is thought to have a role in regulation of the circadian rhythm) 60 . The disease genes underlying the other GWAS susceptibility loci have yet to be identified.…”

Section: Epidemiologymentioning

confidence: 99%

Renal cell carcinoma

Hsieh

Purdue

Signoretti

et al. 2017

Nat Rev Dis Primers

1,804

1,599

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Renal cell carcinoma (RCC) denotes cancer originated from renal epithelium and accounts for >90% of cancers in the kidney. The disease encompasses >10 histological and molecular subtypes, of which clear cell RCC (ccRCC) is most common and accounts for most cancer-related deaths. Although somatic VHL mutations have been described for some time, more-recent cancer genomic studies have identified mutations in epigenetics regulatory genes and demonstrated marked intratumour heterogeneity, which could have prognostic, predictive and therapeutic relevance. Localized RCC can be successfully managed with surgery whereas metastatic RCC is refractory to conventional chemotherapy. However, over the past decade, marked advances in treatment of metastatic RCC have been made, with targeted agents including sorafenib, sunitinib, bevacizumab, pazopanib and axitini that inhibit vascular endothelial growth factor (VEGF) and its receptor(VEGFR) and everolimus and temsirolimus, which inhibit mTOR complex 1, being approved. Since 2015, agents with additional targets aside from VEGFR have been approved, such as cabozantinib and lenvatinib; immunotherapies such as nivolumab have also been added to the armamentarium for metastatic RCC. Here, we provide an overview of the molecular biology of RCC, with a focus on ccRCC, as well as updates to complement current clinical guidelines and an outline of potential future directions for RCC research and therapy.

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“…Interestingly, the location of this SNP (14q24) is deleted in one quarter to half of patients [30], and dysregulation of other components of BAF and PBAF complexes are common features of ccRCC. The same group also identified BHLHE41 , a gene encoding a basic helix-loop-helix protein located in the 12p12.1 susceptibility locus, from GWAS [31]. The ccRCC risk allele associated with this gene increased its expression, and the authors provided functional evidence that ectopic expression of BHLHE41 increased xenograft tumor growth.…”

Section: Genetics Of Ccrccmentioning

confidence: 99%

Genetic and metabolic hallmarks of clear cell renal cell carcinoma

Sanchez

Simon

2018

Biochimica et Biophysica Acta (BBA) - Reviews on Cancer

111

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Clear cell renal cell carcinoma (ccRCC) is a malignancy characterized by deregulated hypoxia-inducible factor signaling, mutation of several key chromatin modifying enzymes, and numerous alterations in cellular metabolism. Pre-clinical studies have historically been limited to cell culture models, however, the identification of critical tumor suppressors and oncogenes from large-scale patient sequencing data has led to several new genetically engineered mouse models with phenotypes reminiscent of ccRCC. In this review, we summarize recent literature on these topics and discuss how they inform targeted therapeutic approaches for the treatment of ccRCC.

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Functional characterization of the 12p12.1 renal cancer-susceptibility locus implicates BHLHE41

Cited by 31 publications

References 51 publications

Allelic imbalance reveals widespread germline-somatic regulatory differences and prioritizes risk loci in Renal Cell Carcinoma

Allelic imbalance reveals widespread germline-somatic regulatory differences and prioritizes risk loci in Renal Cell Carcinoma

Renal cell carcinoma

Genetic and metabolic hallmarks of clear cell renal cell carcinoma

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