Signatures of Co-Deregulated Genes and Their Transcriptional Regulators in Kidney Cancers

Ioanna Ioannou; Angeliki Chatziantoniou; Constantinos Drenios; Panayiota Christodoulou; Malamati Kourti; Apostolos Zaravinos

doi:10.3390/ijms24076577

Signatures of Co-Deregulated Genes and Their Transcriptional Regulators in Kidney Cancers

Int J Mol Sci. 2023 Mar 31;24(7):6577. doi: 10.3390/ijms24076577.

Authors

Ioanna Ioannou^{1

2}, Angeliki Chatziantoniou^{1

2}, Constantinos Drenios¹, Panayiota Christodoulou³, Malamati Kourti^{1

4}, Apostolos Zaravinos^{1

2}

Affiliations

¹ Department of Life Sciences, School of Sciences, European University Cyprus, Nicosia 2404, Cyprus.
² Cancer Genetics, Genomics and Systems Biology Group, Basic and Translational Cancer Research Center (BTCRC), Nicosia 1516, Cyprus.
³ School of Medicine, European University Cyprus, Nicosia 2404, Cyprus.
⁴ Angiogenesis and Cancer Drug Discovery Group, Basic and Translational Cancer Research Center (BTCRC), Nicosia 1516, Cyprus.

Abstract

There are several studies on the deregulated gene expression profiles in kidney cancer, with varying results depending on the tumor histology and other parameters. None of these, however, have identified the networks that the co-deregulated genes (co-DEGs), across different studies, create. Here, we reanalyzed 10 Gene Expression Omnibus (GEO) studies to detect and annotate co-deregulated signatures across different subtypes of kidney cancer or in single-gene perturbation experiments in kidney cancer cells and/or tissue. Using a systems biology approach, we aimed to decipher the networks they form along with their upstream regulators. Differential expression and upstream regulators, including transcription factors [MYC proto-oncogene (MYC), CCAAT enhancer binding protein delta (CEBPD), RELA proto-oncogene, NF-kB subunit (RELA), zinc finger MIZ-type containing 1 (ZMIZ1), negative elongation factor complex member E (NELFE) and Kruppel-like factor 4 (KLF4)] and protein kinases [Casein kinase 2 alpha 1 (CSNK2A1), mitogen-activated protein kinases 1 (MAPK1) and 14 (MAPK14), Sirtuin 1 (SIRT1), Cyclin dependent kinases 1 (CDK1) and 4 (CDK4), Homeodomain interacting protein kinase 2 (HIPK2) and Extracellular signal-regulated kinases 1 and 2 (ERK1/2)], were computed using the Characteristic Direction, as well as GEO2Enrichr and X2K, respectively, and further subjected to GO and KEGG pathways enrichment analyses. Furthermore, using CMap, DrugMatrix and the LINCS L1000 chemical perturbation databases, we highlight putative repurposing drugs, including Etoposide, Haloperidol, BW-B70C, Triamterene, Chlorphenesin, BRD-K79459005 and β-Estradiol 3-benzoate, among others, that may reverse the expression of the identified co-DEGs in kidney cancers. Of these, the cytotoxic effects of Etoposide, Catecholamine, Cyclosporin A, BW-B70C and Lasalocid sodium were validated in vitro. Overall, we identified critical co-DEGs across different subtypes in kidney cancer, and our results provide an innovative framework for their potential use in the future.

Keywords: Characteristic Direction; GEO2Enrichr; KICH; KIRC; KIRP; X2K; co-deregulated genes; drug repurposing; kidney cancer; single-drug perturbation; single-gene perturbation; tumor heterogeneity.

MeSH terms

Carrier Proteins
Etoposide
Humans
Hydroxyurea
Kidney Neoplasms* / genetics
Protein Serine-Threonine Kinases
Signal Transduction* / genetics

Substances

Etoposide
BW B70C
Hydroxyurea
HIPK2 protein, human
Carrier Proteins
Protein Serine-Threonine Kinases

Grants and funding

This research received no external funding.