Randomized Phase II Study Evaluating the Addition of Pembrolizumab to Radium-223 in Metastatic Castration-resistant Prostate Cancer.
Atish D ChoudhuryLucia KwakAlexander CheungKathryn M AllaireJaqueline Marquez GarciaDavid D YangAbhishek TripathiJacqueline M KilarMeredith FlynnBrianna MaynardRebecca ReichelAmanda F PaceBrandon K ChenEliezer Van AllenKerry L KilbridgeXiao X WeiBradley Alexander McGregorMark M PomerantzRupal S BhattChristopher J SweeneyGlenn J BubleyHeather A JaceneMary-Ellen TaplinFranklin W HuangLauren C HarshmanLawrence FongPublished in: Cancer immunology research (2024)
The checkpoint immunotherapeutic pembrolizumab induces responses in a small minority of patients with metastatic castration-resistant prostate cancer (mCRPC). Radium-223 (R223) may increase immunogenicity of bone metastases and increase pembrolizumab (P) activity. In a randomized phase II study, we assessed the effect of R223+P compared with R223 on tumor immune infiltration, safety, and clinical outcomes in patients with mCRPC. The primary endpoint was differences in CD4+ and CD8+ T-cell infiltrate in 8-week versus baseline bone metastasis biopsies; secondary endpoints were safety, radiographic progression-free survival (rPFS), and overall survival (OS). Of the 42 treated patients (29 R223+P, 13 R223), 18 R223+P and 8 R223 patients had evaluable paired tumor biopsies. Median fold-change of CD4+ T cells was -0.7 (range: -9.3 to 4.7) with R223+P and 0.1 (-11.1 to 3.7) with R223 (P = 0.66); for CD8+ T cells, median fold-change was -0.6 (-7.4 to 5.3) with R223+P and -1.3 (-3.1 to 4.8) with R223 (P = 0.66). Median rPFS and OS was 6.1 (95% confidence interval: 2.7-11.0) and 16.9 months [12.7-not reached (NR)], respectively, with R223+P and 5.7 (2.6-NR) and 16.0 (9.0-NR), respectively, with R223. Although R223+P was well tolerated with no unexpected toxicity, the combination did not improve efficacy. High-dimensional flow cytometry demonstrated minimal immune modulation with R223, whereas R223+P induced CTLA-4 expression on circulating CD4+ T cells. Clinical responders possessed lower circulating frequencies of Ki67+ T and myeloid cells at baseline and higher circulating frequencies of TIM-3+ T and myeloid cells by week 9. Although R223+P did not induce T-cell infiltration into the tumor microenvironment, exhaustion of induced peripheral T-cell immune responses may dampen the combination's clinical activity.
Keyphrases
- phase ii study
- end stage renal disease
- newly diagnosed
- open label
- immune response
- induced apoptosis
- free survival
- ejection fraction
- chronic kidney disease
- flow cytometry
- placebo controlled
- dendritic cells
- squamous cell carcinoma
- acute myeloid leukemia
- prognostic factors
- locally advanced
- poor prognosis
- dna damage
- cell cycle arrest
- randomized controlled trial
- diabetic rats
- neoadjuvant chemotherapy
- toll like receptor
- patient reported outcomes
- cell cycle
- patient reported
- epidermal growth factor receptor
- phase iii
- binding protein
- pi k akt