Oestrogen receptor-independent actions of oestrogen in cancer.
Prarthana GopinathRevathi Paramasivam OviyaGopisetty GopalPublished in: Molecular biology reports (2023)
Oestrogen, the primary female sex hormone, plays a significant role in tumourigenesis. The major pathway for oestrogen is via binding to its receptor [oestrogen receptor (ERα or β)], followed by nuclear translocation and transcriptional regulation of target genes. Almost 70% of breast tumours are ER + , and endocrine therapies with selective ER modulators (tamoxifen) have been successfully applied. As many as 25% of tamoxifen-treated patients experience disease relapse within 5 years upon completion of chemotherapy. In such cases, the ER-independent oestrogen actions provide a plausible explanation for the resistance, as well as expands the existing horizon of available drug targets. ER-independent oestrogen signalling occurs via one of the following pathways: signalling through membrane receptors, oxidative catabolism giving rise to genotoxic metabolites, effects on mitochondria and redox balance, and induction of inflammatory cytokines. The current review focuses on the non-classical oestrogen signalling, its role in cancer, and its clinical significance.
Keyphrases
- estrogen receptor
- breast cancer cells
- endoplasmic reticulum
- papillary thyroid
- end stage renal disease
- newly diagnosed
- ejection fraction
- chronic kidney disease
- cell death
- squamous cell carcinoma
- gene expression
- binding protein
- transcription factor
- electronic health record
- drug induced
- positive breast cancer
- genome wide