Prostate-Specific Membrane Antigen-Targeted Therapies for Prostate Cancer: Towards Improving Therapeutic Outcomes - Beyond the Abstract

Discovered in 1987, Prostate-specific membrane antigen (PSMA) glycoprotein, also known as folate hydrolase (FOLH1), has become pivotal in targeting therapeutic payloads to prostate cancer cells. Its prominence lies in its significantly heightened expression—ranging from 100 to 1000 times higher—in prostate adenocarcinoma compared to the normal prostate epithelium.1



Various methods developed and tested in clinical trials aim to target cancer cells expressing PSMA, showing promising outcomes, with the effectiveness of PSMA-targeted therapies heavily reliant on the level of PSMA expressed on the cell surface. Yet, PSMA heterogeneity across multiple levels (interpatient, intertumoral, and intratumoral) has been documented, contributing to the development of resistance against PSMA-targeted therapies.2-4

Understanding the molecular mechanisms governing PSMA regulation is crucial for designing strategies to enhance its expression. HOXB13 and AR are identified as pivotal transcription factors influencing PSMA expression positively and negatively, respectively 3. Moreover, recent findings highlight the role of epigenetic regulation in controlling FOLH1 transcription.2,3 Yet, the complete understanding of how PSMA expression is regulated remains unclear. Within the review, we utilized data from our recently developed Prostate Cancer Transcriptome Atlas5 to compile a roster of transcriptional regulators highly associated with PSMA. This list may offer potential candidate genes involved in its regulation.

In addition, in the review, we rationalize combination therapies, as several established therapeutic approaches not only have the potential to increase PSMA levels but also to enhance DNA damage caused by existing radioligands (Figure 1).

Therapeutic modalities such as AR inhibition not only can increase PSMA levels but also impair DNA repair mechanisms, potentially improving the effectiveness of PSMA-targeted radionuclide therapy (RLT).6,7 The PSMAddition trial in metastatic hormone-sensitive prostate cancer and the ENZA-p trial in castration resistant prostate cancer are ongoing to explore this combination therapy.8,9

Chemotherapy remains a primary treatment option for prostate cancer and neuroendocrine prostate cancer (NEPC) patients. Interestingly, certain chemotherapeutic drugs that induce DNA damage have been found to upregulate PSMA protein levels, suggesting a possibility to enhance PSMA-targeted therapy outcomes through chemotherapy-induced PSMA upregulation.10

Poly (ADP-ribose) polymerase inhibitors (PARPi) have shown effectiveness in inducing synthetic lethality in prostate cancer cells with DNA repair abnormalities. Combining PARPi with PSMA-targeted RLT might amplify the therapeutic effects, as PARPi are crucial for repairing single-strand DNA breaks induced by beta minus particle emitters used in RLT.11 Currently, the LuPARP trial is investigating this combinatorial strategy.12

Immune checkpoint inhibitors have shown efficacy in a subset of prostate cancer patients with high mutational burden and microsatellite instability (MSI). Combining these inhibitors with PSMA-targeted RLT may enhance immune responses through the radiation-induced neoantigens formation on cancer cells, potentially broadening the application of immunotherapy in prostate cancer treatment.13 Multiple ongoing trials are assessing the combination of immune checkpoint inhibitors with PSMA-RLT.14-16

The observed increase in PSMA expression following DNA double-strand breaks suggests the possibility of synergizing PSMA-targeted RLT with itself. A dosing regimen involving sequential PSMA-RLT injections exploiting the upregulation induced by the initial dose is a potential strategy.

In conclusion, a better understanding of PSMA expression is mandatory to fight intra- and intertumoral PSMA heterogeneity as the identification of new regulators of PSMA could reveal novel ways to increase PSMA expression, for example by activating or inhibiting a positive or a negative PSMA regulator, respectively, and augment PSMA-targeted therapies. In addition, this will provide the basis for synergistic combination therapies.


Figure 1. Synergism of different therapeutic approaches with PSMA-targeted therapies.

Written by: Matteo Corpetti,1 Cristina Müller,2 Himisha Beltran,3 Johann de Bono,4 Jean-Philippe Theurillat5

  1. Institute of Oncology Research, Bellinzona, Switzerland; Faculty of Biomedical Sciences, Università della Svizzera italiana, Lugano, Switzerland.
  2. Department of Chemistry and Applied Biosciences, ETH Zurich, Zurich, Switzerland; Center for Radiopharmaceutical Sciences ETH-PSI, Paul Scherrer Institute, Villigen-PSI, Switzerland.
  3. Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA; Harvard Medical School, Boston, MA, USA.
  4. The Institute of Cancer Research, London, UK; The Royal Marsden Hospital, London, UK.
  5. Institute of Oncology Research, Bellinzona, Switzerland; Faculty of Biomedical Sciences, Università della Svizzera italiana, Lugano, Switzerland.
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