Publication

Anti-tumour activity of platinum compounds in advanced prostate cancer—a systematic literature review

Journal Paper/Review - Apr 6, 2016

Units
Keywords
castration-resistant prostate cancer, platinum, cisplatin, carboplatin, oxaliplatin, satraplatin
Contact

Citation
Gillessen Sommer S, Omlin A, Hager S. Anti-tumour activity of platinum compounds in advanced prostate cancer—a systematic literature review. Annals of Oncology 2016; 27:975-984.
Type
Journal Paper/Review (Deutsch)
Journal
Annals of Oncology 2016; 27
Publication Date
Apr 6, 2016
Pages
975-984
Publisher
Oxford University Press
Brief description/objective

Background: For men with advanced castration-resistant prostate cancer (CRPC), several treatment options are available, including androgen receptor (AR) pathway inhibitors (abiraterone acetate, enzalutamide), taxanes (docetaxel, cabazitaxel) and the radionuclide (radium-223). However, cross-resistance is a clinically relevant problem. Platinum compounds have been tested in a number of clinical trials in molecularly unselected prostate cancer patients. Advances in CRPC molecular profiling have shown that a significant proportion of patients harbour DNA repair defects, which may serve as predictive markers for sensitivity to platinum agents.
Objective: To systematically identify and analyse clinical trials that have evaluated platinum agents in advanced prostate
cancer patients.
Methods: PubMed was searched to identify published clinical trials of platinum agents in advanced prostate cancer.
The PRIMSA statement was followed for the systematic review process. Identified trials are analysed for study design, statistical plan, assessments of anti-tumour activity and the potential value of predictive biomarkers.
Results: A total of 163 references were identified by the literature search and 72 publications that met the selection criteria were included in this review; of these 33 used carboplatin, 27 cisplatin, 6 satraplatin, 4 oxaliplatin and 2 other platinum compounds. Overall, anti-tumour activity varies in the range of 10%–40% for objective response and 20%–70% for PSA decline ≥50%. Response seemed highest for the combinations of carboplatin with taxanes or oxaliplatin with gemcitabine. The interpretation of the clinical data is limited by differences in response criteria used and patient populations studied.
Conclusion: Platinum compounds have moderate anti-tumour activity in molecularly unselected patients with advanced prostate cancer. Translational evidence of DNA repair deficiency should be leveraged in future studies to select prostate cancer patients most likely to benefit from platinum-based therapy.