SiRCle (Signature Regulatory Clustering) model integration reveals mechanisms of phenotype regulation in renal cancer

Ariane Mora; Christina Schmidt; Brad Balderson; Christian Frezza; Mikael Bodén

doi:10.1186/s13073-024-01415-3

Genome Medicine (Dec 2024)

SiRCle (Signature Regulatory Clustering) model integration reveals mechanisms of phenotype regulation in renal cancer

Ariane Mora,
Christina Schmidt,
Brad Balderson,
Christian Frezza,
Mikael Bodén

Affiliations

Ariane Mora: School of Chemistry and Molecular Biosciences, University of Queensland
Christina Schmidt: Medical Research Council Cancer Unit, Hutchison/MRC Research Centre, University of Cambridge
Brad Balderson: School of Chemistry and Molecular Biosciences, University of Queensland
Christian Frezza: University of Cologne, Faculty of Medicine and University Hospital Cologne, Institute for Metabolomics in Ageing, Cluster of Excellence Cellular Stress Responses in Aging-associated Diseases (CECAD)
Mikael Bodén: School of Chemistry and Molecular Biosciences, University of Queensland

DOI: https://doi.org/10.1186/s13073-024-01415-3
Journal volume & issue: Vol. 16, no. 1
pp. 1 – 26

Abstract

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Abstract Background Clear cell renal cell carcinoma (ccRCC) tumours develop and progress via complex remodelling of the kidney epigenome, transcriptome, proteome and metabolome. Given the subsequent tumour and inter-patient heterogeneity, drug-based treatments report limited success, calling for multi-omics studies to extract regulatory relationships, and ultimately, to develop targeted therapies. Yet, methods for multi-omics integration to reveal mechanisms of phenotype regulation are lacking. Methods Here, we present SiRCle (Signature Regulatory Clustering), a method to integrate DNA methylation, RNA-seq and proteomics data at the gene level by following central dogma of biology, i.e. genetic information proceeds from DNA, to RNA, to protein. To identify regulatory clusters across the different omics layers, we group genes based on the layer where the gene’s dysregulation first occurred. We combine the SiRCle clusters with a variational autoencoder (VAE) to reveal key features from omics’ data for each SiRCle cluster and compare patient subpopulations in a ccRCC and a PanCan cohort. Results Applying SiRCle to a ccRCC cohort, we showed that glycolysis is upregulated by DNA hypomethylation, whilst mitochondrial enzymes and respiratory chain complexes are translationally suppressed. Additionally, we identify metabolic enzymes associated with survival along with the possible molecular driver behind the gene’s perturbations. By using the VAE to integrate omics’ data followed by statistical comparisons between tumour stages on the integrated space, we found a stage-dependent downregulation of proximal renal tubule genes, hinting at a loss of cellular identity in cancer cells. We also identified the regulatory layers responsible for their suppression. Lastly, we applied SiRCle to a PanCan cohort and found common signatures across ccRCC and PanCan in addition to the regulatory layer that defines tissue identity. Conclusions Our results highlight SiRCle’s ability to reveal mechanisms of phenotype regulation in cancer, both specifically in ccRCC and broadly in a PanCan context. SiRCle ranks genes according to biological features. https://github.com/ArianeMora/SiRCle_multiomics_integration .

Published in Genome Medicine

ISSN: 1756-994X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General): Genetics
Website: https://genomemedicine.biomedcentral.com/

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