Low tolerance for transcriptional variation at cohesin genes is accompanied by functional links to disease-relevant pathways

2022

Preprint

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Preeclampsia (PE) is a relatively common but severe pregnancy disorder that is characterized by hypertension (HTN) and either proteinuria (PRO), or other organ damage. There are very limited effective treatments for PE, and it is associated with substantial effects on the health of both the mother and fetus. 25 genetic variants have been associated (p < 1 × 10−6) with PE in the latest genome-wide association studies (GWAS). By overlapping the regulatory impacts of the PE-associated genetic variants with the regulatory impacts of HTN- and PRO-associated genetic variants, we were able to identify shared functional impacts between PE and HTN. We identified significant variation of the mean LOUEF scores for genes targeted by cis- and trans-acting eQTLs, consistent with an enrichment for regulatory interactions with target genes intolerant to loss-of-function mutations. Signaling pathways were enriched within the protein-protein interaction networks (PPINs) that were constructed using proteins encoded by the eQTL targeted genes. Finally, tissue-specific analyses of eQTLs specific to whole blood and arteries detected dysregulation of PE-relevant regulatory pathways. Collectively, these results are consistent with a model in which predisposition to HTN and PRO lays a molecular groundwork toward risk for PE pathogenesis. These findings inform on possible therapeutic targets for future studies.

Section: Introductionmentioning

confidence: 99%

Spatially Constrained Gene Regulation Identifies Key Genetic Contributions of Preeclampsia, Hypertension and Proteinuria

Boom

2022

Preprint

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“…However, the GTEx catalogue lists thousands of genetic variants in healthy individuals that are associated with local control of RAD21 expression (cis-eQTLs) 20 . Our previous work found that many of these variants in cis-eQTLs are also associated with co-regulation of a network of genes involved in complex disease processes 21 . Our results indicated spatial eQTLs as identifying disease associations through mechanisms alternative to those disease associations found via GWAS.…”

Section: Introductionmentioning

confidence: 99%

Genetic Variation as a Long-Distance Modulator of RAD21 Expression in Humans

Horsfield

2021

Preprint

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Mutations and changes in expression in RAD21 are common across cancers types and outside of cancer can result in cohesinopathy. As such, exploration of variants that modify RAD21 enhancer activity, across the genome, may also provide insights into mechanisms by which distinct variants impact healthy human development and disease. We searched 42,953,834 genomic variants for a spatial-eQTL association with the transcription of RAD21. We identified 123 significant associations (FDR < 0.05), which are local (cis) or long-distance (trans) regulators of RAD21 expression. The 123 variants co-regulate a further seven genes, enriched for having Sp2 transcription factor binding sites in their promoter regions. The Sp2 transcription factor and six of the seven genes had previously been associated with cancer onset, progression, and metastasis. Our results suggest that genome-wide variation in non-coding regions impacts on RAD21 transcript levels in addition to other genes, which then could impact on oncogenesis and the process of ubiquitination. This identification of distant co-regulation of oncogenes represents a strategy for discovery of novel genetic regions which impact cancer onset and a potential for diagnostics.

Genetic variation as a long-distance modulator of RAD21 expression in humans

Horsfield

2022

Sci Rep

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Somatic mutations and changes in expression of RAD21 are common in many types of cancer. Moreover, sub-optimal levels of RAD21 expression in early development can result in cohesinopathies. Altered RAD21 levels can result directly from mutations in the RAD21 gene. However, whether DNA variants outside of the RAD21 gene could control its expression and thereby contribute to cancer and developmental disease is unknown. In this study, we searched for genomic variants that modify RAD21expression to determine their potential to contribute to development or cancer by RAD21 dysregulation. We searched 42,953,834 genomic variants for a spatial-eQTL association with the transcription of RAD21. We identified 123 significant associations (FDR < 0.05), which are local (cis) or long-distance (trans) regulators of RAD21 expression. The 123 variants co-regulate a further seven genes (AARD, AKAP11, GRID1, KCNIP4, RCN1, TRIOBP, and USP32), enriched for having Sp2 transcription factor binding sites in their promoter regions. The Sp2 transcription factor and six of the seven genes had previously been associated with cancer onset, progression, and metastasis. Our results suggest that genome-wide variation in non-coding regions impacts on RAD21 transcript levels in addition to other genes, which then could impact on oncogenesis and the process of ubiquitination. This identification of distant co-regulation of oncogenes represents a strategy for discovery of novel genetic regions influencing cancer onset and a potential for diagnostics.