Aligning germline and somatic mutations in prostate cancer. Are genetics changing practice?

Olivier Cussenot; Geraldine Cancel-Tassin; Srinivasa R Rao; Dan J Woodcock; Alastair D Lamb; Ian G Mills; Freddie C Hamdy

doi:10.1111/bju.16120

Aligning germline and somatic mutations in prostate cancer. Are genetics changing practice?

BJU Int. 2023 Nov;132(5):472-484. doi: 10.1111/bju.16120. Epub 2023 Jul 27.

Authors

Olivier Cussenot^{1

2

3}, Geraldine Cancel-Tassin^{1

2}, Srinivasa R Rao³, Dan J Woodcock³, Alastair D Lamb³, Ian G Mills³, Freddie C Hamdy³

Affiliations

¹ Centre de Recherche sur les Pathologies Prostatiques et Urologiques (CeRePP), Paris, France.
² GRC 5 Predictive Onco-Urology, Sorbonne University, Paris, France.
³ Nuffield Department of Surgical Sciences, University of Oxford, Oxford, UK.

PMID: 37410655
DOI: 10.1111/bju.16120

Abstract

Objective: To review the current status of germline and somatic (tumour) genetic testing for prostate cancer (PCa), and its relevance for clinical practice.

Methods: A narrative synthesis of various molecular profiles related to their clinical context was carried out. Current guidelines for genetic testing and its feasibility in clinical practice were analysed. We report the main identified genetic sequencing results or functional genomic scores for PCa published in the literature or obtained from the French PROGENE study.

Results: The molecular alterations observed in PCa are mostly linked to disruption of the androgen receptor (AR) pathway or DNA repair deficiency. The main known germline mutations affect the BReast CAncer gene 2 (BRCA2) and homeobox B13 (HOXB13) genes, whereas AR and tumour protein p53 (TP53) are the genes with most frequent somatic alterations in tumours from men with metastatic PCa. Molecular tests are now available for detecting some of these germline or somatic alterations and sometimes recommended by guidelines, but their utilisation must combine rationality and feasibility. They can guide specific therapies, notably for the management of metastatic disease. Indeed, following androgen deprivation, targeted therapies for PCa currently include poly-(ADP-ribose)-polymerase (PARP) inhibitors, immune checkpoint inhibitors, and prostate-specific membrane antigen (PSMA)-guided radiotherapy. The genetic tests currently approved for targeted therapies remain limited to the detection of BRCA1 and BRCA2 mutation and DNA mismatch repair deficiency, while large panels are recommended for germline analyses, not only for inherited cancer predisposing syndrome, but also for metastatic PCa.

Conclusions: Further consensus aligning germline with somatic molecular analysis in metastatic PCa is required, including genomics scars, emergent immunohistochemistry, or functional pre-screen imaging. With rapid advances in knowledge and technology in the field, continuous updating of guidelines to help the clinical management of these individuals, and well-conducted studies to evaluate the benefits of genetic testing are needed.

Keywords: clinical practice; genetics; germline mutation; prostate cancer; somatic biomarker.

Publication types

Review