PC consists of two well-established phases, an initial hormono-sensitive phase followed by a castration-resistant one, so different models to represent both contexts were selected. To contextualize castration-resistant PC we used a PDX line coming from a brain metastasis collected during the patient autopsy. This model represents an aggressive form of the disease as by the time the sample was collected the patient had become resistant to different previous treatments. Additionally, since hormone-sensitive PDX models are complex to grow in in vivo models, we explored the hormone-sensitive context by using organoids coming from a PDX line originating from a primary tumour in a metastatic patient in the hormono-sensitive phase of the disease. Both castration-resistant and hormone-sensitive pre-clinical models were submitted to different sequential treatment strategies simulating frequent treatment sequences administered in clinical practice. Interestingly, so far we have observed that in the castration-resistant model one of the therapeutic sequences caused a significant remission of the tumour volume, indicating that this tumour, even while being in a highly advanced stage, was still sensitive to that specific treatment option. In the hormono-sensitive context, viability analysis after treatment exposure was also performed revealing a variety of sensitivities to different agents, including drugs that belong to the same group of medicine.
The molecular analysis of treated organoids and PDX samples and its validation in patients’ samples have provided us with more specific information about treatment-leaded changes under different regimens. Metabolism has resulted a crucial process in tumor cell survival, which is strongly modulated by regimens that include cabazitaxel. Altogether, results reveal the efficacy of cabazitaxel treatment, alone or under sequential regimens, in an aggressive tumor context. Targeting metabolic pathways together with cabazitaxel treatment could be a potential strategy in order to overcome taxane resistance and to increase treatment efficacy in advanced PC.
These results were submitted and selected as an oral presentation to the European congress ESUR21. They have also resulted in a publication in the journal Cancers. A second manuscript is in preparation.