Abstract
Simple SummaryProstate cancer (PCa) is the most commonly diagnosed non-skin cancer in men and one of the leading causes of cancer-related death. The driver of PCa proliferation and growth is the androgen receptor (AR) and inhibiting this receptor is the standard of care for patients, following surgery or radiotherapy. Unfortunately, the effectiveness of current therapeutics is temporary, with the cancer eventually developing drug resistance. Among the mechanisms of resistance are the arising mutations in the AR that make the receptor promiscuously activated by drugs or non-specific ligands, thus promoting cancer progression. The aim of this study is to characterize the responses of 44 AR mutants, derived from PCa patients, to available steroids that activate the receptor as well as to various treatments currently used in the clinic. This work will help create a tool to guide the medical team in selecting the best personalized treatment option for each patient.Resistance to drug treatments is common in prostate cancer (PCa), and the gain-of-function mutations in human androgen receptor (AR) represent one of the most dominant drivers of progression to resistance to AR pathway inhibitors (ARPI). Previously, we evaluated the in vitro response of 24 AR mutations, identified in men with castration-resistant PCa, to five AR antagonists. In the current work, we evaluated 44 additional PCa-associated AR mutants, reported in the literature, and thus expanded the study of the effect of darolutamide to a total of 68 AR mutants. Unlike other AR antagonists, we demonstrate that darolutamide exhibits consistent efficiency against all characterized gain-of-function mutations in a full-length AR. Additionally, the response of the AR mutants to clinically used bicalutamide and enzalutamide, as well as to major endogenous steroids (DHT, estradiol, progesterone and hydrocortisone), was also investigated. As genomic profiling of PCa patients becomes increasingly feasible, the developed “AR functional encyclopedia” could provide decision-makers with a tool to guide the treatment choice for PCa patients based on their AR mutation status.
Highlights
The emergence of drug resistance in prostate cancer (PCa) is a prominent factor of its progression to castration-resistant PCa (CRPC)
In PCa there is a 4-fold difference in mutation rates in metastases compared to primary tumours [11], and a subset of metastatic PCa presents a hypermutated mismatch repair (MMR) leading to oncogene activation and tumour heterogeneity [12]
We have expanded the list of functionally characterized androgen receptor (AR) mutants with an additional 44 variants reported in
Summary
The emergence of drug resistance in prostate cancer (PCa) is a prominent factor of its progression to castration-resistant PCa (CRPC). A recent study [9] demonstrated that downregulation of DNA mismatch repair (MMR) and homologous recombination (HR) play a significant role in adaptive mutability in colorectal cancers, occurring as a response to therapeutic pressure. Such adaptive mutability has been reported for epidermal growth factor receptor (EGFR) in non-small cell lung cancers [10]. Adaptive mutability could rapidly contribute to the emergence of acquired drug-resistant sub-clones in advanced PCa
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